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对人癌前和恶性结直肠肿瘤细胞系中存在及分泌的组织蛋白酶B和L进行免疫检测。

Immunodetection of cathepsins B and L present in and secreted from human pre-malignant and malignant colorectal tumour cell lines.

作者信息

Maciewicz R A, Wardale R J, Etherington D J, Paraskeva C

机构信息

AFRC Institute of Food Research-Bristol Laboratory, Langford, Bristol, Avon, UK.

出版信息

Int J Cancer. 1989 Mar 15;43(3):478-86. doi: 10.1002/ijc.2910430323.

DOI:10.1002/ijc.2910430323
PMID:2647640
Abstract

Pre-malignant and malignant human colorectal tumour epithelial cell lines both secreted precursor forms of the 2 cysteine proteinases, cathepsins B and L. The amount of proteinases secreted by these cell lines varied according to the cell density. Comparison at similar cell densities showed that the pre-malignant, adenoma-derived cell line (PC/AA) secreted as much, or more, of both cathepsin B and L precursors as did the malignant, carcinoma-derived cell line (PC/JW/FI). However, mature forms of cathepsins B and L were detected in the culture media of only the carcinoma-derived cell line, thus indicating that the invasive potential of a tumour may be related to its ability to process extracellularly the secreted precursor enzyme to a mature and consequently active enzyme, rather than to the amount of proteinase synthesized and/or secreted. Similar results were obtained using 2 other epithelium-derived tumour cell lines, HT/29 (carcinoma) and SP/AN (adenoma). Immunolocation studies showed that cathepsin B was lysosomal while cathepsin L appeared to have a distribution more consistent with a plasma membrane association. Purified human cathepsins B and L (mature form) were capable of solubilizing an isolated basement membrane matrix (bovine anterior lens capsule) in vitro, thus indicating that the secreted mature enzymes and the membrane-associated cathepsin L could potentially degrade basal laminae or sub-endothelial basement membranes in vivo.

摘要

癌前和恶性人类结直肠肿瘤上皮细胞系均分泌半胱氨酸蛋白酶组织蛋白酶B和L的前体形式。这些细胞系分泌的蛋白酶量根据细胞密度而变化。在相似细胞密度下进行比较发现,癌前的、源自腺瘤的细胞系(PC/AA)分泌的组织蛋白酶B和L前体与源自恶性癌的细胞系(PC/JW/FI)一样多,甚至更多。然而,仅在源自癌的细胞系的培养基中检测到组织蛋白酶B和L的成熟形式,因此表明肿瘤的侵袭潜力可能与其将分泌的前体酶在细胞外加工成成熟且因此有活性的酶的能力有关,而非与合成和/或分泌的蛋白酶量有关。使用另外两种源自上皮的肿瘤细胞系HT/29(癌)和SP/AN(腺瘤)也获得了相似结果。免疫定位研究表明,组织蛋白酶B位于溶酶体中,而组织蛋白酶L的分布似乎更符合与质膜相关。纯化的人组织蛋白酶B和L(成熟形式)能够在体外溶解分离的基底膜基质(牛晶状体前囊),因此表明分泌的成熟酶和与膜相关的组织蛋白酶L在体内可能降解基底层或内皮下基底膜。

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