An endogenous human peptide derived from α1-antitrypsin as a novel pharmacological inhibitor of Bordetella pertussis toxin - UTU Research Portal

A1 Refereed original research article in a scientific journal

An endogenous human peptide derived from α1-antitrypsin as a novel pharmacological inhibitor of Bordetella pertussis toxin

Authors: Lietz, Stefanie; Sokolowski, Lena-Marie; Beyschlag, Alexander; Rosenau, Helena; Siewert, Annika; Alfonso, Armando A. Rodríguez; Preising, Nico; Ständker, Ludger; Wiese, Sebastian; Köhler, Janet; Weidinger, Gilbert; Münch, Jan; Pulliainen, Arto T.; Ernst, Katharina; Barth, Holger

Publisher: Springer Science and Business Media LLC

Publication year: 2025

Journal: Naunyn-Schmiedeberg's Archives of Pharmacology

ISSN: 0028-1298

eISSN: 1432-1912

DOI: https://doi.org/10.1007/s00210-025-04744-1

Publication's open availability at the time of reporting: Open Access

Publication channel's open availability : Partially Open Access publication channel

Web address : https://doi.org/10.1007/s00210-025-04744-1

Self-archived copy’s web address: https://research.utu.fi/converis/portal/detail/Publication/505616746

Self-archived copy's licence: CC BY

Self-archived copy's version: Publisher`s PDF

Abstract

Pertussis, also known as whooping cough, is a highly infectious respiratory disease caused by the bacterium Bordetella pertussis. The bacterial virulence factor, pertussis toxin (PT), is associated with the manifestation of the characteristic symptoms of pertussis and the severe form of this disease. Increasing case numbers and the lack of treatment options highlight the need to develop novel pharmacological strategies, e.g., the generation of specific PT inhibitors. Recently, we identified the endogenous human protein alpha(1)-antitrypsin (alpha(1)AT) as an inhibitor of PT from a screening of a human hemofiltrate protein/peptide library. In the present work, we tested an in-house alpha(1)AT peptide bank to identify an alpha(1)AT region with anti-PT activity. Then, we compared the sequences of the positive hits from the peptide bank with all known alpha(1)AT fragments in the hemofiltrate samples to find new active peptides. In total, 36 peptides were tested for their PT inhibition, leading to the identification of an endogenous alpha(1)AT fragment, alpha(1)AT HF, derived from hemofiltrate with anti-PT activity. This peptide had no toxic effects on HeLa cells and in vivo on zebrafish embryos, rendering it an attractive lead compound for further evaluation to treat pertussis in the future.

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Funding information in the publication:
Open Access funding enabled and organized by Projekt DEAL. This work was supported by the Deutsche Forschungsgemeinschaft (DFG, German Research Foundation)—project number 316249678-SFB1279 (A07, funding to H.B. (former K.E.); Z01, funding to A.A.R.A. and L.S., A02, funding to J.M., Z02, funding to G.W.). S.L. is a member of the International Graduate School in Molecular Medicine Ulm (IGradU). A.B. is a member of the “Promotionsprogramm Experimentelle Medizin” of the IGradU.