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对无虹膜患者进行涉及威尔姆斯瘤基因缺失的分子分析。

Molecular analysis of aniridia patients for deletions involving the Wilms' tumor gene.

作者信息

Drechsler M, Meijers-Heijboer E J, Schneider S, Schurich B, Grond-Ginsbach C, Tariverdian G, Kantner G, Blankenagel A, Kaps D, Schroeder-Kurth T

机构信息

Institut für Humangenetik, Universität Heidelberg, Germany.

出版信息

Hum Genet. 1994 Oct;94(4):331-8. doi: 10.1007/BF00201588.

Abstract

A human aniridia candidate (AN) gene on chromosome 11p13 has been cloned and characterized. The AN gene is the second cloned gene of the contiguous genes syndrome WAGR (Wilms' tumor, aniridia, genitourinary malformations, mental retardation) on chromosome 11p13, WT1 being the first gene cloned. Knowledge about the position of the AN and WT1 genes on the map of 11p13 makes the risk assessment for Wilms' tumor development in AN patients possible. In this study, we analyzed familial and sporadic aniridia patients for deletions in 11p13 by cytogenetic analyses, in situ hybridization, and pulsed field gel electrophoresis (PFGE). Cytogenetically visible deletions were found in 3/11 sporadic AN cases and in one AN/WT patient, and submicroscopic deletions were identified in two sporadic AN/WT patients and in 1/9 AN families. The exact extent of the deletions was determined with PFGE and, as a result, we could delineate the risk for Wilms' tumor development. Future analyses of specific deletion endpoints in individual AN cases with the 11p13 deletion should result in a more precise risk assessment for these patients.

摘要

位于11号染色体p13区域的一个人类无虹膜候选(AN)基因已被克隆并进行了特征分析。AN基因是11号染色体p13区域连续基因综合征WAGR(Wilms瘤、无虹膜、泌尿生殖系统畸形、智力迟钝)中第二个被克隆的基因,WT1是第一个被克隆的基因。了解AN基因和WT1基因在11p13图谱上的位置,使得对无虹膜患者发生Wilms瘤的风险评估成为可能。在本研究中,我们通过细胞遗传学分析、原位杂交和脉冲场凝胶电泳(PFGE)对家族性和散发性无虹膜患者11p13区域的缺失情况进行了分析。在11例散发性AN病例中有3例以及1例AN/WT患者中发现了细胞遗传学可见的缺失,在2例散发性AN/WT患者和1/9的AN家族中鉴定出了亚显微缺失。用PFGE确定了缺失的精确范围,结果我们能够描绘出发生Wilms瘤的风险。未来对11p13缺失的个别AN病例中特定缺失端点的分析,应该能为这些患者带来更精确的风险评估。

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