Next Article in Journal
Recent Advances in Environmentally Friendly and Green Degumming Processes of Silk for Textile and Non-Textile Applications
Next Article in Special Issue
Development and Characterization of PEGylated Fatty Acid-Block-Poly(ε-caprolactone) Novel Block Copolymers and Their Self-Assembled Nanostructures for Ocular Delivery of Cyclosporine A
Previous Article in Journal
Microfluidic Rheometry and Particle Settling: Characterizing the Effect of Polymer Solution Elasticity
Previous Article in Special Issue
Development of Polymer-Based Nanoformulations for Glioblastoma Brain Cancer Therapy and Diagnosis: An Update
 
 
Search for Articles:
Title / Keyword
Author / Affiliation / Email
Journal
Article Type
 
 
Advanced Search
 
Section
Special Issue
Volume
Issue
Number
Page
 
Journals
Polymers
Volume 14
Issue 4
10.3390/polym14040658
polymers-logo
Submit to this Journal Review for this Journal Propose a Special Issue
Article Menu

Article Menu

share Share announcement Help format_quote Cite question_answer Discuss in SciProfiles thumb_up
...
Endorse textsms
...
Comment
first_page
settings
Order Article Reprints
Font Type:
Arial Georgia Verdana
Font Size:
Aa Aa Aa
Line Spacing:
Column Width:
Background:
Review

Paclitaxel Drug Delivery Systems: Focus on Nanocrystals’ Surface Modifications

by
Razan Haddad
1,*,
Nasr Alrabadi
2,*,
Bashar Altaani
1 and
Tonglei Li
3
1
Department of Pharmaceutical Technology, Faculty of Pharmacy, Jordan University of Science and Technology, Irbid 22110, Jordan
2
Department of Pharmacology, Faculty of Medicine, Jordan University of Science and Technology, Irbid 22110, Jordan
3
Department of Industrial and Physical Pharmacy, Purdue University, West Lafayette, IN 47907, USA
*
Authors to whom correspondence should be addressed.
Polymers 2022, 14(4), 658; https://doi.org/10.3390/polym14040658
Submission received: 19 December 2021 / Revised: 28 January 2022 / Accepted: 3 February 2022 / Published: 9 February 2022
(This article belongs to the Special Issue Drug-Loaded Colloidal Systems in Nanomedicine II)
Browse Figures
Versions Notes

Abstract

:
Paclitaxel (PTX) is a chemotherapeutic agent that belongs to the taxane family and which was approved to treat various kinds of cancers including breast cancer, ovarian cancer, advanced non-small-cell lung cancer, and acquired immunodeficiency syndrome (AIDS)-related Kaposi’s sarcoma. Several delivery systems for PTX have been developed to enhance its solubility and pharmacological properties involving liposomes, nanoparticles, microparticles, micelles, cosolvent methods, and the complexation with cyclodextrins and other materials that are summarized in this article. Specifically, this review discusses deeply the developed paclitaxel nanocrystal formulations. As PTX is a hydrophobic drug with inferior water solubility properties, which are improved a lot by nanocrystal formulation. Based on that, many studies employed nano-crystallization techniques not only to improve the oral delivery of PTX, but IV, intraperitoneal (IP), and local and intertumoral delivery systems were also developed. Additionally, superior and interesting properties of PTX NCs were achieved by performing additional modifications to the NCs, such as stabilization with surfactants and coating with polymers. This review summarizes these delivery systems by shedding light on their route of administration, the methods used in the preparation and modifications, the in vitro or in vivo models used, and the advantages obtained based on the developed formulations.

1. Introduction

Currently, cancer is considered a serious disease that is globally widespread, and it is one of the most life-threatening illnesses [1], accounting for about 10 million deaths in 2020 [2]. Additionally, the economic burden of this disease is enormous, and it is anticipated to increase in the future [3,4]. On the other hand, chemotherapeutic agents are considered effective at fighting cancer and preventing its development and progress [5]. However, there is still an urgent need for more therapeutic options or strategies to improve the currently available treatments in terms of safety and efficacy.
The improvements of chemotherapeutic agents mainly depend on two research lines [5]. The first one is related to explaining cancer-specific mechanisms and molecular targets, such as signal transduction inhibitors concerning essential processes of cells such as growth, survival, and differentiation. These substances may have the ability to prevent the injuries caused by cancer cells, including proliferation and tissue invasion [6]. The second line is considering the enhancement of the available cytotoxic drugs which act on abundant targets (e.g., DNA or tubulin) [5]. These cytotoxic drugs are either natural products or their derivatives obtained from plants, marine species, and microorganisms, but unfortunately, these drugs are still toxic to normal cells [7]. Therefore, the improvement of their efficacy and safety is always warranted.
Eventually, many anticancer agents were obtained. but most of them are inefficient and cause severe side effects. Therefore, there is an emerging need to develop new therapeutic agents or delivery approaches. Several drug delivery systems based on nanotechnology modalities have been obtained for different anticancer drugs such as solid lipid nanoparticles, liposomes, micelles, polymeric nanoparticles, nano-emulsions, implants, and nanocrystals [8,9,10]. All these approaches are aimed at either enhancing the efficacy or reducing the side effects of the currently available chemotherapeutic agents. Finding novel and appropriate drug delivery systems is crucial, especially for chemotherapies where intravenous delivery remains the main route used for drug administration [8]. This returns to the fact that most anticancer drugs have low solubility or gastrointestinal tract (GIT) toxic side effects over oral administration, which in turn can reduce their oral absorption below the therapeutic effective levels [10].

2. Paclitaxel

Paclitaxel (PTX) is an important chemotherapeutic agent that belongs to the taxane family. Taxanes were initially obtained from plants of the genus Taxus. PTX was first derived from the bark of the Pacific yew (Taxus brevifolia), which is an evergreen tree and small to medium in size and also known as western yew, native to the Pacific Northwest of North America [11,12]. PTX was approved by the United States (US) Food and Drug Administration (FDA) to treat various kinds of cancers including breast cancer, ovarian cancer, advanced non-small-cell lung cancer, and acquired immunodeficiency syndrome (AIDS)-related Kaposi’s sarcoma [13]. In general, PTX is not well tolerated and related to serious adverse drug effects such as hypersensitivity reactions, hematological toxicity, peripheral sensory neuropathy, and myalgia or arthralgia [13], even though PTX has been used for two decades either as a single drug or in combination with other chemotherapeutics.
The antitumor activity of paclitaxel comes from its high binding affinity to microtubules, stabilizing and improving the polymerization of tubulin and destruction of the dynamics of the spindle microtubule [14,15]. Such activities provide effective inhibition of cell mitosis, intracellular transport, and motility, which end up with cell death by apoptosis. However, the clinical developments of the natural form of paclitaxel have been restricted due to its physicochemical properties, particularly its very low solubility [16]. Additionally, the absence of modifiable functional moieties in its structure makes the chemical alteration of the natural paclitaxel very complicated when attempting to enhance its solubility [17]. Considering that, the selection of a proper delivery system to paclitaxel is considered very crucial to improving its clinical development, safety, and efficiency.
Regarding the chemical structure of PTX (Figure 1), its 20-carbon compound (C20) belongs to the diterpene class of natural compounds [18]. The anticancer activity is mainly recognized for ring A, ring D (the oxetane ring), the C2 benzoyl group, and some components such as the C3′ amide-acyl group and the OH group at C2′, which attaches on the side chain to C13 [19]. On the other hand, other groups slightly affect the therapeutic activity of PTX such as the carbonyl group on C9 and the acetyl group on C10. Moreover, the specified conformation of the paclitaxel molecule is provided by the acetyl group [19].
PTX has poor aqueous solubility, low permeability, and as it is a P-gp substrate, it also has limited capabilities for being delivered via the oral route [20,21,22,23]. The poor permeability of PTX is related to the following molecular factors: its molecular weight is more than 500, the hydrogen bond acceptor (HBA) is greater than 10, and the polar surface area (PSA) is more than 140 A2, which results in a permeability coefficient value in the range of 10−6 cm/s [24,25]. Therefore, PTX is administered parentally via the intravenous (IV) route with a suitable cosolvent (cremophor EL and ethanol), which unfortunately ends up with several direct, problematic, adverse effects such as acro-anesthesia and neurovirulence, causing pain and high cost [26,27,28,29].

3. PTX Formulations

To improve the benefit and delivery of PTX, several formulations have been developed. The most commonly used delivery system is a cosolvent strategy based on a 50:50 mixture of ethanol and Cremophor EL™ (a polyoxyethylated castor oil). Taxol® is the first generic product of paclitaxel, and it consists of this cosolvent mixture. Although this method overcomes the problem of solubility, Cremophor EL has been associated with non-linear pharmacokinetics and serious and dose-limiting toxicities, such as hypersensitivity, neurotoxicity, and nephrotoxicity [11]. Due to these adverse effects, Taxol® is given slowly in 135- or 175-mg/m2 doses by infusion over 3–24 h every 3 weeks [30,31].
Abraxane™ is another marketed drug of PTX, which was produced by Abraxis BioScience (later obtained by the Celgene company) and approved by the FDA in 2005 [32]. The formulation of PTX in this product is performed with human serum albumin (HSA) [33]. HSA is the most abundant plasma protein in the blood, with a large half-life that reaches up to 19 h and which can bind hydrophobic substances irreversibly, transport them through the body, and deliver them to the cell surface [34]. Additionally, HSA plays a significant role in cellular uptake and transcytosis, as it is bound to gp60 and other proteins which are highly expressed in malignant cells, such as secreted proteins acidic and rich in cysteine (SPARC). Nevertheless, it is still ambiguous how exactly HAS improved the biological response of PTX. However, it is significantly clear that the removal of Cremphor EL contributes to the ability to administer a higher dose of PTX with an analogous toxicity [35]. Moreover, Abraxane™ has a linear pharmacokinetic profile and a higher intratumoral concentration by 33% in comparison with Taxol®, based on results obtained by the Abraxis BioSciences company [36].
Another marketed drug of PTX is Lipusu™, which was formulated by Luye Pharmaceutical Co. Ltd. and approved in China in 2003. It is a liposome composed of PTX, lecithin, and cholesterol. In comparison with Taxol®, Lipusu™ has similar activities toward breast cancer, non-small cell lung, and gastric cancer but with considerably lesser side effects [37,38].
Finally, Genexol-PM™ is marketed by Samyang Corporation and was approved in South Korea in 2007. It is composed of PTX and poly (ethylene glycol)-b-poly (lactic acid) (PEG-b-PLA) block copolymers. Clinical studies showed that Genexol-PM™ has dose-dependent pharmacokinetics and good tolerance, especially for patients with advanced pancreatic cancer or metastatic breast cancer [39,40,41].

4. Drug Delivery of PTX

As previously mentioned, the physicochemical properties and the nature of PTX complicated its formulations. Consequently, several delivery systems for PTX have been developed to enhance its solubility and pharmacological properties involving micelles, liposomes, nanoparticles, the prodrug approach, emulsions, implants, and nanocrystals [42,43,44,45]. Figure 2 summarizes the most common strategies utilized for PTX delivery systems.

4.1. Micelles

Generally, micelles consist of polar heads that encounter the outside aqueous environment and non-polar tails, which form the interior hydrophobic core. Above the critical micelle concentration, micelles spontaneously form, and drugs with low solubility encapsulate efficiently in the lipidic core [46,47]. The properties of micelles and the hydrophobic regions can be modified and tailored by using various polymer structures [48]. The targeted delivery of PTX micelles developed using an Asn-Gly-Arg (NGR) peptide, which covalently bonds to PEG chains to deliver PTX through a brain tumor [49]. Moreover, the oral delivery of PTX was obtained using multi-functional chitosan polymeric micelles [50]. The development of redox-sensitive PEG2000-S-S-PTX micelles resulted in a reduction of PTX cytotoxicity in ovarian and breast cancer cells [51].

4.2. Liposomes

The liposome is a spherical structure with a membrane composed of a single or multiple phospholipid bilayers. It has an aqueous core to encapsulate hydrophilic drugs, while the hydrophobic drug can be loaded in the region of the bilayer membrane. Liposomes have been used to deliver PTX because they showed that they can enhance solubility and efficacy by modulating its pharmacokinetic properties. Additionally, the used excipients are clinically approved [52]. LipusuTM is the first injected PTX liposome, and it has been used in China to treat non-small cell lung cancer, breast cancer, and other cancers [19]. It maintains the original activity of PTX but with a significant reduction in the side effects. Moreover, LEP-ETU is another liposome loaded with PTX. Based on the phase I study, LEP-ETU showed little difference in the pharmacokinetic properties in comparison to Taxol® while being safer at higher doses [53].
Long-term instability is the main obstacle related to liposomes. Despite liposomes having the ability to deliver cytotoxic compounds to certain tissues, they can be eliminated by the mononuclear phagocytic system (MPS) in the spleen and liver [54]. Interestingly, the average circulation time of liposomes can be enhanced by 10 folders with PEGylation, which results in an improvement of the half-life of PTX and its antitumor properties [55,56,57]. The PEGylated liposome can be also modified by active targeting strategies to improve its efficacy [58,59]. This can be obtained by covalently binding species to the surface of the liposomes, such as the peptides [60], proteins [61], and tissue-specific antibodies [62]. Specifically, a multifunctional peptide was incorporated to the surface of the liposomes loaded with PTX, which improved its targeting activity and also its efficacy [59]. Moreover, triphenylphosphonium (TPP) was incorporated into the surface of the PEGylated PTX liposomes, which consequently enhanced their cytotoxicity and antitumor efficacy and provided efficient mitochondrial targeting in cancer cells [58]. Moreover, PTX loaded to a pH-sensitive lipid that was incorporated into a liposomal membrane prevented liposome degradation by lysozymes and consequently caused more suppression of tumors by providing more PTX accumulation at pH of 7.4 instead of 5.5 [63,64].

