BRD4 interacts with NIPBL and BRD4 is mutated in a Cornelia de Lange-like syndrome.
Gabrielle OlleyMorad AnsariHemant BenganiGraeme R GrimesJames RhodesAlex von KriegsheimAna BlatnikFiona J StewartEmma WakelingNicola CarrollAlison RossSoo-Mi Parknull nullWendy A BickmoreMadapura M PradeepaDavid R FitzPatrickPublished in: Nature genetics (2018)
We found that the clinical phenotype associated with BRD4 haploinsufficiency overlapped with that of Cornelia de Lange syndrome (CdLS), which is most often caused by mutation of NIPBL. More typical CdLS was observed with a de novo BRD4 missense variant, which retained the ability to coimmunoprecipitate with NIPBL, but bound poorly to acetylated histones. BRD4 and NIPBL displayed correlated binding at super-enhancers and appeared to co-regulate developmental gene expression.