Diversely evolved xibalbin variants from remipede venom inhibit potassium channels and activate PKA-II and Erk1/2 signaling.

Pinheiro-Junior, Ernesto Lopes; Alirahimi, Ehsan; Peigneur, Steve; Isensee, Jörg; Schiffmann, Susanne; Erkoc, Pelin; Fürst, Robert; Vilcinskas, Andreas; Sennoner, Tobias; Koludarov, Ivan; Hempel, Benjamin-Florian; Tytgat, Jan; Hucho, Tim; von Reumont, Björn M

Pinheiro-Junior, Ernesto Lopes; Alirahimi, Ehsan; Peigneur, Steve; Isensee, Jörg; Schiffmann, Susanne; Erkoc, Pelin; Fürst, Robert; Vilcinskas, Andreas; Sennoner, Tobias; Koludarov, Ivan; Hempel, Benjamin-Florian; Tytgat, Jan; Hucho, Tim; von Reumont, Björn M.

Afiliação

Pinheiro-Junior EL; Toxicology and Pharmacology - Campus Gasthuisberg, University of Leuven (KU Leuven), Herestraat 49, PO Box 922, 3000, Louvain, Belgium.
Alirahimi E; Department of Anesthesiology and Intensive Care Medicine, University Cologne, Translational Pain Research, University Hospital of Cologne, Cologne, Germany.
Peigneur S; Toxicology and Pharmacology - Campus Gasthuisberg, University of Leuven (KU Leuven), Herestraat 49, PO Box 922, 3000, Louvain, Belgium.
Isensee J; Department of Anesthesiology and Intensive Care Medicine, University Cologne, Translational Pain Research, University Hospital of Cologne, Cologne, Germany.
Schiffmann S; Fraunhofer Institute for Translational Medicine and Pharmacology ITMP, Theodor-Stern-Kai 7, 60596, Frankfurt Am Main, Germany.
Erkoc P; Institute of Pharmaceutical Biology, Goethe University Frankfurt, Max-Von-Laue-Str. 9, 60438, Frankfurt, Germany.
Fürst R; LOEWE Center for Translational Biodiversity Genomics (LOEWE-TBG), Senckenberganlage 25, 60325, Frankfurt, Germany.
Vilcinskas A; Institute of Pharmaceutical Biology, Goethe University Frankfurt, Max-Von-Laue-Str. 9, 60438, Frankfurt, Germany.
Sennoner T; LOEWE Center for Translational Biodiversity Genomics (LOEWE-TBG), Senckenberganlage 25, 60325, Frankfurt, Germany.
Koludarov I; LOEWE Center for Translational Biodiversity Genomics (LOEWE-TBG), Senckenberganlage 25, 60325, Frankfurt, Germany.
Hempel BF; Department of Bioresources, Fraunhofer Institute for Molecular Biology and Applied Ecology (IME-BR), Ohlebergsweg 14, 35394, Giessen, Germany.
Tytgat J; Department of Informatics, Bioinformatics and Computational Biology, i12, Technical University of Munich, Boltzmannstr. 3, 85748, Garching, Munich, Germany.
Hucho T; Department of Informatics, Bioinformatics and Computational Biology, i12, Technical University of Munich, Boltzmannstr. 3, 85748, Garching, Munich, Germany.
von Reumont BM; Freie Unveristät Berlin, Veterinary Centre for Resistance Research (TZR), Robert-Von-Ostertag Str. 8, 14163, Berlin, Germany.

BMC Biol ; 22(1): 164, 2024 Jul 29.

Article em En | MEDLINE | ID: mdl-39075558

ABSTRACT

ABSTRACT

BACKGROUND:

The identification of novel toxins from overlooked and taxonomically exceptional species bears potential for various pharmacological applications. The remipede Xibalbanus tulumensis, an underwater cave-dwelling crustacean, is the only crustacean for which a venom system has been described. Its venom contains several xibalbin peptides that have an inhibitor cysteine knot (ICK) scaffold.

RESULTS:

Our screenings revealed that all tested xibalbin variants particularly inhibit potassium channels. Xib1 and xib13 with their eight-cysteine domain similar to spider knottins also inhibit voltage-gated sodium channels. No activity was noted on calcium channels. Expanding the functional testing, we demonstrate that xib1 and xib13 increase PKA-II and Erk1/2 sensitization signaling in nociceptive neurons, which may initiate pain sensitization. Our phylogenetic analysis suggests that xib13 either originates from the common ancestor of pancrustaceans or earlier while xib1 is more restricted to remipedes. The ten-cysteine scaffolded xib2 emerged from xib1, a result that is supported by our phylogenetic and machine learning-based analyses.

CONCLUSIONS:

Our functional characterization of synthesized variants of xib1, xib2, and xib13 elucidates their potential as inhibitors of potassium channels in mammalian systems. The specific interaction of xib2 with Kv1.6 channels, which are relevant to treating variants of epilepsy, shows potential for further studies. At higher concentrations, xib1 and xib13 activate the kinases PKA-II and ERK1/2 in mammalian sensory neurons, suggesting pain sensitization and potential applications related to pain research and therapy. While tested insect channels suggest that all probably act as neurotoxins, the biological function of xib1, xib2, and xib13 requires further elucidation. A novel finding on their evolutionary origin is the apparent emergence of X. tulumensis-specific xib2 from xib1. Our study is an important cornerstone for future studies to untangle the origin and function of these enigmatic proteins as important components of remipede but also other pancrustacean and arthropod venoms.

Assuntos

Canais de Potássio; Animais; Canais de Potássio/metabolismo; Canais de Potássio/genética; Sistema de Sinalização das MAP Quinases/efeitos dos fármacos; Filogenia; Camundongos; Proteínas Quinases Dependentes de AMP Cíclico/metabolismo; Proteínas Quinases Dependentes de AMP Cíclico/genética; Evolução Molecular; Humanos; Venenos de Artrópodes/química

Palavras-chave

Electrophysiology; HCI screening; ICK; Knottin; Marine venoms; Venomous crustaceans; Xibalbanus; Xibalbin1; Xibalbin13; Xibalbin2

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Texto completo: 1 Base de dados: MEDLINE Assunto principal: Canais de Potássio Limite: Animals / Humans Idioma: En Revista: BMC Biol Assunto da revista: BIOLOGIA Ano de publicação: 2024 Tipo de documento: Article País de afiliação: Bélgica

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