Abstract
CGI-58 is a lipid droplet-associated protein that, when mutated, causes Chanarin-Dorfman syndrome in humans, which is characterized by excessive storage of triglyceride in various tissues. However, the molecular mechanisms underlying the defect remain elusive. CGI-58 was previously reported to catalyze the resynthesis of phosphatidic acid as a lysophosphatidic acid acyltransferase. In addition to triglyceride, phosphatidic acid is also used a substrate for the synthesis of various mitochondrial phospholipids. In this report, we investigated the propensity of CGI-58 in the remodeling of various phospholipids. We found that the recombinant CGI-58 overexpressed in mammalian cells or purified from Sf9 insect cells catalyzed efficiently the reacylation of lysophosphatidylglycerol to phosphatidylglycerol (PG), which requires acyl-CoA as the acyl donor. In contrast, the recombinant CGI-58 was devoid of acyltransferase activity toward other lysophospholipids. Accordingly, overexpression and knockdown of CGI-58 adversely affected the endogenous PG level in C2C12 cells. PG is a substrate for the synthesis of cardiolipin, which is required for mitochondrial oxidative phosphorylation and mitophagy. Consequently, overexpression and knockdown of CGI-58 adversely affected autophagy and mitophagy in C2C12 cells. In support for a key role of CGI-58 in mitophagy, overexpression of CGI-58 significantly stimulated mitochondrial fission and translocation of PINK1 to mitochondria, key steps involved in mitophagy. Furthermore, overexpression of CGI-58 promoted mitophagic initiation through activation of 5'-AMP-activated protein kinase and inhibition of mTORC1 mammalian target of rapamycin complex 1 signaling, the positive and negative regulators of autophagy, respectively. Together, these findings identified novel molecular mechanisms by which CGI-58 regulates lipid homeostasis, because defective autophagy is implicated in dyslipidemia and fatty liver diseases.
Highlights
CGI-58 plays an essential role in lipid homeostasis with poorly defined mechanisms
CGI-58 Is a Novel lysophosphatidylglycerol acyltransferase (LPGAT)—Previous studies indicated that CGI-58 catalyzes the synthesis of phosphatidic acid as a lysophosphatidic acid acyltransferase (LPAAT) enzyme
To confirm the LPGAT activity was not caused by a compensatory response of the endogenous LPGAT enzymes, we analyzed LPGAT activity of the purified recombinant CGI-58, which was overexpressed in Sf9 insect cells and purified using anti-FLAG antibody agarose resin
Summary
CGI-58 plays an essential role in lipid homeostasis with poorly defined mechanisms. Results: CGI-58 promotes autophagy as a novel lysophosphatidylglcyerol acyltransferase. Conclusion: CGI-58 regulates lipid homeostasis in part by promoting autophagy. Significance: Our findings provide potential molecular mechanisms by which CGI-58 mutations cause dyslipidemia. Overexpression and knockdown of CGI-58 adversely affected autophagy and mitophagy in C2C12 cells. Overexpression of CGI-58 promoted mitophagic initiation through activation of 5-AMP-activated protein kinase and inhibition of mTORC1 mammalian target of rapamycin complex 1 signaling, the positive and negative regulators of autophagy, respectively. Together, these findings identified novel molecular mechanisms by which CGI-58
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