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Creatine kinase B controls futile creatine cycling in thermogenic fat

Authors :
Christien B. Dykstra
Linus T.-Y. Tsai
Karen Reue
Janane F. Rahbani
Laurent Vergnes
Anna Roesler
Lawrence Kazak
Mark P. Jedrychowski
Bozena Samborska
Bruce M. Spiegelman
Mohammed Faiz Hussain
Source :
Nature
Publication Year :
2020

Abstract

Obesity increases the risk of mortality because of metabolic sequelae such as type 2 diabetes and cardiovascular disease1. Thermogenesis by adipocytes can counteract obesity and metabolic diseases2,3. In thermogenic fat, creatine liberates a molar excess of mitochondrial ADP—purportedly via a phosphorylation cycle4—to drive thermogenic respiration. However, the proteins that control this futile creatine cycle are unknown. Here we show that creatine kinase B (CKB) is indispensable for thermogenesis resulting from the futile creatine cycle, during which it traffics to mitochondria using an internal mitochondrial targeting sequence. CKB is powerfully induced by thermogenic stimuli in both mouse and human adipocytes. Adipocyte-selective inactivation of Ckb in mice diminishes thermogenic capacity, increases predisposition to obesity, and disrupts glucose homeostasis. CKB is therefore a key effector of the futile creatine cycle. Upon induction by thermogenic stimuli, creatine kinase B traffics to mitochondria to trigger the futile creatine cycle in thermogenic fat.

Details

ISSN :
14764687
Volume :
590
Issue :
7846
Database :
OpenAIRE
Journal :
Nature
Accession number :
edsair.doi.dedup.....edde8a4ba37f0da3658b9cc6524ff3e7