The RASSF1A tumor suppressor binds and activates proapoptotic MST kinases. The Salvador adaptor protein couples MST kinases to the LATS kinases to form the hippo pathway. Upon activation by RASSF1A, LATS1 phosphorylates the transcriptional regulator YAP, which binds to p73 and activates its proapoptotic effects. However, although serving as an adaptor for MST and LATS, Salvador can also bind RASSF1A. The functional role of the RASSF1A/Salvador interaction is unclear. Although Salvador is a novel tumor suppressor in Drosophila and mice, its role in human systems remains largely unknown. Here we show that Salvador promotes apoptosis in human cells and that Salvador inactivation deregulates the cell cycle and enhances the transformed phenotype. Moreover, we show that although the salvador gene is seldom mutated or epigenetically inactivated in human cancers, it is frequently down-regulated posttranscriptionally. Surprisingly, we also find that although RASSF1A requires the presence of Salvador for full apoptotic activity and to activate p73, this effect does not require a direct interaction of RASSF1A with MST kinases or the activation of the hippo pathway. Thus, we confirm a role for Salvador as a human tumor suppressor and RASSF1A effector and show that Salvador allows RASSF1A to modulate p73 independently of the hippo pathway.
Salvador protein is a tumor suppressor effector of RASSF1A with hippo pathway-independent functions.
Salvador 蛋白是 RASSF1A 的肿瘤抑制效应因子,具有不依赖于 hippo 通路的功能
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作者:Donninger Howard, Allen Nadia, Henson Adrianna, Pogue Jennifer, Williams Andrew, Gordon Laura, Kassler Susannah, Dunwell Thomas, Latif Farida, Clark Geoffrey J
| 期刊: | Journal of Biological Chemistry | 影响因子: | 3.900 |
| 时间: | 2011 | 起止号: | 2011 May 27; 286(21):18483-91 |
| doi: | 10.1074/jbc.M110.214874 | 研究方向: | 肿瘤 |
| 信号通路: | Hippo | ||
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