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Angiomotin family proteins are novel activators of the LATS2 kinase tumor suppressor 总被引:1,自引:0,他引:1
Paramasivam M Sarkeshik A Yates JR Fernandes MJ McCollum D 《Molecular biology of the cell》2011,22(19):3725-3733
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Hata S Hirayama J Kajiho H Nakagawa K Hata Y Katada T Furutani-Seiki M Nishina H 《The Journal of biological chemistry》2012,287(26):22089-22098
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Chan SW Lim CJ Chong YF Pobbati AV Huang C Hong W 《The Journal of biological chemistry》2011,286(9):7018-7026
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《Cellular signalling》2014,26(11):2504-2513
The Hippo pathway plays an important role in both physical and pathogenesis processes. As crucial downstream effectors of Hippo pathway, YAP is inhibited by Lats1/2 through phosphorylation. However, upstream signals that regulate the Hippo pathway have been still poorly understood. Here, we found that knockdown of CD44 reduced YAP expression and nuclear localization, but nearly had no effect on its upstream effectors, Mst1 and Lats1. Downregulated CD44 expression also significantly decreased the expression of YAP downstream effectors CTGF, Cyr61 and EDN1 at mRNA level. Our next study showed that knockdown of CD44 inhibited RhoA expression, which was consistent with RhoA knockdown mediated YAP downregulation. Furthermore, we demonstrated that over expression of the constitutively active RhoA (RhoA-V14) could block the YAP expression decrease mediated by CD44 knockdown. Moreover, downregulation of CD44 significantly promoted cell apoptosis and inhibited cell proliferation, cell cycle progression and migration, which were consistent with the effects of RNAi-mediated YAP knockdown in both A549 and HepG2 cells. Overall, data are presented showing that CD44 could act through RhoA signaling to regulate YAP expression and this study also provide new insights into the regulatory mechanisms of the Hippo–YAP pathway. 相似文献
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