Peptide Drug Discovery and Development

A special issue of Pharmaceuticals (ISSN 1424-8247).

Deadline for manuscript submissions: closed (20 September 2013) | Viewed by 70036

Special Issue Editors


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Guest Editor
Department of Chemical and Biological Engineering, Rensselaer Polytechnic Institute, 3217 CBIS, 110 8th St., Troy, NY 12180, USA
Interests: drug discovery; drug delivery; peptide engineering; high throughput screening; vaccine design; biomaterials and diagnostics

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Guest Editor
Georg Speyer Haus, Institute for Tumor Biology and Experimental Therapy, Paul Ehrlich Str. 42, D-60596 Frankfurt am Main, Germany
Interests: cytokine signal transduction; peptide inhibitors of oncoproteins; breast cancer research; experimental tumor therapy

Special Issue Information

Dear Colleagues,

The journal “Pharmaceuticals” is planning to publish a special issue covering the topic “Peptide drug discovery and development” and we are inviting you to contribute an article to this volume.

Peptides represent an attractive class of molecules for the design of new drugs, lead structures, drug carriers and excepients. Recent developments in peptide synthesis techniques and high-throughput screening platforms have created enthusiasm and interest in the design and discovery of novel peptides for a broad range of biological and pharmacological applications. Advances in peptide engineering have helped to overcome traditional limitations in peptide drug development such as poor systemic stability, rapid clearance and low binding affinities to biological targets. Currently there are nearly one hundred peptide based drug candidates in clinical trials, a dramatic increase compared to a decade ago. These developments signal a ‘second wave’ in peptide drug development.

The past two decades have also witnessed the derivation of chemically modified peptide constructs. They make use of non-natural amino acids, sugars and peptide bonds to provide  natural peptide backbones with desirable structural and functional properties. These ‘peptidomimetics’ have created exciting opportunities to engineer unique and complementary physical, chemical, structural and biological activities within the peptide sequence. The ability of peptides to recognize structural domains which are not limited to conventional drug binding pockets, makes them exciting leads for drug discovery. Peptide based drugs will therefore have a significant impact in the near future for the treatment of a broad range of indications including cancer, infectious diseases, neurodegenerative diseases and inflammation.

We would like you to share your contributions to the advances and opportunities in this burgeoning field of peptide drug discovery and development for this special issue. Areas of interest include:

  • Discovery of peptide drugs, prodrugs, formulations and drug carriers
  • Peptide drugs in oncology, neurology, inflammation and other physiological disorders
  • Peptide based vaccines and immunomodulating agents
  • In vitro and in vivo validation of peptide drugs
  • Advances in synthetic peptide design and screening techniques
  • Design and engineering of peptidomimetics and other novel hybrid peptide constructs
  • Approaches for improving peptide stability and target recognition
  • Peptide Theranostics

Dr. Pankaj Karande
Prof. Dr. Bernd Groner
Guest Editors

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Published Papers (2 papers)

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Review

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Review
Antimicrobial Peptides
by Ali Adem Bahar and Dacheng Ren
Pharmaceuticals 2013, 6(12), 1543-1575; https://doi.org/10.3390/ph6121543 - 28 Nov 2013
Cited by 1077 | Viewed by 52785
Abstract
The rapid increase in drug-resistant infections has presented a serious challenge to antimicrobial therapies. The failure of the most potent antibiotics to kill “superbugs” emphasizes the urgent need to develop other control agents. Here we review the history and new development of antimicrobial [...] Read more.
The rapid increase in drug-resistant infections has presented a serious challenge to antimicrobial therapies. The failure of the most potent antibiotics to kill “superbugs” emphasizes the urgent need to develop other control agents. Here we review the history and new development of antimicrobial peptides (AMPs), a growing class of natural and synthetic peptides with a wide spectrum of targets including viruses, bacteria, fungi, and parasites. We summarize the major types of AMPs, their modes of action, and the common mechanisms of AMP resistance. In addition, we discuss the principles for designing effective AMPs and the potential of using AMPs to control biofilms (multicellular structures of bacteria embedded in extracellular matrixes) and persister cells (dormant phenotypic variants of bacterial cells that are highly tolerant to antibiotics). Full article
(This article belongs to the Special Issue Peptide Drug Discovery and Development)
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636 KiB  
Review
Database-Guided Discovery of Potent Peptides to Combat HIV-1 or Superbugs
by Guangshun Wang
Pharmaceuticals 2013, 6(6), 728-758; https://doi.org/10.3390/ph6060728 - 27 May 2013
Cited by 90 | Viewed by 15904
Abstract
Antimicrobial peptides (AMPs), small host defense proteins, are indispensable for the protection of multicellular organisms such as plants and animals from infection. The number of AMPs discovered per year increased steadily since the 1980s. Over 2,000 natural AMPs from bacteria, protozoa, fungi, plants, [...] Read more.
Antimicrobial peptides (AMPs), small host defense proteins, are indispensable for the protection of multicellular organisms such as plants and animals from infection. The number of AMPs discovered per year increased steadily since the 1980s. Over 2,000 natural AMPs from bacteria, protozoa, fungi, plants, and animals have been registered into the antimicrobial peptide database (APD). The majority of these AMPs (>86%) possess 11–50 amino acids with a net charge from 0 to +7 and hydrophobic percentages between 31–70%. This article summarizes peptide discovery on the basis of the APD. The major methods are the linguistic model, database screening, de novo design, and template-based design. Using these methods, we identified various potent peptides against human immunodeficiency virus type 1 (HIV-1) or methicillin-resistant Staphylococcus aureus (MRSA). While the stepwise designed anti-HIV peptide is disulfide-linked and rich in arginines, the ab initio designed anti-MRSA peptide is linear and rich in leucines. Thus, there are different requirements for antiviral and antibacterial peptides, which could kill pathogens via different molecular targets. The biased amino acid composition in the database-designed peptides, or natural peptides such as θ-defensins, requires the use of the improved two-dimensional NMR method for structural determination to avoid the publication of misleading structure and dynamics. In the case of human cathelicidin LL-37, structural determination requires 3D NMR techniques. The high-quality structure of LL-37 provides a solid basis for understanding its interactions with membranes of bacteria and other pathogens. In conclusion, the APD database is a comprehensive platform for storing, classifying, searching, predicting, and designing potent peptides against pathogenic bacteria, viruses, fungi, parasites, and cancer cells. Full article
(This article belongs to the Special Issue Peptide Drug Discovery and Development)
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