Abstract
Mitochondrial solute carrier family 25 member 10 (Slc25a10) transports dicarboxylates such as malate or succinate across the mitochondrial inner membrane. Although fatty acid synthesis in adipose tissue or the liver is initiated by citrate transport in exchange for malate across the mitochondrial membrane, the transporter responsible for supplying malate during citrate transport has not been identified. In the present study, we clarified the role of Slc25a10 in supplying malate for citrate transport and examined the effect of Slc25a10 suppression on the lipogenic pathway and lipid accumulation. We have reported an Slc25a10 increase in white adipose tissue in obese mouse models and a decrease in a fasted mouse model using expression profiles. Next, we examined the effect of Slc25a10 suppression by small interfering RNA on citrate transport in the lipogenic cell lines HepG2 and 3T3-L1. We observed that inhibition of malate transport by Slc25a10 suppression significantly reduced the citrate transport from the mitochondria to the cytosol. We also found that suppression of Slc25a10 down-regulated the lipogenic pathway, indicated by decreases in ACC1 expression and malonyl-CoA level. Furthermore, suppression of Slc25a10 decreased triglyceride lipid accumulation in adipose-differentiated 3T3-L1 cells. These results suggested that Slc25a10 plays an important role in supplying malate for citrate transport required for fatty acid synthesis and indicated that inhibition of Slc25a10 might effectively reduce lipid accumulation in adipose tissues.
Highlights
The mechanism involving the supply of cytosolic malate for the citrate transporter, which antiports the cytosolic malate and mitochondrial citrate, remains to be elucidated
We found that Slc25a10 plays a crucial role in supplying malate for the citrate transport required for fatty acid synthesis
We focused on Slc25a10, hypothesizing that the carrier is involved in the initial steps of fatty acid synthesis
Summary
The mechanism involving the supply of cytosolic malate for the citrate transporter, which antiports the cytosolic malate and mitochondrial citrate, remains to be elucidated. Suppression of Slc25a10 Reduces Malate Transport Activity in Isolated Mitochondria—To analyze the function of Slc25a10 in lipogenesis and examine the effect of inhibition on de novo fatty acid synthesis, we designed siRNA for human and mouse Slc25a10. After suppression of Slc25a10 expression by siRNA, mitochondria were isolated from HepG2 and 3T3-L1, and the malate exchange rate was measured.
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