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Published May 1, 2012 | Published + Supplemental Material
Journal Article Open

Lysocardiolipin acyltransferase 1 (ALCAT1) controls mitochondrial DNA fidelity and biogenesis through modulation of MFN2 expression

Li, Jia
Liu, Xiaolei
Wang, Huayan
Zhang, Weiping
Chan, David C. ORCID icon
Shi, Yuguang

Abstract

Oxidative stress causes mitochondrial fragmentation and dysfunction in age-related diseases through unknown mechanisms. Cardiolipin (CL) is a phospholipid required for mitochondrial oxidative phosphorylation. The function of CL is determined by its acyl composition, which is significantly altered by the onset of age-related diseases. Here, we examine a role of acyl-CoA:lysocardiolipin acyltransferase lysocardiolipin acyltransferase 1 (ALCAT1), a lysocardiolipin acyltransferase that catalyzes pathological CL remodeling, in mitochondrial biogenesis. We show that overexpression of ALCAT1 causes mitochondrial fragmentation through oxidative stress and depletion of mitofusin mitofusin 2 (MFN2) expression. Strikingly, ALCAT1 overexpression also leads to mtDNA instability and depletion that are reminiscent of MFN2 deficiency. Accordingly, expression of MFN2 completely rescues mitochondrial fusion defect and respiratory dysfunction. Furthermore, ablation of ALCAT1 prevents mitochondrial fragmentation from oxidative stress by up-regulating MFN2 expression, mtDNA copy number, and mtDNA fidelity. Together, these findings reveal an unexpected role of CL remodeling in mitochondrial biogenesis, linking oxidative stress by ALCAT1 to mitochondrial fusion defect.

Additional Information

© 2012 National Academy of Sciences. Edited by Tak W. Mak, The Campbell Family Institute for Breast Cancer Research, Ontario Cancer Institute at Princess Margaret Hospital, University Health Network, Toronto, ON, Canada, and approved March 23, 2012 (received for review December 5, 2011). Published online before print April 16, 2012. We thank Mr. Roland Myers for EM analysis and Dr. Jaeseok Han for technical help with MEF isolation. This study was supported, in part, by National Institutes of Health Grants DK076685 (to Y.S.) and GM062967 (to D.C.C.) and a scholarship from the Chinese National Scholarship Council (to J.L.). Author contributions: Y.S. designed research; J.L. and X.L. performed research; H.W., W.Z., and D.C.C. contributed new reagents/analytic tools; J.L., X.L., D.C.C., and Y.S. analyzed data; and J.L. and Y.S. wrote the paper.

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Published - Li2012p18148P_Natl_Acad_Sci_Usa.pdf

Supplemental Material - pnas.201120043SI.pdf

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Created:
August 19, 2023
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October 17, 2023