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细胞核组织蛋白酶L的定位及其与结直肠癌疾病进展和不良预后的关系。

Localization of nuclear cathepsin L and its association with disease progression and poor outcome in colorectal cancer.

作者信息

Sullivan Shane, Tosetto Miriam, Kevans David, Coss Alan, Wang Laimun, O'Donoghue Diarmuid, Hyland John, Sheahan Kieran, Mulcahy Hugh, O'Sullivan Jacintha

机构信息

Centre for Colorectal Disease, St. Vincent's University Hospital, Dublin, Dublin, Ireland.

出版信息

Int J Cancer. 2009 Jul 1;125(1):54-61. doi: 10.1002/ijc.24275.

Abstract

Previous in vitro studies have identified a nuclear isoform of Cathepsin L. The aim of this study was to examine if nuclear Cathepsin L exists in vivo and examine its association with clinical, pathological and patient outcome data. Cellular localization (nuclear and cytoplasmic) and expression levels v of Cathespin L in 186 colorectal cancer cases using immunohistochemistry. The molecular weight and activity of nuclear and cytoplasmic Cathepsin L in vivo and in vitro were assessed by Western blotting and ELISA, respectively. Epithelial nuclear staining percentage (p = 0.04) and intensity (p = 0.006) increased with advancing tumor stage, whereas stromal cytoplasmic staining decreased (p = 0.02). Using multivariate statistical analysis, survival was inversely associated with staining intensity in the epithelial cytoplasm (p = 0.01) and stromal nuclei (p = 0.007). In different colorectal cell lines and in vivo tumors, pro- and active Cathepsin L isoforms were present in both the cytoplasm and nuclear samples, with pro-Cathepsin L at 50 kDa and active Cathepsin L at 25 kDa. Purified nuclear and cytoplasmic fractions from cell lines and tumors showed active Cathepsin L activity. The identification of nuclear Cathepsin L may play an important prognostic role in colorectal disease progression and patient outcome. Moreover, these findings suggest that altering active nuclear Cathepsin L may significantly influence disease progression.

摘要

先前的体外研究已鉴定出组织蛋白酶L的一种核异构体。本研究的目的是检测核组织蛋白酶L在体内是否存在,并研究其与临床、病理及患者预后数据的关联。采用免疫组织化学方法检测186例结直肠癌病例中组织蛋白酶L的细胞定位(核和细胞质)及表达水平。分别通过蛋白质印迹法和酶联免疫吸附测定法评估体内和体外核及细胞质组织蛋白酶L的分子量和活性。上皮细胞核染色百分比(p = 0.04)和强度(p = 0.006)随肿瘤分期进展而增加,而基质细胞质染色减少(p = 0.02)。使用多变量统计分析,生存率与上皮细胞质(p = 0.01)和基质细胞核(p = 0.007)中的染色强度呈负相关。在不同的结直肠癌细胞系和体内肿瘤中,细胞质和核样本中均存在组织蛋白酶L的前体和活性异构体,前体组织蛋白酶L为50 kDa,活性组织蛋白酶L为25 kDa。从细胞系和肿瘤中纯化的核及细胞质组分显示出活性组织蛋白酶L活性。核组织蛋白酶L的鉴定可能在结直肠癌疾病进展和患者预后中发挥重要的预后作用。此外,这些发现表明改变活性核组织蛋白酶L可能会显著影响疾病进展。

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