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酸性胞质蛋白优先被导入大鼠肝脏溶酶体。

Acidic cytosolic proteins are preferentially imported into rat liver lysosomes.

作者信息

Aniento F, Roche E, Knecht E

机构信息

Departamento de Bioquímica y Biología Molecular, Universidad de Valencia, Burjassot, Spain.

出版信息

Electrophoresis. 1997 Dec;18(14):2638-44. doi: 10.1002/elps.1150181420.

Abstract

Previous studies have reported that lysosomes isolated from human diploid fibroblasts and from rat liver can selectively import and degrade specific proteins. We have now reinvestigated this selectivity using an in vitro assay with rat liver lysosomes and an extract of cytosolic proteins prepared from cultured cells labeled to equilibriums with [35S-]methionine. Analysis by two-dimensional gel electrophoresis and autoradiography of the cytosolic proteins bound to the lysosomal membrane and imported into the lysosomes shows that when all cytosolic proteins are simultaneously present in the in vitro assay the lysosomal uptake also occurs in a specific manner. These findings suggest that isolated lysosomes are able to discriminate among different proteins, selecting those with certain features for lysosomal degradation. Additional characterization of the cytosolic proteins which are selectively imported by lysosomes shows that a common structural feature of most, but not all, of these proteins is an acidic isoelectric point (pI <6.0) and a small or intermediate size. This observation is in agreement with earlier studies which established a relationship between the in vivo half-lives of cytosolic proteins in rat liver and their net charge, with acidic proteins, in general, being degraded more rapidly than neutral or basic proteins. The reasons for this preference are still uncertain, although a possible explanation is presented.

摘要

以往的研究报道,从人二倍体成纤维细胞和大鼠肝脏中分离出的溶酶体能够选择性地摄取和降解特定蛋白质。我们现在使用大鼠肝脏溶酶体和从用[35S-]甲硫氨酸标记至平衡的培养细胞制备的胞质蛋白提取物进行体外测定,重新研究了这种选择性。通过二维凝胶电泳和放射自显影分析与溶酶体膜结合并导入溶酶体的胞质蛋白,结果表明,当所有胞质蛋白同时存在于体外测定中时,溶酶体摄取也以特定方式发生。这些发现表明,分离的溶酶体能够区分不同的蛋白质,选择具有某些特征的蛋白质进行溶酶体降解。对被溶酶体选择性摄取的胞质蛋白的进一步表征表明,这些蛋白中大多数(但不是全部)的一个共同结构特征是酸性等电点(pI <6.0)和小或中等大小。这一观察结果与早期的研究一致,早期研究确立了大鼠肝脏中胞质蛋白的体内半衰期与其净电荷之间的关系,一般来说,酸性蛋白比中性或碱性蛋白降解得更快。尽管提出了一种可能的解释,但这种偏好的原因仍然不确定。

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