N‐terminal modification of an LAH4‐derived peptide increases mRNA delivery in the presence of serum

Author:

Dussouillez Candice12,Lointier Morane3,Sebane Mohammed‐Karim12,Fournel Sylvie12,Bechinger Burkhard3ORCID,Kichler Antoine12ORCID

Affiliation:

1. Laboratoire de Conception et Application de Molécules Bioactives UMR7199 CNRS, Université de Strasbourg, 3BioTeam, Faculté de Pharmacie Illkirch France

2. Inserm UMR_S 1121, EMR 7003 CNRS, Université de Strasbourg, Biomaterials and Bioengineering, Centre de Recherche en Biomédecine de Strasbourg Strasbourg France

3. Université de Strasbourg, CNRS, UMR7177, Institut de Chimie Strasbourg France

Abstract

The recently developed mRNA‐based coronavirus SARS‐CoV‐2 vaccines highlighted the great therapeutic potential of the mRNA technology. Although the lipid nanoparticles used for the delivery of the mRNA are very efficient, they showed, in some cases, the induction of side effects as well as the production of antibodies directed against particle components. Thus, the development of alternative delivery systems is of great interest in the pursuit of more effective mRNA treatments. In the present work, we evaluated the mRNA transfection capacities of a series of cationic histidine‐rich amphipathic peptides derived from LAH4. We found that while the LAH4‐A1 peptide was an efficient carrier for mRNA, its activity was highly serum sensitive. Interestingly, modification of this cell penetrating peptide at the N‐terminus with two tyrosines or with salicylic acid allowed to confer serum resistance to the carrier.

Funder

IDEXLYON

Agence Nationale de la Recherche

Ligue Contre le Cancer

Yellow Sea Fisheries Research Institute, Chinese Academy of Fishery Sciences

Publisher

Wiley

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