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新生大鼠的脂蛋白。低密度脂蛋白与富含载脂蛋白E的高密度脂蛋白的相互发育。

Lipoproteins of the newborn rat. Reciprocal development of low density lipoproteins and apoprotein E-rich high density lipoproteins.

作者信息

Perrin Ansart M C, Vacher D, Girard-Globa A

机构信息

Centre de Recherches sur la Nutrition du CNRS, Meudon, France.

出版信息

J Dev Physiol. 1988 Aug;10(4):321-34.

PMID:3204263
Abstract

Plasma lipids increase sharply with the onset of suckling in the neonatal rat. Much of the variation has been attributed to the high fat content of milk. Apoproteins AI, E and AIV were found in low concentrations in the fetus. They increased during suckling. Apoprotein E and apoprotein AIV did not exceed adult values whereas apoprotein AI concentration in the late suckling period was twice that of the adult. On the contrast, fetal apoprotein B was nearly 2.5-fold above adult concentration and was under the form of LDL, the main lipoprotein class in the late fetal period. Apoprotein B concentration decreased progressively as LDL was replaced by an apoprotein E-rich HDL. The latter class constituted an important transitory cholesterol carrier during the shift from the neonatal lipoprotein pattern dominated by LDL to the typical adult pattern in which HDL are predominant. Lack of active cholesterol ester transfer protein is believed to be one of the reasons for low LDL concentration in adult rats. However, in vitro incubation of radioactively-labelled HDL cholesteryl esters with rat plasma demonstrated that the juveniles' lipoprotein depleted plasma induced as little transfer of the label from HDL to lower density lipoproteins as that of the adult. Thus a transient cholesteryl ester transfer activity could not have contributed to the composition of the LDL pool in the fetus and the early suckling rat. It is more likely that LDL are secreted directly by the liver. Each apolipoprotein exhibited a characteristic developmental pattern different from that of adult rats fed hyperlipidic diets. It therefore appears that each apoprotein is controlled independently by a combination of programmed ontogenic development and nutritional factors leading to the progressive establishment of the adult lipoprotein profile.

摘要

新生大鼠开始哺乳后,血浆脂质会急剧增加。大部分变化归因于乳汁中的高脂肪含量。胎儿体内载脂蛋白AI、E和AIV的浓度较低。哺乳期间它们会增加。载脂蛋白E和载脂蛋白AIV未超过成年大鼠的水平,而哺乳后期载脂蛋白AI的浓度是成年大鼠的两倍。相反,胎儿载脂蛋白B的浓度比成年大鼠高出近2.5倍,且以低密度脂蛋白(LDL)的形式存在,LDL是胎儿后期的主要脂蛋白类别。随着LDL被富含载脂蛋白E的高密度脂蛋白(HDL)取代,载脂蛋白B的浓度逐渐降低。在从以LDL为主导的新生儿脂蛋白模式向以HDL为主导的典型成年模式转变过程中,HDL是重要的过渡性胆固醇载体。成年大鼠LDL浓度较低被认为是缺乏活性胆固醇酯转移蛋白的原因之一。然而,用放射性标记的HDL胆固醇酯与大鼠血浆进行体外孵育表明,幼年大鼠脂蛋白缺乏的血浆诱导的标记物从HDL向低密度脂蛋白的转移与成年大鼠一样少。因此,短暂的胆固醇酯转移活性不可能对胎儿和早期哺乳大鼠LDL池的组成有贡献。更有可能的是,LDL是由肝脏直接分泌的。每种载脂蛋白都呈现出与喂食高脂饮食的成年大鼠不同的特征性发育模式。因此,似乎每种载脂蛋白都是由程序性个体发育和营养因素共同独立控制的,从而逐渐形成成年脂蛋白谱。

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