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The HslV Protease from Leishmania major and Its Activation by C-terminal HslU Peptides

HslVU is an ATP-dependent proteolytic complex present in certain bacteria and in the mitochondrion of some primordial eukaryotes, including deadly parasites such as Leishmania. It is formed by the dodecameric protease HslV and the hexameric ATPase HslU, which binds via the C-terminal end of its subu...

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Autores principales: Kebe, Ndeye Mathy, Samanta, Krishnananda, Singh, Priyanka, Lai-Kee-Him, Joséphine, Apicella, Viviana, Payrot, Nadine, Lauraire, Noémie, Legrand, Baptiste, Lisowski, Vincent, Mbang-Benet, Diane-Ethna, Pages, Michel, Bastien, Patrick, Kajava, Andrey V., Bron, Patrick, Hernandez, Jean-François, Coux, Olivier
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6429459/
https://www.ncbi.nlm.nih.gov/pubmed/30813632
http://dx.doi.org/10.3390/ijms20051021
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author Kebe, Ndeye Mathy
Samanta, Krishnananda
Singh, Priyanka
Lai-Kee-Him, Joséphine
Apicella, Viviana
Payrot, Nadine
Lauraire, Noémie
Legrand, Baptiste
Lisowski, Vincent
Mbang-Benet, Diane-Ethna
Pages, Michel
Bastien, Patrick
Kajava, Andrey V.
Bron, Patrick
Hernandez, Jean-François
Coux, Olivier
author_facet Kebe, Ndeye Mathy
Samanta, Krishnananda
Singh, Priyanka
Lai-Kee-Him, Joséphine
Apicella, Viviana
Payrot, Nadine
Lauraire, Noémie
Legrand, Baptiste
Lisowski, Vincent
Mbang-Benet, Diane-Ethna
Pages, Michel
Bastien, Patrick
Kajava, Andrey V.
Bron, Patrick
Hernandez, Jean-François
Coux, Olivier
author_sort Kebe, Ndeye Mathy
collection PubMed
description HslVU is an ATP-dependent proteolytic complex present in certain bacteria and in the mitochondrion of some primordial eukaryotes, including deadly parasites such as Leishmania. It is formed by the dodecameric protease HslV and the hexameric ATPase HslU, which binds via the C-terminal end of its subunits to HslV and activates it by a yet unclear allosteric mechanism. We undertook the characterization of HslV from Leishmania major (LmHslV), a trypanosomatid that expresses two isoforms for HslU, LmHslU1 and LmHslU2. Using a novel and sensitive peptide substrate, we found that LmHslV can be activated by peptides derived from the C-termini of both LmHslU1 and LmHslU2. Truncations, Ala- and D-scans of the C-terminal dodecapeptide of LmHslU2 (LmC12-U2) showed that five out of the six C-terminal residues of LmHslU2 are essential for binding to and activating HslV. Peptide cyclisation with a lactam bridge allowed shortening of the peptide without loss of potency. Finally, we found that dodecapeptides derived from HslU of other parasites and bacteria are able to activate LmHslV with similar or even higher efficiency. Importantly, using electron microscopy approaches, we observed that the activation of LmHslV was accompanied by a large conformational remodeling, which represents a yet unidentified layer of control of HslV activation.
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spelling pubmed-64294592019-04-10 The HslV Protease from Leishmania major and Its Activation by C-terminal HslU Peptides Kebe, Ndeye Mathy Samanta, Krishnananda Singh, Priyanka Lai-Kee-Him, Joséphine Apicella, Viviana Payrot, Nadine Lauraire, Noémie Legrand, Baptiste Lisowski, Vincent Mbang-Benet, Diane-Ethna Pages, Michel Bastien, Patrick Kajava, Andrey V. Bron, Patrick Hernandez, Jean-François Coux, Olivier Int J Mol Sci Article HslVU is an ATP-dependent proteolytic complex present in certain bacteria and in the mitochondrion of some primordial eukaryotes, including deadly parasites such as Leishmania. It is formed by the dodecameric protease HslV and the hexameric ATPase HslU, which binds via the C-terminal end of its subunits to HslV and activates it by a yet unclear allosteric mechanism. We undertook the characterization of HslV from Leishmania major (LmHslV), a trypanosomatid that expresses two isoforms for HslU, LmHslU1 and LmHslU2. Using a novel and sensitive peptide substrate, we found that LmHslV can be activated by peptides derived from the C-termini of both LmHslU1 and LmHslU2. Truncations, Ala- and D-scans of the C-terminal dodecapeptide of LmHslU2 (LmC12-U2) showed that five out of the six C-terminal residues of LmHslU2 are essential for binding to and activating HslV. Peptide cyclisation with a lactam bridge allowed shortening of the peptide without loss of potency. Finally, we found that dodecapeptides derived from HslU of other parasites and bacteria are able to activate LmHslV with similar or even higher efficiency. Importantly, using electron microscopy approaches, we observed that the activation of LmHslV was accompanied by a large conformational remodeling, which represents a yet unidentified layer of control of HslV activation. MDPI 2019-02-26 /pmc/articles/PMC6429459/ /pubmed/30813632 http://dx.doi.org/10.3390/ijms20051021 Text en © 2019 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Kebe, Ndeye Mathy
Samanta, Krishnananda
Singh, Priyanka
Lai-Kee-Him, Joséphine
Apicella, Viviana
Payrot, Nadine
Lauraire, Noémie
Legrand, Baptiste
Lisowski, Vincent
Mbang-Benet, Diane-Ethna
Pages, Michel
Bastien, Patrick
Kajava, Andrey V.
Bron, Patrick
Hernandez, Jean-François
Coux, Olivier
The HslV Protease from Leishmania major and Its Activation by C-terminal HslU Peptides
title The HslV Protease from Leishmania major and Its Activation by C-terminal HslU Peptides
title_full The HslV Protease from Leishmania major and Its Activation by C-terminal HslU Peptides
title_fullStr The HslV Protease from Leishmania major and Its Activation by C-terminal HslU Peptides
title_full_unstemmed The HslV Protease from Leishmania major and Its Activation by C-terminal HslU Peptides
title_short The HslV Protease from Leishmania major and Its Activation by C-terminal HslU Peptides
title_sort hslv protease from leishmania major and its activation by c-terminal hslu peptides
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6429459/
https://www.ncbi.nlm.nih.gov/pubmed/30813632
http://dx.doi.org/10.3390/ijms20051021
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