巨结肠疾病:关于基因、外显率和产前诊断的见解

X. Wang, M. Camilleri
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引用次数: 13

摘要

这篇小型综述的目的是提供与巨结肠疾病不同表现相关的遗传变异的理解进展,这些疾病可能表现为从短段结肠到全结肠和小肠或广泛的神经节病的一系列失神经支配。该杂志最近发表的一篇文章记录了23例长段巨结肠病患者的潜在基因变异。如先前文献报道的那样,使用与巨结肠疾病或肠神经嵴细胞发育相关的31个基因组来鉴定基因变异。该研究在13名患者的8个基因中发现了潜在的有害变异,检出率为56.5%(13/23名患者)。5例患者存在RET、NRG1和L1CAM的病理变异,其余患者被认为是意义未知的变异。作者试图利用羊膜穿刺术样本对一个家庭中高龄的母亲进行先天性巨结肠疾病的产前诊断,该家庭中存在已知的有害RET突变,表现为父亲(长段先天性巨结肠疾病)和大女儿(全结肠坏疽症)。胎儿有相同的RET变异,但经过几年的随访,没有出现任何先天性巨结肠疾病的症状,这支持了RET突变是不完全外显的常染色体显性基因的结论。这一经验表明,遗传咨询是适当的,以仔细评估产前检查的理由,特别是当长段巨结肠疾病的表型如此多变,这种疾病有可能通过手术治愈。
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Hirschsprung disease: Insights on genes, penetrance, and prenatal diagnosis
The objective of this mini‐review is to provide insights on the advances in the understanding of the genetic variants associated with different manifestations of Hirschsprung disease, which may present with a range of denervation from a short segment of colon to total colonic and small bowel or extensive aganglionosis. A recent article in this journal documented potential gene variants involved in long‐segment Hirschsprung disease in 23 patients. Gene variants were identified using a 31‐gene panel of genes related to Hirschsprung disease or enteric neural crest cell development, as previously reported in the literature. The study identified potentially harmful variants in eight genes across 13 patients, with a detection rate of 56.5% (13/23 patients). Five patients had pathologic variants in RET, NRG1, and L1CAM, and the remainder were considered variants of unknown significance. The authors attempted prenatal diagnosis of Hirschsprung disease utilizing an amniocentesis sample obtained for advanced maternal age in a family with a known deleterious RET mutation, manifested in the father (long‐segment Hirschsprung disease) and older daughter (total colonic aganglionosis). The fetus had the same RET variant but, after several years of follow‐up, has not developed any symptoms of Hirschsprung disease, supporting the conclusion that this RET mutation is an autosomal dominant gene with incomplete penetrance. This experience suggests that genetic counseling is appropriate to carefully assess the justification of prenatal testing, especially, when the phenotype of long‐segment Hirschsprung disease is so variable and the disease is potentially curable with surgery.
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