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Publication : ZNF410 represses fetal globin by singular control of CHD4.

First Author  Vinjamur DS Year  2021
Journal  Nat Genet Volume  53
Issue  5 Pages  719-728
PubMed ID  33859416 Mgi Jnum  J:308797
Mgi Id  MGI:6742249 Doi  10.1038/s41588-021-00843-w
Citation  Vinjamur DS, et al. (2021) ZNF410 represses fetal globin by singular control of CHD4. Nat Genet 53(5):719-728
abstractText  Known fetal hemoglobin (HbF) silencers have potential on-target liabilities for rational beta-hemoglobinopathy therapeutic inhibition. Here, through transcription factor (TF) CRISPR screening, we identify zinc-finger protein (ZNF) 410 as an HbF repressor. ZNF410 does not bind directly to the genes encoding gamma-globins, but rather its chromatin occupancy is concentrated solely at CHD4, encoding the NuRD nucleosome remodeler, which is itself required for HbF repression. CHD4 has two ZNF410-bound regulatory elements with 27 combined ZNF410 binding motifs constituting unparalleled genomic clusters. These elements completely account for the effects of ZNF410 on fetal globin repression. Knockout of ZNF410 or its mouse homolog Zfp410 reduces CHD4 levels by 60%, enough to substantially de-repress HbF while eluding cellular or organismal toxicity. These studies suggest a potential target for HbF induction for beta-hemoglobin disorders with a wide therapeutic index. More broadly, ZNF410 represents a special class of gene regulator, a conserved TF with singular devotion to regulation of a chromatin subcomplex.
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