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氨基酸对分离的大鼠肝细胞中蛋白质降解自噬/溶酶体途径的抑制作用。

Amino acid inhibition of the autophagic/lysosomal pathway of protein degradation in isolated rat hepatocytes.

作者信息

Seglen P O, Gordon P B, Poli A

出版信息

Biochim Biophys Acta. 1980 Jun 5;630(1):103-18. doi: 10.1016/0304-4165(80)90141-5.

DOI:10.1016/0304-4165(80)90141-5
PMID:7388042
Abstract

Protein degradation in isolated rat hepatocytes, as measured by the release of [14C]valine from pre-labelled protein, is partly inhibited by a physiologically balanced mixture of amino acids. The inhibition is largely due to the seven amino acids leucine, phenylalanine, tyrosine, tryptophan, histidine, asparagine and glutamine. When the amino acids are tested individually at different concentrations, asparagine and glutamine are the strongest inhibitors. However, when various combinations are tested, a mixture of the first five amino acids as well as a combination of leucine and asparagine inhibit protein degradation particularly strongly. The inhibition brought about by asparagine plus leucine is not additive to the inhibition by propylamine, a lysosomotropic inhibitor; thus indicating that the amino acids act exclusively upon the lysosomal pathway of protein degradation. Following a lag of about 15 min the effect of asparagine plus leucine is maximal and equal to the effect of propylamine, suggesting that their inhibition of the lysosomal pathway is complete as well as specific. Degradation of endocytosed 125I-labelled asialofetuin is not affected by asparagine plus leucine, indicating that the amino acids do not affect lysosomes directly, but rather inhibit autophagy at a step prior to the fusion of autophagic vacuoles with lysosomes. The aminotransferase inhibitor, aminooxyacetate, does not prevent the inhibitory effect of any of the amino acids, i.e. amino acid metabolites are apparently not involved.

摘要

通过预标记蛋白质中[14C]缬氨酸的释放来测定,分离的大鼠肝细胞中的蛋白质降解受到生理平衡的氨基酸混合物的部分抑制。这种抑制主要归因于七种氨基酸,即亮氨酸、苯丙氨酸、酪氨酸、色氨酸、组氨酸、天冬酰胺和谷氨酰胺。当分别以不同浓度测试这些氨基酸时,天冬酰胺和谷氨酰胺是最强的抑制剂。然而,当测试各种组合时,前五种氨基酸的混合物以及亮氨酸和天冬酰胺的组合对蛋白质降解的抑制作用特别强。天冬酰胺加亮氨酸所产生的抑制作用与溶酶体促透剂丙胺的抑制作用并非相加关系;因此表明这些氨基酸仅作用于蛋白质降解的溶酶体途径。经过约15分钟的延迟后,天冬酰胺加亮氨酸的作用达到最大值,且与丙胺的作用相同,这表明它们对溶酶体途径的抑制是完全且特异的。内吞的125I标记去唾液酸胎球蛋白的降解不受天冬酰胺加亮氨酸的影响,这表明这些氨基酸并非直接影响溶酶体,而是在自噬泡与溶酶体融合之前的某个步骤抑制自噬作用。转氨酶抑制剂氨基氧乙酸并不能阻止任何一种氨基酸的抑制作用,即氨基酸代谢产物显然未参与其中。

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