On allosteric modulation of P-type Cu(+)-ATPases

Daniel Mattle; Oleg Sitsel; Henriette Elisabeth Autzen; Gabriele Meloni; Pontus Gourdon; Poul Nissen

doi:10.1016/j.jmb.2013.03.008

On allosteric modulation of P-type Cu(+)-ATPases

Daniel Mattle, Oleg Sitsel, Henriette Elisabeth Autzen, Gabriele Meloni, Pontus Gourdon, Poul Nissen

Aarhus University

Research output: Contribution to journal › Article › peer-review

Abstract

P-type ATPases perform active transport of various compounds across biological membranes and are crucial for ion homeostasis and the asymmetric composition of lipid bilayers. Although their functional cycle share principles of phosphoenzyme intermediates, P-type ATPases also show subclass-specific sequence motifs and structural elements that are linked to transport specificity and mechanistic modulation. Here we provide an overview of the Cu(+)-transporting ATPases (of subclass PIB) and compare them to the well-studied sarco(endo)plasmic reticulum Ca(2+)-ATPase (of subclass PIIA). Cu(+) ions in the cell are delivered by soluble chaperones to Cu(+)-ATPases, which expose a putative "docking platform" at the intracellular interface. Cu(+)-ATPases also contain heavy-metal binding domains providing a basis for allosteric control of pump activity. Database analysis of Cu(+) ligating residues questions a two-site model of intramembranous Cu(+) binding, and we suggest an alternative role for the proposed second site in copper translocation and proton exchange. The class-specific features demonstrate that topological diversity in P-type ATPases may tune a general energy coupling scheme to the translocation of compounds with remarkably different properties.

Original language	English
Pages (from-to)	2299-308
Journal	Journal of Molecular Biology
Volume	425
Issue number	13
DOIs	https://doi.org/10.1016/j.jmb.2013.03.008
Publication status	Published - 2013 Jul 10
Externally published	Yes

Free keywords

Adenosine Triphosphatases
Allosteric Regulation
Binding Sites
Cation Transport Proteins
Crystallography, X-Ray
Ion Transport
Models, Biological
Models, Molecular
Molecular Dynamics Simulation
Protein Conformation
Journal Article
Research Support, Non-U.S. Gov't
Review

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10.1016/j.jmb.2013.03.008

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title = "On allosteric modulation of P-type Cu(+)-ATPases",

abstract = "P-type ATPases perform active transport of various compounds across biological membranes and are crucial for ion homeostasis and the asymmetric composition of lipid bilayers. Although their functional cycle share principles of phosphoenzyme intermediates, P-type ATPases also show subclass-specific sequence motifs and structural elements that are linked to transport specificity and mechanistic modulation. Here we provide an overview of the Cu(+)-transporting ATPases (of subclass PIB) and compare them to the well-studied sarco(endo)plasmic reticulum Ca(2+)-ATPase (of subclass PIIA). Cu(+) ions in the cell are delivered by soluble chaperones to Cu(+)-ATPases, which expose a putative {"}docking platform{"} at the intracellular interface. Cu(+)-ATPases also contain heavy-metal binding domains providing a basis for allosteric control of pump activity. Database analysis of Cu(+) ligating residues questions a two-site model of intramembranous Cu(+) binding, and we suggest an alternative role for the proposed second site in copper translocation and proton exchange. The class-specific features demonstrate that topological diversity in P-type ATPases may tune a general energy coupling scheme to the translocation of compounds with remarkably different properties.",

keywords = "Adenosine Triphosphatases, Allosteric Regulation, Binding Sites, Cation Transport Proteins, Crystallography, X-Ray, Ion Transport, Models, Biological, Models, Molecular, Molecular Dynamics Simulation, Protein Conformation, Journal Article, Research Support, Non-U.S. Gov't, Review",

author = "Daniel Mattle and Oleg Sitsel and Autzen, {Henriette Elisabeth} and Gabriele Meloni and Pontus Gourdon and Poul Nissen",

year = "2013",

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doi = "10.1016/j.jmb.2013.03.008",

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T1 - On allosteric modulation of P-type Cu(+)-ATPases

AU - Mattle, Daniel

AU - Sitsel, Oleg

AU - Autzen, Henriette Elisabeth

AU - Meloni, Gabriele

AU - Gourdon, Pontus

AU - Nissen, Poul

PY - 2013/7/10

Y1 - 2013/7/10

N2 - P-type ATPases perform active transport of various compounds across biological membranes and are crucial for ion homeostasis and the asymmetric composition of lipid bilayers. Although their functional cycle share principles of phosphoenzyme intermediates, P-type ATPases also show subclass-specific sequence motifs and structural elements that are linked to transport specificity and mechanistic modulation. Here we provide an overview of the Cu(+)-transporting ATPases (of subclass PIB) and compare them to the well-studied sarco(endo)plasmic reticulum Ca(2+)-ATPase (of subclass PIIA). Cu(+) ions in the cell are delivered by soluble chaperones to Cu(+)-ATPases, which expose a putative "docking platform" at the intracellular interface. Cu(+)-ATPases also contain heavy-metal binding domains providing a basis for allosteric control of pump activity. Database analysis of Cu(+) ligating residues questions a two-site model of intramembranous Cu(+) binding, and we suggest an alternative role for the proposed second site in copper translocation and proton exchange. The class-specific features demonstrate that topological diversity in P-type ATPases may tune a general energy coupling scheme to the translocation of compounds with remarkably different properties.

AB - P-type ATPases perform active transport of various compounds across biological membranes and are crucial for ion homeostasis and the asymmetric composition of lipid bilayers. Although their functional cycle share principles of phosphoenzyme intermediates, P-type ATPases also show subclass-specific sequence motifs and structural elements that are linked to transport specificity and mechanistic modulation. Here we provide an overview of the Cu(+)-transporting ATPases (of subclass PIB) and compare them to the well-studied sarco(endo)plasmic reticulum Ca(2+)-ATPase (of subclass PIIA). Cu(+) ions in the cell are delivered by soluble chaperones to Cu(+)-ATPases, which expose a putative "docking platform" at the intracellular interface. Cu(+)-ATPases also contain heavy-metal binding domains providing a basis for allosteric control of pump activity. Database analysis of Cu(+) ligating residues questions a two-site model of intramembranous Cu(+) binding, and we suggest an alternative role for the proposed second site in copper translocation and proton exchange. The class-specific features demonstrate that topological diversity in P-type ATPases may tune a general energy coupling scheme to the translocation of compounds with remarkably different properties.

KW - Adenosine Triphosphatases

KW - Allosteric Regulation

KW - Binding Sites

KW - Cation Transport Proteins

KW - Crystallography, X-Ray

KW - Ion Transport

KW - Models, Biological

KW - Models, Molecular

KW - Molecular Dynamics Simulation

KW - Protein Conformation

KW - Journal Article

KW - Research Support, Non-U.S. Gov't

KW - Review

U2 - 10.1016/j.jmb.2013.03.008

DO - 10.1016/j.jmb.2013.03.008

M3 - Article

C2 - 23500486

SN - 1089-8638

VL - 425

SP - 2299

EP - 2308

JO - Journal of Molecular Biology

JF - Journal of Molecular Biology

IS - 13

ER -

On allosteric modulation of P-type Cu(+)-ATPases

Abstract

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