Two unrelated girls with intellectual disability associated with a truncating mutation in the PPM1D penultimate exon

Two unrelated girls with intellectual disability associated with a truncating mutation in the PPM1D penultimate exon

PPM1D truncating mutations in the last and penultimate exons of the gene have been associated with intellectual disability (ID) syndrome. Only 15 affected patients to-date have been reported with mild-to-severe ID, autistic behavior, anxiety and dysmorphic features. Here, we describe the clinical ch...

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Veröffentlicht in:Brain & development (Tokyo. 1979) 2019-06, Vol.41 (6), p.538-541
Hauptverfasser: Kuroda, Yukiko, Murakami, Hiroaki, Yokoi, Takayuki, Kumaki, Tatsuro, Enomoto, Yumi, Tsurusaki, Yoshinori, Kurosawa, Kenji
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De novo mutation
Dysmorphic
Intellectual disability
Last exon
PPM1D
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container_end_page 541
container_issue 6
container_start_page 538
container_title Brain & development (Tokyo. 1979)
container_volume 41
creator Kuroda, Yukiko
Murakami, Hiroaki
Yokoi, Takayuki
Kumaki, Tatsuro
Enomoto, Yumi
Tsurusaki, Yoshinori
Kurosawa, Kenji
description PPM1D truncating mutations in the last and penultimate exons of the gene have been associated with intellectual disability (ID) syndrome. Only 15 affected patients to-date have been reported with mild-to-severe ID, autistic behavior, anxiety and dysmorphic features. Here, we describe the clinical characteristics and underlying genetics of two unrelated girls with moderate developmental delay and dysmorphic features associated with novel mutations in PPM1D exon 5. The dysmorphic features demonstrated by these two patients are consistent with previously reported patients, including broad forehead, thin upper lip, brachydactyly, and hypoplastic nails. We identified a de novo PPM1D mutation in exon 5 of each patient (c.1250_1251insACCA p.V419Tfs*16 and c.1256_1257insCAAG p.S421Qfs*14) by panel sequencing for 4,813 disease-related genes. Both patients also had frameshift mutations (at different positions) that resulted in the same estimated termination codon at 434. These additional reports add to the growing literature on PPM1D-associated ID syndrome and help delineate the clinical phenotype and genetic basis.
doi_str_mv 10.1016/j.braindev.2019.02.007
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subjects De novo mutation
Dysmorphic
Intellectual disability
Last exon
PPM1D
title Two unrelated girls with intellectual disability associated with a truncating mutation in the PPM1D penultimate exon
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