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人表皮中的蛋白酶体核糖核酸酶活性。

Proteasomal RNase activity in human epidermis.

作者信息

Horikoshi T, Page J, Lei G, Brysk H, Arany I, Tyring S K, Brysk M M

机构信息

Department of Dermatology, University of Texas Medical Branch, Galveston 77555, USA.

出版信息

In Vivo. 1998 Mar-Apr;12(2):155-8.

PMID:9627796
Abstract

The proteasome is a cytoplasmic high-molecular-weight structure composed of several smaller protein and RNA subunits. It has been associated with non-lysosomal pathways of intracellular degradation, expressing multicatalytic proteinase activities and specific RNase activity. By standard methods, we have isolated andpartially purified proteasomes from human epidermis. We obtained the expected multiple 24-32 kDa subunits by SDS-PAGE, and evidence of RNA. Proteasomes degraded casein, as well as chromogens for t-PA and trypsin but not for chymotrypsin, these proteolytic activities overlap, but do not coincide with those observed in other organs. We found that human epidermal 28 S and 18 S rRNAs were degraded, but yeast RNA was not. By means of zymography, we demonstrated, for the first time, that RNase activity persists after dissociation of the proteasome on the gel and that it co-localizes to the same range of molecular weight subunits as the proteinase activity.

摘要

蛋白酶体是一种细胞质中的高分子量结构,由几个较小的蛋白质和RNA亚基组成。它与细胞内降解的非溶酶体途径相关,具有多种催化蛋白酶活性和特定的核糖核酸酶活性。通过标准方法,我们从人表皮中分离并部分纯化了蛋白酶体。通过SDS-PAGE,我们获得了预期的多个24 - 32 kDa亚基以及RNA的证据。蛋白酶体可降解酪蛋白,以及组织型纤溶酶原激活物(t-PA)和胰蛋白酶的色原底物,但不能降解胰凝乳蛋白酶的色原底物,这些蛋白水解活性有重叠,但与在其他器官中观察到的活性不一致。我们发现人表皮的28 S和18 S rRNA被降解,但酵母RNA未被降解。通过酶谱分析,我们首次证明,蛋白酶体在凝胶上解离后,核糖核酸酶活性仍然存在,并且它与蛋白酶活性共定位于相同分子量范围的亚基。

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