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体外通过(去)磷酸化和底物供应对肝脏和肠道酰基辅酶A:胆固醇酰基转移酶活性的双重调节

Dual modulation of hepatic and intestinal acyl-CoA: cholesterol acyltransferase activity by (de-)phosphorylation and substrate supply in vitro.

作者信息

Suckling K E, Stange E F, Dietschy J M

出版信息

FEBS Lett. 1983 Jan 10;151(1):111-6. doi: 10.1016/0014-5793(83)80354-8.

Abstract

Acyl-CoA: cholesterol acyltransferase (ACAT) activity in microsomes from rat liver and rat intestinal epithelial cells was increased by incubation of the microsomes with the 100 000 x g supernatant fraction in the presence of ATP/MgCl2 and NaF. The measured activity was further increased by including cholesterol-rich liposomes in the preincubation. The ACAT activity in rat liver microsomes could be inhibited by preincubation in the presence of 100 000 x g supernatant and MgCl2 and microsomes preactivated by ATP/MgCl2 could also be inhibited in this way. The results suggest that ACAT activity in vitro is modulated by substrate supply and also reversibly by an ATP-dependent process which may be protein phosphorylation.

摘要

在ATP/MgCl₂和NaF存在的情况下,将大鼠肝脏和大鼠肠上皮细胞微粒体与100000×g上清液组分一起孵育,可使微粒体中的酰基辅酶A:胆固醇酰基转移酶(ACAT)活性增加。预孵育时加入富含胆固醇的脂质体,测得的活性会进一步增加。在100000×g上清液和MgCl₂存在的情况下进行预孵育,可抑制大鼠肝脏微粒体中的ACAT活性,并且经ATP/MgCl₂预激活的微粒体也能以这种方式被抑制。结果表明,体外ACAT活性受底物供应调节,也受一个可能是蛋白质磷酸化的ATP依赖性过程可逆调节。

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