4.3. Nanoparticles

4.3.1. Solid Lipid Nanoparticles

Generally, solid lipid nanoparticles (SLN) are obtained from solid lipids, such as complex glyceride, highly purified triglycerides, and waxes [65]. Several kinds of lipids and surfactants can be used for SLN production and engineering. More specifically, lipids such as phospholipids and glycerides and surfactants such as tween 80, sodium glycolate, lecithin, and poloxamer 188 are considered suitable for IV injection [66]. There are several advantages related to the SLN, such as the simplicity of the preparation method and the scaling up, biocompatibility, stability, low cost, low toxicity, controlled drug release, and versatile chemistry [52].
To obtain high drug loading and the slow release of PTX, SLN should obtain high drug solubility and miscibility [67]. The cellular uptake and cytotoxicity properties of PTX-loaded SLN can be vary based on the lipid materials used. For instance, studies showed that the cellular uptake of SLN was concentration- and time-dependent and related to the melting point of the lipidic materials, the length of its hydrocarbon chain, and the particle size [68,69,70]. PTX-loaded PEGylated steric acid SLN proved to have a high cellular uptake and up to 10-fold greater cytotoxicity in comparison with PTX. Moreover, SLN showed an ability to affect P-gp-mediated multidrug resistance (MDR), as PTX loaded SLN provided an inhibition of P-gp activity and a rapid depletion of ATP [71,72].
As with the other noncompaction systems, surface modification of the particles by different chemical moieties is useful for obtaining prolonged SLN circulation by avoiding the clearance with the reticuloendothelial system (RES) [52].

4.3.2. Polymeric Nanoparticles

Polymers have been used in nanoparticle preparation to provide them with suitable properties and characteristics. Examples of some of the polymers that are commonly used in developing paclitaxel nanoparticles are poly (lactic-co-glycolic acid) (PLGA) and chitosan, which will be discussed in the following sections.

Poly Lactic-co-Glycolic Acid (PLGA)

Poly (lactic-co-glycolic acid) (PLGA) is a biocompatible, biodegradable, nontoxic synthetic polymer derived from poly (lactic acid) (PLA) and poly (glycolic acid) (PGA) [73,74]. It has been approved by the US Food and Drug Administration (FDA) for drug delivery, as it has superior properties in the delivery of many therapeutic agents. PLGA is a very useful and successful polymer in nanomedicine and the nano-delivery of drugs. In addition, it has a favorable ability to target tumors and DNA [73,75,76,77]. PLGA is available commercially with various molecular weights and copolymer ratios. Based on that, the duration of the degradation can vary, as can the release time. Glycolic acid is more hydrophilic than lactic acid, and thus PLGA with higher glycolic acid is more hydrophilic and can adsorb water more and degrade faster [78,79]. The loading of PTX to PLGA nanoparticles has been obtained by various methods such as emulsion solvent evaporation [77], interfacial deposition methods [80], and the nanoprecipitation method [81]. Studies showed that PTX loaded to the PLGA nanoparticles had superior antitumor properties and efficacy in comparison with Taxol® [81,82]. Moreover, surface modification of the nanoparticles has a crucial impact on their properties, such as efficacy and targeting. The delivery of PTX was improved by surface modification of PLGA nanoparticles with albumin, as the circulation time of these nanoparticles in the blood was increased even as it became more toxic in the in vitro study [83]. The targeted delivery of PTX to breast cancer cells was developed by loading it into PLGA nanoparticles coated with hyaluronic acid (HA), and the results showed that the cellular uptake was increased using this system [84]. Moreover, PTX has been loaded to lipid PLGA hybrid nanoparticles, and the results showed that the release profile was affected with this lipid coat. Also, these nanoparticles provided a prolongation in the circulation time in the blood [85].

Chitosan

Chitosan is a natural polysaccharide polymer produced by the diacylation of chitin. It has many attractive properties such as non-toxicity, biocompatibility, biodegradability, and bio-adhesivity, which necessitates its use in drug delivery [86,87]. The solubility of chitosan in acidic solutions and its limited solubility in biological solutions (pH 7.4) are considered the main drawbacks of its application in drug delivery. Lately, many chitosan derivatives have been prepared by adding various hydrophobic or hydrophilic groups to the chitosan structure [88,89]. Moreover, studies showed that chitosan has antitumor properties, and it can affect the cancer cells by interfering with its metabolism, inhibiting its growth, or inducing its apoptosis [90].
Chitosan has been introduced to many PTX delivery systems, and it improved various aspects (e.g., decreasing the toxicity and enhancing the efficiency and targeting capabilities) [91,92,93]. A study showed that the PTX-loaded micelle based on N-octyl-O-sulfate chitosan (OSC), which is a novel derivative of water-soluble chitosan used for the delivery of PTX, has superior toxic properties, as lower side effects were observed, and the AUC was about 3.5 lower than the marketed drug Taxol® while preserving the antitumor efficacy at equivalent doses [94]. Additionally, other studies showed that the targeted delivery of PTX chitosan nanoparticles had been achieved in combination with other polymers such as PEGylated chitosan nanoparticles grafted with Arg-Gly-Asp (RGD) [92], poly NIPAAm [95], transferrin [96], and biotinylated N-palmitoyl chitosan [97].

4.4. Prodrug Approach

Prodrugs are derivatives of a drug molecule that can be transformed chemically or enzymatically in the body to release the active ingredient that possesses pharmacological effects [98]. Differing from other delivery systems or formulations, prodrugs are usually formulated by chemical linkage with proper quality control and less variation from batch to batch. Generally, prodrugs are developed to overcome problems related to the parent drug itself, such as poor aqueous solubility, limited permeability, inadequate oral absorption and delivery, non-targeting, and toxic side effects [99,100].
The PTX prodrug is usually fabricated at the carbon no. 123; 2′or 7-OH group [100]. PTX prodrugs are constructed using various strategies, such as polymer-based prodrugs, which are formulated using polymers such as PEG [101], PLA [102,103,104], poly(amidoamine) [PAMAM] [105], N-(2-hydroxypropyl) methacry’lamide (HPMA) [106], and poly(L-glutamic acid) (PGA) [107]. Moreover, a protein-based prodrug of PTX has been developed using different proteins, such as the marketed product Abraxane™, which is tumor-targeted and formulated using CREKA and LyP-1 [108]. Additionally, PTX prodrugs were obtained using transferrin (Tf) and Fmoc-L-glutamic acid 5-tert-butyl ester (linker) to specifically target tumor tissues and cells [109]. Similarly, peptide-based prodrugs of PTX were also formulated such as the Tat-based self-assembling peptide, which is used to deliver PTX intracellularly [110], the tumor-homing cell-penetrating peptide (CPP) [111], and recombinant chimeric polypeptides (CPs) [112]. Additionally, PTX prodrugs can be obtained using small molecules such as docosahexaenoic acid (DHA) [113], conjugated linoleic acids (CLAs) [114], and oligo(lactic acid)8 [115]. Finally, hybrid prodrugs for PTX also exist, which are a combination of two drugs or more that is capable of producing synergistic effects, reducing the adverse effects related to a high dose of a single drug, and overcoming the multidrug resistance mechanism of cancer cells during treatment [116]. PTX hybrid prodrugs were delivered using other anticancer drugs such as doxorubicin (DOX) [117], camptothecin (CPT) [118], and the nucleic acid oligonucleotide [119].

4.5. Emulsions

Generally, macroemulsions are defined as the dispersion of one liquid in another liquid and it is considered a two-phase system [120]. They are turbid or opaque, viscus, and thermodynamically unstable, and their preparation is complicated as sheer is needed. On the other hand, microemulsions are translucent, thermodynamically stable, have a lower viscosity, and form spontaneously [121]. Based on the name, nano-emulsions should have a droplet size lower than microemulsions. As a matter of fact, nano-emulsions have a droplet size of 20–200 nm and a narrow particle size distribution [122,123,124].
A TocosolTM nano-emulsion was established early in 2000. It was formulated using an a-tocopherol isomer of vitamin E as a solubilizing agent for PTX and vitamin E TPGS as an emulsifier. Unfortunately, studies in phase III showed that the overall response rate was only 37%, while it was 45% with Taxol®. Based on that, the TocosolTM nano-emulsion was terminated [125]. Recently, Shakhwar et al. tried to reform a TocosolTM nano-emulsion using the c-tocotrienol (c-T3) isomer instead of a-tocopherol and the PEGylated c-T3 surfactant instead of vitamin E TPGS. Their results showed that the reformulated PTX was more active toward pancreatic tumor cell lines than the previous formulation [126].
Moreover, self-emulsifying drug delivery systems (SEDDSs) and self-microemulsifying drug delivery systems (SMEDDSs) are combinations of the non-aqueous components of emulsions and microemulsions, respectively [127], such as oils, surfactants, and if present, cosurfactant or cosolvents. These mixtures can be readily dispersed when diluted with an aqueous phase (gastric fluids) in the body and then spontaneously emulsified to form fine oil-in-water (O/W) microemulsions. This process can be sped up by slight mechanical agitation, and in vivo, this can be obtained by gastrointestinal motility [18,122,128]. A novel SMEDDS was developed for oral delivery of PTX, and it was administered to patients with advanced cancer and compared with orally administered Taxol®. The SMEDDS was co-administered with cyclosporin A to inhibit P-gp and CYP3A4. This formula was safe and well-tolerated by patients and had comparable bioavailability to oral Taxol®. In addition, the T-max of the SMEDDS was lower than the orally delivered Taxol®. This means that the absorption was higher in the novel formula, and this may be related to the added excipients [129]. In another study, the oral delivery of PTX was designed as an SEDDS. In this study, tocopheryl polyethylene glycol succinate was used to assist the emulsification. The results indicated that this system had higher G2M cell cycle arrest, apoptosis, mitochondrial membrane potential disruption, and ROS production in comparison with Taxol®. Moreover, the oral bioavailability of the SEDDS was about fourfold greater than Taxol®. Considerable reductions in the volumes and weights of the tumors were detected in syngeneic mammary tumors in SD rats. Additionally, this system was safe, stable, and caused low lung metastasis [130].

4.6. Implants

Drug-loaded polymeric implants are considered a pioneering approach in drug delivery. Active ingredients can be delivered to malignant cells using biodegradable polymers in continuous, sustained, and predictable patterns. Owing to their nature, biodegradable polymers do not need to be removed surgically after their application and thus eliminate complications associated with the long-term safety of implanted devices with non-biodegradable polymers. Additionally, the postsurgical local insertion of a biodegradable implant device loaded with an anticancer drug can avoid the further spread of cancer cells while avoiding toxic chemotherapy adverse effects in the patient [131]. Recently, an in situ depot-forming implant (ISFI) has been developed which can be injected as a liquid and then subsequently solidified [132,133]. In this way, an effective dosage form can be delivered with the avoidance of surgical insertion [134]. Moreover, ISFIs have relatively simpler preparation conditions and fewer complications than solid implants [135,136]. The PTX ISFI was formulated using PLGA to improve its efficiency and toxicity. This formula provided an in vitro sustained release of PTX for 28 days [137].

4.7. Nanocrystals

Nanocrystal formulations have become more attractive for the delivery of chemotherapies due to their superior properties in comparison with other nano-delivery approaches [138,139,140]. Nanocrystals eliminate the need for chemical carriers, therefore eradicating any toxic side effects induced by the excipients used for solubilization or coating and also providing about 100% drug loading, which ensures suitable concentrations of the drug even at low doses [141]. Additionally, due to the stable and uniform physical properties of crystalline particles, the enhancement of the pharmacokinetics and biodistribution properties of the anticancer drugs are anticipated [142,143,144,145].
Nanocrystals can be produced either by top-down or bottom-up methods. The top-down technique involves utilizing a high mechanical energy force to produce nanocrystals from large crystals by media milling or high-pressure homogenization [142,143]. These techniques are generally used to formulate insoluble drugs, especially those used for oral drug delivery [146,147]. In the high-pressure homogenization method, large drug crystals are forced across fluidic pressure and an impact valve, which leads the drug crystals to break down into tinier particles. The control of the particle size is achieved through the pressure and space among the impact valves. On the other hand, in media milling, the grinding of large crystals of the drug is obtained using solid particles like yttrium-stabilized zirconia, cerium, highly crosslinked polystyrene resin-coated beads, and stainless steel [142].
In the bottom-up approach, which involves the antisolvent perception method, nanocrystals can be produced directly from the drug solution. When the drug solution is mixed with an antisolvent with poor drug solubility, in such a case, the decrease in solubility leads to nucleation and crystal growth of the drug, and these are the two critical steps of this method [148]. As more nuclei form during the nucleation stage, then the growth of each nucleus is lower, and based on that, the nucleation step needs to be monitored carefully. The ultrasonic waves produced by sonication can help reduce the size of the nanocrystals by decreasing the particle agglomeration, achieved by breaking down the contact between particles. Consequently, perception and ultrasonication (PU) are commonly used in the bottom-up method [149,150].
The anti-solvent method produced nanocrystals with a smaller size that were cost-effective, simpler, and easy to scale up in comparison with other methods of the top-down approach [151,152]. However, various factors during nanocrystal preparation can be controlled to influence the size and morphology of nanocrystals obtained by the antisolvent method, such as the drug concentration, drug solution flow rate, temperature, solvent-to-antisolvent volume ratio, stirring speed, and the ultrasound wave characteristics [152,153,154]. In addition, the addition of surfactants and polymers during the crystallization process has an impact on the size or the shape of the drug’s nanocrystals [155]. This shows that engineering the modifications of nanocrystals according to our preference and usefulness is possible. Moreover, a combination of both approaches—the top-down and bottom-up methods—can also possibly obtain NCs with a smaller size (<100 nm), narrow distribution, and less production time [156]. In addition, the shape of nanocrystals is also considered important in controlling the activity and toxicity of anticancer drugs. For instance, the rod shape of some drug nanocrystals has superior anticancer activity and toxicity in comparison with the spherical shape [157]. Another study showed that the needle shape of some drug nanocrystals provides better accumulation in some cancers, which may be referred to as an increasing ability of these nanocrystals to be entrapped [144]. Moreover, the size of the nanocrystals is very critical for the in vivo performance of drugs. For instance, smaller nanocrystals have more dissolution rates than larger ones. Conversely, larger nanocrystals may provide sustained release behavior, which results in greater drug accumulation in tumors similar to drug depots. On the other hand, the smaller one is more stable because of the lower accumulation. Finally, the surface treatment or coating of nanocrystals with a polymer or surfactant can further improve the anticancer properties of the nanocrystals and the stability [10,158].
Manipulation during the preparation of the nanocrystals is possible and might end up in unexpected favorable outcomes. Therefore, this indicates the significance of controlling nanocrystals’ properties based on the efficiency, effectiveness, and safety of the anticancer drug, as these can be improved and manipulated indirectly during nanocrystal preparation, especially in the case of the nanocoating.

