[X-linked intellectual disability syndrome with macrocephaly due to BRWD3 gene deletion].

IF 0.8 4区 医学 Q4 CLINICAL NEUROLOGY
I Arroyo-Carrera, R Romero-Peguero, R Martín-Fernández, A Ramajo-Polo, V García-Navas Núñez
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引用次数: 0

Abstract

Introduction: Pathogenic variants in BRWD3 gene have been described as a rare cause of syndromic X-linked intellectual disability. Its phenotype shows neurodevelopmental delay with intellectual disability in all reported patients, facial dysmorphic features, macrocephaly, overgrowth and obesity. The great majority of cases yield point variants in the gene, only three large deletions including only the BRWD3 gene have been reported. The BRWD3 protein is an epigenetic reader that regulates chromatin remodeling. We report a boy with a compatible phenotype and a deletion including only this gene.

Case report: Boy, without family and perinatal pathological background, with neurodevelopmental delay: psychomotor delay, speech delay and intellectual disability, macrocephaly (p > 99) and obesity. Phenotype with facial dysmorphic features: wide forehead, deep set eyes, bulbous nose, prominent ears and pointed chin. The array-CGH analysis showed a 586 kb deletion at Xq21.1 including only one gene with associated disorder, BRWD3. Afterwards, the deletion was also identified in his asymptomatic mother and sister.

Conclusions: Our patient confirms that the haploinsufficiency due to BRWD3 deletion is a causal genetic mechanism of the BRWD3-related syndromic X-linked intellectual disability. It is important to recognize the phenotype for the diagnosis and follow up of the patients, and also to carry out the family genetic analysis in order to identify and give genetic counselling to the women who also have the genetic defect, because the majority of them are asymptomatic, as the mother and sister of our patient.

[BRWD3基因缺失导致的伴有巨脑畸形的X连锁智力残疾综合征]。
简介BRWD3基因的致病变异已被描述为导致X连锁智力障碍综合征的罕见病因。其表型表现为神经发育迟缓,所有报道的患者均有智力障碍、面部畸形、巨颅症、过度生长和肥胖。绝大多数病例的基因都是点变异,仅有三例大缺失病例的报道,其中只包括 BRWD3 基因。BRWD3 蛋白是一种调控染色质重塑的表观遗传读取器。我们报告了一名男孩的相合表型和仅包括该基因的缺失:病例报告:男孩,无家族和围产期病理背景,神经发育迟缓:精神运动发育迟缓、语言发育迟缓和智力障碍,巨脑畸形(P > 99)和肥胖。表型具有面部畸形特征:宽额头、深眼窝、隆鼻、突出的耳朵和尖下巴。阵列-CGH分析显示,Xq21.1处有一个586 kb的缺失,其中只有一个基因与相关疾病有关,即BRWD3。之后,在他无症状的母亲和姐姐身上也发现了该基因缺失:结论:我们的患者证实,BRWD3 基因缺失导致的单倍性缺失是 BRWD3 相关综合征 X 连锁智力障碍的致病遗传机制。认识到这一表型对于患者的诊断和随访非常重要,同时也要进行家族遗传分析,以确定哪些妇女也存在遗传缺陷,并为她们提供遗传咨询,因为她们中的大多数人都没有症状,就像我们患者的母亲和姐姐一样。
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来源期刊
Revista de neurologia
Revista de neurologia 医学-临床神经学
CiteScore
2.50
自引率
8.30%
发文量
117
审稿时长
3-8 weeks
期刊介绍: Revista de Neurología fomenta y difunde el conocimiento generado en lengua española sobre neurociencia, tanto clínica como experimental.
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