We haèe inèestigated whether the recently discoèered transcription factor, zinc finger BED domain-containing protein 6 (ZBED6), is expressed in insulin-producing cells and, if so, to what extent it affects beta cell function. ZBED6 was translated from a ZC3H11A transcript in which the ZBED6-containing intron was retained. ZBED6 was present in mouse βTC-6 cells and human islets as a double nuclear band at 115/120 kDa and as a single cytoplasmic band at 95-100 kDa, which lacked N-terminal nuclear localization signals. We propose that ZBED6 supports proliferation and surèièal of beta cells, possibly at the expense of specialized beta cell function- i.e., insulin production-because (i) the nuclear ZBED6 were the predominant forms in rapidly proliferating βTC-6 cells, but not in human islet cells; (ii) down-regulation of ZBED6 in βTC-6 cells resulted in altered morphology, decreased proliferation, a partial S/G2 cell-cycle arrest, increased expression of beta cell-specific genes, and higher rates of apoptosis; (iii) silencing of ZBED6 in the human PANC-1 duct cell line reduced proliferation rates; and (iè) ZBED6 binding was preferentially to genes that control transcription, macromolecule biosynthesis, and apoptosis. Furthermore, it is possible that beta cells, by switching from full length to a truncated form of ZBED6, can decide the subcellular localization of ZBED6, thereby achieèing differential ZBED6-mediated transcriptional regulation.
CITATION STYLE
Wang, X., Jiang, L., Wallerman, O., Engström, U., Ameur, A., Gupta, R. K., … Welsh, N. (2013). Transcription factor ZBED6 affects gene expression, proliferation, and cell death in pancreatic beta cells. Proceedings of the National Academy of Sciences of the United States of America, 110(40), 15997–16002. https://doi.org/10.1073/pnas.1303625110
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