5. PTX Nanocrystals

As PTX is a hydrophobic drug with inferior water solubility properties, it is improved greatly by nanocrystal formulation [159]. Based on that, many studies employed the nano-crystallization techniques not only to improve the oral delivery of PTX, but IV, intraperitoneal (IP), and local and intertumoral delivery systems were also developed. Additionally, superior and interesting properties of the PTX NCs were achieved by performing additional modifications to the NCs, such as stabilizing them with surfactants and polymers or coating them with polymers. Table 1, Table 2 and Table 3 summarize these modified delivery systems by classifying them into three main categories, according to their route of administration: either IV (Table 1), oral (Table 2), or local and intraperitoneal (Table 3) delivery systems. Additionally, the summary tables shed light on the methods used in the preparation of these modified NCs, the in vitro or in vivo models used, and the advantages obtained based on the developed formulations. Nearly the majority of these NCs had a rode-like shape with drug-loading capabilities (>50%), and their size was between <50 and 500 nm (mainly 100–300 nm). The most common route of administration for these novel formulas was the intravenous (IV) route (Table 1), and the most common method of preparation was the antisolvent or precipitation method. The most common cancer cell lines or types of cancer tested were breast cancer (MCF-7 cell lines), followed by ovarian and then lung cancer. Finally, the aims for modifications were mainly focused on providing more solubility and tumor and cancer cell targeting, less elimination and side effects, and more anti-cancer effects with a smaller dose. In addition, it appears that the NCs’ formulation provided a suitable method for multiple drug combinations.

6. Future Aspects

It is worth mentioning that the nanocrystals are formed by weak, non-covalent interactions. This leads drug nanocrystals to continue to dissolve, albeit slowly, when in contact with water. As such, any surface-coated materials on drug nanocrystals will eventually be detached during the dissolution process. This not only makes it a challenging task to develop surface-treated nanocrystals but also results in transient target-homing effects.
In this regard, the concept of hybrid nanocrystals may overcome this limitation by physically integrating guest molecules among the crystal lattices of nanocrystals. Small molecules such as fluorescent dyes have been demonstrated in vitro and in vivo of paclitaxel nanocrystals. It is thus possible to utilize larger molecules as a guest in making hybrid nanocrystals.
Finally, it is pertinent to understand and eventually predict drug release and dissolution kinetics of paclitaxel nanocrystals in a biological environment. This may be aided by in vitro experimentation and physics-based simulation. One ultimate goal in developing paclitaxel nanocrystals is precision medicine for cancer treatment, which can only be enabled by a thorough understanding of the interactions and the pharmacokinetic characteristics of drug nanocrystals in tissues and cells.

7. Conclusions and Remarks

Several delivery systems for paclitaxel drugs have been developed to enhance their solubility and pharmacological properties. Of these delivery systems, nanocrystal formulations are considered a promising modality that can also have the advantage of providing a suitable platform for surface modifications. Based on that, many studies employed nano-crystallization techniques not only to improve the oral delivery of PTX but also to improve the IV, intraperitoneal (IP), and local and intertumoral delivery systems, where the applications of surface modifications can be of greater value in terms of targeted delivery. Moreover, these systems can provide 100% loading and releasing capacities for the drugs as well as gain the advantages of being formulated as particles that have different circulation patterns, fates, cellular uptake mechanisms, and sometimes preferable efficacy and safety profiles compared with free drugs. Finally, more studies are needed to understand the molecular basis for the formation and interaction of these nanocrystals with biological systems, and consequently providing better platforms for useful modifications in the future.

Author Contributions

Conceptualization, R.H. and N.A.; methodology, R.H. and N.A.; software, R.H.; validation, R.H., N.A., B.A. and T.L.; formal analysis, R.H. and N.A.; investigation, R.H.; resources, R.H.; data curation, R.H., N.A., B.A. and T.L.; writing—original draft preparation, R.H.; writing—review and editing, N.A. and T.L.; visualization, N.A.; supervision, N.A., B.A. and T.L.; project administration, N.A. and B.A.; funding acquisition, N.A. and B.A. All authors have read and agreed to the published version of the manuscript.

Funding

This research was funded by Jordan University of Science and Technology, grant number [298/2021].

Informed Consent Statement

Not applicable.

Data Availability Statement

Not applicable.

Conflicts of Interest

The authors declare no conflict of interest.

