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大鼠肝脏中视黄醇的酯化作用。细胞视黄醇结合蛋白和细胞视黄醇结合蛋白II可能参与其中。

Esterification of retinol in rat liver. Possible participation by cellular retinol-binding protein and cellular retinol-binding protein II.

作者信息

Ong D E, MacDonald P N, Gubitosi A M

机构信息

Department of Biochemistry, Vanderbilt University School of Medicine, Nashville, Tennessee 37232.

出版信息

J Biol Chem. 1988 Apr 25;263(12):5789-96.

PMID:3281946
Abstract

Retinol bound to cellular retinol-binding protein (CRBP) was available for esterification by liver microsomes in the absence of exogenous acyl donors. Moreover, exogenous acyl-CoA gave little or no stimulation of ester production over what was observed with the endogenous acyl donor. In contrast, unbound retinol was esterified in an acyl-CoA-dependent reaction. The presence of two different enzyme activities, acyl-CoA-dependent and -independent, was demonstrated by differential sensitivities to several enzyme inhibitors. The enzyme reaction with retinol-CRBP and endogenous acyl donor produced retinyl esters normally found in vivo in liver. In addition, rates of esterification with this system were sufficient to maintain liver stores. Liver also contains cellular retinol-binding protein, type II (CRBP(II] during the perinatal period. Radioimmunoassay revealed highest levels of CRBP(II) in liver 3-4 days after birth. Examination of retinol esterification by microsomes from the liver of 3-day-old rats revealed a retinyl ester synthase activity with lower Km and higher Vmax than that found in the adult. The activity could use either retinol-CRBP or retinol-CRBP(II) and an endogenous acyl donor. The microsomes from 3-day-old liver had greater esterifying ability than microsomes from adult liver, perhaps due to the presence of two retinyl ester synthase enzymes.

摘要

在没有外源性酰基供体的情况下,与细胞视黄醇结合蛋白(CRBP)结合的视黄醇可被肝微粒体用于酯化。此外,与内源性酰基供体相比,外源性酰基辅酶A对酯生成的刺激作用很小或没有。相反,未结合的视黄醇在依赖酰基辅酶A的反应中被酯化。对几种酶抑制剂的不同敏感性证明了两种不同酶活性的存在,即依赖酰基辅酶A和不依赖酰基辅酶A的活性。视黄醇-CRBP与内源性酰基供体的酶反应产生了肝脏中正常存在于体内的视黄酯。此外,该系统的酯化速率足以维持肝脏储存。在围产期肝脏中还含有II型细胞视黄醇结合蛋白(CRBP(II))。放射免疫分析显示出生后3-4天肝脏中CRBP(II)水平最高。对3日龄大鼠肝脏微粒体视黄醇酯化的研究表明,与成年大鼠相比,视黄酯合酶活性的Km较低,Vmax较高。该活性可以使用视黄醇-CRBP或视黄醇-CRBP(II)以及内源性酰基供体。3日龄肝脏的微粒体比成年肝脏的微粒体具有更强的酯化能力,这可能是由于存在两种视黄酯合酶。

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