Disruption of PHF21A causes syndromic intellectual disability with craniofacial anomalies, epilepsy, hypotonia, and neurobehavioral problems including autism.
Hyung-Goo KimJill A RosenfeldDaryl A ScottGerard BénédicteJonathan D LabonneJason BrownMarianne McGuireSonal MahidaSakkubai NaiduJacqueline GutierrezGaetan LescaVincent des PortesAnge-Line BruelArthur SorlinFan XiaYline CapriEric MullerDianalee McKnightErin TortiFranz RüschendorfOliver HummelZeyaul IslamPrasanna R KolatkarLawrence C LaymanDuchwan RyuIl-Keun KongSuneeta Madan-KhetarpalCheol-Hee KimPublished in: Molecular autism (2019)
Deleterious nonsense, frameshift, and missense mutations disrupting the AT Hook domain and/or an intrinsically disordered region in PHF21A were found to be associated with autism spectrum disorder, epilepsy, hypotonia, neurobehavioral problems, tapering fingers, clinodactyly, and syndactyly, in addition to intellectual disability and craniofacial anomalies. This suggests that PHF21A is involved in autism spectrum disorder and intellectual disability, and its haploinsufficiency causes a diverse neurological phenotype.