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首页> 外文期刊>Molecular and Cellular Biochemistry >The β-subunit of ATP synthase is involved in cellular uptake and resecretion of apoA-I but does not control apoA-I-induced lipid efflux in adipocytes
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The β-subunit of ATP synthase is involved in cellular uptake and resecretion of apoA-I but does not control apoA-I-induced lipid efflux in adipocytes

机译:ATP合酶的β亚基参与apoA-I的细胞摄取和分泌,但不控制apoA-I诱导的脂肪细胞脂质外排

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Cellular uptake and resecretion of apoA-I (apoA-I recycling) could be an important factor in determining the circulating plasma levels of apoA-I and/or HDL. Using a novel method to study protein recycling, we have recently demonstrated recycling of apoA-I by adipocytes and suggested that this is a receptor mediated process independent of ABCA1 function. In the present study, it is shown that apoA-I recycling by adipocytes can be blocked by a monoclonal antibody against the β-subunit of ATP synthase, a protein that had been previously identified as an apoA-I receptor. Investigation of the cellular recycling of two other proteins, an apolipoprotein and a small globular protein, showed that recycling of apoA-I is a selective process. The present study also shows that blocking apoA-I recycling has no effect on the rate of apoA-I-induced cholesterol or phospholipid efflux. It is concluded that cellular recycling of apoA-I is a selective process that involves the ectopically expressed β-subunit of ATP synthase. The physiological function of apoA-I recycling remains to be elucidated. However, this study shows that the process of apoA-I uptake and resecretion is not required for apoA-I lipidation.
机译:细胞对apoA-I的摄取和分泌(apoA-I回收)可能是确定apoA-I和/或HDL循环血浆水平的重要因素。使用一种新颖的方法来研究蛋白质的回收利用,我们最近证明了脂肪细胞对apoA-I的回收利用,并表明这是一种独立于ABCA1功能的受体介导的过程。在本研究中,研究表明,脂肪细胞对apoA-I的循环利用可以被针对ATP合酶的β-亚基的单克隆抗体所阻断,后者是一种先前被确定为apoA-I受体的蛋白质。对另外两种蛋白质(载脂蛋白和小球状蛋白)的细胞再循环研究表明,apoA-I的再循环是一个选择性过程。本研究还表明,阻断apoA-I的再循环对apoA-I诱导的胆固醇或磷脂外排率没有影响。结论是,apoA-I的细胞再循环是一个选择性过程,涉及异位表达的ATP合酶的β-亚基。 apoA-I回收的生理功能仍有待阐明。但是,这项研究表明apoA-I脂化不需要apoA-I的吸收和分泌过程。

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