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组织蛋白酶B及其在癌症进展中的作用。

Cathepsin B and its role(s) in cancer progression.

作者信息

Podgorski Izabela, Sloane Bonnie F

机构信息

Department of Pharmacology, Wayne State University School of Medicine, Detroit, MI 48201, USA.

出版信息

Biochem Soc Symp. 2003(70):263-76. doi: 10.1042/bss0700263.

Abstract

Experimental and clinical evidence has linked cathepsin B with tumour invasion and metastasis. Cathepsin B expression is increased in many human cancers at the mRNA, protein and activity levels. In addition, cathepsin B is frequently overexpressed in premalignant lesions, an observation that associates this protease with local invasive stages of cancer. Increased expression of cathepsin B in primary cancers, and especially in preneoplastic lesions, suggests that this enzyme might have pro-apoptotic features. Expression of cathepsin B is regulated at many different levels, from gene amplification, use of alternative promoters, increased transcription and alternative splicing, to increased stability and translatability of transcripts. During the transition to malignancy, a change in the localization of cathepsin B occurs, as demonstrated by the presence of cathepsin B-containing vesicles at the cell periphery and at the basal pole of polarized cells. Due to increased expression of cathepsin B and changes in intracellular trafficking, increased secretion of procathepsin B from tumours is observed. Active cathepsin B is also secreted from tumours, a mechanism likely to be facilitated by lysosomal exocytosis or extracellular processing by surface activators. Cathepsin B is localized to caveolae on the tumour surface, where binding to the annexin II heterotetramer occurs. Activation of cathepsin B on the cell surface leads to the regulation of downstream proteolytic cascade(s).

摘要

实验和临床证据表明组织蛋白酶B与肿瘤侵袭和转移有关。在许多人类癌症中,组织蛋白酶B在mRNA、蛋白质和活性水平上的表达均增加。此外,组织蛋白酶B在癌前病变中经常过度表达,这一观察结果将这种蛋白酶与癌症的局部侵袭阶段联系起来。组织蛋白酶B在原发性癌症中,尤其是在癌前病变中的表达增加,表明这种酶可能具有促凋亡特性。组织蛋白酶B的表达在许多不同水平上受到调控,从基因扩增、使用替代启动子、转录增加和可变剪接,到转录本稳定性和可翻译性增加。在向恶性肿瘤转变过程中,组织蛋白酶B的定位发生变化,如在细胞周边和极化细胞的基底极存在含组织蛋白酶B的囊泡所示。由于组织蛋白酶B表达增加和细胞内运输变化,观察到肿瘤中组织蛋白酶原B的分泌增加。活性组织蛋白酶B也从肿瘤中分泌,这种机制可能通过溶酶体胞吐作用或表面激活剂的细胞外加工而得到促进。组织蛋白酶B定位于肿瘤表面的小窝,在那里与膜联蛋白II异源四聚体结合。细胞表面组织蛋白酶B的激活导致下游蛋白水解级联反应的调控。

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