References

  1. WHO. Cancer-Fact Fheets. Available online: www.who.int/mediacentre/factsheets/fs297/en/12/9/20182/3/2020 (accessed on 2 March 2020).
  2. World Health Organization. Available online: https://www.who.int/news-room/fact-sheets/detail/cancer (accessed on 5 March 2021).
  3. Patterson, R.; Fischman, V.G.; Wasserman, I.; Siu, J.; Shrime, M.G.; Fagan, J.J.; Koch, W.; Alkire, B.C. Global Burden of Head and Neck Cancer: Economic Consequences, Health, and the Role of Surgery. Otolaryngol. Neck Surg. 2020, 162, 296–303. [Google Scholar] [CrossRef] [PubMed]
  4. Smith, G.L.; Lopez-Olivo, M.; Advani, P.G.; Ning, M.S.; Geng, Y.; Giordano, S.H.; Volk, R.J. Financial Burdens of Cancer Treatment: A Systematic Review of Risk Factors and Outcomes. J. Natl. Compr. Cancer Netw. 2019, 17, 1184–1192. [Google Scholar] [CrossRef] [PubMed]
  5. Altmann, K.-H.; Gertsch, J. Anticancer drugs from nature—Natural products as a unique source of new microtubule-stabilizing agents. Nat. Prod. Rep. 2007, 24, 327–357. [Google Scholar] [CrossRef] [PubMed]
  6. Rowinsky, E.K. Signal events: Cell signal transduction and its inhibition in cancer. Oncologist 2003, 8, 5–17. [Google Scholar] [CrossRef]
  7. Yue, Q.-X.; Liu, X.; Guo, D.-A. Microtubule-Binding Natural Products for Cancer Therapy. Planta Med. 2010, 76, 1037–1043. [Google Scholar] [CrossRef] [Green Version]
  8. Hollis, C.P.; Li, T. Hybrid Nanocrystal as a Versatile Platform for Cancer Theranostics. In Biomaterials for Cancer Thera-peutics: Diagnosis, Prevention and Therapy; Woodhead Publishinged: Cambridge, UK, 2013. [Google Scholar]
  9. Chaturvedi, V.K.; Singh, A.; Singh, V.K.; Singh, M.P. Cancer Nanotechnology: A New Revolution for Cancer Diagnosis and Therapy. Curr. Drug Metab. 2019, 20, 416–429. [Google Scholar] [CrossRef]
  10. Lu, Y.; Chen, Y.; A Gemeinhart, R.; Wu, W.; Li, T. Developing nanocrystals for cancer treatment. Nanomedicine 2015, 10, 2537–2552. [Google Scholar] [CrossRef] [Green Version]
  11. Miele, E.; Spinelli, G.P.; Miele, E.; Tomao, F.; Tomao, S. Albumin-bound formulation of paclitaxel (Abraxane® ABI-007) in the treatment of breast cancer. Int. J. Nanomed. 2009, 4, 99. [Google Scholar]
  12. Heinig, U.; Scholz, S.; Jennewein, S. Getting to the bottom of Taxol biosynthesis by fungi. Fungal Divers. 2013, 60, 161–170. [Google Scholar] [CrossRef] [Green Version]
  13. Markman, M. Managing taxane toxicities. Support. Care Cancer 2003, 11, 144–147. [Google Scholar] [CrossRef]
  14. Rowinsky, E.K.; Cazenave, L.A.; Donehower, R.C. Taxol: A Novel Investigational Antimicrotubule Agent. JNCI J. Natl. Cancer Inst. 1990, 82, 1247–1259. [Google Scholar] [CrossRef] [PubMed]
  15. Schiff, P.; Horwitz, S.B. Taxol stabilizes microtubules in mouse fibroblast cells. Proc. Natl. Acad. Sci. USA 1980, 77, 1561–1565. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  16. Yoncheva, K.; Calleja, P.; Agüeros, M.; Petrov, P.; Miladinova, I.; Tsvetanov, C.; Irache, J.M. Stabilized micelles as delivery vehicles for paclitaxel. Int. J. Pharm. 2012, 436, 258–264. [Google Scholar] [CrossRef] [Green Version]
  17. Deepa, G.; Ashwanikumar, N.; Pillai, J.J.; Kumar, G.S.V. Polymer nanoparticles-a novel strategy for administration of paclitaxel in cancer chemotherapy. Curr. Med. Chem. 2012, 19, 6207–6213. [Google Scholar] [CrossRef]
  18. Ezrahi, S.; Aserin, A.; Garti, N. Basic principles of drug delivery systems—The case of paclitaxel. Adv. Colloid Interface Sci. 2019, 263, 95–130. [Google Scholar] [CrossRef]
  19. Zhang, Z.; Mei, L.; Feng, S.-S. Paclitaxel drug delivery systems. Expert Opin. Drug Deliv. 2013, 10, 325–340. [Google Scholar] [CrossRef]
  20. Schiff, P.; Fant, J.; Horwitz, S.B. Promotion of microtubule assembly in vitro by taxol. Nature 1979, 277, 665–667. [Google Scholar] [CrossRef]
  21. Stinchcombe, T.E. Nanoparticle albumin-bound paclitaxel: A novel Cremphor-EL®-free formulation of paclitaxel. Nanomedicine 2007, 2, 415–423. [Google Scholar] [CrossRef]
  22. Ghadi, R.; Dand, N. BCS class IV drugs: Highly notorious candidates for formulation development. J. Control. Release 2017, 248, 71–95. [Google Scholar] [CrossRef]
  23. Malingré, M.M.; Beijnen, J.H.; Schellens, J.H. Oral delivery of taxanes. Investig. New Drugs 2001, 19, 155–162. [Google Scholar] [CrossRef]
  24. Lee, J.; Lee, S.C.; Acharya, G.; Chang, C.; Park, K. Hydrotropic Solubilization of Paclitaxel: Analysis of Chemical Structures for Hydrotropic Property. Pharm. Res. 2003, 20, 1022–1030. [Google Scholar] [CrossRef] [PubMed]
  25. Thomas, V.H.; Bhattachar, S.; Hitchingham, L.; Zocharski, P.; Naath, M.; Surendran, N.; Stoner, C.L.; El-Kattan, A. The road map to oral bioavailability: An industrial perspective. Expert Opin. Drug Metab. Toxicol. 2006, 2, 591–608. [Google Scholar] [CrossRef] [PubMed]
  26. Bradley, J.D.; Paulus, R.; Komaki, R.; Masters, G.; Blumenschein, G.; Schild, S.; Bogart, J.; Hu, C.; Forster, K.; Magliocco, A.; et al. Standard-dose versus high-dose conformal radiotherapy with concurrent and consolidation carboplatin plus paclitaxel with or without cetuximab for patients with stage IIIA or IIIB non-small-cell lung cancer (RTOG 0617): A randomised, two-by-two factorial phase 3 study. Lancet Oncol. 2015, 16, 187–199. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  27. Song, W.; Tang, Z.; Li, M.; Lv, S.; Sun, H.; Deng, M.; Liu, H.; Chen, X. Polypeptide-based combination of paclitaxel and cisplatin for enhanced chemotherapy efficacy and reduced side-effects. Acta Biomater. 2014, 10, 1392–1402. [Google Scholar] [CrossRef] [PubMed]
  28. Brotto, L.; Brundage, M.; Hoskins, P.; Vergote, I.; Cervantes, A.; Casado, H.A.; Poveda, A.; Eisenhauer, E.; Tu, N. Randomized study of sequential cisplatin-topotecan/carboplatin-paclitaxel versus carboplatin-paclitaxel: Effects on quality of life. Support Care Cancer 2016, 24, 1241–1249. [Google Scholar] [CrossRef] [PubMed]
  29. Zhang, R.; Yang, J.; Sima, M.; Zhou, Y.; Kopeček, J. Sequential combination therapy of ovarian cancer with degradable N-(2-hydroxypropyl)methacrylamide copolymer paclitaxel and gemcitabine conjugates. Proc. Natl. Acad. Sci. USA 2014, 111, 12181–12186. [Google Scholar] [CrossRef] [Green Version]
  30. Panchagnula, R. Pharmaceutical aspects of paclitaxel. Int. J. Pharm. 1998, 172, 1–15. [Google Scholar] [CrossRef]
  31. Marupudi, N.; E Han, J.; Li, K.W.; Renard, V.M.; Tyler, B.M.; Brem, H. Paclitaxel: A review of adverse toxicities and novel delivery strategies. Expert Opin. Drug Saf. 2007, 6, 609–621. [Google Scholar] [CrossRef]
  32. Green, R.M.; Manikhas, M.G.; Orlov, S.; Afanasyev, B.; Makhson, M.A.; Bhar, P.; Hawkins, J.M. Abraxane®, a novel Cremophor®-free, albumin-bound particle form of paclitaxel for the treatment of advanced non-small-cell lung cancer. Ann. Oncol. 2006, 17, 1263–1268. [Google Scholar] [CrossRef]
  33. Gradishar, W.J. Albumin-bound paclitaxel: A next-generation taxane. Expert Opin. Pharmacother. 2006, 7, 1041–1053. [Google Scholar] [CrossRef]
  34. Paál, K.; Müller, J.; Hegedûs, L. High affinity binding of paclitaxel to human serum albumin. JBIC J. Biol. Inorg. Chem. 2001, 268, 2187–2191. [Google Scholar] [CrossRef] [PubMed]
  35. Singh, S.; Dash, A.K. Paclitaxel in cancer treatment: Perspectives and prospects of its delivery challenges. Crit. Rev. Ther. Drug Carr. Syst. 2009, 26, 333–372. [Google Scholar] [CrossRef] [PubMed]
  36. Gradishar, W.J.; Tjulandin, S.; Davidson, N.; Shaw, H.; Desai, N.; Bhar, P.; Hawkins, M.; O’Shaughnessy, J. Phase III Trial of Nanoparticle Albumin-Bound Paclitaxel Compared with Polyethylated Castor Oil–Based Paclitaxel in Women with Breast Cancer. J. Clin. Oncol. 2005, 23, 7794–7803. [Google Scholar] [CrossRef] [PubMed]
  37. Chen, Q.; Zhang, Q.-Z.; Liu, J.; Li, L.-Q.; Zhao, W.-H.; Wang, Y.-J.; Zhou, Q.-H.; Li, L. Multi-center prospective randomized trial on paclitaxel liposome and traditional taxol in the treatment of breast cancer and non-small-cell lung cancer. Zhonghua Zhong Liu Za Zhi Chinese J. Oncol. 2003, 25, 190–192. [Google Scholar]
  38. Xu, X.; Wang, L.; Xu, Q.H.; Huang, E.X.; Qian, D.Y.; Xiang, J. Clinical comparison between paclitaxel liposome (Lipusu®) and paclitaxel for treatment of patients with meta-static gastric cancer. Asian Pac. J. Cancer Prev. 2013, 14, 2591–2594. [Google Scholar] [CrossRef] [Green Version]
  39. Kim, T.-Y.; Kim, D.-W.; Chung, J.-Y.; Shin, S.G.; Kim, S.-C.; Heo, D.S.; Kim, N.K.; Bang, Y.-J. Phase I and Pharmacokinetic Study of Genexol-PM, a Cremophor-Free, Polymeric Micelle-Formulated Paclitaxel, in Patients with Advanced Malignancies. Clin. Cancer Res. 2004, 10, 3708–3716. [Google Scholar] [CrossRef] [Green Version]
  40. Lim, W.T.; Tan, E.H.; Toh, C.K.; Hee, S.W.; Leong, S.S.; Ang, P.C.S.; Wong, N.S.; Chowbay, B. Phase I pharmacokinetic study of a weekly liposomal paclitaxel formulation (Genexol®-PM) in patients with solid tumors. Ann. Oncol. 2009, 21, 382–388. [Google Scholar] [CrossRef]
  41. Saif, M.W.; Podoltsev, N.A.; Rubin, M.S.; Figueroa, J.A.; Lee, M.Y.; Kwon, J.; Rowen, E.; Yu, J.; Kerr, R.O. Phase II Clinical Trial of Paclitaxel Loaded Polymeric Micelle in Patients with Advanced Pancreatic Cancer. Cancer Investig. 2010, 28, 186–194. [Google Scholar] [CrossRef]
  42. Sartori, S.; Caporale, A.; Rechichi, A.; Cufari, D.; Cristallini, C.; Barbani, N.; Giusti, P.; Ciardelli, G. Biodegradable paclitaxel-loaded microparticles prepared from novel block copolymers: Influence of polymer composition on drug encapsulation and release. J. Pept. Sci. 2013, 19, 205–213. [Google Scholar] [CrossRef]
  43. He, H.; Chen, S.; Zhou, J.; Dou, Y.; Song, L.; Che, L.; Zhou, X.; Chen, X.; Jia, Y.; Zhang, J.; et al. Cyclodextrin-derived pH-responsive nanoparticles for delivery of paclitaxel. Biomaterials 2013, 34, 5344–5358. [Google Scholar] [CrossRef]
  44. Wang, H.; Cheng, G.; Du, Y.; Ye, L.; Chen, W.; Zhang, L.; Wang, T.; Tian, J.; Fu, F. Hypersensitivity reaction studies of a polyethoxylated castor oil-free, liposome-based alternative paclitaxel formulation. Mol. Med. Rep. 2013, 7, 947–952. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  45. Xia, X.-J.; Guo, R.-F.; Liu, Y.-L.; Zhang, P.-X.; Zhou, C.-P.; Jin, D.-J.; Wang, R.-Y. Formulation, Characterization and Hypersensitivity Evaluation of an Intravenous Emulsion Loaded with a Paclitaxel-Cholesterol Complex. Chem. Pharm. Bull. 2011, 59, 321–326. [Google Scholar] [CrossRef] [Green Version]
  46. Torchilin, V.P. Micellar Nanocarriers: Pharmaceutical Perspectives. Pharm. Res. 2007, 24, 1. [Google Scholar] [CrossRef] [PubMed]
  47. May, S.; Ben-Shaul, A. Molecular Theory of Lipid-Protein Interaction and the Lα-HII Transition. Biophys. J. 1999, 76, 751–767. [Google Scholar] [CrossRef] [Green Version]
  48. Lukyanov, A.N.; Torchilin, V.P. Micelles from lipid derivatives of water-soluble polymers as delivery systems for poorly soluble drugs. Adv. Drug Deliv. Rev. 2004, 56, 1273–1289. [Google Scholar] [CrossRef] [PubMed]
  49. Zhao, B.J.; Ke, X.Y.; Huang, Y.; Chen, X.M.; Zhao, X.; Zhao, B.X.; Lu, W.L.; Lou, J.N.; Zhang, X.; Zhang, Q. The antiangiogenic efficacy of NGR-modified PEG–DSPE micelles containing paclitaxel (NGR-M-PTX) for the treatment of glioma in rats. J. Drug Target. 2011, 19, 382–390. [Google Scholar] [CrossRef]
  50. Chen, T.; Tu, L.; Wang, G.; Qi, N.; Wu, W.; Zhang, W.; Feng, J. Multi-functional chitosan polymeric micelles as oral paclitaxel delivery systems for enhanced bioavailability and anti-tumor efficacy. Int. J. Pharm. 2020, 578, 119105. [Google Scholar] [CrossRef]
  51. Mutlu-Agardan, N.B.; Sarisozen, C.; Torchilin, V. Cytotoxicity of Novel Redox Sensitive PEG 2000-SS-PTX Micelles against Drug-Resistant Ovarian and Breast Cancer Cells. Pharm. Res. 2020, 37, 65. [Google Scholar] [CrossRef]
  52. Feng, L.; Mumper, R.J. A critical review of lipid-based nanoparticles for taxane delivery. Cancer Lett. 2013, 334, 157–175. [Google Scholar] [CrossRef] [Green Version]
  53. Fetterly, G.J.; Grasela, T.H.; Sherman, J.W.; Dul, J.L.; Grahn, A.; LeComte, D.; Fiedler-Kelly, J.; Damjanov, N.; Fishman, M.; Kane, M.P.; et al. Pharmacokinetic/Pharmacodynamic Modeling and Simulation of Neutropenia during Phase I Development of Liposome-Entrapped Paclitaxel. Clin. Cancer Res. 2008, 14, 5856–5863. [Google Scholar] [CrossRef] [Green Version]
  54. Crosasso, P.; Ceruti, M.; Brusa, P.; Arpicco, S.; Dosio, F.; Cattel, L. Preparation, characterization and properties of sterically stabilized paclitaxel-containing liposomes. J. Control. Release 2000, 63, 19–30. [Google Scholar] [CrossRef]
  55. Klibanov, A.L.; Maruyama, K.; Torchilin, V.P.; Huang, L. Amphipathic polyethyleneglycols effectively prolong the circulation time of liposomes. FEBS Lett. 1990, 268, 235–237. [Google Scholar] [CrossRef] [Green Version]
  56. Yoshizawa, Y.; Kono, Y.; Ogawara, K.-I.; Kimura, T.; Higaki, K. PEG liposomalization of paclitaxel improved its in vivo disposition and anti-tumor efficacy. Int. J. Pharm. 2011, 412, 132–141. [Google Scholar] [CrossRef] [PubMed]
  57. Abu Lila, A.; Kiwada, H.; Ishida, T. The accelerated blood clearance (ABC) phenomenon: Clinical challenge and approaches to manage. J. Control. Release 2013, 172, 38–47. [Google Scholar] [CrossRef]
  58. Biswas, S.; Dodwadkar, N.S.; Deshpande, P.; Torchilin, V.P. Liposomes loaded with paclitaxel and modified with novel triphenylphosphonium-PEG-PE conjugate possess low toxicity, target mitochondria and demonstrate enhanced antitumor effects in vitro and in vivo. J. Control. Release 2012, 159, 393–402. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  59. Liu, Y.; Ran, R.; Chen, J.; Kuang, Q.; Tang, J.; Mei, L.; Zhang, Q.; Gao, H.; Zhang, Z.; He, Q. Paclitaxel loaded liposomes decorated with a multifunctional tandem peptide for glioma targeting. Biomaterials 2014, 35, 4835–4847. [Google Scholar] [CrossRef]
  60. Luo, L.-M.; Huang, Y.; Zhao, B.-X.; Zhao, X.; Duan, Y.; Du, R.; Yu, K.-F.; Song, P.; Zhao, Y.; Zhang, X.; et al. Anti-tumor and anti-angiogenic effect of metronomic cyclic NGR-modified liposomes containing paclitaxel. Biomaterials 2013, 34, 1102–1114. [Google Scholar] [CrossRef]
  61. Qin, L.I.; Wang, C.Z.; Fan, H.J.; Zhang, C.J.; Zhang, H.W.; Lv, M.H.; Cui, S.D. A dual-targeting liposome conjugated with transferrin and arginine-glycine-aspartic acid peptide for glio-ma-targeting therapy. Oncol. Lett. 2014, 8, 2000–2006. [Google Scholar] [CrossRef] [Green Version]
  62. Büyükköroğlu, G.; Şenel, B.; Başaran, E.; Gezgin, S. Development of paclitaxel-loaded liposomal systems with anti-her2 antibody for targeted therapy. Trop. J. Pharm. Res. 2016, 15, 895. [Google Scholar] [CrossRef] [Green Version]
  63. Chen, D.; Jiang, X.; Liu, J.; Jin, X.; Zhang, C.; Ping, Q. In vivo evaluation of novel pH-sensitive mPEG-Hz-Chol conjugate in liposomes: Pharmacokinetics, tissue distribution, efficacy assessment. Artif. Cells Blood Substit. Biotechnol. 2010, 38, 136–142. [Google Scholar] [CrossRef]
