2016
DOI: 10.1016/j.ajhg.2016.07.019
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Mutations in MBOAT7 , Encoding Lysophosphatidylinositol Acyltransferase I, Lead to Intellectual Disability Accompanied by Epilepsy and Autistic Features

Abstract: The risk of epilepsy among individuals with intellectual disability (ID) is approximately ten times that of the general population. From a cohort of >5,000 families affected by neurodevelopmental disorders, we identified six consanguineous families harboring homozygous inactivating variants in MBOAT7, encoding lysophosphatidylinositol acyltransferase (LPIAT1). Subjects presented with ID frequently accompanied by epilepsy and autistic features. LPIAT1 is a membrane-bound phospholipid-remodeling enzyme that tran… Show more

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Cited by 76 publications
(87 citation statements)
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“…Ataxic gait which could be accompanied by abnormal cerebellar tests was a universal finding in our patients. However, incoordination was not reported in the case series of Johansen et al Our patients were normocephalic documented in seven of 12 cases, similar to the patients reported by Johansen et al Similar facial features, strabismus and hypopigmented macules were additional clinical findings seen our patients which were not documented in the prior series …”
Section: Discussionsupporting
confidence: 87%
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“…Ataxic gait which could be accompanied by abnormal cerebellar tests was a universal finding in our patients. However, incoordination was not reported in the case series of Johansen et al Our patients were normocephalic documented in seven of 12 cases, similar to the patients reported by Johansen et al Similar facial features, strabismus and hypopigmented macules were additional clinical findings seen our patients which were not documented in the prior series …”
Section: Discussionsupporting
confidence: 87%
“…We present clinical and neuroimaging findings of 12 patients with MBOAT7 gene defect, which is the second series reported in literature. Johansen et al reported 16 patients with MBOAT7 gene defect from six families . In our series 12 patients come from seven families and parents are relatives in all patients compatible with autosomal recessive inheritance.…”
Section: Discussionmentioning
confidence: 71%
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“…Unless indicated, these variants were absent in 194 unrelated Pakistani exomes with non-cognitive Mendelian phenotypes and in ~ 1000 unrelated individuals in the GME Variome Project. References per known gene: ALG3 (Riess et al 2013); ASPM (Kousar et al 2010); BCKDK (Novarino et al 2012); CRADD (Di Donato et al 2016; Harel et al 2017); CWF19L1 (Burns et al 2014; Nguyen et al 2016; Evers et al 2016); CYB5R3 (Ewenczyk et al 2008); GAN (Kuhlenbäumer et al 2002; Tazir et al 2009); LRP2 (Vasli et al 2016); MBOAT7 (Johansen et al 2016); MLYCD (Salomons et al 2007); PNKP (Shen et al 2010); SPTBN2 (Lise et al 2012); TUSC3 (Garshasbi et al 2008, 2011; Khan et al 2011; Loddo et al 2013; Al-Amri et al 2016); WDR62 (Wang et al 2017). …”
Section: Figmentioning
confidence: 99%
“…Mutations responsible for ID were identified in three of the seven families, and several other candidates were also revealed. In addition, the genes DENND5A (DENN domain-containing protein 5A) and MBOAT7 (Lysophospholipid acyltransferase 7) were newly implicated in a distinctive subtype of epileptic encephalopathy and ID in studies of consanguineous families (Han et al 2016;Johansen et al 2016).…”
Section: Introductionmentioning
confidence: 99%