Cardiolipin Remodeling by ALCAT1 Links Oxidative Stress and Mitochondrial Dysfunction to Obesity

Oxidative stress causes mitochondrial dysfunction and metabolic complications through unknown mechanisms. Cardiolipin (CL) is a key mitochondrial phospholipid required for oxidative phosphorylation. Oxidative damage to CL from pathological remodeling is implicated in the etiology of mitochondrial dy...

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Published inCell metabolism Vol. 12; no. 2; pp. 154 - 165
Main Authors Li, Jia, Romestaing, Caroline, Han, Xianlin, Li, Yuan, Hao, Xinbao, Wu, Yinyuan, Sun, Chao, Liu, Xiaolei, Jefferson, Leonard S., Xiong, Jingwei, LaNoue, Kathryn F., Chang, Zhijie, Lynch, Christopher J., Wang, Huayan, Shi, Yuguang
Format Journal Article
LanguageEnglish
Published United States Elsevier Inc 04.08.2010
Subjects
Acyltransferases - deficiency
Acyltransferases - genetics
Acyltransferases - metabolism
Animals
Cardiolipins - metabolism
Cell Line
HUMDISEASE
Insulin Resistance
Mice
Mitochondria - metabolism
Mitochondria - physiology
Obesity - etiology
Obesity - metabolism
Oxidative Stress
Phosphorylation
Reactive Oxygen Species - metabolism
SIGNALING
Up-Regulation
HUMDISEASE
SIGNALING
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Summary:Oxidative stress causes mitochondrial dysfunction and metabolic complications through unknown mechanisms. Cardiolipin (CL) is a key mitochondrial phospholipid required for oxidative phosphorylation. Oxidative damage to CL from pathological remodeling is implicated in the etiology of mitochondrial dysfunction commonly associated with diabetes, obesity, and other metabolic diseases. Here, we show that ALCAT1, a lyso-CL acyltransferase upregulated by oxidative stress and diet-induced obesity (DIO), catalyzes the synthesis of CL species that are highly sensitive to oxidative damage, leading to mitochondrial dysfunction, ROS production, and insulin resistance. These metabolic disorders were reminiscent of those observed in type 2 diabetes and were reversed by rosiglitazone treatment. Consequently, ALCAT1 deficiency prevented the onset of DIO and significantly improved mitochondrial complex I activity, lipid oxidation, and insulin signaling in ALCAT1−/− mice. Collectively, these findings identify a key role of ALCAT1 in regulating CL remodeling, mitochondrial dysfunction, and susceptibility to DIO. ► ALCAT1 expression is upregulated by oxidative stress and the onset of diet-induced obesity ► ALCAT1 catalyzes the synthesis of cardiolipin species commonly found in metabolic diseases ► ALCAT1 causes oxidative stress and mitochondrial dysfunction when overexpressed in C2C12 cells ► ALCAT1−/− mice are resistant to DIO and the related mitochondrial defects and oxidative stress
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These authors contributed equally to the work
ISSN:1550-4131
1932-7420
DOI:10.1016/j.cmet.2010.07.003