Calcium Orthophosphate-Containing Biocomposites and Hybrid Biomaterials for Biomedical Applications
Abstract
:1. Introduction
Inorganic Phases | wt % | Bioorganic Phases | wt % |
---|---|---|---|
CaPO4 (biological apatite) | ~60 | collagen type I | ~20 |
water | ~9 | non-collagenous proteins: osteocalcin, osteonectin, osteopontin, thrombospondin, morphogenetic proteins, sialoprotein, serum proteins | ~3 |
carbonates | ~4 | other traces: polysaccharides, lipids, cytokines | balance |
citrates | ~0.9 | primary bone cells: osteoblasts, osteocytes, osteoclasts | balance |
sodium | ~0.7 | ||
magnesium | ~0.5 | ||
other traces: Cl−, F−, K+ Sr2+, Pb2+, Zn2+, Cu2+, Fe2+ | balance |
2. General Information and Knowledge
Inorganic | Bioorganic |
---|---|
hardness, brittleness | elasticity, plasticity |
high density | low density |
thermal stability | permeability |
hydrophilicity | hydrophobicity |
high refractive index | selective complexation |
mixed valence slate (red-ox) | chemical reactivity |
strength | bioactivity |
3. The Major Constituents
3.1. CaPO4
Ca/P Molar Ratio | Compound | Formula | Solubility at 25 °C, −log (Ks) | Solubility at 25 °C, g/L | pH Stability Range in Aqueous Solutions at 25 °C |
---|---|---|---|---|---|
0.5 | Monocalcium phosphate monohydrate (MCPM) | Ca(H2PO4)2·H2O | 1.14 | ~18 | 0.0–2.0 |
0.5 | Monocalcium phosphate anhydrous (MCPA or MCP) | Ca(H2PO4)2 | 1.14 | ~17 | [c] |
1.0 | Dicalcium phosphate dihydrate (DCPD), mineral brushite | CaHPO4·2H2O | 6.59 | ~0.088 | 2.0–6.0 |
1.0 | Dicalcium phosphate anhydrous (DCPA or DCP), mineral monetite | CaHPO4 | 6.90 | ~0.048 | [c] |
1.33 | Octacalcium phosphate (OCP) | Ca8(HPO4)2(PO4)4·5H2O | 96.6 | ~0.0081 | 5.5–7.0 |
1.5 | α-Tricalcium phosphate (α-TCP) | α-Ca3(PO4)2 | 25.5 | ~0.0025 | [a] |
1.5 | β-Tricalcium phosphate (β-TCP) | β-Ca3(PO4)2 | 28.9 | ~0.0005 | [a] |
1.2–2.2 | Amorphous calcium phosphates (ACP) | CaxHy(PO4)z·nH2O, n = 3–4.5; 15%–20% H2O | [b] | [b] | ~5–12 [d] |
1.5–1.67 | Calcium-deficient hydroxyapatite (CDHA or Ca-def HA) [e] | Ca10−x(HPO4)x(PO4)6−x(OH)2−x (0 < x < 1) | ~85 | ~0.0094 | 6.5–9.5 |
1.67 | Hydroxyapatite (HA, HAp or OHAp) | Ca10(PO4)6(OH)2 | 116.8 | ~0.0003 | 9.5–12 |
1.67 | Fluorapatite (FA or FAp) | Ca10(PO4)6F2 | 120.0 | ~0.0002 | 7–12 |
1.67 | Oxyapatite (OA, OAp or OXA) [f], mineral voelckerite | Ca10(PO4)6O | ~69 | ~0.087 | [a] |
2.0 | Tetracalcium phosphate (TTCP or TetCP), mineral hilgenstockite | Ca4(PO4)2O | 38–44 | ~0.0007 | [a] |
- [a] These compounds cannot be precipitated from aqueous solutions.
- [b] Cannot be measured precisely. However, the following values were found: 25.7 ± 0.1 (pH = 7.40), 29.9 ± 0.1 (pH = 6.00), 32.7 ± 0.1 (pH = 5.28). The comparative extent of dissolution in acidic buffer is: ACP >> α-TCP >> β-TCP > CDHA >> HA > FA.
- [c] Stable at temperatures above 100 °C.
- [d] Always metastable.
- [e] Occasionally, it is called “precipitated HA (PHA)”.
- [f] Existence of OA remains questionable.
