Short-Chained Linear Scorpion Peptides: A Pool for Novel Antimicrobials-Reference-Cited by-同舟云学术

Short-Chained Linear Scorpion Peptides: A Pool for Novel Antimicrobials

Published:2024-05-05 Issue:5 Volume:13 Page:422
ISSN:2079-6382
Container-title:Antibiotics
language:en
Short-container-title:Antibiotics

Author:

Panayi Tolis¹²,Diavoli Spiridoula²,Nicolaidou Vicky¹^ORCID,Papaneophytou Christos¹^ORCID,Petrou Christos²^ORCID,Sarigiannis Yiannis²^ORCID

Affiliation:

1. Department of Life Sciences, School of Life and Health Sciences, University of Nicosia, 2417 Nicosia, Cyprus

2. Department of Health Sciences, School of Life and Health Sciences, University of Nicosia, 2417 Nicosia, Cyprus

Abstract

Scorpion venom peptides are generally classified into two main groups: the disulfide bridged peptides (DBPs), which usually target membrane-associated ion channels, and the non-disulfide bridged peptides (NDBPs), a smaller group with multifunctional properties. In the past decade, these peptides have gained interest because most of them display functions that include antimicrobial, anticancer, haemolytic, and anti-inflammatory activities. Our current study focuses on the short (9–19 amino acids) antimicrobial linear scorpion peptides. Most of these peptides display a net positive charge of 1 or 2, an isoelectric point at pH 9–10, a broad range of hydrophobicity, and a Grand Average of Hydropathy (GRAVY) Value ranging between −0.05 and 1.7. These features allow these peptides to be attracted toward the negatively charged phospholipid head groups of the lipid membranes of target cells, a force driven by electrostatic interactions. This review outlines the antimicrobial potential of short-chained linear scorpion venom peptides. Additionally, short linear scorpion peptides are in general more attractive for large-scale synthesis from a manufacturing point of view. The structural and functional diversity of these peptides represents a good starting point for the development of new peptide-based therapeutics.

Publisher

MDPI AG

Link

https://www.mdpi.com/2079-6382/13/5/422/pdf

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