Topoisomeric Membrane-Active Peptides: A Review of the Last Two Decades

Author:

Carrera-Aubesart Adam1,Gallo Maria1ORCID,Defaus Sira1ORCID,Todorovski Toni12ORCID,Andreu David1ORCID

Affiliation:

1. Department of Medicine and Life Sciences, Universitat Pompeu Fabra, 08003 Barcelona, Spain

2. Department of Biotechnology, University of Rijeka, 51000 Rijeka, Croatia

Abstract

In recent decades, bioactive peptides have been gaining recognition in various biomedical areas, such as intracellular drug delivery (cell-penetrating peptides, CPPs) or anti-infective action (antimicrobial peptides, AMPs), closely associated to their distinct mode of interaction with biological membranes. Exploiting the interaction of membrane-active peptides with diverse targets (healthy, tumoral, bacterial or parasitic cell membranes) is opening encouraging prospects for peptides in therapeutics. However, ordinary peptides formed by L-amino acids are easily decomposed by proteases in biological fluids. One way to sidestep this limitation is to use topoisomers, namely versions of the peptide made up of D-amino acids in either canonic (enantio) or inverted (retroenantio) sequence. Rearranging peptide sequences in this fashion provides a certain degree of native structure mimicry that, in appropriate contexts, may deliver desirable biological activity while avoiding protease degradation. In this review, we will focus on recent accounts of membrane-active topoisomeric peptides with therapeutic applications as CPP drug delivery vectors, or as antimicrobial and anticancer candidates. We will also discuss the most common modes of interaction of these peptides with their membrane targets.

Funder

La Caixa Health Foundation

European Union

Publisher

MDPI AG

Subject

Pharmaceutical Science

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