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6 results on '"Sara Košenina"'

1. Structural and functional insight into the interaction of Clostridioides difficile toxin B and FZD7

Author

Julia Kinsolving, Julien Bous, Pawel Kozielewicz, Sara Košenina, Rawan Shekhani, Lukas Grätz, Geoffrey Masuyer, Yuankai Wang, Pål Stenmark, Min Dong, and Gunnar Schulte

Subjects
CP: Molecular biology, Biology (General), QH301-705.5
Abstract

Summary: The G protein-coupled receptors of the Frizzled (FZD) family, in particular FZD1,2,7, are receptors that are exploited by Clostridioides difficile toxin B (TcdB), the major virulence factor responsible for pathogenesis associated with Clostridioides difficile infection. We employ a live-cell assay examining the affinity between full-length FZDs and TcdB. Moreover, we present cryoelectron microscopy structures of TcdB alone and in complex with full-length FZD7, which reveal that large structural rearrangements of the combined repetitive polypeptide domain are required for interaction with FZDs and other TcdB receptors, constituting a first step for receptor recognition. Furthermore, we show that bezlotoxumab, an FDA-approved monoclonal antibody to treat Clostridioides difficile infection, favors the apo-TcdB structure and thus disrupts binding with FZD7. The dynamic transition between the two conformations of TcdB also governs the stability of the pore-forming region. Thus, our work provides structural and functional insight into how conformational dynamics of TcdB determine receptor binding.

Published
2024
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2. Structural Analysis of Botulinum Neurotoxins Type B and E by Cryo-EM

Author

Sara Košenina, Markel Martínez-Carranza, Jonathan R. Davies, Geoffrey Masuyer, and Pål Stenmark

Subjects
Clostridium botulinum, botulism, botulinum neurotoxin, BoNT/B, BoNT/E, cryo-EM, Medicine
Abstract

Botulinum neurotoxins (BoNTs) are the causative agents of a potentially lethal paralytic disease targeting cholinergic nerve terminals. Multiple BoNT serotypes exist, with types A, B and E being the main cause of human botulism. Their extreme toxicity has been exploited for cosmetic and therapeutic uses to treat a wide range of neuromuscular disorders. Although naturally occurring BoNT types share a common end effect, their activity varies significantly based on the neuronal cell-surface receptors and intracellular SNARE substrates they target. These properties are the result of structural variations that have traditionally been studied using biophysical methods such as X-ray crystallography. Here, we determined the first structures of botulinum neurotoxins using single-particle cryogenic electron microscopy. The maps obtained at 3.6 and 3.7 Å for BoNT/B and /E, respectively, highlight the subtle structural dynamism between domains, and of the binding domain in particular. This study demonstrates how the recent advances made in the field of single-particle electron microscopy can be applied to bacterial toxins of clinical relevance and the botulinum neurotoxin family in particular.

Published
2021
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3. Crystal structure of the <scp>OrfX1</scp> – <scp>OrfX3</scp> complex from the <scp>PMP1</scp> neurotoxin gene cluster

Author

Pål Stenmark and Sara Košenina

Subjects
Structural Biology, Genetics, Biophysics, Cell Biology, Molecular Biology, Biochemistry
Abstract

Paraclostridial mosquitocidal protein 1 (PMP1) is a member of the clostridial neurotoxin (CNT) family, which includes botulinum and tetanus neurotoxins. PMP1 has unique selectivity for anopheline mosquitos and is the only known member of the family that targets insects. PMP1 is encoded in an orfX gene cluster, which in addition to the toxin, consists of OrfX1, OrfX2, OrfX3, P47 and NTNH, which have been shown to aid in PMP1 toxicity. We here show that OrfX1 and OrfX3 form a complex and present its structure at 2.7 Å. The OrfX1-OrfX3 complex mimics the structure of full-length OrfX2 and belongs to the lipid-binding TULIP protein superfamily. With this report, the structures of all proteins encoded in the orfX gene cluster of CNTs are now determined.

Published
2022
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4. Crystal structure of the catalytic domain of the Weissella oryzae botulinum‐like toxin

Author

Sara Košenina, Pål Stenmark, Sicai Zhang, Min Dong, and Geoffrey Masuyer

Subjects
Botulinum Toxins, Protein Conformation, Stereochemistry, Biophysics, Crystal structure, Crystallography, X-Ray, Immunoglobulin light chain, medicine.disease_cause, Biochemistry, Catalysis, 03 medical and health sciences, Structural Biology, Catalytic Domain, Genetics, medicine, Molecular Biology, Biological sciences, 030304 developmental biology, 0303 health sciences, Chemistry, Toxin, Zinc ion, 030302 biochemistry & molecular biology, Weissella oryzae, Cell Biology, Structural biology, Weissella
Abstract

Botulinum neurotoxins (BoNTs) are the most potent toxins known. So far, eight serotypes have been identified that all act as zinc-dependent endopeptidases targeting SNARE proteins and inhibiting the release of neurotransmitters. Recently, the first botulinum toxin-like protein was identified outside the Clostridial genus, designated BoNT/Wo in the genome of Weissella oryzae. Here, we report the 1.6 A X-ray crystal structure of the light chain of BoNT/Wo (LC/Wo). LC/Wo presents the core fold common to BoNTs but has an unusually wide, open and negatively charged catalytic pocket, with an additional Ca2+ ion besides the zinc ion and a unique s-hairpin motif. The structural information will help establish the substrate profile of BoNT/Wo and help our understanding of how BoNT evolved.

Published
2019
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