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Crystal structure of bacterial cytotoxic necrotizing factor CNF(Y) reveals molecular building blocks for intoxication

Cytotoxic necrotizing factors (CNFs) are bacterial single‐chain exotoxins that modulate cytokinetic/oncogenic and inflammatory processes through activation of host cell Rho GTPases. To achieve this, they are secreted, bind surface receptors to induce endocytosis and translocate a catalytic unit into...

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Autores principales: Chaoprasid, Paweena, Lukat, Peer, Mühlen, Sabrina, Heidler, Thomas, Gazdag, Emerich‐Mihai, Dong, Shuangshuang, Bi, Wenjie, Rüter, Christian, Kirchenwitz, Marco, Steffen, Anika, Jänsch, Lothar, Stradal, Theresia E B, Dersch, Petra, Blankenfeldt, Wulf
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7883292/
https://www.ncbi.nlm.nih.gov/pubmed/33410511
http://dx.doi.org/10.15252/embj.2020105202
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author Chaoprasid, Paweena
Lukat, Peer
Mühlen, Sabrina
Heidler, Thomas
Gazdag, Emerich‐Mihai
Dong, Shuangshuang
Bi, Wenjie
Rüter, Christian
Kirchenwitz, Marco
Steffen, Anika
Jänsch, Lothar
Stradal, Theresia E B
Dersch, Petra
Blankenfeldt, Wulf
author_facet Chaoprasid, Paweena
Lukat, Peer
Mühlen, Sabrina
Heidler, Thomas
Gazdag, Emerich‐Mihai
Dong, Shuangshuang
Bi, Wenjie
Rüter, Christian
Kirchenwitz, Marco
Steffen, Anika
Jänsch, Lothar
Stradal, Theresia E B
Dersch, Petra
Blankenfeldt, Wulf
author_sort Chaoprasid, Paweena
collection PubMed
description Cytotoxic necrotizing factors (CNFs) are bacterial single‐chain exotoxins that modulate cytokinetic/oncogenic and inflammatory processes through activation of host cell Rho GTPases. To achieve this, they are secreted, bind surface receptors to induce endocytosis and translocate a catalytic unit into the cytosol to intoxicate host cells. A three‐dimensional structure that provides insight into the underlying mechanisms is still lacking. Here, we determined the crystal structure of full‐length Yersinia pseudotuberculosis CNF(Y). CNF(Y) consists of five domains (D1–D5), and by integrating structural and functional data, we demonstrate that D1–3 act as export and translocation module for the catalytic unit (D4–5) and for a fused β‐lactamase reporter protein. We further found that D4, which possesses structural similarity to ADP‐ribosyl transferases, but had no equivalent catalytic activity, changed its position to interact extensively with D5 in the crystal structure of the free D4–5 fragment. This liberates D5 from a semi‐blocked conformation in full‐length CNF(Y), leading to higher deamidation activity. Finally, we identify CNF translocation modules in several uncharacterized fusion proteins, which suggests their usability as a broad‐specificity protein delivery tool.
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spelling pubmed-78832922021-02-19 Crystal structure of bacterial cytotoxic necrotizing factor CNF(Y) reveals molecular building blocks for intoxication Chaoprasid, Paweena Lukat, Peer Mühlen, Sabrina Heidler, Thomas Gazdag, Emerich‐Mihai Dong, Shuangshuang Bi, Wenjie Rüter, Christian Kirchenwitz, Marco Steffen, Anika Jänsch, Lothar Stradal, Theresia E B Dersch, Petra Blankenfeldt, Wulf EMBO J Articles Cytotoxic necrotizing factors (CNFs) are bacterial single‐chain exotoxins that modulate cytokinetic/oncogenic and inflammatory processes through activation of host cell Rho GTPases. To achieve this, they are secreted, bind surface receptors to induce endocytosis and translocate a catalytic unit into the cytosol to intoxicate host cells. A three‐dimensional structure that provides insight into the underlying mechanisms is still lacking. Here, we determined the crystal structure of full‐length Yersinia pseudotuberculosis CNF(Y). CNF(Y) consists of five domains (D1–D5), and by integrating structural and functional data, we demonstrate that D1–3 act as export and translocation module for the catalytic unit (D4–5) and for a fused β‐lactamase reporter protein. We further found that D4, which possesses structural similarity to ADP‐ribosyl transferases, but had no equivalent catalytic activity, changed its position to interact extensively with D5 in the crystal structure of the free D4–5 fragment. This liberates D5 from a semi‐blocked conformation in full‐length CNF(Y), leading to higher deamidation activity. Finally, we identify CNF translocation modules in several uncharacterized fusion proteins, which suggests their usability as a broad‐specificity protein delivery tool. John Wiley and Sons Inc. 2021-01-07 2021-02-15 /pmc/articles/PMC7883292/ /pubmed/33410511 http://dx.doi.org/10.15252/embj.2020105202 Text en © 2021 The Authors. Published under the terms of the CC BY NC ND 4.0 license This is an open access article under the terms of the http://creativecommons.org/licenses/by-nc-nd/4.0/ License, which permits use and distribution in any medium, provided the original work is properly cited, the use is non‐commercial and no modifications or adaptations are made.
spellingShingle Articles
Chaoprasid, Paweena
Lukat, Peer
Mühlen, Sabrina
Heidler, Thomas
Gazdag, Emerich‐Mihai
Dong, Shuangshuang
Bi, Wenjie
Rüter, Christian
Kirchenwitz, Marco
Steffen, Anika
Jänsch, Lothar
Stradal, Theresia E B
Dersch, Petra
Blankenfeldt, Wulf
Crystal structure of bacterial cytotoxic necrotizing factor CNF(Y) reveals molecular building blocks for intoxication
title Crystal structure of bacterial cytotoxic necrotizing factor CNF(Y) reveals molecular building blocks for intoxication
title_full Crystal structure of bacterial cytotoxic necrotizing factor CNF(Y) reveals molecular building blocks for intoxication
title_fullStr Crystal structure of bacterial cytotoxic necrotizing factor CNF(Y) reveals molecular building blocks for intoxication
title_full_unstemmed Crystal structure of bacterial cytotoxic necrotizing factor CNF(Y) reveals molecular building blocks for intoxication
title_short Crystal structure of bacterial cytotoxic necrotizing factor CNF(Y) reveals molecular building blocks for intoxication
title_sort crystal structure of bacterial cytotoxic necrotizing factor cnf(y) reveals molecular building blocks for intoxication
topic Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7883292/
https://www.ncbi.nlm.nih.gov/pubmed/33410511
http://dx.doi.org/10.15252/embj.2020105202
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