Department of Biochemistry and Molecular Biology, University of Southern Denmark, 5230 Odense M, Denmark.
J Biol Chem. 2011 Feb 4;286(5):3460-72. doi: 10.1074/jbc.M110.161109. Epub 2010 Nov 24.
The acyl-CoA-binding protein (ACBP)/diazepam binding inhibitor is an intracellular protein that binds C(14)-C(22) acyl-CoA esters and is thought to act as an acyl-CoA transporter. In vitro analyses have indicated that ACBP can transport acyl-CoA esters between different enzymatic systems; however, little is known about the in vivo function in mammalian cells. We have generated mice with targeted disruption of ACBP (ACBP(-/-)). These mice are viable and fertile and develop normally. However, around weaning, the ACBP(-/-) mice go through a crisis with overall weakness and a slightly decreased growth rate. Using microarray analysis, we show that the liver of ACBP(-/-) mice displays a significantly delayed adaptation to weaning with late induction of target genes of the sterol regulatory element-binding protein (SREBP) family. As a result, hepatic de novo cholesterogenesis is decreased at weaning. The delayed induction of SREBP target genes around weaning is caused by a compromised processing and decreased expression of SREBP precursors, leading to reduced binding of SREBP to target sites in chromatin. In conclusion, lack of ACBP interferes with the normal metabolic adaptation to weaning and leads to delayed induction of the lipogenic gene program in the liver.
酰基辅酶 A 结合蛋白 (ACBP)/地西泮结合抑制剂是一种细胞内蛋白,可结合 C(14)-C(22)酰基辅酶 A 酯,并被认为可作为酰基辅酶 A 转运体。体外分析表明 ACBP 可以在不同的酶系统之间转运酰基辅酶 A 酯;然而,关于其在哺乳动物细胞中的体内功能知之甚少。我们已经生成了靶向敲除 ACBP(ACBP(-/-))的小鼠。这些小鼠具有活力和生育能力,并且正常发育。然而,在断奶期间,ACBP(-/-)小鼠会经历一场危机,表现为全身虚弱和生长速度略有下降。通过微阵列分析,我们表明 ACBP(-/-)小鼠的肝脏在断奶时表现出明显的适应延迟,固醇调节元件结合蛋白 (SREBP) 家族的靶基因延迟诱导。结果,肝内新生胆固醇合成在断奶时减少。断奶时 SREBP 靶基因的延迟诱导是由于 SREBP 前体的加工受损和表达减少,导致 SREBP 与染色质中靶位点的结合减少所致。总之,缺乏 ACBP 会干扰正常的代谢适应断奶,并导致肝脏中脂肪生成基因程序的延迟诱导。
