Absence of subtelomeric rearrangements in selected patients with mental retardation as assessed by multiprobe T FISH.

Suely Rodrigues dos Santos, Dértia Villalba Freire-Maia
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引用次数: 4

Abstract

Background: Mental retardation (MR) is a heterogeneous condition that affects 2-3% of the general population and is a public health problem in developing countries. Chromosomal abnormalities are an important cause of MR and subtelomeric rearrangements (STR) have been reported in 4-35% of individuals with idiopathic MR or an unexplained developmental delay, depending on the screening tests and patient selection criteria used. Clinical checklists such as that suggested by de Vries et al. have been used to improve the predictive value of subtelomeric screening.

Findings: Fifteen patients (1-20 years old; five females and ten males) with moderate to severe MR from a genetics outpatient clinic of the Gaffrée and Guinle Teaching Hospital (HUGG) of the Federal University of Rio de Janeiro State (UNIRIO) were screened with Multiprobe T FISH after normal high resolution karyotyping. No subtelomeric rearrangements were detected even though the clinical score of the patients ranged from four to seven.

Conclusion: In developing countries, FISH-based techniques such as Multiprobe T FISH are still expensive. Although Multiprobe T FISH is a good tool for detecting STR, in this study it did not detect STR in patients with unexplained MR/developmental delay even though these patients had a marked chromosomal imbalance. Our findings also show that clinical scores are not reliable predictors of STR.

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通过多探针T - FISH评估选定的智力迟钝患者的亚端粒重排缺失。
背景:智力迟钝(MR)是一种异质性疾病,影响总人口的2-3%,是发展中国家的一个公共卫生问题。染色体异常是MR和亚端粒重排(STR)的重要原因,据报道,在4-35%的特发性MR或不明原因的发育迟缓患者中,这取决于筛查试验和使用的患者选择标准。临床检查表(如de Vries等人建议的)已被用于提高亚端粒筛选的预测价值。结果:15例患者(1-20岁;对来自里约热内卢州联邦大学(UNIRIO) gaffr和Guinle教学医院(HUGG)遗传学门诊的5名女性和10名男性患有中度至重度MR的患者进行Multiprobe T FISH筛查,正常高分辨率核型分析。即使患者的临床评分在4到7分之间,也没有检测到亚端粒重排。结论:在发展中国家,基于FISH的技术,如Multiprobe T FISH仍然很昂贵。虽然Multiprobe T FISH是一种检测STR的好工具,但在本研究中,它没有检测出原因不明的MR/发育迟缓患者的STR,即使这些患者有明显的染色体失衡。我们的研究结果还表明,临床评分并不是STR的可靠预测指标。
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