3.2. Polymers
Polymer | Thermal Properties (°C) | Tensile Modulus (GРa) | Degradation Time (Months) |
---|---|---|---|
polyglycolic acid (PGA) | Tg = 35–40 | 7.06 | 6–12 (strength loss within 3 weeks) |
Tm = 225–230 | |||
L-polylactic acid (LPLA) | Tg = 60–65 | 2.7 | >24 |
Tm = 173–178 | |||
D,L-polylactic acid (DLPLA) | Tg = 55–60 | 1.9 | 12–16 |
amorphous | |||
85/15 D,L-polylactic-co-glycolic acid (85/15 DLPLGA) | Tg = 50–55 | 2.0 | 5–6 |
amorphous | |||
75/25 D,L-polylactic-co-glycolic acid (75/25 DLPLGA) | Tg = 50–55 | 2.0 | 4–5 |
amorphous | |||
65/35 D,L-polylactic-co-glycolic acid (65/35 DLPLGA) | Tg = 45–50 | 2.0 | 3–4 |
amorphous | |||
50/50 D,L-polylactic-co-glycolic acid (50/50 DLPLGA) | Tg = 45–50 | 2.0 | 1–2 |
amorphous | |||
poly(ε-caprolactone) (PCL) | Tg = (−60)–(−65) | 0.4 | >24 |
Tm = 58–63 |
3.3. Inorganic Materials and Compounds
3.3.1. Metals
3.3.2. Glasses and Glass-Ceramics
3.3.3. Ceramics
3.3.4. Carbon
4. Biocomposites and Hybrid Biomaterials Containing CaPO4
- biocomposites with polymers;
- self-setting formulations;
- formulations based on nanodimensional CaPO4 and nanodimensional biocomposites;
- biocomposites with collagen;
- formulations with other bioorganic compounds and/or biological macromolecules;
- injectable bone substitutes (IBS);
- biocomposites with inorganic compounds, carbon and metals;
- functionally graded formulations;
- biosensors.
4.1. Biocomposites with Polymers
4.1.1. Apatite-Based Formulations
4.1.2. TCP-Based Formulations
4.1.3. Formulations Based on Other Types of CaPO4
4.2. Self-Setting Formulations
4.3. Formulations Based on Nanodimensional CaPO4 and Nanodimensional Biocomposites
4.4. Biocomposites with Collagen
4.5. Formulations with Other Bioorganic Compounds
4.6. Injectable Bone Substitutes (IBS)
Producer | Product name | Composition | Form |
---|---|---|---|
ApaTech (UK) | Actifuse™ | HA, polymer and aqueous solution | pre-mixed |
Actifuse™ Shape; Actifuse™ ABX | Si-substituted CaPO4 and a polymer | pre-mixed | |
Baxter (US) | TricOs Τ; TricOs | BCP (60% HA, 40% β-TCP) granules and Tissucol (fibrin glue) | to be mixed |
Berkeley Advanced Biomaterials | Bi-Ostetic Putty | not disclosed | not disclosed |
BioForm (US) | Calcium hydroxylapatite implant | HA powder embedded in a mixture of glycerine, water and CMC | pre-mixed |
Biomatlante (FR) | In’Oss™ | BCP granules (60% HA, 40% β-TCP; 0.08–0.2 mm) and 2% HPMC | pre-mixed |
MBCP Gel® | BCP granules (60% HA, 40% β-TCP; 0.08–0.2 mm) and 2% HPMC | pre-mixed | |
Hydr’Os | BCP granules (60% HA, 40% β-TCP; micro- and nano-sized particles) and saline solution | pre-mixed | |
Degradable solutions (CH) | Easy graft™ | β-TCP or BCP granules (0.45–l.0 mm) coated with 10 μm PLGA, N-methyl-2-pyrrolydone | to be mixed |
Dentsply (US) | Pepgen P-15® flow | HA (0.25–0.42 mm), P-15 peptide and aqueous Na hyaluronate solution | to be mixed |
DePuy Spine (US) | Healos® Fx | HA (20%–30%) and collagen | to be mixed |
Fluidinova (P) | nanoXIM TCP | β-TCP (5% or 15%) and water | pre-mixed |
nanoXIM HA | HA (5%, 15%, 30% or 40%) and water | pre-mixed | |
Integra LifeSciences (US) | Mozaik Osteoconductive Scaffold | β-TCP (80%) and type 1 collagen (20%) | to be mixed |
Mathys Ltd (CH) | Ceros® Putty/cyclOS® Putty | β-TCP granules (0.125–0.71 mm; 94%) and recombinant Na hyaluronate powder (6%) | to be mixed |
Medtronic (US) | Mastergraft® | BCP (85% HA, 15% β-TCP) and bovine collagen | to be mixed |
Merz Aesthetics (GER) | RADIESSE® | HA particles suspended in a gel | pre-mixed |
Osartis / ΑΑΡ (GER) | Ostim® | Nanocrystalline HA (35%) and water (65%) | pre-mixed |
Smith & Nephew (US) | JAXTCP | β-TCP granules and an aqueous solution of 1.75% CMC and 10% glycerol | to be mixed |
Stryker (US) | Calstrux™ | β-TCP granules and CMC | to be mixed |
Teknimed (FR) | Nanogel | HA (100 – 200 nm) (30%) and water (70%) | pre-mixed |
Therics (US) | Therigraft™ Putty | β-TCP granules and polymer | pre-mixed |
Zimmer (US) | Collagraft | BCP granules (65% HA, 35% β-TCP; 0.5–1.0 mm), bovine collagen and bone marrow aspirate | to be mixed |
