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TSPYL2 is an essential component of the REST/NRSF transcriptional complex for TGF? signaling activation.


ABSTRACT: REST/NRSF is a transcriptional repressor of neuronal genes that has been implicated in development and cancer. In epithelial tissues, REST acts as a tumor suppressor and in breast cancer, loss of REST is associated with disease recurrence and poor prognosis. Here, we identify TSPYL2 (also known as CDA1 and DENTT) as a novel component of the REST protein complex. We show that REST and TSPYL2 are regulators of TGF? signaling and that cell-cycle arrest induced by TGF? requires both REST and TSPYL2. Importantly, knockdown of REST or TSPYL2 resulted in transformation of human mammary epithelial cells. Mechanistically, we demonstrate that the TSPYL2/REST complex promotes TGF? signaling by repressing the expression of genes, such as the proto-oncogene neurotrophic tyrosine kinase receptor C (TrkC). These data provide insight into the role of REST as a tumor suppressor in epithelial tissues through the regulation of the TGF? pathway.

SUBMITTER: Epping MT 

PROVIDER: S-EPMC4495358 | biostudies-literature | 2015 Aug

REPOSITORIES: biostudies-literature

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TSPYL2 is an essential component of the REST/NRSF transcriptional complex for TGFβ signaling activation.

Epping M T MT   Lunardi A A   Nachmani D D   Castillo-Martin M M   Thin T H TH   Cordon-Cardo C C   Pandolfi P P PP  

Cell death and differentiation 20150123 8


REST/NRSF is a transcriptional repressor of neuronal genes that has been implicated in development and cancer. In epithelial tissues, REST acts as a tumor suppressor and in breast cancer, loss of REST is associated with disease recurrence and poor prognosis. Here, we identify TSPYL2 (also known as CDA1 and DENTT) as a novel component of the REST protein complex. We show that REST and TSPYL2 are regulators of TGFβ signaling and that cell-cycle arrest induced by TGFβ requires both REST and TSPYL2.  ...[more]

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