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大多数雅各布森综合征缺失断点发生在FRA11B远端。

Most Jacobsen syndrome deletion breakpoints occur distal to FRA11B.

作者信息

Michaelis R C, Velagaleti G V, Jones C, Pivnick E K, Phelan M C, Boyd E, Tarleton J, Wilroy R S, Tunnacliffe A, Tharapel A T

机构信息

Greenwood Genetic Center, South Carolina, USA.

出版信息

Am J Med Genet. 1998 Mar 19;76(3):222-8.

PMID:9508241
Abstract

Recent studies have identified a (CCG)n repeat in the 5' untranslated region of the CBL2 protooncogene (11q23.3) and have demonstrated that expansion of this repeat causes expression of the folate-sensitive fragile site FRA11B. It has also been demonstrated that FRA11B is the site of breakage in some cases of Jacobsen syndrome (JS) involving terminal deletions of chromosome 11q. We report on 2 patients with JS and a 46,XX,del(11)(q23.3) karyotype. In both cases, microsatellite and fluorescence in situ hybridization analyses indicated that the deletion breakpoint was approximately 1.5-3 Mb telomeric to FRA11B. There was no evidence of expansion of the CBL2 (CCG)n repeat in the parents of either patient. The deleted chromosome was of paternal origin in both cases, although it was of maternal origin in the cases reported to be caused by FRA11B. These findings and those in previously reported patients suggest that the breakpoint for most 11q deletions in JS patients is telomeric to FRA11B, which raises the possibility that there may be other fragile sites in 11q23.3 in addition to FRA11B. These findings also support previous evidence that there may be a propensity for breakpoints to differ depending on the parental origin of the deleted chromosome.

摘要

近期研究已在CBL2原癌基因(11q23.3)的5'非翻译区鉴定出一个(CCG)n重复序列,并证明该重复序列的扩增会导致叶酸敏感型脆性位点FRA11B的表达。研究还表明,在一些涉及11号染色体q末端缺失的雅各布森综合征(JS)病例中,FRA11B是断裂位点。我们报告了2例JS患者,其核型为46,XX,del(11)(q23.3)。在这两例中,微卫星和荧光原位杂交分析表明,缺失断点位于FRA11B端粒约1.5 - 3 Mb处。两例患者的父母均无CBL2(CCG)n重复序列扩增的证据。两例中缺失的染色体均来自父方,而在报道由FRA11B导致的病例中,缺失染色体来自母方。这些发现以及先前报道患者的发现表明,JS患者中大多数11q缺失的断点位于FRA11B的端粒,这增加了11q23.3除FRA11B外可能存在其他脆性位点的可能性。这些发现也支持了先前的证据,即根据缺失染色体的亲本来源,断点可能存在差异倾向。

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