SINHCAF/FAM60A and SIN3A specifically repress HIF-2{alpha} expression

The SIN3A–HDAC (histone deacetylase) complex is a master transcriptional repressor, required for development but often deregulated in disease. Here, we report that the recently identified new component of this complex, SINHCAF (SIN3A and HDAC-associated factor)/FAM60A (family of homology 60A), links the SIN3A–HDAC co-repressor complex function to the hypoxia response. We show that SINHCAF specifically represses HIF-2α mRNA and protein expression, via its interaction with the transcription factor SP1 (specificity protein 1) and recruitment of HDAC1 to the HIF-2α promoter. SINHCAF control over HIF-2α results in functional cellular changes in in vitro angiogenesis and viability. Our analysis reveals an unexpected link between SINHCAF and the regulation of the hypoxia response.

http://www.biochemj.org/cgi/content/short/475/12/2073?rss=1

Source: Biochemical Journal - June 29, 2018 Category: Biochemistry Authors: Biddlestone, J., Batie, M., Bandarra, D., Munoz, I., Rocha, S. Tags: Research Articles Source Type: research

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