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HM3人结肠癌细胞中两种不同类型粘蛋白的生物合成。

Biosynthesis of two distinct types of mucin in HM3 human colon cancer cells.

作者信息

Ohara S, Byrd J C, Gum J R, Kim Y S

机构信息

Gastrointestinal Research Laboratory, VA Medical Center, San Francisco, CA.

出版信息

Biochem J. 1994 Feb 1;297 ( Pt 3)(Pt 3):509-16. doi: 10.1042/bj2970509.

Abstract

Mucins, high-M(r) glycoproteins with a large amount of O-glycosidically linked carbohydrate, protect the colonic epithelial surface and are altered in ulcerative colitis and colon cancer. At least two mucin genes, MUC2 and MUC3, are expressed at high levels in the human intestine. As an experimental model for studying the biosynthesis of human intestinal mucins, we used HM3 colon cancer cells. When mature mucins labelled with [3H]glucosamine or [3H]threonine were analysed by gel filtration, it was found that secreted mucins (M(r) > 10(8) were larger than soluble cellular mucins (M(r) approx. 5 x 10(6)). Only secreted mucin was sensitive to reduction. Both MUC2 and MUC3 proteins, identified by labelling with [3H]threonine or [35S]cysteine and immunoprecipitation with antibodies to synthetic mucin peptides, were already of large size (M(r) > 180,000) by the earliest labelling time (5 min). The MUC3 precursor was completely degraded by trypsin, but the MUC2 precursor had a trypsin-resistant fragment of M(r) approx. 240,000 containing threonine and cysteine. The trypsin-resistant MUC2 fragment contained N-linked carbohydrate, as indicated by a decrease in size as a result of peptidyl N-glycosidase digestion or tunicamycin treatment of HM3 cells. These results show that HM3 colon cancer cells produce at least two distinct human intestinal mucins. They also indicate that the mechanisms of biosynthesis of intestinal mucins differ from those of other mucin-like glycoproteins that have been studied.

摘要

黏蛋白是一类高分子量糖蛋白,带有大量O-糖苷键连接的碳水化合物,可保护结肠上皮表面,且在溃疡性结肠炎和结肠癌中会发生改变。至少有两个黏蛋白基因,即MUC2和MUC3,在人类肠道中高水平表达。作为研究人类肠道黏蛋白生物合成的实验模型,我们使用了HM3结肠癌细胞。当用[3H]葡萄糖胺或[3H]苏氨酸标记的成熟黏蛋白通过凝胶过滤进行分析时,发现分泌型黏蛋白(M(r)>10(8))比可溶性细胞黏蛋白(M(r)约为5×10(6))更大。只有分泌型黏蛋白对还原敏感。通过用[3H]苏氨酸或[35S]半胱氨酸标记以及用针对合成黏蛋白肽的抗体进行免疫沉淀鉴定的MUC2和MUC3蛋白,在最早的标记时间(5分钟)时就已经是大尺寸(M(r)>180,000)。MUC3前体被胰蛋白酶完全降解,但MUC2前体有一个M(r)约为240,000的抗胰蛋白酶片段,含有苏氨酸和半胱氨酸。抗胰蛋白酶的MUC2片段含有N-连接的碳水化合物,这可通过肽基N-糖苷酶消化或衣霉素处理HM3细胞后尺寸减小来表明。这些结果表明HM3结肠癌细胞产生至少两种不同的人类肠道黏蛋白。它们还表明肠道黏蛋白的生物合成机制与已研究的其他黏蛋白样糖蛋白不同。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/441c/1137863/b898c351bedc/biochemj00094-0091-a.jpg

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