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Cystatin C peptidomimetic derivative with antimicrobial and immunoregulatory properties as a potential wound supportive compound
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Journal of Tissue Science and Engineering

ISSN: 2157-7552

Open Access

Cystatin C peptidomimetic derivative with antimicrobial and immunoregulatory properties as a potential wound supportive compound


5th International Conference on Tissue Engineering & Regenerative Medicine

September 12-14, 2016 Berlin, Germany

Milena Deptula, Michal Pikula, Maria Smuzynska, Adam Krzystyniak, Maciej Zielinski, Paulina Langa, Adriana Schumacher, Franciszek Kasprzykowski, Miroslawa Cichorek, Piotr Trzonkowski and Sylwia Rodziewicz-Motowidlo

Medical University of Gdansk, Poland
University of Gdansk, Poland
Nencki Institute of Experimental Biology, Poland

Posters & Accepted Abstracts: J Tissue Sci Eng

Abstract :

Wound infections are one of the biggest challenges for pharmaceutical industry and modern medicine. They can hinder the healing process, cause chronic wounds formation and systematic inflammations. Due to the bacteria developing resistance to currently used antibiotics, there is an increasing demand for new chemotherapeutics against opportunistic pathogens. Cystapep 1 (A-20) is a human cystatin C derivative structurally based upon its N terminal fragment. This compound shows strong antibacterial properties against S. aureus and S. pyogenes which are associated with skin-related infections. A-20 effect on human primary keratinocytes proliferation, cytotoxity and allergic potential has been analyzed. The XTT and LDH assays were used to determine the effect of A-20 on proliferation and cytotoxicity of normal human keratinocytes. Allergic potential of A-20 peptide was assessed using ELISPOT technique (IL-4, IL-5 and IL-13 releasing by human PBMCs) and basophil activation test (CD63, CD203c and CCR3 antigens expression by basophils). The studies show that A-20 is not cytotoxic to human keratinocytes and does not inhibit their proliferation in concentrations upto 50 �¼g/mL. At the same time, A-20 can stimulate proliferation of keratinocytes in lower concentrations. Moreover, it does not activate PBMCs or basophils in vitro. Additinally, A-20 inhibits IL-4 and IL-13 production by concavalin stimulated PBMCs in vitro. The obtained data led to a conclusion that A-20 can be helpful in treating wound infections caused by S. aureus and S. pyogenes and therefore enhance wound healing.

Biography :

Milena Deptula is currently working at the Department of Embryology in Medical University of Gdansk and a Participant in STRATEGMED research project entitled “Novel technologies for pharmacological stimulation of regeneration". She has completed her Engineer and Master’s degree in the field of Cancer Stem-like Cells Biology in the Department of Pharmaceutical Technology and Biochemistry at Gdansk University of Technology.

Email: milenadeptula@gumed.edu.pl

Google Scholar citation report
Citations: 807

Journal of Tissue Science and Engineering received 807 citations as per Google Scholar report

Journal of Tissue Science and Engineering peer review process verified at publons

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