Design and validation of neuronal exocytosis blocking peptides as potential novel antiperspirants

Author:

Butron Laura1,Nikolaeva‐Koleva Magdalena2ORCID,Sempere Ana2,Rivero Verónica1,Fernandez‐Ballester Gregorio1,Espinosa Ana2,Vergassola Matteo3,Mastrocola Elena3,Zucchi Sara3,Ragni Lorella3,Fernández‐Carvajal Asia1,Mangano Giorgina4,Ferrer‐Montiel Antonio1,Devesa Isabel2

Affiliation:

1. Instituto de Investigación, Desarrollo e Innovación en Biotecnología Sanitaria de Elche (IDiBE) Universitas Miguel Hernández 03202 Elche Alicante Spain

2. AntalGenics SL, Ed. Quorum III UMH Scientific Park 03202 Elche Alicante Spain

3. Angelini Pharma S.p.A. Global R&D PLCM Preclinical Development Ancona Italy

4. Senior Scientific Consultant Rome Italy

Abstract

AbstractThermoregulation and heat dissipation by sweat production and evaporation are vital for human survival. However, hyperhidrosis or excessive perspiration might affect people's quality of life by causing discomfort and stress. The prolonged use of classical antiperspirants, anticholinergic medications or botulinum toxin injections for persistent hyperhidrosis might produce diverse side effects that limit their clinical use. Inspired by botox molecular mode of action, we used an in silico molecular modelling approach to design novel peptides to target neuronal acetylcholine exocytosis by interfering with the Snapin‐SNARE complex formation. Our exhaustive design rendered the selection of 11 peptides that decreased calcium‐dependent vesicle exocytosis in rat DRG neurons, reducing αCGRP release and TRPV1 inflammatory sensitization. The most potent peptides were palmitoylated peptides SPSR38‐4.1 and SPSR98‐9.1 that significantly suppressed acetylcholine release in vitro in human LAN‐2 neuroblastoma cells. Noteworthy, local acute and chronic administration of SPSR38‐4.1 peptide significantly decreased, in a dose‐dependent manner, pilocarpine‐induced sweating in an in vivo mouse model. Taken together, our in silico approach lead to the identification of active peptides able to attenuate excessive sweating by modulating neuronal acetylcholine exocytosis, and identified peptide SPSR38‐4.1 as a promising new antihyperhidrosis candidate for clinical development.

Funder

Angelini Pharma

Publisher

Wiley

Subject

Dermatology,Molecular Biology,Biochemistry

Cited by 2 articles. 订阅此论文施引文献 订阅此论文施引文献,注册后可以免费订阅5篇论文的施引文献,订阅后可以查看论文全部施引文献

1. Design and Validation of Novel Potential Antiperspirant Peptides Blocking M3-Gαq Sweat Signaling Cascade;International Journal of Peptide Research and Therapeutics;2024-07-15

2. Influence of permeability enhancers on in vitro peptides delivery through STRAT-M® membranes;Journal of Drug Delivery Science and Technology;2023-11

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