  64. Monteiro, L.O.; Malachias, A.; Pound-Lana, G.; Magalhaes-Paniago, R.; Mosqueira, V.C.; Oliveira, M.C.; de Barros, A.L.B.; Leite, E.A. Paclitaxel-loaded pH-sensitive liposome: New insights on structural and physicochemical characterization. Langmuir 2018, 34, 5728–5737. [Google Scholar] [CrossRef]
  65. Qi, J.; Lu, Y.; Wu, W. Absorption, Disposition and Pharmacokinetics of Solid Lipid Nanoparticles. Curr. Drug Metab. 2012, 13, 418–428. [Google Scholar] [CrossRef]
  66. Shahgaldian, P.; Da Silva, E.; Coleman, A.W.; Rather, B.; Zaworotko, M.J. Para-acyl-calix-arene based solid lipid nanoparticles (SLNs): A detailed study of preparation and stability parameters. Int. J. Pharm. 2003, 253, 23–38. [Google Scholar] [CrossRef]
  67. Yegin, A.B.; Benoît, J.-P.; Lamprecht, A. Paclitaxel-loaded lipid nanoparticles prepared by solvent injection or ultra-sound emulsification. Drug Dev. Ind. Pharm. 2006, 32, 1089–1094. [Google Scholar] [CrossRef] [PubMed]
  68. Yuan, H.; Miao, J.; Du, Y.-Z.; You, J.; Hu, F.-Q.; Zeng, S. Cellular uptake of solid lipid nanoparticles and cytotoxicity of encapsulated paclitaxel in A549 cancer cells. Int. J. Pharm. 2008, 348, 137–145. [Google Scholar] [CrossRef] [PubMed]
  69. Xu, W.; Bae, E.J.; Lee, M.-K. Enhanced anticancer activity and intracellular uptake of paclitaxel-containing solid lipid nanoparticles in multidrug-resistant breast cancer cells. Int. J. Nanomed. 2018, 13, 7549–7563. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  70. Valsalakumari, R.; Yadava, S.K.; Szwed, M.; Pandya, A.D.; Mælandsmo, G.M.; Torgersen, M.L.; Iversen, T.-G.; Skotland, T.; Sandvig, K.; Giri, J. Mechanism of cellular uptake and cytotoxicity of paclitaxel loaded lipid nanocapsules in breast cancer cells. Int. J. Pharm. 2021, 597, 120217. [Google Scholar] [CrossRef]
  71. Dong, X.; Mattingly, C.A.; Tseng, M.T.; Cho, M.J.; Liu, Y.; Adams, V.R.; Mumper, R.J. Doxorubicin and Paclitaxel-Loaded Lipid-Based Nanoparticles Overcome Multidrug Resistance by Inhibiting P-Glycoprotein and Depleting ATP. Cancer Res. 2009, 69, 3918–3926. [Google Scholar] [CrossRef] [Green Version]
  72. Tammam, S.N. Lipid Based Nanoparticles as Inherent Reversing Agents of Multidrug Resistance in Cancer. Curr. Pharm. Des. 2017, 23, 6714–6729. [Google Scholar] [CrossRef]
  73. Pandey, A.; Jain, D.S.; Chakraborty, S. Poly Lactic-Co-Glycolic Acid (PLGA) Copolymer and Its Pharmaceutical Application. Handb. Polym. Pharm. Technol. 2015, 2, 151–172. [Google Scholar]
  74. Astete, C.E.; Sabliov, C.M. Synthesis and characterization of PLGA nanoparticles. J. Biomater. Sci. Polym. Ed. 2006, 17, 247–289. [Google Scholar] [CrossRef] [PubMed]
  75. Berthet, M.; Gauthier, Y.; Lacroix, C.; Verrier, B.; Monge, C. Nanoparticle-based dressing: The future of wound treatment? Trends Biotechnol. 2017, 35, 770–784. [Google Scholar] [CrossRef] [PubMed]
  76. Rezvantalab, S.; Drude, N.; Moraveji, M.K.; Güvener, N.; Koons, E.K.; Shi, Y.; Lammers, T.; Kiessling, F. PLGA-Based Nanoparticles in Cancer Treatment. Front. Pharmacol. 2018, 9, 1260. [Google Scholar] [CrossRef] [Green Version]
  77. Jin, C.; Wu, H.; Liu, J.; Bai, L.; Guo, G. The effect of paclitaxel-loaded nanoparticles with radiation on hypoxic MCF-7 cells. J. Clin. Pharm. Ther. 2007, 32, 41–47. [Google Scholar] [CrossRef]
  78. Dinarvand, R.; Sepehri, N.; Manouchehri, S.; Rouhani, H.; Atyabi, F. Polylactide-co-glycolide nanoparticles for controlled delivery of anticancer agents. Int. J. Nanomed. 2011, 6, 877–895. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  79. Mirakabad, F.S.T.; Nejati-Koshki, K.; Akbarzadeh, A.; Yamchi, M.R.; Milani, M.; Zarghami, N.; Zeighamian, V.; Rahimzadeh, A.; Alimohammadi, S.; Hanifehpour, Y.; et al. PLGA-Based Nanoparticles as Cancer Drug Delivery Systems. Asian Pac. J. Cancer Prev. 2014, 15, 517–535. [Google Scholar] [CrossRef] [Green Version]
  80. Fonseca, C.; Simões, S.; Gaspar, R. Paclitaxel-loaded PLGA nanoparticles: Preparation, physicochemical characterization and in vitro anti-tumoral activity. J. Control. Release 2002, 83, 273–286. [Google Scholar] [CrossRef] [Green Version]
  81. Danhier, F.; Lecouturier, N.; Vroman, B.; Jérôme, C.; Marchand-Brynaert, J.; Feron, O.; Préat, V. Paclitaxel-loaded PEGylated PLGA-based nanoparticles: In vitro and in vivo evaluation. J. Control. Release 2009, 133, 11–17. [Google Scholar] [CrossRef]
  82. Mo, Y.; Lim, L.-Y. Paclitaxel-loaded PLGA nanoparticles: Potentiation of anticancer activity by surface conjugation with wheat germ agglutinin. J. Control. Release 2005, 108, 244–262. [Google Scholar] [CrossRef]
  83. Esfandyari-Manesh, M.; Mostafavi, S.H.; Majidi, R.F.; Koopaei, M.N.; Ravari, N.S.; Amini, M.; Darvishi, B.; Ostad, S.N.; Atyabi, F.; Dinarvand, R. Improved anticancer delivery of paclitaxel by albumin surface modification of PLGA nano-particles DARU. J. Pharm. Sci. 2015, 23, 28. [Google Scholar]
  84. Cerqueira, B.B.S.; Lasham, A.; Shelling, A.N.; Al-Kassas, R. Development of biodegradable PLGA nanoparticles surface engineered with hyaluronic acid for targeted delivery of paclitaxel to triple negative breast cancer cells. Mater. Sci. Eng. C 2017, 76, 593–600. [Google Scholar] [CrossRef] [PubMed]
  85. Godara, S.; Lather, V.; Kirthanashri, S.V.; Awasthi, R.; Pandita, D. Lipid-PLGA hybrid nanoparticles of paclitaxel: Preparation, characterization, in vitro and in vivo evaluation. Mater. Sci. Eng. C 2020, 109, 110576. [Google Scholar] [CrossRef]
  86. Kim, C.; Lee, A.S.C.; Kang, S.W.; Kwon, I.C.; Kim, A.Y.-H.; Jeong, S.Y. Synthesis and the Micellar Characteristics of Poly(ethylene oxide)−Deoxycholic Acid Conjugates1. Langmuir 2000, 16, 4792–4797. [Google Scholar] [CrossRef]
  87. Kim, C.; Lee, S.C.; Kwon, I.C.; Chung, H.; Jeong, S.Y. Complexation of Poly (2-ethyl-2-oxazoline)-b lock-poly (ε-caprolactone) Micelles with Multifunctional Car-boxylic Acids. Macromolecules 2002, 35, 193–200. [Google Scholar] [CrossRef]
  88. Patel, N.K.; Sinha, V.K. Synthesis, Characterization and Optimization of Water-Soluble Chitosan Derivatives. Int. J. Polym. Mater. Polym. Biomater. 2009, 58, 548–560. [Google Scholar] [CrossRef]
  89. Chen, X.-G.; Park, H.-J. Chemical characteristics of O-carboxymethyl chitosans related to the preparation conditions. Carbohydr. Polym. 2003, 53, 355–359. [Google Scholar] [CrossRef]
  90. Cao, J.; Zhou, N. Progress in antitumor studies of chitosan. Chin. J. Biochem. Pharm. 2005, 26, 127. [Google Scholar]
  91. Gupta, U.; Sharma, S.; Khan, I.; Gothwal, A.; Sharma, A.K.; Singh, Y.; Chourasia, M.K.; Kumar, V. Enhanced apoptotic and anticancer potential of paclitaxel loaded biodegradable nanoparticles based on chitosan. Int. J. Biol. Macromol. 2017, 98, 810–819. [Google Scholar] [CrossRef]
  92. Lv, P.-P.; Ma, Y.-F.; Yu, R.; Yue, H.; Ni, D.-Z.; Wei, W.; Ma, G.-H. Targeted Delivery of Insoluble Cargo (Paclitaxel) by PEGylated Chitosan Nanoparticles Grafted with Arg-Gly-Asp (RGD). Mol. Pharm. 2012, 9, 1736–1747. [Google Scholar] [CrossRef]
  93. Ashrafizadeh, M.; Ahmadi, Z.; Mohamadi, N.; Zarrabi, A.; Abasi, S.; Dehghannoudeh, G.; Tamaddondoust, R.N.; Khanbabaei, H.; Mohammadinejad, R.; Thakur, V.K. Chitosan-based advanced materials for docetaxel and paclitaxel delivery: Recent advances and future directions in cancer theranostics. Int. J. Biol. Macromol. 2020, 145, 282–300. [Google Scholar] [CrossRef]
  94. Zhang, C.; Qu, G.; Sun, Y.; Wu, X.; Yao, Z.; Guo, Q.; Ding, Q.; Yuan, S.; Shen, Z.; Ping, Q.; et al. Pharmacokinetics, biodistribution, efficacy and safety of N-octyl-O-sulfate chitosan micelles loaded with paclitaxel. Biomaterials 2008, 29, 1233–1241. [Google Scholar] [CrossRef] [PubMed]
  95. Li, F.; Wu, H.; Zhang, H.; Li, F.; Gu, C.H.; Yang, Q. Antitumor drug Paclitaxel-loaded pH-sensitive nanoparticles targeting tumor extracellular pH. Carbohydr. Polym. 2009, 77, 773–778. [Google Scholar] [CrossRef]
  96. Nag, M.; Gajbhiye, V.; Kesharwani, P.; Jain, N.K. Transferrin functionalized chitosan-PEG nanoparticles for targeted delivery of paclitaxel to cancer cells. Colloids Surfaces B Biointerfaces 2016, 148, 363–370. [Google Scholar] [CrossRef] [PubMed]
  97. Ursachi, V.C.; Dodi, G.; Rusu, A.G.; Mihai, C.T.; Verestiuc, L.; Balan, V. Paclitaxel-Loaded Magnetic Nanoparticles Based on Biotinylated N-Palmitoyl Chitosan: Synthesis, Characterization and Preliminary In Vitro Studies. Molecules 2021, 26, 3467. [Google Scholar] [CrossRef]
  98. Rautio, J.; Kumpulainen, H.; Heimbach, T.; Oliyai, R.; Oh, D.; Järvinen, T.; Savolainen, J. Prodrugs: Design and clinical applications. Nat. Rev. Drug Discov. 2008, 7, 255–270. [Google Scholar] [CrossRef]
  99. Ettmayer, P.; Amidon, G.L.; Clement, A.B.; Testa, B. Lessons Learned from Marketed and Investigational Prodrugs. J. Med. Chem. 2004, 47, 2393–2404. [Google Scholar] [CrossRef]
  100. Skwarczynski, M.; Hayashi, Y.; Kiso, Y. Paclitaxel Prodrugs: Toward Smarter Delivery of Anticancer Agents. J. Med. Chem. 2006, 49, 7253–7269. [Google Scholar] [CrossRef]
  101. Li, C.; Yu, D.; Inoue, T.; Yang, D.J.; Milas, L.; Hunter, N.R.; Kim, E.E.; Wallace, S. Synthesis and evaluation of water-soluble polyethylene glycol-paclitaxel conjugate as a paclitaxel prodrug. Anticancer Drugs 1996, 7, 642–648. [Google Scholar] [CrossRef]
  102. Yu, Y.; Chen, C.-K.; Law, W.-C.; Mok, J.; Zou, J.; Prasad, P.N.; Cheng, C. Well-Defined Degradable Brush Polymer–Drug Conjugates for Sustained Delivery of Paclitaxel. Mol. Pharm. 2013, 10, 867–874. [Google Scholar] [CrossRef]
  103. Yu, Y.; Zou, J.; Yu, L.; Ji, W.; Li, Y.; Law, W.C.; Cheng, C. Functional polylactide-g-paclitaxel–poly (ethylene glycol) by azide–alkyne click chemistry. Macromolecules 2011, 44, 4793–4800. [Google Scholar] [CrossRef]
  104. Tong, R.; Cheng, J. Paclitaxel-initiated, controlled polymerization of lactide for the formulation of polymeric nanoparticulate delivery vehicles. Angew. Chem. Int. Ed. 2008, 47, 4830–4834. [Google Scholar] [CrossRef]
  105. Satsangi, A.; Roy, S.S.; Satsangi, R.K.; Vadlamudi, R.K.; Ong, J.L. Design of a Paclitaxel Prodrug Conjugate for Active Targeting of an Enzyme Upregulated in Breast Cancer Cells. Mol. Pharm. 2014, 11, 1906–1918. [Google Scholar] [CrossRef] [PubMed]
  106. Erez, R.; Segal, E.; Miller, K.; Satchi-Fainaro, R.; Shabat, D. Enhanced cytotoxicity of a polymer–drug conjugate with triple payload of paclitaxel. Bioorg. Med. Chem. 2009, 17, 4327–4335. [Google Scholar] [CrossRef] [PubMed]
  107. Singer, J.W. Paclitaxel poliglumex (XYOTAX™, CT-2103): A macromolecular taxane. J. Control. Release 2005, 109, 120–126. [Google Scholar] [CrossRef] [PubMed]
  108. Karmali, P.P.; Kotamraju, V.R.; Kastantin, M.; Black, M.; Missirlis, D.; Tirrell, M.; Ruoslahti, E. Targeting of albumin-embedded paclitaxel nanoparticles to tumors. Nanomed. Nanotechnol. Biol. Med. 2009, 5, 73–82. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  109. Shan, L.; Shan, X.; Zhang, T.; Zhai, K.; Gao, G.; Chen, X.; Gu, Y. Transferrin-conjugated paclitaxel prodrugs for targeted cancer therapy. RSC Adv. 2016, 6, 77987–77998. [Google Scholar] [CrossRef]
  110. Zhang, P.; Cheetham, A.G.; Lin, Y.-A.; Cui, H. Self-Assembled Tat Nanofibers as Effective Drug Carrier and Transporter. ACS Nano 2013, 7, 5965–5977. [Google Scholar] [CrossRef] [Green Version]
  111. Tian, R.; Wang, H.; Niu, R.; Ding, D. Drug delivery with nanospherical supramolecular cell penetrating peptide–taxol conjugates containing a high drug loading. J. Colloid Interface Sci. 2015, 453, 15–20. [Google Scholar] [CrossRef]
  112. Bhattacharyya, J.; Bellucci, J.J.; Weitzhandler, I.; McDaniel, J.; Spasojevic, I.; Li, X.; Lin, C.-C.; Chi, J.-T.; Chilkoti, A. A paclitaxel-loaded recombinant polypeptide nanoparticle outperforms Abraxane in multiple murine cancer models. Nat. Commun. 2015, 6, 7939. [Google Scholar] [CrossRef]
  113. Bradley, M.; Swindell, C.; Anthony, F.; Witman, P.; Devanesan, P.; Webb, N.; Baker, S.; Wolff, A.; Donehower, R. Tumor targeting by conjugation of DHA to paclitaxel. J. Control. Release 2001, 74, 233–236. [Google Scholar] [CrossRef]
  114. Ke, X.-Y.; Zhao, B.-J.; Zhao, X.; Wang, Y.; Huang, Y.; Chen, X.-M.; Zhao, B.-X.; Zhao, S.-S.; Zhang, X.; Zhang, Q. The therapeutic efficacy of conjugated linoleic acid—Paclitaxel on glioma in the rat. Biomaterials 2010, 31, 5855–5864. [Google Scholar] [CrossRef] [PubMed]
  115. Tam, T.Y.; Gao, J.; Kwon, G.S. Oligo (lactic acid) n-paclitaxel prodrugs for poly (ethylene glycol)-block-poly (lactic acid) micelles: Loading, release, and backbiting conversion for anticancer activity. J. Am. Chem. Soc. 2016, 138, 8674–8677. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  116. Su, H.; Koo, J.M.; Cui, H. One-component nanomedicine. J. Control. Release 2015, 219, 383–395. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  117. Ajaj, K.A.; Biniossek, M.L.; Kratz, F. Development of protein-binding bifunctional linkers for a new generation of dual-acting prodrugs. Bioconjug. Chem. 2009, 20, 390–396. [Google Scholar] [CrossRef]
  118. Cheetham, A.G.; Zhang, P.; Lin, Y.-A.; Lin, R.; Cui, H. Synthesis and self-assembly of a mikto-arm star dual drug amphiphile containing both paclitaxel and camptothecin. J. Mater. Chem. B 2014, 2, 7316–7326. [Google Scholar] [CrossRef] [Green Version]
  119. Tan, X.; Lu, X.; Jia, F.; Liu, X.; Sun, Y.; Logan, J.K.; Zhang, K. Blurring the Role of Oligonucleotides: Spherical Nucleic Acids as a Drug Delivery Vehicle. J. Am. Chem. Soc. 2016, 138, 10834–10837. [Google Scholar] [CrossRef]
  120. Berg, J. An Introduction to Interfaces of Colloids: The Bridge to Nanoscience; World Scientific Publishing Co.: Singapore, 2009. [Google Scholar]
  121. Paul, B.K.; Moulik, S.P. Microemulsions: An overview. J. Dispers. Sci. Technol. 1997, 18, 301–367. [Google Scholar] [CrossRef]
  122. Lawrence, M.J.; Warisnoicharoen, W. Recent Advances in Microemulsions as Drug Delivery Vehicles. In Nanoparticulates Drug Carr; World Scientific: Singapore, 2006; pp. 125–171. [Google Scholar]
  123. Forgiarini, A.M.; Esquena, J.; Gonzalez, C.; Solans, C. Formation of Nano-emulsions by Low-Energy Emulsification Methods at Constant Temperature. Langmuir 2001, 17, 2076–2083. [Google Scholar] [CrossRef]
  124. Kunieda, H.; Solans, C. Nano-Emulsions: Where Macro-and Microemulsions Meet; Imperial College Press: London, UK, 2001. [Google Scholar]
  125. Ma, P.; Mumper, R.J. Paclitaxel nano-delivery systems: A comprehensive review. J. Nanomed. Nano Technol. 2013, 4, 1000164. [Google Scholar] [CrossRef] [Green Version]
  126. Shakhwar, S.; Darwish, R.; Kamal, M.M.; Nazzal, S.; Pallerla, S.; Abu Fayyad, A. Development and evaluation of paclitaxel nanoemulsion for cancer therapy. Pharm. Dev. Technol. 2020, 25, 510–516. [Google Scholar] [CrossRef]
  127. Narang, A.S.; Delmarre, D.; Gao, D. Stable drug encapsulation in micelles and microemulsions. Int. J. Pharm. 2007, 345, 9–25. [Google Scholar] [CrossRef] [PubMed]
  128. Pouton, C.W. Formulation of self-emulsifying drug delivery systems. Adv. Drug Deliv. Rev. 1997, 25, 47–58. [Google Scholar] [CrossRef]
