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FMR2的鉴定,一种与FRAXE CCG重复序列和CpG岛相关的新基因。

Identification of FMR2, a novel gene associated with the FRAXE CCG repeat and CpG island.

作者信息

Gu Y, Shen Y, Gibbs R A, Nelson D L

机构信息

Department of Molecular and Human Genetics, Human Genome Center, Baylor College of Medicine, Houston, Texas 77030, USA.

出版信息

Nat Genet. 1996 May;13(1):109-13. doi: 10.1038/ng0596-109.

Abstract

Five folate-sensitive fragile sites have been identified at the molecular level to date. Each is characterized by an expanded and methylated trinucleotide repeat CGG (CCG). Of the three X chromosome sites, FRAXA, FRAXE and FRAXF, the former two are associated with mental retardation in their expanded forms. FRAXA expansion results in fragile X syndrome due to down regulation of expression of the FMR1 gene, which carries the hypermutable CGG repeat in the 5' untranslated portion of its first exon. Mild mental retardation without consistent physical findings has been found associated with expanded CCG repeats at FRAXE. We have identified a large gene (FMR2) transcribed distally from the CpG island at FRAXE, and down-regulated by repeat expansion and methylation. The gene is novel, expressed in adult brain and placenta, and shows similarity with another human protein, MLLT2, expressed from a gene at chromosome 4q21 involved in translocations found in acute lymphoblastic leukaemia (ALL) cells. Identification of this gene will facilitate further studies to determine the role of its product in FRAXE associated mental deficiency.

摘要

迄今为止,已在分子水平上鉴定出五个对叶酸敏感的脆性位点。每个位点的特征都是三核苷酸重复序列CGG(CCG)的扩增和甲基化。在三个X染色体位点FRAXA、FRAXE和FRAXF中,前两个位点在其扩增形式下与智力迟钝有关。FRAXA扩增导致脆性X综合征,这是由于FMR1基因的表达下调所致,该基因在其第一个外显子的5'非翻译部分携带高度可变的CGG重复序列。已发现FRAXE处CCG重复序列扩增与无一致身体体征的轻度智力迟钝有关。我们在FRAXE的CpG岛远端鉴定出一个大基因(FMR2),该基因因重复序列扩增和甲基化而下调。该基因是新发现的,在成人大脑和胎盘中表达,并与另一种人类蛋白质MLLT2相似,后者由4q21染色体上的一个基因表达,该基因参与急性淋巴细胞白血病(ALL)细胞中的易位。该基因的鉴定将有助于进一步研究以确定其产物在FRAXE相关智力缺陷中的作用。

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