Membrane‐acting biomimetic peptoids against visceral leishmaniasis

Vivek Kumar; Jennifer S. Lin; Natalia Molchanova; John A. Fortkort; Carolin Reckmann; Stefan Bräse; Håvard Jenssen; Annelise E. Barron; Archana Chugh

doi:10.1002/2211-5463.13562

FEBS Open Bio (Mar 2023)

Membrane‐acting biomimetic peptoids against visceral leishmaniasis

Vivek Kumar,
Jennifer S. Lin,
Natalia Molchanova,
John A. Fortkort,
Carolin Reckmann,
Stefan Bräse,
Håvard Jenssen,
Annelise E. Barron,
Archana Chugh

Affiliations

Vivek Kumar: Kusuma School of Biological Sciences Indian Institute of Technology Delhi India
Jennifer S. Lin: Department of Bioengineering Stanford University, Schools of Medicine and of Engineering CA USA
Natalia Molchanova: The Molecular Foundry, Lawrence Berkeley National Laboratory CA USA
John A. Fortkort: Department of Bioengineering Stanford University, Schools of Medicine and of Engineering CA USA
Carolin Reckmann: Institute of Biological and Chemical Systems – Functional Molecular Systems (IBCS‐FMS) Karlsruhe Institute of Technology (KIT) Germany
Stefan Bräse: Institute of Biological and Chemical Systems – Functional Molecular Systems (IBCS‐FMS) Karlsruhe Institute of Technology (KIT) Germany
Håvard Jenssen: Department of Science and Environment Roskilde University Denmark
Annelise E. Barron: Department of Bioengineering Stanford University, Schools of Medicine and of Engineering CA USA
Archana Chugh: Kusuma School of Biological Sciences Indian Institute of Technology Delhi India

DOI: https://doi.org/10.1002/2211-5463.13562
Journal volume & issue: Vol. 13, no. 3
pp. 519 – 531

Abstract

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Visceral leishmaniasis (VL) is among the most neglected tropical diseases in the world. Drug cell permeability is essential for killing the intracellular residing parasites responsible for VL, making cell‐permeating peptides a logical choice to address VL. Unfortunately, the limited biological stability of peptides restricts their usage. Sequence‐specific oligo‐N‐substituted glycines (‘peptoids’) are a class of peptide mimics that offers an excellent alternative to peptides in terms of ease of synthesis and good biostability. We tested peptoids against the parasite Leishmania donovani in both forms, that is, intracellular amastigotes and promastigotes. N‐alkyl hydrophobic chain addition (lipidation) and bromination of oligopeptoids yielded compounds with good antileishmanial activity against both forms, showing the promise of these antiparasitic peptoids as potential drug candidates to treat VL.

Published in FEBS Open Bio

ISSN: 2211-5463 (Online)
Publisher: Wiley
Country of publisher: United Kingdom
LCC subjects: Science: Biology (General)
Website: https://febs.onlinelibrary.wiley.com/journal/22115463

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