SEC61B regulates calcium flux and platelet hyperreactivity in diabetes

Yvonne Kong; Rajan Rehan; Cesar L. Moreno; Søren Madsen; Yunwei Zhang; Huiwen Zhao; Miao Qi; Callum B. Houlahan; Siân P. Cartland; Declan Robertshaw; Vincent Trang; Frederick Jun Liang Ong; Michael Liu; Edward Cheng; Imala Alwis; Alexander Dupuy; Michelle Cielesh; Kristen C. Cooke; Meg Potter; Jacqueline Stöckli; Grant Morahan; Maggie Kalev-Zylinska; Matthew T. Rondina; Sol Schulman; Jean Y H Yang; G. Gregory Neely; Simone M. Schoenwaelder; Shaun P Jackson; David E. James; Mary M. Kavurma; Samantha L. Hocking; Stephen M. Twigg; James C. Weaver; Mark Larance; Freda H. Passam

doi:10.1172/JCI184597

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SEC61B regulates calcium flux and platelet hyperreactivity in diabetes

Journal article

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Peer reviewed

SEC61B regulates calcium flux and platelet hyperreactivity in diabetes

Yvonne Kong, Rajan Rehan, Cesar L. Moreno, Søren Madsen, Yunwei Zhang, Huiwen Zhao, Miao Qi, Callum B. Houlahan, Siân P. Cartland, Declan Robertshaw, …

The Journal of clinical investigation, Vol.135(16), e184597

2025

DOI: https://doi.org/10.1172/JCI184597

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Abstract

Platelet hyperreactivity increases the risk of cardiovascular thrombosis in diabetes and failure of antiplatelet drug therapies. Elevated basal and agonist-induced calcium flux is a fundamental cause of platelet hyperreactivity in diabetes; however, the mechanisms responsible for this remain largely unknown. Using a high-sensitivity, unbiased proteomic platform, we consistently detected over 2,400 intracellular proteins and identified proteins that were differentially released by platelets in type 2 diabetes. We identified that SEC61 translocon subunit β (SEC61B) was increased in platelets from humans and mice with hyperglycemia and in megakaryocytes from mice with hyperglycemia. SEC61 is known to act as an endoplasmic reticulum (ER) calcium leak channel in nucleated cells. Using HEK293 cells, we showed that SEC61B overexpression increased calcium flux into the cytosol and decreased protein synthesis. Concordantly, platelets in hyperglycemic mice mobilized more calcium and had decreased protein synthesis. Platelets in both humans and mice with hyperglycemia had increased ER stress. ER stress induced the expression of platelet SEC61B and increased cytosolic calcium. Inhibition of SEC61 with anisomycin decreased platelet calcium flux and inhibited platelet aggregation in vitro and in vivo. These studies demonstrate the existence of a mechanism whereby ER stress–induced upregulation of platelet SEC61B leads to increased cytosolic calcium, potentially contributing to platelet hyperreactivity in diabetes. This study identifies SEC61 as a novel endoplasmic reticulum calcium leak channel in platelets. Upregulation of SEC61B contributes to platelet hyperreactivity in diabetes.

Details

Title: SEC61B regulates calcium flux and platelet hyperreactivity in diabetes
Authors/Creators: Yvonne Kong
Rajan Rehan
Cesar L. Moreno
Søren Madsen
Yunwei Zhang
Huiwen Zhao
Miao Qi
Callum B. Houlahan
Siân P. Cartland
Declan Robertshaw
Vincent Trang
Frederick Jun Liang Ong
Michael Liu
Edward Cheng
Imala Alwis
Alexander Dupuy
Michelle Cielesh
Kristen C. Cooke
Meg Potter
Jacqueline Stöckli
Grant Morahan
Maggie Kalev-Zylinska
Matthew T. Rondina
Sol Schulman
Jean Y H Yang
G. Gregory Neely
Simone M. Schoenwaelder
Shaun P Jackson
David E. James
Mary M. Kavurma
Samantha L. Hocking
Stephen M. Twigg
James C. Weaver
Mark Larance
Freda H. Passam
Publication Details: The Journal of clinical investigation, Vol.135(16), e184597
Publisher: American Society for Clinical Investigation
Identifiers: 991005806848707891
Murdoch Affiliation: School of Mathematics, Statistics, Chemistry and Physics
Language: English
Resource Type: Journal article

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