Finally, Figure 8 summarizes our results and proposes a potential mechanism of find more the proproliferative and proinvasive functions of YAP in ccRCC by its interaction with the endothelin axis and the tumor microenvironment. Our data presented here suggest widespread deregulation of the Hippo signaling pathway in human ccRCC. In a considerable subset of cases, this was found to be due to down-regulation of the upstream regulator SAV1 and consecutive nuclear accumulation of YAP. In this regard, our data are in line with a recent report by Matsuura and colleagues, who describe down-regulation of SAV1
in high-grade ccRCC [19]. Of note, copy number loss on chromosome 14q22, i.e., in the region of the SAV1 gene, have been previously described in high-grade ccRCC by different groups [19], [20] and [21]. In addition, truncating mutations of this upstream member of the Hippo network are present in a subset selleck chemicals of VHL-wt ccRCCs [22] and [23]. However, our data presented here also hint at the existence of other alternative mechanisms of pathway perturbation in human ccRCC, since in a considerable subset of cases in which marked, albeit not exclusively nuclear staining for YAP was observed this was not accompanied by loss of SAV1 expression. Moreover, our data suggest an important role of Hippo signaling in mediating proliferation as well as migration and invasion, both
in vitro and in vivo, with obvious impact on the metastatic potential of ccRCC. In line with our observations, conditional knockout of NF2, an upstream activator of the Cobimetinib molecular weight growth inhibitory Hippo pathway, in the proximal tubular epithelium of Villin-Cre;Nf2(lox/lox)
mice leads to intratubular neoplasia and invasive carcinoma that resembles human RCC in a mouse model of RCC [24]. Recent reports also linked the renal cilia-associated proteins NPHP4 and NPHP9 to Hippo signaling in both oncogenically transformed and normal kidney epithelial cells. These proteins were found to prevent Lats-dependent phosphorylation of YAP, thus controlling YAP activation and mediating cell proliferation [25] and [26]. Of note, Lamar et al. recently described enhanced metastatic potential of breast cancer as well as melanoma cells with increased YAP/TEAD activity; they concluded that YAP can promote metastasis through its TEAD-interaction domain [27]. To the best of our knowledge, our data presented here for the first time hint at a possible link between Hippo signaling and increased invasiveness and metastatic potential in ccRCC. As a next step, we thought to further dissect the underlying mechanism by which YAP exerts its proproliferative and potentially proinvasive properties in ccRCC on a molecular level and to identify downstream effectors of Hippo signaling in this entity, since this might have important implications in exploiting this pathway as potential therapeutic target in future work.
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