Department of Pediatric Neurology, Medical University of Silesia, Katowice, Poland.
Department of Medical Genetics, Medical University of Warsaw, Warsaw, Poland.
Clin Genet. 2018 Oct;94(3-4):381-385. doi: 10.1111/cge.13410. Epub 2018 Aug 2.
The HNRNPH2-associated disease (mental retardation, X-linked, syndromic, Bain type [MRXSB, MIM #300986]) is caused by de novo mutations in the X-linked HNRNPH2 gene. MRXSB has been described in six female patients with dysmorphy, developmental delay, intellectual disability, autism, hypotonia and seizures. The reported HNRNPH2 mutations were clustered in the small domain encoding nuclear localization signal; in particular, the p.Arg206Trp was found in four independent de novo events. HNRNPH1 is a conserved autosomal paralogue of HNRNPH2 with a similar function in regulation of pre-mRNAs splicing but so far it has not been associated with human disease. We describe a boy with a disease similar to MRXSB in whom a novel de novo mutation c.616C>T (p.Arg206Trp) in HNRNPH1 was found (ie, the exact paralogue of the recurrent HNRNPH2 mutation). We propose that defective function of HNRNPH2 and HNRNPH1 nuclear localization signal has similar clinical consequences. An important difference between the two diseases is that the HNRNPH1-associated syndrome may occur in boys (as in the case of our proband) which is well explained by the autosomal (chr5q35.3) rather than X-linked localization of the HNRNPH2 gene.
HNRNPH2 相关疾病(智力障碍,X 连锁,综合征型,贝恩型[MRXSB,MIM #300986])是由 X 连锁 HNRNPH2 基因中的新生突变引起的。MRXSB 已在六名女性患者中被描述,这些患者存在畸形、发育迟缓、智力障碍、自闭症、低张力和癫痫发作。报道的 HNRNPH2 突变集中在编码核定位信号的小结构域中;特别是,p.Arg206Trp 在四个独立的新生事件中被发现。HNRNPH1 是 HNRNPH2 的保守常染色体同源物,具有类似的调节前体 mRNA 剪接的功能,但迄今为止尚未与人类疾病相关。我们描述了一名男孩,其疾病与 MRXSB 相似,在他的 HNRNPH1 中发现了一个新的新生突变 c.616C>T(p.Arg206Trp)(即,与反复发生的 HNRNPH2 突变相同的同源物)。我们提出,HNRNPH2 和 HNRNPH1 核定位信号的功能缺陷具有相似的临床后果。两种疾病之间的一个重要区别是,HNRNPH1 相关综合征可能发生在男孩中(如我们的先证者),这很好地解释了 HNRNPH2 基因的常染色体(chr5q35.3)而非 X 连锁定位。
