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人结肠癌中质膜相关神经节苷脂唾液酸酶(Neu3)的上调及其在抑制细胞凋亡中的作用。

Up-regulation of plasma membrane-associated ganglioside sialidase (Neu3) in human colon cancer and its involvement in apoptosis suppression.

作者信息

Kakugawa Yoichiro, Wada Tadashi, Yamaguchi Kazunori, Yamanami Hideaki, Ouchi Kiyoaki, Sato Ikuro, Miyagi Taeko

机构信息

Division of Biochemistry, Research Institute, Department of Surgery, Miyagi Prefectural Cancer Center, Natori, Miyagi 981-1293, Japan.

出版信息

Proc Natl Acad Sci U S A. 2002 Aug 6;99(16):10718-23. doi: 10.1073/pnas.152597199. Epub 2002 Jul 29.

Abstract

Human plasma membrane-associated sialidase (Neu3) is unique in specifically hydrolyzing gangliosides, thought to participate in cell differentiation and transmembrane signaling, thereby playing crucial roles in the regulation of cell surface functions. We have discovered levels of mRNA for this sialidase to be increased in restricted cases of human colon cancer by 3- to 100-fold compared with adjacent nontumor mucosa (n = 32), associated with significant elevation in sialidase activity in tumors (n = 50). In situ hybridization showed the sialidase expression in epithelial elements of adenocarcinomas. In cultured human colon cancer cells, the sialidase level was down-regulated in the process of differentiation and apoptosis induced by sodium butyrate, whereas lysosomal sialidase (Neu1) was up-regulated. Transfection of the sialidase gene into colon cancer cells inhibited apoptosis and was accompanied by increased Bcl-2 and decreased caspase expression. Colon cancer exhibited a marked accumulation of lactosylceramide, a possible sialidase product, and addition of the glycolipid to the culture reduced apoptotic cells during sodium butyrate treatment. These results indicate that high expression of the sialidase in cancer cells leads to protection against programmed cell death, probably modulation of gangliosides. This finding provides a possible sialidase target for diagnosis and therapy of colon cancer.

摘要

人血浆膜相关唾液酸酶(Neu3)在特异性水解神经节苷脂方面独具特色,据认为其参与细胞分化和跨膜信号传导,从而在细胞表面功能调节中发挥关键作用。我们发现,在部分人类结肠癌病例中,该唾液酸酶的mRNA水平相较于相邻的非肿瘤黏膜升高了3至100倍(n = 32),且肿瘤中的唾液酸酶活性显著升高(n = 50)。原位杂交显示腺癌上皮细胞中存在唾液酸酶表达。在培养的人结肠癌细胞中,丁酸钠诱导的分化和凋亡过程中唾液酸酶水平下调,而溶酶体唾液酸酶(Neu1)上调。将唾液酸酶基因转染至结肠癌细胞可抑制凋亡,并伴随Bcl-2表达增加和半胱天冬酶表达减少。结肠癌中乳糖神经酰胺(一种可能的唾液酸酶产物)明显蓄积,在丁酸钠处理期间向培养物中添加该糖脂可减少凋亡细胞。这些结果表明,癌细胞中唾液酸酶的高表达可防止程序性细胞死亡,可能是通过调节神经节苷脂实现的。这一发现为结肠癌的诊断和治疗提供了一个可能的唾液酸酶靶点。

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