4.7. Biocomposites with Inorganic Compounds, Carbon and Metals
4.8. Functionally Graded Formulations
4.9. Biosensors
5. Interactions among the Phases
6. Bioactivity and Biodegradation
7. Some Challenges and Critical Issues
- There are not enough reliable experimental and clinical data supporting the long-term performance of biocomposites with respect to monolithic traditional materials;
- The design of biocomposites and hybrid biomaterials is far more complex than that of conventional monolithic materials because of the large number of additional design variables to be considered;
- The available fabrication methods may limit the possible reinforcement configurations, may be time consuming, expensive, highly skilled and may require special cleaning and sterilization processes;
- There are no satisfactory standards yet for biocompatibility testing of the biocomposite implants because the ways in which the components of any biocomposite interact to living tissues are not completely understood;
- There are no adequate standards for the assessment of biocomposite fatigue performance because the fatigue behavior of such materials is far more complex and difficult to predict than that of traditional materials [197].
- Optimizing biocomposite processing conditions;
- Optimization of interfacial bonding and strength equivalent to natural bone;
- Optimization of the surface properties and pore size to maximize bone growth;
- Maintaining the adequate volume of the construct in vivo to allow bone formation to take place;
- Withstanding the load-bearing conditions;
- Matching the bioresorbability of the grafts and their biomechanical properties while forming new bone;
- Understanding the molecular mechanisms by which the cells and the biocomposite matrix interact with each other in vivo to promote bone regeneration;
- Supporting angiogenesis and vascularization for the growth of healthy bone cells and subsequent tissue formation and remodeling.
8. Conclusions
Conflicts of Interest
Abbreviations
A-W | apatite-wollastonite |
BMP | bone morphogenetic protein |
BSA | bovine serum albumin |
CMC | carboxymethylcellulose |
EVOH | a copolymer of ethylene and vinyl alcohol |
IBS | injectable bone substitute |
HDPE | high-density polyethylene |
HPMC | hydroxypropylmethylcellulose |
PA | polyamide |
PAA | polyacrylic acid |
PBT | polybutyleneterephthalate |
PCL | poly(ε-caprolactone) |
PDLLA | poly(D,L-lactic acid) |
PE | polyethylene |
PEEK | polyetheretherketone |
PEG | polyethylene glycol |
PGA | polyglycolic acid |
PHB | polyhydroxybutyrate |
PHBHV | poly(hydroxybutyrate-co-hydroxyvalerate) |
PHEMA | polyhydroxyethyl methacrylate |
PLA | polylactic acid |
PLGA | poly(lactic-co-glycolic) acid |
PLGC | co-polyester lactide-co-glycolide-co-ε-caprolactone |
PLLA | poly(L-lactic acid) |
PMMA | polymethylmethacrylate |
PP | polypropylene |
PPF | poly(propylene-co-fumarate) |
PSZ | partially stabilized zirconia |
PTMC | poly(trimethylene carbonate) |
PU | polyurethane |
PVA | polyvinyl alcohol |
PVAP | polyvinyl alcohol phosphate |
SEVA-C | a blend of EVOH with starch |
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Dorozhkin, S.V. Calcium Orthophosphate-Containing Biocomposites and Hybrid Biomaterials for Biomedical Applications. J. Funct. Biomater. 2015, 6, 708-832. https://doi.org/10.3390/jfb6030708
Dorozhkin SV. Calcium Orthophosphate-Containing Biocomposites and Hybrid Biomaterials for Biomedical Applications. Journal of Functional Biomaterials. 2015; 6(3):708-832. https://doi.org/10.3390/jfb6030708
Chicago/Turabian StyleDorozhkin, Sergey V. 2015. "Calcium Orthophosphate-Containing Biocomposites and Hybrid Biomaterials for Biomedical Applications" Journal of Functional Biomaterials 6, no. 3: 708-832. https://doi.org/10.3390/jfb6030708
APA StyleDorozhkin, S. V. (2015). Calcium Orthophosphate-Containing Biocomposites and Hybrid Biomaterials for Biomedical Applications. Journal of Functional Biomaterials, 6(3), 708-832. https://doi.org/10.3390/jfb6030708