  129. Veltkamp, S.A.; Thijssen, B.; Garrigue, J.S.; Lambert, G.; Lallemand, F.; Binlich, F.; Huitema, A.D.; Nuijen, B.; Nol, A.; Beijnen, J.H.; et al. A novel self-microemulsifying formulation of paclitaxel for oral administration to patients with advanced cancer. Br. J. Cancer 2006, 95, 729–734. [Google Scholar] [CrossRef]
  130. Meher, J.G.; Dixit, S.; Pathan, D.K.; Singh, Y.; Chandasana, H.; Pawar, V.K.; Sharma, M.; Bhatta, R.S.; Konwar, R.; Kesharwani, P.; et al. Paclitaxel-loaded TPGS enriched self-emulsifying carrier causes apoptosis by modulating survivin ex-pression and inhibits tumour growth in syngeneic mammary tumours. Artif. Cells Nanomed. Biotechnol. 2018, 46, S344–S358. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  131. Park, E.-S.; Maniar, M.; Shah, J.C. Biodegradable polyanhydride devices of cefazolin sodium, bupivacaine, and taxol for local drug delivery: Preparation, and kinetics and mechanism of in vitro release. J. Control. Release 1998, 52, 179–189. [Google Scholar] [CrossRef]
  132. Bode, C.; Kranz, H.; Siepmann, F.; Siepmann, J. In-situ forming PLGA implants for intraocular dexamethasone delivery. Int. J. Pharm. 2018, 548, 337–348. [Google Scholar] [CrossRef]
  133. Kamali, H.; Khodaverdi, E.; Hadizadeh, F.; Mohajeri, S.A. In-vitro, ex-vivo, and in-vivo evaluation of buprenorphine HCl release from an in situ forming gel of PLGA-PEG-PLGA using N-methyl-2-pyrrolidone as solvent. Mater. Sci. Eng. C 2019, 96, 561–575. [Google Scholar] [CrossRef]
  134. Samy, W.M.; I Ghoneim, A.; A Elgindy, N. Novel microstructured sildenafil dosage forms as wound healing promoters. Expert Opin. Drug Deliv. 2014, 11, 1525–1536. [Google Scholar] [CrossRef]
  135. Kempe, S.; Mäder, K. In situ forming implants—An attractive formulation principle for parenteral depot formulations. J. Control. Release 2012, 161, 668–679. [Google Scholar] [CrossRef]
  136. Packhaeuser, C.B.; Schnieders, J.; Oster, C.G.; Kissel, T. In situ forming parenteral drug delivery systems: An overview. Eur. J. Pharm. Biopharm. Drug Dispos. 2004, 58, 445–455. [Google Scholar] [CrossRef]
  137. Amini-Fazl, M.S. Biodegradation study of PLGA as an injectable in situ depot-forming implant for controlled release of paclitaxel. Polym. Bull. 2021, 3, 1–14. [Google Scholar] [CrossRef]
  138. Hollis, C.P.; Li, T. Nanocrystals Production, Characterization, and Application for Cancer Therapy. In Pharmaceutical Sciences Encyclopedia: Drug Discovery, Development, Manufacturing; Wiley & Sons, Inc.: New York, NY, USA, 2013; pp. 181–206. [Google Scholar]
  139. Wong, J.; Brugger, A.; Khare, A.; Chaubal, M.; Papadopoulos, P.; Rabinow, B.; Kipp, J.; Ning, J. Suspensions for intravenous (IV) injection: A review of development, preclinical and clinical aspects. Adv. Drug Deliv. Rev. 2008, 60, 939–954. [Google Scholar] [CrossRef] [PubMed]
  140. Rabinow, B.E. Nanosuspensions in drug delivery. Nat. Rev. Drug Discov. 2004, 3, 785–796. [Google Scholar] [CrossRef]
  141. Müller, H.R.; Gohla, S.; Keck, C.M. State of the art of nanocrystals—Special features, production, nanotoxicology aspects and intracellular delivery. Eur. J. Pharm. Biopharm. Drug Dispos. 2011, 78, 1–9. [Google Scholar] [CrossRef] [PubMed]
  142. Shegokar, R.; Müller, R.H. Nanocrystals: Industrially feasible multifunctional formulation technology for poorly soluble actives. Int. J. Pharm. 2010, 399, 129–139. [Google Scholar] [CrossRef] [PubMed]
  143. Merisko-Liversidge, E.; Liversidge, G.G.; Cooper, E.R. Nanosizing: A formulation approach for poorly-water-soluble compounds. Eur. J. Pharm. Sci. 2003, 18, 113–120. [Google Scholar] [CrossRef]
  144. Zhang, H.; Hollis, C.P.; Zhang, Q.; Li, T. Preparation and antitumor study of camptothecin nanocrystals. Int. J. Pharm. 2011, 415, 293–300. [Google Scholar] [CrossRef]
  145. Wang, J.; Muhammad, N.; Li, T.; Wang, H.; Liu, Y.; Liu, B.; Zhan, H. Hyaluronic Acid-Coated Camptothecin Nanocrystals for Targeted Drug Delivery to Enhance Anticancer Efficacy. Mol. Pharm. 2020, 17, 2411–2425. [Google Scholar] [CrossRef]
  146. Gao, L.; Liu, G.; Ma, J.; Wang, X.; Zhou, L.; Li, X.; Wang, F. Application of Drug Nanocrystal Technologies on Oral Drug Delivery of Poorly Soluble Drugs. Pharm. Res. 2013, 30, 307–324. [Google Scholar] [CrossRef]
  147. Sinha, B.; Müller, R.H.; Möschwitzer, J.P. Bottom-up approaches for preparing drug nanocrystals: Formulations and factors affecting particle size. Int. J. Pharm. 2013, 453, 126–141. [Google Scholar] [CrossRef]
  148. Xia, D.; Quan, P.; Piao, H.; Piao, H.; Sun, S.; Yin, Y.; Cui, F. Preparation of stable nitrendipine nanosuspensions using the precipitation–ultrasonication method for enhancement of dissolution and oral bioavailability. Eur. J. Pharm. Sci. 2010, 40, 325–334. [Google Scholar] [CrossRef] [PubMed]
  149. Hollis, C.P.; Li, T. Nanocrystals production, characterization, and application for cancer therapy. Pharm. Sci. Encycl. Drug Discov. Dev. Manuf. 2010, 1–26. [Google Scholar]
  150. De Castro, M.L.; Priego-Capote, F. Ultrasound-assisted crystallization (sonocrystallization). Ultrason. Sonochem. 2007, 14, 717–724. [Google Scholar] [CrossRef] [PubMed]
  151. Kakran, M.; Sahoo, N.G.; Tan, I.-L.; Li, L. Preparation of nanoparticles of poorly water-soluble antioxidant curcumin by antisolvent precipitation methods. J. Nanopart. Res. 2012, 14, 757. [Google Scholar] [CrossRef]
  152. Lonare, A.A.; Patel, S.R. Antisolvent crystallization of poorly water soluble drugs. Int. J. Chem. Eng. Appl. 2013, 4, 337. [Google Scholar] [CrossRef] [Green Version]
  153. Pawar, N.; Agrawal, S.; Methekar, R. Modeling, Simulation, and Influence of Operational Parameters on Crystal Size and Morphology in Semibatch Antisolvent Crystallization of α-Lactose Monohydrate. Cryst. Growth Des. 2018, 18, 4511–4521. [Google Scholar] [CrossRef]
  154. Crisp, J.; Dann, S.; Blatchford, C. Antisolvent crystallization of pharmaceutical excipients from aqueous solutions and the use of preferred orientation in phase identification by powder X-ray diffraction. Eur. J. Pharm. Sci. 2011, 42, 568–577. [Google Scholar] [CrossRef]
  155. Sharma, C.; Desai, M.; Patel, S.R. Effect of surfactants and polymers on morphology and particle size of telmisartan in ultrasound-assisted anti-solvent crystallization. Chem. Pap. 2019, 73, 1685–1694. [Google Scholar] [CrossRef]
  156. Miao, X.; Yang, W.; Feng, T.; Lin, J.; Huang, P. Drug nanocrystals for cancer therapy. Nanomed. Nanobiotechnol. 2018, 10, e1499. [Google Scholar] [CrossRef]
  157. Zhou, M.; Zhang, X.; Yu, C.; Nan, X.; Chen, X.; Zhang, X.-H. Shape regulated anticancer activities and systematic toxicities of drug nanocrystals in vivo. Nanomed. Nanotechnol. Biol. Med. 2016, 12, 181–189. [Google Scholar] [CrossRef]
  158. Lu, Y.; Wang, Z.-H.; Li, T.; McNally, H.; Park, K.; Sturek, M. Development and evaluation of transferrin-stabilized paclitaxel nanocrystal formulation. J. Control. Release 2014, 176, 76–85. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  159. Liu, J.; Tu, L.; Cheng, M.; Feng, J.; Jin, Y. Mechanisms for oral absorption enhancement of drugs by nanocrystals. J. Drug Deliv. Sci. Technol. 2020, 56, 101607. [Google Scholar] [CrossRef]
  160. Park, J.; Sun, B.; Yeo, Y. Albumin-coated nanocrystals for carrier-free delivery of paclitaxel. J. Control. Release 2017, 263, 90–101. [Google Scholar] [CrossRef] [PubMed]
  161. Park, J.; Park, J.E.; Hedrick, V.E.; Wood, K.V.; Bonham, C.; Lee, W.; Yeo, Y. A Comparative In Vivo Study of Albumin-Coated Paclitaxel Nanocrystals and Abraxane. Small 2018, 14, 1703670. [Google Scholar] [CrossRef] [PubMed]
  162. Sohn, J.S.; Yoon, D.S.; Sohn, J.Y.; Park, J.S.; Choi, J.S. Development and evaluation of targeting ligands surface modified paclitaxel nanocrystals. Mater. Sci. Eng. C 2017, 72, 228–237. [Google Scholar] [CrossRef]
  163. Sharma, S.; Singh, J.; Verma, A.; Teja, B.V.; Shukla, R.P.; Singh, S.K.; Sharma, V.; Konwar, R.; Mishra, P.R. Hyaluronic acid anchored paclitaxel nanocrystals improves chemotherapeutic efficacy and inhibits lung metastasis in tumor-bearing rat model. RSC Adv. 2016, 6, 73083–73095. [Google Scholar] [CrossRef]
  164. Zhang, H.; Hu, H.; Zhang, H.; Dai, W.; Wang, X.; Wang, X.; Zhang, Q. Effects of PEGylated paclitaxel nanocrystals on breast cancer and its lung metastasis. Nanoscale 2015, 7, 10790–10800. [Google Scholar] [CrossRef]
  165. Polomska, A.; Gauthier, M.A.; Leroux, J.C. In Vitro and In Vivo Evaluation of PEGylated Layer-by-Layer Polyelectro-lyte-Coated Paclitaxel Nanocrystals. Small 2017, 13, 1602066. [Google Scholar] [CrossRef]
  166. Zhao, J.; Du, J.; Wang, J.; An, N.; Zhou, K.; Hu, X.; Dong, Z.; Liu, Y. Folic Acid and Poly(ethylene glycol) Decorated Paclitaxel Nanocrystals Exhibit Enhanced Stability and Breast Cancer-Targeting Capability. ACS Appl. Mater. Interfaces 2021, 13, 14577–14586. [Google Scholar] [CrossRef]
  167. Wang, D.; Wang, Y.; Zhao, G.; Zhuang, J.; Wu, W. Improving systemic circulation of paclitaxel nanocrystals by surface hybridization of DSPE-PEG2000. Colloids Surfaces B Biointerfaces 2019, 182, 110337. [Google Scholar] [CrossRef]
  168. Guo, F.; Shang, J.; Zhao, H.; Lai, K.; Li, Y.; Fan, Z.; Hou, Z.; Su, G. Cube-shaped theranostic paclitaxel prodrug nanocrystals with surface functionalization of SPC and MPEG-DSPE for imaging and chemotherapy. Colloids Surfaces B Biointerfaces 2017, 160, 649–660. [Google Scholar] [CrossRef] [PubMed]
  169. Choi, J.-S.; Park, J.-S. Effects of paclitaxel nanocrystals surface charge on cell internalization. Eur. J. Pharm. Sci. 2016, 93, 90–96. [Google Scholar] [CrossRef] [PubMed]
  170. Liu, H.; Ma, Y.; Liu, D.; Fallon, J.K.; Liu, F. The Effect of Surfactant on Paclitaxel Nanocrystals: An In Vitro and In Vivo Study. J. Biomed. Nanotechnol. 2016, 12, 147–153. [Google Scholar] [CrossRef] [PubMed]
  171. Noh, J.-K.; Naeem, M.; Cao, J.; Lee, E.H.; Kim, M.-S.; Jung, Y.; Yoo, J.-W. Herceptin-functionalized pure paclitaxel nanocrystals for enhanced delivery to HER2-postive breast cancer cells. Int. J. Pharm. 2016, 513, 543–553. [Google Scholar] [CrossRef] [PubMed]
  172. Gao, W.; Chen, Y.; Thompson, D.H.; Park, K.; Li, T. Impact of surfactant treatment of paclitaxel nanocrystals on biodistribution and tumor accumulation in tumor-bearing mice. J. Control. Release 2016, 237, 168–176. [Google Scholar] [CrossRef]
  173. Han, X.; Su, R.; Huang, X.; Wang, Y.; Kuang, X.; Zhou, S.; Liu, H. Triphenylphosphonium-modified mitochondria-targeted paclitaxel nanocrystals for overcoming multidrug resistance. Asian J. Pharm. Sci. 2019, 14, 569–580. [Google Scholar] [CrossRef]
  174. Mei, D.; Gong, L.; Zou, Y.; Yang, D.; Liu, H.; Liang, Y.; Sun, N.; Zhao, L.; Zhang, Q.; Lin, Z. Platelet membrane-cloaked paclitaxel-nanocrystals augment postoperative chemotherapeutical efficacy. J. Control. Release 2020, 324, 341–353. [Google Scholar] [CrossRef] [PubMed]
  175. Huang, Z.-G.; Lv, F.-M.; Wang, J.; Cao, S.-J.; Liu, Z.-P.; Liu, Y.; Lu, W.-Y. RGD-modified PEGylated paclitaxel nanocrystals with enhanced stability and tumor-targeting capability. Int. J. Pharm. 2019, 556, 217–225. [Google Scholar] [CrossRef]
  176. Wang, J.; Lv, F.M.; Wang, D.L.; Du, J.L.; Guo, H.Y.; Chen, H.N.; Zhao, S.J.; Liu, Z.P.; Liu, Y. Synergistic Antitumor Effects on Drug-Resistant Breast Cancer of Paclitaxel/Lapatinib Composite Nano-crystals. Molecules 2020, 25, 604. [Google Scholar] [CrossRef] [Green Version]
  177. Sharma, S.; Verma, A.; Pandey, G.; Mittapelly, N.; Mishra, P.R. Investigating the role of Pluronic-g-Cationic polyelectrolyte as functional stabilizer for nanocrystals: Impact on Paclitaxel oral bioavailability and tumor growth. Acta Biomater. 2015, 26, 169–183. [Google Scholar] [CrossRef]
  178. Sharma, S.; Verma, A.; Teja, B.V.; Shukla, P.; Mishra, P.R. Development of stabilized Paclitaxel nanocrystals: In-vitro and in-vivo efficacy studies. Eur. J. Pharm. Sci. 2015, 69, 51–60. [Google Scholar] [CrossRef] [PubMed]
  179. Han, S.; Li, X.; Zhou, C.; Hu, X.; Zhou, Y.; Jin, Y.; Liu, Q.; Wang, L.; Li, X.; Liu, Y. Further Enhancement in Intestinal Absorption of Paclitaxel by Using Transferrin-Modified Paclitaxel Nano-crystals. ACS Appl. Bio Mater. 2020, 3, 4684–4695. [Google Scholar] [CrossRef] [PubMed]
  180. Liu, R.; Chang, Y.-N.; Xing, G.; Li, M.; Zhao, Y. Study on orally delivered paclitaxel nanocrystals: Modification, characterization and activity in the gastrointestinal tract. R. Soc. Open Sci. 2017, 4, 170753. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  181. Lin, Z.; Xu, S.; Gao, W.; Hu, H.; Chen, M.; Wang, Y.; He, B.; Dai, W.; Zhang, H.; Wang, X.; et al. A comparative investigation between paclitaxel nanoparticle- and nanocrystal-loaded thermosensitive PECT hydrogels for peri-tumoural administration. Nanoscale 2016, 8, 18782–18791. [Google Scholar] [CrossRef]
  182. Tiet, P.; Li, J.; Abidi, W.; Mooney, R.; Flores, L.; Aramburo, S.; Batalla-Covello, J.; Gonzaga, J.; Tsaturyan, L.; Kang, Y.; et al. Silica Coated Paclitaxel Nanocrystals Enable Neural Stem Cell Loading for Treatment of Ovarian Cancer. Bioconjug. Chem. 2019, 30, 1415–1424. [Google Scholar] [CrossRef]
  183. Huang, X.; Shi, Q.; Du, S.; Lu, Y.; Han, N. Poly-tannic acid coated paclitaxel nanocrystals for combinational photothermal-chemotherapy. Colloids Surfaces B Biointerfaces 2021, 197, 111377. [Google Scholar] [CrossRef]
  184. Lin, Z.; Mei, D.; Chen, M.; Wang, Y.; Chen, X.; Wang, Z.; He, B.; Zhang, H.; Wang, X.; Dai, W.; et al. A comparative study of thermo-sensitive hydrogels with water-insoluble paclitaxel in molecule, nanocrystal and microcrystal dispersions. Nanoscale 2015, 7, 14838–14847. [Google Scholar] [CrossRef]
  185. Sun, B.; Taha, M.S.; Ramsey, B.; Torregrosa-Allen, S.; Elzey, B.D.; Yeo, Y. Intraperitoneal chemotherapy of ovarian cancer by hydrogel depot of paclitaxel nanocrystals. J. Control. Release 2016, 235, 91–98. [Google Scholar] [CrossRef] [Green Version]
  186. Zhao, D.; Hu, C.; Fu, Q.; Lv, H. Combined chemotherapy for triple negative breast cancer treatment by paclitaxel and niclosamide nano-crystals loaded thermosensitive hydrogel. Eur. J. Pharm. Sci. 2021, 167, 105992. [Google Scholar] [CrossRef]
Polymers 14 00658 g001 550
Figure 1. The chemical structure of a PTX drug.
Figure 1. The chemical structure of a PTX drug.
Polymers 14 00658 g001
Polymers 14 00658 g002 550
Figure 2. The most common developed strategies to improve the delivery of paclitaxel drugs. SLN: solid lipid nanoparticles.
Figure 2. The most common developed strategies to improve the delivery of paclitaxel drugs. SLN: solid lipid nanoparticles.
Polymers 14 00658 g002
Table
Table 1. Modified PTX NC formulations for intravenous (IV) drug delivery.
Table 1. Modified PTX NC formulations for intravenous (IV) drug delivery.
PTX NCMethod of PreparationThe Models Used and the Reference or Control FormulaBenefits, Aims, and Other NotesRefs.
Albumin-coated PTX-NC
(Alb-PTX NCs)		NC crystallized in the medium containing Pluronic F-127 and then coated with albumin
“Cim-F-alb”		The new formula was compared to Abraxane and solvent-dissolved PTX

