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临床病理学中的比较基因组杂交阵列:进展与挑战

Comparative genomic hybridization arrays in clinical pathology: progress and challenges.

作者信息

Gunn Shelly R, Robetorye Ryan S, Mohammed Mansoor S

机构信息

Department of Pathology, University of Texas Health Science Center, San Antonio, Texas 78229-3900, USA.

出版信息

Mol Diagn Ther. 2007;11(2):73-7. doi: 10.1007/BF03256225.

Abstract

Array-based comparative genomic hybridization (array CGH) genome scanning is a powerful method for the global detection of gains and losses of genetic material in both congenital and neoplastic disorders. When used as a clinical diagnostic test, array CGH combines the whole genome perspective of traditional G-banded cytogenetics with the targeted identification of cryptic chromosomal abnormalities characteristic of fluorescence in situ hybridization (FISH). However, the presence of structural variants in the human genome can complicate analysis of patient samples, and array CGH does not provide morphologic information about chromosome structure, balanced translocations, or the actual chromosomal location of segmental duplications. Identification of such anomalies has significant diagnostic and prognostic implications for the patient. We therefore propose that array CGH should be used as a guide to the presence of genomic structural rearrangements in germline and tumor genomes that can then be further characterized by FISH or G-banding, depending on the clinical scenario. In this article, we share some of our experiences with diagnostic array CGH and discuss recent progress and challenges involved with the integration of array CGH into clinical laboratory medicine.

摘要

基于微阵列的比较基因组杂交(array CGH)基因组扫描是一种用于全面检测先天性和肿瘤性疾病中遗传物质增减的强大方法。当用作临床诊断测试时,array CGH将传统G带细胞遗传学的全基因组视角与荧光原位杂交(FISH)特有的隐秘染色体异常的靶向识别相结合。然而,人类基因组中结构变异的存在会使患者样本分析变得复杂,并且array CGH无法提供有关染色体结构、平衡易位或节段性重复实际染色体位置的形态学信息。识别此类异常对患者具有重要的诊断和预后意义。因此,我们建议将array CGH用作检测种系和肿瘤基因组中基因组结构重排的指南,然后根据临床情况通过FISH或G带进一步对其进行特征描述。在本文中,我们分享了一些诊断性array CGH的经验,并讨论了将array CGH整合到临床检验医学中所涉及的最新进展和挑战。

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