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胰岛素样生长因子II通过p70 S6激酶途径保护成肌细胞免受顺铂诱导的凋亡的作用。

Effect of insulin-like growth factor II on protecting myoblast cells against cisplatin-induced apoptosis through p70 S6 kinase pathway.

作者信息

Wan Xiaolin, Helman Lee J

机构信息

Molecular Oncology Section, Pediatric Oncology Branch, NCI, National Institutes of Health, Bethesda, MD 20892-1928, USA.

出版信息

Neoplasia. 2002 Sep-Oct;4(5):400-8. doi: 10.1038/sj.neo.7900242.

DOI:10.1038/sj.neo.7900242
PMID:12192598
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1564119/
Abstract

Insulin-like growth factor (IGF-II) is overexpressed in a variety of human tumors and has both mitogenic and antiapoptotic activity. Although the mechanisms of IGF-II-induced proliferation have been well studied, the mechanisms underlying its survival signaling have been less well characterized. In this report, we investigated the role of IGF-II on cisplatin-induced apoptosis. We found that IGF-II overexpression was associated with an increase in p70 ribosomal protein S6 kinase (p70 S6K). Cisplatin treatment of C2C12 mouse myoblasts led to cell death associated with an inhibition of p70 S6K activity. Endogenous or exogenous IGF-II addition to C2C12 cells caused protection to cisplatin-induced apoptosis. This protection was associated in both cases with an increase in p70 S6K basal activity as well as resistance to cisplatin-induced decreased activity. Blockade of p70 S6K activation by rapamycin abrogated the IGF-II-mediated protection of cells to cisplatin-induced apoptosis. Furthermore, treatment of IGF-II-overexpressing Rh30 and CTR rhabdomyosarcoma cells with rapamycin restored sensitivity to cisplatin-induced apoptosis. These data together suggest that IGF-II-associated protection to cisplatin-induced apoptosis is mediated through an activation of the p70 S6K pathway. Thus, inhibition of the p70 S6 pathway may enhance chemotherapy-induced apoptosis in the treatment of IGF-II-overexpressing tumors.

摘要

胰岛素样生长因子(IGF-II)在多种人类肿瘤中过表达,具有促有丝分裂和抗凋亡活性。尽管IGF-II诱导增殖的机制已得到充分研究,但其生存信号传导的潜在机制仍不太清楚。在本报告中,我们研究了IGF-II在顺铂诱导的细胞凋亡中的作用。我们发现IGF-II过表达与p70核糖体蛋白S6激酶(p70 S6K)的增加有关。用顺铂处理C2C12小鼠成肌细胞导致细胞死亡,并伴有p70 S6K活性的抑制。向C2C12细胞中添加内源性或外源性IGF-II可保护细胞免受顺铂诱导的凋亡。在这两种情况下,这种保护都与p70 S6K基础活性的增加以及对顺铂诱导的活性降低的抗性有关。雷帕霉素阻断p70 S6K的激活消除了IGF-II介导的细胞对顺铂诱导凋亡的保护作用。此外,用雷帕霉素处理IGF-II过表达的Rh30和CTR横纹肌肉瘤细胞可恢复对顺铂诱导凋亡的敏感性。这些数据共同表明,IGF-II对顺铂诱导凋亡的相关保护作用是通过p70 S6K途径的激活介导的。因此,抑制p70 S6途径可能会增强化疗诱导的凋亡,用于治疗IGF-II过表达的肿瘤。