Anticryptococcal activity and mechanistic studies of short amphipathic peptides

Author:

Aaghaz Shams1,Sharma Komal1,Maurya Indresh K.2,Rudramurthy Shivaprakash M.3,Singh Shreya3,Kumar Vinod4,Tikoo Kulbhushan4,Jain Rahul12ORCID

Affiliation:

1. Department of Medicinal Chemistry National Institute of Pharmaceutical Education and Research Nagar Punjab India

2. Center for Infectious Diseases National Institute of Pharmaceutical Education and Research Nagar Punjab India

3. Department of Medical Microbiology Post Graduate Institute of Medical Education and Research Chandigarh Punjab India

4. Department of Pharmacology and Toxicology National Institute of Pharmaceutical Education and Research Nagar Punjab India

Abstract

AbstractCryptococcus neoformans, an opportunistic fungal pathogen, causes cryptococcosis in immunocompromised persons. A series of modified L‐histidines‐containing peptides are synthesized that exhibit promising activity against C. neoformans. Analog 11d [L‐His(2‐adamantyl)‐L‐Trp‐L‐His(2‐phenyl)‐OMe] produced potency with an IC50 of 3.02 µg/ml (MIC = 5.49 µg/ml). This peptide is noncytotoxic and nonhaemolytic at the MIC and displays synergistic effects with amphotericin B at subinhibitory concentration. Mechanistic investigation of 11d using microscopic tools indicates cell wall and membrane disruption of C. neoformans, while flow cytometric analysis confirms cell death by apoptosis. This study indicates that 11d exhibits antifungal potential and acts via the rapid onset of action.

Publisher

Wiley

Subject

Drug Discovery,Pharmaceutical Science

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