In vitro models including Biolayer interferometry analysisCell culture models: J774A.1 macrophages and SPARC+ B16F10 melanoma cells

In vivo model: mouse model of B16F10 melanoma		High drug loading (90%) and serum stability
Equivalent cytotoxicity.
More stability in undiluted serum.
Less interaction with serum proteins.

In cell culture studies, demonstrated suitable cell interaction profiles (depressed uptake by macrophages and great uptake by melanoma cells).

In the in vivo studies, exhibited prolonged plasma t1/2 and superior accumulation in tumors by about 1.5 and 4.6 times, respectively.
Exhibited superior antitumor efficacy.		[160,161]
Surface modified PTX-NCs with apo-transferrin (Tf) or hyaluronic acid (HA)PTX NCs were prepared by the nanoprecipitation
Method, and then the surface was modified by grafting with Tf or HA		The new formula was compared to PTX-NC and pure PTX drug

In vitro models: drug release in PBS with or without tween 80
Cell culture models: HaCaT normal cells and MCF-7 cancer cells		PTX release was faster.

Improve the cellular uptake, permeability, and cell growth inhibition (60%) against the cancer cells.
The effect on the normal cells was inferior.
Provide targeted delivery to cancer cells.		[162]
Hyaluronic acid (HA) coated PTX NCsThe NCs were prepared by the top-down method using homogenizationThe new formula was compared to Taxol® and heparin-coated PTX NCs

In vitro models: 2D monolayer and 3D spheroids
Cell culture models: MDA-MB 231 cells

In vivo model: LA-7 tumor-bearing rat model		Exhibited superior in vitro efficacy.

HA-PTX NCs incur receptor-mediated endocytosis by binding to CD44 receptors.

The in vivo studies indicated significantly prolonged blood circulation time of PTX.
Exhibited superior efficacy with reduced lung metastasis and toxicity.		[163]
PEGylated PTX NCsThe NCs were prepared by the antisolvent precipitation method combined with probe sonicationThe new formula was compared to PTX NCs and Taxol®

In vivo model: breast cancer xenografted mice model and a model of lung tumor metastasis quantified by the luciferase activity		Superior stability under both storage and physiological conditions.

In vivo studies showed significant improvement of the antitumor activity in facing in situ or metastatic tumors.		[164]
PEGylated polyelectrolyte multilayer-coated PTX NCsThe layer-by-layer method was used to coat PTX NCs with alternating
layers of oppositely charged polyelectrolytes, utilizing a PEGylated copolymer as the upper layer, and PTX NCs were prepared by a wet milling approach		The new formula was compared to Abraxane and PTX NCs

In vitro models: physiologically relevant media and human RBC hemolysis

Cell culture models: HT-29 cells

In vivo model: NMRI-nu mice bearing HT-29 subcutaneous xenografts		Slowed down the dissolution.
Offered colloidal stability in physiologically simulated media.

Showed no innate effect on cell viability using HT-29 cells.

No hemolytic activity was detected.

Quickly eliminated from the bloodstream and accumulated in the liver and spleen (mononuclear phagocyte organs).
Poor tumor accumulation.		[165]
PTX NCs modified with PEG and folic acid (FA)(PTX NCs-PEG-FA)PTX NCs were prepared by thin-film hydration method, which is a bottom-up method, and then modified with both PEG and
FA derivatives using thin-film hydration technique		The new formula was compared to Taxol®, PTX NCs, and PTX NCs-PEG

In vitro models: plasma
Cell culture models: 4T1 breast cancer cells

In vivo model: PK rat model and 4T1 orthotopic breast cancer-bearing nude mice		More size stability in plasma.
Improved cellular uptake and growth inhibition in cells.

An in vivo pharmacokinetic study showed a significant increase in the circulation of PTX.
In vivo cancer model showed that it significantly enhanced the accumulation of PTX in the tumor and effectively inhibited tumor growth. 		[166]
Surface hybridization of PTX NCs by DSPE-PEG 2000PTX NCs were prepared by anti-solvent method, and DSPE-PEG 2000 was incorporated by hybridizationThe new formula was compared to PTX solution and PTX NCs

In vitro models: in vitro release study

In vivo model: PK rats’ model		Similar size with an increased negative charge.
The in vitro study showed that the release of PTX was significantly slower.

The pharmacokinetics studies showed a greater area under the curve (AUC) and a lower clearance rate.		[167]
Cube-shaped PTX NC prodrug with surface functionalization of SPC and MPEG-DSPEPTX was labeled with fluorophore conjugate 4-chloro-7-nitro-1, 2, 3-benzoxadiazole (NBD-Cl) (PTX-NBD), which was synthesized by a nucleophilic substitution reaction of PTX with NBD-Cl in high yield. The PTX-NBD NCs were prepared by the anti-solvent method followed by surface functionalization of SPC and MPEG-DSPE.The new formula was compared to free PTX-NBD and the sphere-shaped PTX-NBD nanocrystals with surface functionalization of SPC and MPEG-DSPE (PTX-NBD@PC-PEG NSs)

Cell culture models: HeLa cells		The cube-shaped PTX-NBD@PC-PEG NCs exhibited better drug loading and stability properties.

It showed a remarkable decrease in burst release, efficiently enhanced cellular uptake, and had a better ability to kill cancer cells in vitro using HeLa cells.

These NCs can be useful for cell imaging and chemotherapy.		[168]
Surface-modified
PTX with positively charged poly(allylamine hydrochloride)
(PAH)		Nano-precipitation method (bottom-up approach) was employed to prepare PTX NCs, and the surface-modified NCs were obtained by an absorption method with the positively charged polymerThe new formula was compared to pure PTX, PTX NCs, and negatively charged poly (sodium 4-styrene sulfonate) PSS PTX NCs

In vitro models: PBS (pH 7.4) containing 0.5% (w/v) tween 80 and bovine serum albumin (BSA)
Cell culture models: A549 cells		Higher drug release.
Stronger interaction with bovine serum albumin.

