Gedeon A K, Baker E, Robinson H, Partington M W, Gross B, Manca A, Korn B, Poustka A, Yu S, Sutherland G R
Department of Cytogenetics and Molecular Genetics, Adelaide Children's Hospital, South Australia.
Nat Genet. 1992 Aug;1(5):341-4. doi: 10.1038/ng0892-341.
We describe a patient with typical clinical features of the fragile X syndrome, but without cytogenetic expression of the fragile X or an amplified CCG trinucleotide repeat fragment. The patient has a previously uncharacterized submicroscopic deletion encompassing the CCG repeat, the entire FMR1 gene and about 2.5 megabases of flanking sequences. This finding confirms that the fragile X phenotype can exist, without amplification of the CCG repeat or cytogenetic expression of the fragile X, and that fragile X syndrome is a genetically homogeneous disorder involving FMR1. We also found random X-inactivation in the mother of the patient who was shown to be a carrier of this deletion.
我们描述了一名患有脆性X综合征典型临床特征的患者,但该患者并无脆性X的细胞遗传学表现或CCG三核苷酸重复片段的扩增。该患者存在一个先前未被描述的亚显微缺失,其涵盖了CCG重复序列、整个FMR1基因以及约2.5兆碱基的侧翼序列。这一发现证实,即使没有CCG重复序列的扩增或脆性X的细胞遗传学表现,脆性X表型也可能存在,并且脆性X综合征是一种涉及FMR1的基因同质性疾病。我们还在该患者的母亲(已被证明是这种缺失的携带者)中发现了随机X染色体失活现象。