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Expansion of the spectrum of ITGB6-related disorders to adolescent alopecia, dentogingival abnormalities and intellectual disability.


ABSTRACT: Alopecia with mental retardation (APMR) is a very rare disorder. In this study, we report on a consanguineous Pakistani family (AP91) with mild-to-moderate intellectual disability, adolescent alopecia and dentogingival abnormalities. Using homozygosity mapping, linkage analysis and exome sequencing, we identified a novel rare missense variant c.898G>A (p.(Glu300Lys)) in ITGB6, which co-segregates with the phenotype within the family and is predicted to be deleterious. Structural modeling shows that Glu300 lies in the ?-propeller domain, and is surrounded by several residues that are important for heterodimerization with ? integrin. Previous studies showed that ITGB6 variants can cause amelogenesis imperfecta in humans, but patients from family AP91 who are homozygous for the c.898G>A variant present with neurological and dermatological features, indicating a role for ITGB6 beyond enamel formation. Our study demonstrates that a rare deleterious variant within ITGB6 causes not only dentogingival anomalies but also intellectual disability and alopecia.

SUBMITTER: Ansar M 

PROVIDER: S-EPMC4970676 | biostudies-literature | 2016 Aug

REPOSITORIES: biostudies-literature

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Expansion of the spectrum of ITGB6-related disorders to adolescent alopecia, dentogingival abnormalities and intellectual disability.

Ansar Muhammad M   Jan Abid A   Santos-Cortez Regie Lyn P RL   Wang Xin X   Suliman Muhammad M   Acharya Anushree A   Habib Rabia R   Abbe Izoduwa I   Ali Ghazanfar G   Lee Kwanghyuk K   Smith Joshua D JD   Nickerson Deborah A DA   Shendure Jay J   Bamshad Michael J MJ   Ahmad Wasim W   Leal Suzanne M SM  

European journal of human genetics : EJHG 20151223 8


Alopecia with mental retardation (APMR) is a very rare disorder. In this study, we report on a consanguineous Pakistani family (AP91) with mild-to-moderate intellectual disability, adolescent alopecia and dentogingival abnormalities. Using homozygosity mapping, linkage analysis and exome sequencing, we identified a novel rare missense variant c.898G>A (p.(Glu300Lys)) in ITGB6, which co-segregates with the phenotype within the family and is predicted to be deleterious. Structural modeling shows t  ...[more]

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