Greater cellular internalization, uptake, and cytotoxicity.		[169]
A non-covalent transferrin-stabilized PTX NCsThe NCs were prepared by the antisolvent precipitation method augmented by sonicationThe new formula was compared to PTX solution, PTX NCs, and Taxol®

Cell culture models: human KB epidermal carcinoma cells and SKOV-3 ovarian cancer cells

In vivo model: mice inoculated with KB cells		The in vivo efficacy studies on KB-bearing mice showed a significantly superior tumor inhibition rate compared with PTX NCs and less efficacy than Taxol, but with a better toxicity profile. However, in cellular models, it showed similar efficacy 72 h after treatment.[158]
PTX NCs stabilized by D-α-tocopheryl polyethylene glycol 1000 succinate (TPGS)The NCs were prepared by three-phase nanoparticle engineering technology (3PNET)The new formula was compared to Taxol® and PTX/Pluronic F127 (F127) NCs

Cell culture models: P-glycoprotein-overexpressing PTX-resistant (H460/TaxR) cancer cells

In vivo model: PK using CD-1 mice		The greater the amount of TPGS in the formula, the greater cytotoxicity and cellular internalization.
TPGS PTX NCs demonstrated a significantly sustained and prolonged in vitro release pattern.

PK studies indicated more rapid clearance. However, they were more effective in promoting the accumulation of PTX in drug-resistant tumors.		[170]
Herceptin (HCT)-functionalized PTX NCsPTX NCs were prepared by sono-precipitation approach, and then HCT was coated, applying a facile non-covalent techniqueThe new formula was compared to PTX NCs and PTX powder

In vitro models: release study
Cell culture models: HER2-positive breast cancer cell lines		Exhibited a sustained release pattern comparable to PTX NCs.

Demonstrated a higher binding affinity, greater cell-specific internalization, and inhibition of growth to HER2-positive breast cancer cell lines.		[171]
PTX-NCs coated with Pluronic® F68 (PEG-PPG-PEG block polymer)The NCs were prepared by the anti-solvent methodThe new formula was compared to Taxol® and PTX NCs

In vivo model: tumor-bearing (HT-29 and KB cells) mice and female nude outbred mice		These NCs exhibited similar or better antitumor efficacy and lower toxicity in comparison with Taxol.
The in vivo study showed a significant enhancement in the blood circulation of PTX and accumulation in tumor tissue. However, the definite amount that reached the tumor was still minimal for the administered dose.
The maximum amount of the coated NCs was significantly obtained in the liver compared with the other organs relative to the uncoated PTX NCs.		[172]
Triphenylphosphonium (TPP+)-stabilized PTX NCs
(TPP+ PTX NCs)		Precipitation-resuspending methodThe new formula was compared to free PTX and unmodified PTX NCs

In vitro cell culture models: 2D monolayer and 3D multicellular spheroids (MCs) of MCF-7 cells and MCF-7/ADR cells		A mitochondria-targeted system was developed.
Showed the strongest cytotoxicity that was associated with a reduction in mitochondrial membrane potential.
Showed greater penetration and superior growth inhibition.		[173]
Platelet membrane-coated or cloaked PEG-PTX NCs
(PPNCs)		The modified emulsion-lyophilized crystallization methodThe new formula was compared to PTX NCs

Platelet aggregation was examined using a spectrophotometric method

In vitro drug releasee
Cell culture models: 4T1 breast cancer cells
In vivo model: BALB/c mice injected with 4T1 cells model		Minor risk of thrombus formation after injection was observed.

Higher cellular uptake and greater cytotoxicity.

In vivo studies showed the ability to deliver a higher dose of the drug and target the site of the coagulation (surgery or vascular disrupting), which improved the antitumor efficacy and decreased toxicities.		[174]
RGD peptide -PEGylated PTX NCs coated by polydopamine (PDA)
(NC@PDA-PEG-RGD)		The NCs were prepared using modified antisolvent–sonication methodThe new formula was compared to free PTX, PTX NCs, PTX NCs-PEG, and PTX NCs-PDA-PEG

In vitro models: plasma for size stabilityCell culture models: A549 lung cancer cell line

In vivo model: nude mice A549 bearing cancer model		More size stability in plasma.

Showed superior cellular uptake, growth inhibition, and cytotoxicity on A549 lung cancer cell line.

In vivo demonstrated significantly greater accumulation in the tumor and slower tumor growth.		[175]
PTX and lapatinib (LAPA) composite nanocrystals with PDA and PEG modification(cNC@PDA-PEG)PEG coat was introduced into the cNC via PDA) coat to get PEGylated composite NCs (cNC@PDA-PEG). The NCs were prepared using the bottom-up method or precipitation-resuspending method.The new formula was compared to free PTX and unmodified PTX NCs

In vitro models: plasma and blood
Cell culture models: MCF-7/ADR cancer cells		cNC@PDA-PEG had optimum size and stability.
The in vitro release study showed that both PTX and LAPA were released completely from cNC@PDA-PEG in 3 days, while only 30% of the drug was released from bulk drugs or unmodified NCs.

Showed negligible hemocytolysis and improved therapeutic effect on MCF-7/ADR through endocytosis of whole NCs.		[176]
Table
Table 2. Modified PTX NC formulations for oral drug delivery.
Table 2. Modified PTX NC formulations for oral drug delivery.
PTX NCMethod of PreparationThe Models Used and the Reference or Control FormulaBenefits, Aims, and Other NotesRef.
Pluronic-grafted chitosan as a stabilizer for PTX NC
(Pl-g-CH PTX NCs)		A novel Pluronic-grafted chitosan copolymer was established and then utilized as a functional stabilizer for PTX NCs. Generally, the NCs were prepared using a high-pressure homogenizer.The new formula was compared to Taxol®

Cell culture models: Caco-2 cells and B16 F10 murine melanoma cells

In vivo model for oral PK evaluation: Wistar ratsIn vivo model for efficacy study: healthy Balb/C mice injected with B16 F10 murine melanoma model		Improving intra-cellular accumulation.
Improving the absorption by the transcellular and paracellular routes.
Showed a P-gp inhibitory property.

The in vivo model demonstrated more anti-tumor efficacy and growth reduction after oral delivery, and this was related to the enhancement in the systemic circulation as both the absorption and bioavailability were improved significantly.		[177]
PTX NCs stabilized by tween 80 or low molecular weight synthetic polymer sodium polystyrene sulfonate (PSS)The top-down method was performed using a microfluidizer as a high-pressure homogenizer that was used to prepare the NCs without using any organic solventThe new formula was compared to formulas stabilized with high molecular weight polymers glycol chitosan (GC) and sodium alginate (SA), as well as with PTX solution and PTX-NCs

Cell culture models: MCF7 and MDA-MB breast cancer cell lines

In vivo model: PK in male Wistar rat model		The prepared NCs were more suitable, efficient, and exhibited a considerable increase in the dissolution rate, which indicated an enhancement in its bioavailability.
The in vitro cell culture study showed more efficiency and potency in killing and inhibiting the growth of the cancer cells.
In vivo pharmacokinetic studies demonstrated a considerable increase in AUC0–t, Cmax, and MRT and a decrease in Tmax.		[178]
Transferrin (TF)-modified PTX NCsPTX NCs were prepared using the precipitation–resuspension methodThe new formula was compared to Taxol® and unmodified PTX NCs

In vitro models: in situ intestinal perfusion study
Cell culture models: Caco-2 cells and MCF-7 cancer cells

In vivo model: PK Sprague Dawley rat model		Showed an enhancement of cellular monolayer penetration.
Had superior suppression in MCF-7 cell growth.

Showed an enhancement of intestinal absorption.
The pharmacokinetic studies also demonstrated greater Cmax and AUC than both PTX NCs and Taxol® while having the lowest tmax.		[179]
Poly(sodium pstyrenesulfonate) (PSS)-modified PTX NCsNot mentionedIn vitro models: interactions with biomolecules in oral delivery pathways
Cell culture models: Caco-2 cell lines		Suitable mono-dispersion and stability in the gastrointestinal tract (GIT) environments for at least 24 h.
No substantial interactions with pepsin or trypsin enzymes were detected in the GIT environments.
PSS-modified PTX NCs passed through the mimical intestinal epithelial cell (Caco-2 cell lines) with about 25% transmittance. However, the concentration of the NCs should be controlled to avoid toxic effects on the cells.		[180]
Table
Table 3. Modified PTX NC formulations for local and intraperitoneal drug delivery.
Table 3. Modified PTX NC formulations for local and intraperitoneal drug delivery.
PTX NCRoute of AdministrationMethod of PreparationThe Models Used and the Reference or Control FormulaBenefits, Aims, and Other NotesRef.
PTX NC-loaded PECT hydrogelsLocal delivery and peritumoral administrationPTX NCs were prepared by three-phase nanoparticle engineering technology (3PNET), while PTX-NC-based PECT (PTX-NC-PECT) gel was prepared based on the “cold” methodThe new formula was compared to a nanoparticle-based system (PTX-NP-PECT) and controlled hydrogel of Pluronic® F127

In vitro models: release study

In vivo model: MCF-7 tumor-bearing mouse models		High loading capacity of the drug.
In vitro release was more effective and homogeneous.

In vivo near-infrared fluorescence (NIRF) imaging indicated the ability to maintain the payloads of 1,1-dioctadecyltetramethyl indotricarbocyanine iodide (DiR) at a peri-tumoral site for about 21 days.
Exhibited the most complete release system with the greatest anti-tumor efficacy and apoptosis effect.		[181]
Silica-coated PTX NCs
Si		Intra-peritoneal (IP)Precipitation–resuspending
method		The new formula was compared to uncoated PTX-NC or Abraxane

Cell culture model: neural stem cells and OVCAR-8 cells

In vivo model: athymic nude mice which inoculated with 2 M OVCAR-8.eGFP.ffluc human ovarian cancer cells		More effective in loading neural stem
cells (NSCs).

In vivo studies showed that loaded NSCs preserved their migratory ability and, for low PTX dose, were more effective against ovarian tumors.		[182]
Poly-tannic acid-coated PTX NCs
(PTA-PTX NCs)		Intertumoral injectionThe NCs were prepared using the thin-film hydration method followed by probe sonicationThe new formula was compared with or without laser irradiation to PTX

Cell culture models: 4T1, A549, and HepG2 cells

In vivo model: 4T1 tumor-bearing mice		PTX NCs were prepared to act as a chemo-therapeutic agent and poly-tannic acid (pTA)-coated PTX NCs in the presence of Fe3+ acting as a potential agent for photothermal therapy (PTT).

The cellular uptake was significantly improved.
A synergistic effect with laser irradiation was observed.
Demonstrated mild photothermal effect in vivo and the greatest effect in tumor inhibition upon laser irradiation.		[183]
PTX NC with F127 hydrogelIntertumoral injectionPrecipitation–resuspending
method. The cold method was used for hydrogel preparation.		The new formula was compared to PTX or PTX microcrystal-based hydrogels

In vitro erosion of the hydrogels and drug release

In vivo model: 4T1 tumor-bearing BALB/c mice		PTX NCs gel offered optimum properties with high drug loading combined with moderate drug release and erosion profiles.
Superior anti-tumor efficacy in 4T1 tumor-bearing BALB/c mice.		[184]
In situ cross-linkable hydrogel depot containing PTX NCsIntraperitoneal (IP)Anti-solvent and temperature-induced crystallization methodThe new formula was compared to Taxol® and microparticulate PTX precipitates (PPT)

Cell culture models: SKOV3 cells

In vivo model: healthy Balb/c mice for toxicity studies and Balb/c mice (SKOV3-Luc) cell-bearing mice for the efficacy study		Superior killing efficiency and more toxicity in SKOV3 cell line.

The in vivo study indicated improved dissolution, cellular uptake, and lower maximum tolerated dose.
It also showed that a single IP dose was sufficient in extending the survival of tumor-bearing mice.		[185]
PTX-NCs combined with niclosamide (NLM) NLM-NCs co-loaded PLGA-PEG-PLGA thermosensitive hydrogel
(PN-NCs-Ts)		Intratumoral injectionPTX-NCs were prepared by the “3PNET” methodThe new formula was compared to PTX-NCs, PTX-NCs-Ts Gel, NLM-NCs, NLM-NCs-Ts gel, and PN–NCs-Ts gel

In vitro drug release

Cell culture models: MDA-MB-231 cells

In vivo model: BALB/c nude mice inoculated with MDA-MB-231 cells		Sustained and significantly delayed drug release both in vitro and in vivo.
The combination with NLM improved PTX cellular uptake, apoptosis, and provided inhibition of cell migration.
The in vivo studies showed significant inhibition of tumor growth with acceptable safety and effectively overcoming it. Triple-negative breast cancer (TNBC) progress and drastically prevented breast cancer stem cells (BCSCs).		[186]
Publisher’s Note: MDPI stays neutral with regard to jurisdictional claims in published maps and institutional affiliations.

Share and Cite

MDPI and ACS Style

Haddad, R.; Alrabadi, N.; Altaani, B.; Li, T. Paclitaxel Drug Delivery Systems: Focus on Nanocrystals’ Surface Modifications. Polymers 2022, 14, 658. https://doi.org/10.3390/polym14040658

AMA Style

Haddad R, Alrabadi N, Altaani B, Li T. Paclitaxel Drug Delivery Systems: Focus on Nanocrystals’ Surface Modifications. Polymers. 2022; 14(4):658. https://doi.org/10.3390/polym14040658

Chicago/Turabian Style

Haddad, Razan, Nasr Alrabadi, Bashar Altaani, and Tonglei Li. 2022. "Paclitaxel Drug Delivery Systems: Focus on Nanocrystals’ Surface Modifications" Polymers 14, no. 4: 658. https://doi.org/10.3390/polym14040658

APA Style

Haddad, R., Alrabadi, N., Altaani, B., & Li, T. (2022). Paclitaxel Drug Delivery Systems: Focus on Nanocrystals’ Surface Modifications. Polymers, 14(4), 658. https://doi.org/10.3390/polym14040658

Note that from the first issue of 2016, this journal uses article numbers instead of page numbers. See further details here.

Article Metrics

Back to TopTop