Structure-based dynamic arrays in regulatory domains of sodium-calcium exchanger (NCX) isoforms
Abstract Mammalian Na+/Ca2+ exchangers, NCX1 and NCX3, generate splice variants, whereas NCX2 does not. The CBD1 and CBD2 domains form a regulatory tandem (CBD12), where Ca2+ binding to CBD1 activates and Ca2+ binding to CBD2 (bearing the splicing segment) alleviates the Na+-induced inactivation. He...
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doaj-e36e68f88afb4f2581ecb244352f12a32020-12-08T00:56:02ZengNature Publishing GroupScientific Reports2045-23222017-04-017111210.1038/s41598-017-01102-xStructure-based dynamic arrays in regulatory domains of sodium-calcium exchanger (NCX) isoformsMoshe Giladi0Su Youn Lee1Yarden Ariely2Yotam Teldan3Rotem Granit4Roi Strulovich5Yoni Haitin6Ka Young Chung7Daniel Khananshvili8Department of Physiology and Pharmacology, Tel-Aviv UniversitySchool of Pharmacy, Sungkyunkwan UniversityDepartment of Physiology and Pharmacology, Tel-Aviv UniversityDepartment of Physiology and Pharmacology, Tel-Aviv UniversityDepartment of Physiology and Pharmacology, Tel-Aviv UniversityDepartment of Physiology and Pharmacology, Tel-Aviv UniversityDepartment of Physiology and Pharmacology, Tel-Aviv UniversitySchool of Pharmacy, Sungkyunkwan UniversityDepartment of Physiology and Pharmacology, Tel-Aviv UniversityAbstract Mammalian Na+/Ca2+ exchangers, NCX1 and NCX3, generate splice variants, whereas NCX2 does not. The CBD1 and CBD2 domains form a regulatory tandem (CBD12), where Ca2+ binding to CBD1 activates and Ca2+ binding to CBD2 (bearing the splicing segment) alleviates the Na+-induced inactivation. Here, the NCX2-CBD12, NCX3-CBD12-B, and NCX3-CBD12-AC proteins were analyzed by small-angle X-ray scattering (SAXS) and hydrogen-deuterium exchange mass-spectrometry (HDX-MS) to resolve regulatory variances in the NCX2 and NCX3 variants. SAXS revealed the unified model, according to which the Ca2+ binding to CBD12 shifts a dynamic equilibrium without generating new conformational states, and where more rigid conformational states become more populated without any global conformational changes. HDX-MS revealed the differential effects of the B and AC exons on the folding stability of apo CBD1 in NCX3-CBD12, where the dynamic differences become less noticeable in the Ca2+-bound state. Therefore, the apo forms predefine incremental changes in backbone dynamics upon Ca2+ binding. These observations may account for slower inactivation (caused by slower dissociation of occluded Ca2+ from CBD12) in the skeletal vs the brain-expressed NCX2 and NCX3 variants. This may have physiological relevance, since NCX must extrude much higher amounts of Ca2+ from the skeletal cell than from the neuron.https://doi.org/10.1038/s41598-017-01102-x |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Moshe Giladi Su Youn Lee Yarden Ariely Yotam Teldan Rotem Granit Roi Strulovich Yoni Haitin Ka Young Chung Daniel Khananshvili |
spellingShingle |
Moshe Giladi Su Youn Lee Yarden Ariely Yotam Teldan Rotem Granit Roi Strulovich Yoni Haitin Ka Young Chung Daniel Khananshvili Structure-based dynamic arrays in regulatory domains of sodium-calcium exchanger (NCX) isoforms Scientific Reports |
author_facet |
Moshe Giladi Su Youn Lee Yarden Ariely Yotam Teldan Rotem Granit Roi Strulovich Yoni Haitin Ka Young Chung Daniel Khananshvili |
author_sort |
Moshe Giladi |
title |
Structure-based dynamic arrays in regulatory domains of sodium-calcium exchanger (NCX) isoforms |
title_short |
Structure-based dynamic arrays in regulatory domains of sodium-calcium exchanger (NCX) isoforms |
title_full |
Structure-based dynamic arrays in regulatory domains of sodium-calcium exchanger (NCX) isoforms |
title_fullStr |
Structure-based dynamic arrays in regulatory domains of sodium-calcium exchanger (NCX) isoforms |
title_full_unstemmed |
Structure-based dynamic arrays in regulatory domains of sodium-calcium exchanger (NCX) isoforms |
title_sort |
structure-based dynamic arrays in regulatory domains of sodium-calcium exchanger (ncx) isoforms |
publisher |
Nature Publishing Group |
series |
Scientific Reports |
issn |
2045-2322 |
publishDate |
2017-04-01 |
description |
Abstract Mammalian Na+/Ca2+ exchangers, NCX1 and NCX3, generate splice variants, whereas NCX2 does not. The CBD1 and CBD2 domains form a regulatory tandem (CBD12), where Ca2+ binding to CBD1 activates and Ca2+ binding to CBD2 (bearing the splicing segment) alleviates the Na+-induced inactivation. Here, the NCX2-CBD12, NCX3-CBD12-B, and NCX3-CBD12-AC proteins were analyzed by small-angle X-ray scattering (SAXS) and hydrogen-deuterium exchange mass-spectrometry (HDX-MS) to resolve regulatory variances in the NCX2 and NCX3 variants. SAXS revealed the unified model, according to which the Ca2+ binding to CBD12 shifts a dynamic equilibrium without generating new conformational states, and where more rigid conformational states become more populated without any global conformational changes. HDX-MS revealed the differential effects of the B and AC exons on the folding stability of apo CBD1 in NCX3-CBD12, where the dynamic differences become less noticeable in the Ca2+-bound state. Therefore, the apo forms predefine incremental changes in backbone dynamics upon Ca2+ binding. These observations may account for slower inactivation (caused by slower dissociation of occluded Ca2+ from CBD12) in the skeletal vs the brain-expressed NCX2 and NCX3 variants. This may have physiological relevance, since NCX must extrude much higher amounts of Ca2+ from the skeletal cell than from the neuron. |
url |
https://doi.org/10.1038/s41598-017-01102-x |
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