Structure and ion-release mechanism of P(IB-4)-type ATPases

Transition metals, such as zinc, are essential micronutrients in all organisms, but also highly toxic in excessive amounts. Heavy-metal transporting P-type (P(IB)) ATPases are crucial for homeostasis, conferring cellular detoxification and redistribution through transport of these ions across cellul...

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Autores principales: Grønberg, Christina, Hu, Qiaoxia, Mahato, Dhani Ram, Longhin, Elena, Salustros, Nina, Duelli, Annette, Lyu, Pin, Bågenholm, Viktoria, Eriksson, Jonas, Rao, Komal Umashankar, Henderson, Domhnall Iain, Meloni, Gabriele, Andersson, Magnus, Croll, Tristan, Godaly, Gabriela, Wang, Kaituo, Gourdon, Pontus
Formato: Online Artículo Texto
Lenguaje:English
Publicado: eLife Sciences Publications, Ltd 2021
Materias:
Biochemistry and Chemical Biology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8880997/
https://www.ncbi.nlm.nih.gov/pubmed/34951590
http://dx.doi.org/10.7554/eLife.73124
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author Grønberg, Christina
Hu, Qiaoxia
Mahato, Dhani Ram
Longhin, Elena
Salustros, Nina
Duelli, Annette
Lyu, Pin
Bågenholm, Viktoria
Eriksson, Jonas
Rao, Komal Umashankar
Henderson, Domhnall Iain
Meloni, Gabriele
Andersson, Magnus
Croll, Tristan
Godaly, Gabriela
Wang, Kaituo
Gourdon, Pontus
author_facet Grønberg, Christina
Hu, Qiaoxia
Mahato, Dhani Ram
Longhin, Elena
Salustros, Nina
Duelli, Annette
Lyu, Pin
Bågenholm, Viktoria
Eriksson, Jonas
Rao, Komal Umashankar
Henderson, Domhnall Iain
Meloni, Gabriele
Andersson, Magnus
Croll, Tristan
Godaly, Gabriela
Wang, Kaituo
Gourdon, Pontus
author_sort Grønberg, Christina
collection PubMed
description Transition metals, such as zinc, are essential micronutrients in all organisms, but also highly toxic in excessive amounts. Heavy-metal transporting P-type (P(IB)) ATPases are crucial for homeostasis, conferring cellular detoxification and redistribution through transport of these ions across cellular membranes. No structural information is available for the P(IB-4)-ATPases, the subclass with the broadest cargo scope, and hence even their topology remains elusive. Here, we present structures and complementary functional analyses of an archetypal P(IB-4)-ATPase, sCoaT from Sulfitobacter sp. NAS14-1. The data disclose the architecture, devoid of classical so-called heavy-metal-binding domains (HMBDs), and provide fundamentally new insights into the mechanism and diversity of heavy-metal transporters. We reveal several novel P-type ATPase features, including a dual role in heavy-metal release and as an internal counter ion of an invariant histidine. We also establish that the turnover of P(IB)-ATPases is potassium independent, contrasting to many other P-type ATPases. Combined with new inhibitory compounds, our results open up for efforts in for example drug discovery, since P(IB-4)-ATPases function as virulence factors in many pathogens.
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spelling pubmed-88809972022-02-26 Structure and ion-release mechanism of P(IB-4)-type ATPases Grønberg, Christina Hu, Qiaoxia Mahato, Dhani Ram Longhin, Elena Salustros, Nina Duelli, Annette Lyu, Pin Bågenholm, Viktoria Eriksson, Jonas Rao, Komal Umashankar Henderson, Domhnall Iain Meloni, Gabriele Andersson, Magnus Croll, Tristan Godaly, Gabriela Wang, Kaituo Gourdon, Pontus eLife Biochemistry and Chemical Biology Transition metals, such as zinc, are essential micronutrients in all organisms, but also highly toxic in excessive amounts. Heavy-metal transporting P-type (P(IB)) ATPases are crucial for homeostasis, conferring cellular detoxification and redistribution through transport of these ions across cellular membranes. No structural information is available for the P(IB-4)-ATPases, the subclass with the broadest cargo scope, and hence even their topology remains elusive. Here, we present structures and complementary functional analyses of an archetypal P(IB-4)-ATPase, sCoaT from Sulfitobacter sp. NAS14-1. The data disclose the architecture, devoid of classical so-called heavy-metal-binding domains (HMBDs), and provide fundamentally new insights into the mechanism and diversity of heavy-metal transporters. We reveal several novel P-type ATPase features, including a dual role in heavy-metal release and as an internal counter ion of an invariant histidine. We also establish that the turnover of P(IB)-ATPases is potassium independent, contrasting to many other P-type ATPases. Combined with new inhibitory compounds, our results open up for efforts in for example drug discovery, since P(IB-4)-ATPases function as virulence factors in many pathogens. eLife Sciences Publications, Ltd 2021-12-24 /pmc/articles/PMC8880997/ /pubmed/34951590 http://dx.doi.org/10.7554/eLife.73124 Text en © 2021, Grønberg et al https://creativecommons.org/licenses/by/4.0/This article is distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use and redistribution provided that the original author and source are credited.
spellingShingle Biochemistry and Chemical Biology
Grønberg, Christina
Hu, Qiaoxia
Mahato, Dhani Ram
Longhin, Elena
Salustros, Nina
Duelli, Annette
Lyu, Pin
Bågenholm, Viktoria
Eriksson, Jonas
Rao, Komal Umashankar
Henderson, Domhnall Iain
Meloni, Gabriele
Andersson, Magnus
Croll, Tristan
Godaly, Gabriela
Wang, Kaituo
Gourdon, Pontus
Structure and ion-release mechanism of P(IB-4)-type ATPases
title Structure and ion-release mechanism of P(IB-4)-type ATPases
title_full Structure and ion-release mechanism of P(IB-4)-type ATPases
title_fullStr Structure and ion-release mechanism of P(IB-4)-type ATPases
title_full_unstemmed Structure and ion-release mechanism of P(IB-4)-type ATPases
title_short Structure and ion-release mechanism of P(IB-4)-type ATPases
title_sort structure and ion-release mechanism of p(ib-4)-type atpases
topic Biochemistry and Chemical Biology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8880997/
https://www.ncbi.nlm.nih.gov/pubmed/34951590
http://dx.doi.org/10.7554/eLife.73124
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