The pleiotropy associated with de novo variants in CHD4, CNOT3, and SETD5 extends to moyamoya angiopathy.
Amélie C PinardStéphanie GueyDongchuan GuoAlana C CecchiNatasha KharasStephanie WallaceEllen S RegaladoEllen M HostetlerAnjail Z SharriefFrançoise BergamettiManoëlle KossorotoffNathanaelle Ibos-AugéMarkus KraemerMichael J BamshadDeborah A NickersonEdward R SmithElisabeth Tournier-LasserveDianna M MilewiczPublished in: Genetics in medicine : official journal of the American College of Medical Genetics (2019)
These genes encode proteins involved in chromatin remodeling, and taken together with previously reported genes leading to MMA-like cerebrovascular occlusive disease (YY1AP1, SMARCAL1), implicate disrupted chromatin remodeling as a molecular pathway predisposing to early onset, large artery occlusive cerebrovascular disease. Furthermore, these data expand the spectrum of phenotypic pleiotropy due to alterations of CHD4, CNOT3, and SETD5 beyond DD to later onset disease in the cerebrovascular arteries and emphasize the need to assess clinical complications into adulthood for genes associated with DD.