Martínez Francisco, Roselló Mónica, Mayo Sonia, Monfort Sandra, Oltra Silvestre, Orellana Carmen
Unidad de Genética y Diagnostico Prenatal, Hospital Universitario y Politécnico La Fe, Valencia, Spain.
Am J Med Genet A. 2014 Apr;164A(4):918-23. doi: 10.1002/ajmg.a.36371. Epub 2014 Jan 23.
Here we report on two unrelated male patients with syndromic intellectual disability (ID) due to duplication at Xq13.3-q21.1, a region of about 6 Mb and 25 genes. Among these, the most outstanding is ATRX, the causative gene of X-linked alpha-thalassemia/mental retardation. ATRX belongs to the growing list of genes implied in chromatin remodeling causing ID. Many these genes, such as MECP2, are dose-sensitive so that not only deletions and point mutations, but also duplications cause ID. Both patients have severe ID, absent expressive speech, early hypotonia, behavior problems (hyperactivity, repetitive self-stimulatory behavior), postnatal growth deficiency, microcephaly, micrognathia, cryptorchidism, low-set, posteriorly angulated ears, and downslanting palpebral fissures. These findings are also usually present among patients with loss-of-function mutations of the ATRX gene. Completely skewed X inactivation was observed in the only informative carrier mother, a constant finding among female carriers of inactivating point mutations of this gene. Participation of other duplicated genes cannot be excluded; nevertheless we propose that the increased dosage of ATRX is the major pathogenic mechanism of this X-linked disorder, a syndrome reminiscent of MECP2 duplication.
在此,我们报告了两名患有综合征性智力障碍(ID)的男性患者,他们因Xq13.3 - q21.1区域的重复而患病,该区域约6Mb,包含25个基因。其中,最突出的是ATRX,它是X连锁α地中海贫血/智力障碍的致病基因。ATRX属于越来越多的与染色质重塑导致ID相关的基因列表。许多这类基因,如MECP2,对剂量敏感,以至于不仅缺失和点突变,重复也会导致ID。两名患者均有严重ID、无表达性言语、早期肌张力减退、行为问题(多动、重复性自我刺激行为)、出生后生长发育迟缓、小头畸形、小颌畸形、隐睾、低位后倾耳以及睑裂向下倾斜。这些表现通常也见于ATRX基因功能丧失突变的患者中。在唯一提供信息的携带者母亲中观察到完全偏态的X染色体失活,这在该基因失活点突变的女性携带者中是一个常见发现。不能排除其他重复基因的参与;然而,我们认为ATRX剂量增加是这种X连锁疾病的主要致病机制,这是一种类似于MECP2重复综合征的疾病。
