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大鼠乳腺中酰基辅酶A:胆固醇酰基转移酶活性:妊娠和哺乳期的变化

Acyl-CoA: cholesterol acyltransferase activity in the rat mammary gland: variation during pregnancy and lactation.

作者信息

Shand J H, West D W

机构信息

Hannah Research Institute, Ayr, Scotland.

出版信息

Lipids. 1991 Feb;26(2):150-4. doi: 10.1007/BF02544010.

Abstract

Cholesterol esterification by acyl-CoA:cholesterol acyltransferase (ACAT; EC 2.3.1.26) has been studied in microsomes isolated from the mammary glands of rats in late pregnancy, in early and mid-lactation, and following premature weaning. The mammary glands were freeze-clamped and the microsomes prepared in the presence of phosphatase inhibitors to preserve the phosphorylation status of the enzyme. Optimal conditions were established for the assay of enzyme activity in the presence of endogenous cholesterol. Supplementation of the microsomes with exogenous cholesterol as a dispersion in Triton WR-1339 was shown to lead to an increase in enzyme activity. Incubation of microsomes with MgATP led to an increase in ACAT activity which could be reversed by treatment of the microsomes with a phosphoprotein phosphatase preparation from rat liver. The results suggested that ACAT activity in the mammary gland was activated by phosphorylation in a similar way to that observed for the hepatic enzyme. The mammary glands from pregnant animals contained a higher level of ACAT activity than did the glands of the lactating animals and this correlated with the higher cholesteryl ester content of the pregnant glands. The highest level of ACAT activity was found in the weaned animals but the cholesteryl ester content of the microsomes was lower than expected. The influence of progesterone levels and changes in feeding patterns during gestation were considered as factors in these variations in ACAT activity.

摘要

已对从妊娠后期、泌乳早期和中期以及提前断奶后的大鼠乳腺中分离出的微粒体中的酰基辅酶A:胆固醇酰基转移酶(ACAT;EC 2.3.1.26)介导的胆固醇酯化作用进行了研究。将乳腺进行冷冻钳夹,并在存在磷酸酶抑制剂的情况下制备微粒体,以保持该酶的磷酸化状态。确定了在存在内源性胆固醇的情况下测定酶活性的最佳条件。结果表明,用在Triton WR - 1339中分散的外源性胆固醇补充微粒体会导致酶活性增加。将微粒体与MgATP一起孵育会导致ACAT活性增加,而用来自大鼠肝脏的磷蛋白磷酸酶制剂处理微粒体可使其逆转。结果表明,乳腺中的ACAT活性以与肝脏酶类似的方式通过磷酸化被激活。怀孕动物的乳腺中ACAT活性水平高于泌乳动物的乳腺,这与怀孕乳腺中较高的胆固醇酯含量相关。断奶动物的ACAT活性水平最高,但微粒体中的胆固醇酯含量低于预期。妊娠期间孕酮水平和喂养模式变化的影响被认为是这些ACAT活性变化的因素。

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