Incidence of RET mutations in patients with Hirschsprung's disease

IF 2.4 2区医学 Q1 PEDIATRICS

Journal of pediatric surgery Pub Date : 2000-01-01 DOI:10.1016/S0022-3468(00)80031-7

M. Sancandi, I. Ceccherini, M. Costa, M. Fava, B. Chen, Y. Wu, R. Hofstra, T. Laurie, M. Griffths, D. Burge, P.K.H. Tam

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引用次数: 74

Abstract

Background: RET mutations have been reported variously to affect 7% to 41% of Hirschsprung's disease (HSCR) patients depending on familial or sporadic occurrence of the disease, length of aganglionosis and possible association with other disease phenotypes. The authors report a study of the incidence of RET mutations in unselected HSCR patients from two regional centers and correlate their genotypes and phenotypes. Methods: The records of HSCR patients treated in 2 regional centers with a combined population of 5 million were reviewed, and blood samples were obtained from 57 patients. During the same period, 39 patients with similar demographic data refused or provided insufficient blood for study. DNA was extracted, and the 21 exons of the RET proto-oncogene were screened for mutations using denaturing gradient gel electrophoresis (DGGE). Results: Of 57 patients, 48 were sporadic, and 9 were familial. Lengths of aganglionosis were total colonic, 4; long, 11; short, 39; ultrashort, 1; unclassified, 2. Associated anomalies were present in 20. Causative mutations were identified in 4 (7%): missense or “silent” in 3 (exons 5, 11, 13) and deletion in 1. The silent mutation of exon 11 recently has been shown to have effects on correct RET mRNA splicing. One mutation occurred in total colonic aganglionosis (25%), 1 in long segment dysganglionosis (9%), and 2 in short segment aganglionosis (5%). Surprisingly, all these mutations occurred in sporadic cases (10%). Five patients (9%) had rare polymorphic alleles at exon 14 (n = 1) and exon 18 (n = 4). Fifty patients (88%) showed common polymorphic alleles (sequence variants) in 1 or more exons (>4, n = 5). Conclusions: RET mutation as a primary cause for Hirschsprung's disease in the general surgical population is less frequent than previously thought. This observation is compatible with the hypothesis that HSCR could be a polygenic disease caused by additive subclinical effects of more than one gene, including RET. J Pediatr Surg 35:139-143. Copyright © 2000 by W.B. Saunders Company.

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先天性巨结肠病患者RET突变的发生率

背景:据报道，RET突变影响7%至41%的巨结肠病(HSCR)患者，这取决于该疾病的家族性或散发性、神经节病的病程长短以及与其他疾病表型的可能关联。作者报告了来自两个区域中心的未选择的HSCR患者中RET突变发生率的研究，并将其基因型和表型联系起来。方法:回顾性分析2个地区中心共500万HSCR患者的治疗记录，采集57例患者的血液样本。在同一时期，39例人口统计数据相似的患者拒绝或提供的血液不足进行研究。提取DNA，使用变性梯度凝胶电泳(DGGE)筛选RET原癌基因的21个外显子进行突变。结果:57例患者中，散发性48例，家族性9例。神经节病的长度为结肠总长度，4;长,11;短,39;超短,1;“机密”字样,2。20年出现相关异常。4例(7%)被鉴定出致病突变:3例(外显子5、11、13)错义或“沉默”，1例缺失。外显子11的沉默突变最近被证明对正确的RET mRNA剪接有影响。1个突变发生在全结肠神经节失调症(25%)，1个突变发生在长节段神经节失调症(9%)，2个突变发生在短节段神经节失调症(5%)。令人惊讶的是，所有这些突变都发生在散发病例中(10%)。5例(9%)患者在第14外显子(n = 1)和第18外显子(n = 4)有罕见的多态性等位基因。50例(88%)患者在1个或多个外显子(>4, n = 5)中显示常见的多态性等位基因(序列变异)。结论:RET突变作为普通外科人群中先天性巨结肠病的主要原因比以前认为的要少。这一观察结果与HSCR可能是一种多基因疾病的假设相一致，该疾病是由包括RET在内的多个基因的加性亚临床效应引起的。[J]儿科学外科学35:139-143。W.B. Saunders Company版权所有©2000。

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来源期刊

Journal of pediatric surgery 医学-外科

CiteScore

1.10

自引率

12.50%

发文量

569

审稿时长

38 days

期刊介绍： The journal presents original contributions as well as a complete international abstracts section and other special departments to provide the most current source of information and references in pediatric surgery. The journal is based on the need to improve the surgical care of infants and children, not only through advances in physiology, pathology and surgical techniques, but also by attention to the unique emotional and physical needs of the young patient.