A hallmark of phospholamban functional divergence is located in the N-terminal phosphorylation domain

A hallmark of phospholamban functional divergence is located in the N-terminal phosphorylation domain

Sarcoplasmic reticulum Ca2+ pump (SERCA) is a critical component of the Ca2+ transport machinery in myocytes. There is clear evidence for regulation of SERCA activity by PLB, whose activity is modulated by phosphorylation of its N-terminal domain (residues 1–25), but there is less clear evidence for...

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Main Authors: Eli Fernández-de Gortari, Rodrigo Aguayo-Ortiz, Joseph M. Autry, L. Michel Espinoza-Fonseca
Format: Article
Language:English
Published: Elsevier 2020-01-01
Series:Computational and Structural Biotechnology Journal
Subjects:
Calcium pump
Phospholamban
Sarcolipin
Functional divergence
Phosphorylation domain
Molecular dynamics simulations
Online Access:http://www.sciencedirect.com/science/article/pii/S2001037019305136
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spelling doaj-72dd00a178e94cbab4530c66acc069cc2021-01-02T05:08:28ZengElsevierComputational and Structural Biotechnology Journal2001-03702020-01-0118705713A hallmark of phospholamban functional divergence is located in the N-terminal phosphorylation domainEli Fernández-de Gortari0Rodrigo Aguayo-Ortiz1Joseph M. Autry2L. Michel Espinoza-Fonseca3Center for Arrhythmia Research, Department of Internal Medicine, Division of Cardiovascular Medicine, University of Michigan, Ann Arbor, MI 48109, USACenter for Arrhythmia Research, Department of Internal Medicine, Division of Cardiovascular Medicine, University of Michigan, Ann Arbor, MI 48109, USADepartment of Biochemistry, Molecular Biology, and Biophysics, University of Minnesota, Minneapolis, MN 55455, USA; Biophysical Technology Center, University of Minnesota, Minneapolis, MN 55455, USACenter for Arrhythmia Research, Department of Internal Medicine, Division of Cardiovascular Medicine, University of Michigan, Ann Arbor, MI 48109, USA; Corresponding author.Sarcoplasmic reticulum Ca2+ pump (SERCA) is a critical component of the Ca2+ transport machinery in myocytes. There is clear evidence for regulation of SERCA activity by PLB, whose activity is modulated by phosphorylation of its N-terminal domain (residues 1–25), but there is less clear evidence for the role of this domain in PLB’s functional divergence. It is widely accepted that only sarcolipin (SLN), a protein that shares substantial homology with PLB, uncouples SERCA Ca2+ transport from ATP hydrolysis by inducing a structural change of its energy-transduction domain; yet, experimental evidence shows that the transmembrane domain of PLB (residues 26–52, PLB26–52) partially uncouples SERCA in vitro. These apparently conflicting mechanisms suggest that PLB’s uncoupling activity is encoded in its transmembrane domain, and that it is controlled by the N-terminal phosphorylation domain. To test this hypothesis, we performed molecular dynamics simulations (MDS) of the binary complex between PLB26–52 and SERCA. Comparison between PLB26–52 and wild-type PLB (PLBWT) showed no significant changes in the stability and orientation of the transmembrane helix, indicating that PLB26–52 forms a native-like complex with SERCA. MDS showed that PLB26–52 produces key intermolecular contacts and structural changes required for inhibition, in agreement with studies showing that PLB26–52 inhibits SERCA. However, deletion of the N-terminal phosphorylation domain facilitates an order-to-disorder shift in the energy-transduction domain associated with uncoupling of SERCA, albeit weaker than that induced by SLN. This mechanistic evidence reveals that the N-terminal phosphorylation domain of PLB is a primary contributor to the functional divergence among homologous SERCA regulators.http://www.sciencedirect.com/science/article/pii/S2001037019305136Calcium pumpPhospholambanSarcolipinFunctional divergencePhosphorylation domainMolecular dynamics simulations
collection DOAJ
language English
format Article
sources DOAJ
author Eli Fernández-de Gortari
Rodrigo Aguayo-Ortiz
Joseph M. Autry
L. Michel Espinoza-Fonseca
spellingShingle Eli Fernández-de Gortari
Rodrigo Aguayo-Ortiz
Joseph M. Autry
L. Michel Espinoza-Fonseca
A hallmark of phospholamban functional divergence is located in the N-terminal phosphorylation domain
Computational and Structural Biotechnology Journal
Calcium pump
Phospholamban
Sarcolipin
Functional divergence
Phosphorylation domain
Molecular dynamics simulations
author_facet Eli Fernández-de Gortari
Rodrigo Aguayo-Ortiz
Joseph M. Autry
L. Michel Espinoza-Fonseca
author_sort Eli Fernández-de Gortari
title A hallmark of phospholamban functional divergence is located in the N-terminal phosphorylation domain
title_short A hallmark of phospholamban functional divergence is located in the N-terminal phosphorylation domain
title_full A hallmark of phospholamban functional divergence is located in the N-terminal phosphorylation domain
title_fullStr A hallmark of phospholamban functional divergence is located in the N-terminal phosphorylation domain
title_full_unstemmed A hallmark of phospholamban functional divergence is located in the N-terminal phosphorylation domain
title_sort hallmark of phospholamban functional divergence is located in the n-terminal phosphorylation domain
publisher Elsevier
series Computational and Structural Biotechnology Journal
issn 2001-0370
publishDate 2020-01-01
description Sarcoplasmic reticulum Ca2+ pump (SERCA) is a critical component of the Ca2+ transport machinery in myocytes. There is clear evidence for regulation of SERCA activity by PLB, whose activity is modulated by phosphorylation of its N-terminal domain (residues 1–25), but there is less clear evidence for the role of this domain in PLB’s functional divergence. It is widely accepted that only sarcolipin (SLN), a protein that shares substantial homology with PLB, uncouples SERCA Ca2+ transport from ATP hydrolysis by inducing a structural change of its energy-transduction domain; yet, experimental evidence shows that the transmembrane domain of PLB (residues 26–52, PLB26–52) partially uncouples SERCA in vitro. These apparently conflicting mechanisms suggest that PLB’s uncoupling activity is encoded in its transmembrane domain, and that it is controlled by the N-terminal phosphorylation domain. To test this hypothesis, we performed molecular dynamics simulations (MDS) of the binary complex between PLB26–52 and SERCA. Comparison between PLB26–52 and wild-type PLB (PLBWT) showed no significant changes in the stability and orientation of the transmembrane helix, indicating that PLB26–52 forms a native-like complex with SERCA. MDS showed that PLB26–52 produces key intermolecular contacts and structural changes required for inhibition, in agreement with studies showing that PLB26–52 inhibits SERCA. However, deletion of the N-terminal phosphorylation domain facilitates an order-to-disorder shift in the energy-transduction domain associated with uncoupling of SERCA, albeit weaker than that induced by SLN. This mechanistic evidence reveals that the N-terminal phosphorylation domain of PLB is a primary contributor to the functional divergence among homologous SERCA regulators.
topic Calcium pump
Phospholamban
Sarcolipin
Functional divergence
Phosphorylation domain
Molecular dynamics simulations
url http://www.sciencedirect.com/science/article/pii/S2001037019305136
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