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大鼠肺微粒体中的酰基转移酶活性。

Acyltransferase activities in rat lung microsomes.

作者信息

Hasegawa-Sasaki H, Ohno K

出版信息

Biochim Biophys Acta. 1975 Mar 24;380(3):486-95.

PMID:1138876
Abstract

Some properties of acyl-CoA:1-acyl-sn-glycero-3-phosphorylcholine acyl-transferase in rat lung microsomes wed moiety of acyl-CoAs, quite different values were obtained on the Michaelis constant, the maximal velocity, and the activation energy. Moreover, the incorporation of fatty acid from an acyl-CoA was affected in a different manner by the addition of other acyl-CoAs. These results suggested that there are at least two different acyltransferases which are tentatively termed as follows: (1) palmitoyl-CoA: 1-acylglycerophosphorylcholine acyltransferase; and (2) arachidonoyl-CoA: 1-acylglycerophosphorylcholine acyltransferase. A low Km value, a low maximal velocity, and a low value of the activation energy were obtained for the former activity. The activity is readily inhibited by the addition of other acyl-CoAs and also at the higher concentration of palmitoyl-CoA itself. While a high Km value, a high maximal velocity, and a high value of the activation energy were obtained for the latter activity. The activity is not affected by the addition of palmitoyl-CoA or oleoyl-CoA and only slightly inhibited by linoleoyl-CoA, which indicates a high substrate specificity for polyenoyl-CoA especially for arachidonoyl-CoA. It seems that the present result, together with the previous findings obtained in slice experiments and in in vivo studies, do not support the idea that palmitoyl-CoA : 1-acylglycerophosphorylcholine acyltransferase participates in the main pathway for the formation of dipalmitoyllecithin in lung.

摘要

大鼠肺微粒体中酰基辅酶A:1-酰基-sn-甘油-3-磷酸胆碱酰基转移酶的一些特性 对于酰基辅酶A的不同部分,在米氏常数、最大速度和活化能方面获得了截然不同的值。此外,添加其他酰基辅酶A对来自酰基辅酶A的脂肪酸掺入有不同的影响。这些结果表明至少存在两种不同的酰基转移酶,暂命名如下:(1)棕榈酰辅酶A:1-酰基甘油磷酸胆碱酰基转移酶;(2)花生四烯酰辅酶A:1-酰基甘油磷酸胆碱酰基转移酶。前一种活性的米氏常数低、最大速度低且活化能值低。该活性很容易被添加其他酰基辅酶A以及较高浓度的棕榈酰辅酶A本身所抑制。而后一种活性的米氏常数高、最大速度高且活化能值高。该活性不受添加棕榈酰辅酶A或油酰辅酶A的影响,仅被亚油酰辅酶A轻微抑制,这表明对多烯酰辅酶A尤其是花生四烯酰辅酶A具有高底物特异性。似乎目前的结果与先前在切片实验和体内研究中获得的结果一起,并不支持棕榈酰辅酶A:1-酰基甘油磷酸胆碱酰基转移酶参与肺中二棕榈酰卵磷脂形成的主要途径这一观点。

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