先天性巨结肠RET基因突变及相关疾病分析

Mutation of RET proto-oncogene and analysis of correlated disease in patients with Hirschsprung's disease

下载PDF

导出

摘要先天性巨结肠(Hirschsprung's disease,HD)是常见的先天性消化道畸形,其病因尚未明了。最近研究表明原癌基因RET的突变在HD发病中起主要作用。方法:采集30例散发性先天性巨结肠和30例正常儿童的全血标本,提取基因组;采用聚合酶链反应(PCR)和单链构象多态(SSCP)技术分析RET基因的第6、10、16外显子。结果:2例患儿存在第10外显子的突变,其中1例家庭中有MEN2A患者;1例患儿存在第16外显子的突变。结论:RET基因突变可能是导致先天性巨结肠发生的重要原因之一,MEN2A和先天性巨结肠的发生可能有一定联系。 The etiology of Hirschsprung's disease (HD) which is a common congenital malformation of the digestive tract remains unclear. The study recently showed the mutation of RET proto-oncogene can be responsible for the pathogene-sis of HD. 30 children with HD and 30 normal children were enrolled in this study. Genome DNA was isolated from the whole blood of all 60 cases. Exon 6, 10 and 16 of RET proto-oncogene were advanced amplified and analyzed by polymerase chain reaction (PCR) and single-strand conformation polymorphism (SSCP). The results showed that two patients were detected with the mutation of exon 10 and one patient with the mutation of exon 16. One of two patients with the mutation of exon 10 was found to have the patient with multible endocrine neoplasia type 2A(MEN2A) in his family. It is concluded that the mutation of RET proto-oncogene can play an important role in the occurrence of HD, and MEN2A correlate probably with the HD.

作者杜勇单振潮吕怀盛

机构地区宁夏医学院附属医院小儿外科宁夏医学院附属医院病理科

出处《临床儿科杂志》 CAS CSCD 北大核心 2001年第4期221-223,234,共4页 Journal of Clinical Pediatrics

关键词先天性巨结肠 RET基因基因突变相关疾病 HD Hirschsprung's disease RET proto-oncogene mutation correlated disease

分类号 R726.5 [医药卫生—儿科]

引文网络
相关文献

参考文献10

1[1]Matrucciello G, Favre A, Takahashi M, et al. Immunohistochemical localization of RET protein in Hirsch-sprung's disease. J Pediatr Surg, 1995,30(3)∶433-436.
2[2]Heyningen VV. One gene-four syndromes. Nature, 1994,367(1)∶319-320.
3[3]Moorse EW, Robe H, Millar AJW, et al. Familial aspect of Hirschsprung's disease. Eur J Pediatr Surg, 1991,1(2)∶97-101.
4[4]Bacher JA, Sieber WK, Garver KL, et al. A genetic study of Hirschsprung's disease. Am J Genet, 1990,45(5)∶568-571.
5[5]Martucciello G. Hirschsprung's disease as a neurochristopathy. Pediatr Surg Int, 1997,12(1)∶2-10.
6[6]Schuchardt A, Vivette D, Lena LB, et al. Defects in the kidney and enteric nervous system of mice lacking the tyrosine kinase receptor ret. Nature, 1994,367(1)∶380-383.
7[7]Ruth AD, Michael LP, Patric W, et al. Hirschsprung's disease in MEN2A∶increased spectrum of RET exon 10 genotypes and strong genotype-phenotype correlation. Human Molecular Genetics, 1998,7(1)∶129-134.
8[8]Kusafuka T,Puri P. The RET proto-oncogene: a challenge to our understanding of disease pathogenesis. Pediatr Surg Int, 1997,12(1)∶11-18.
9[9]Pacini B,Borrello MG, Greco A, et al. Lose of function effect of RET mutations causing Hirschsprung's disease. Nature Genetics, 1995,10(5)∶35-40.
10[10]Salomon R, Attie T,Peplet A, et al. Germline mutations of the RET ligand GDNF are not sufficient to cause Hirschsprung's disease. Nature Genetics, 1996,14(11)∶345-347.

1许娟,魏明发,史慧芬,王果,李辉,黄尚志.先天性巨结肠RET基因突变的研究[J].中华小儿外科杂志,1999,20(1):7-8. 被引量：10
2易斌,袁继炎,魏明发,王果.应用PCR-SSCP银染技术检测先天性巨结肠症原癌基因RET突变[J].中华实验外科杂志,1999,16(4):340-341. 被引量：1
3许娟,魏明发,史慧芬,王果,李辉,黄尚志.PCR-SSCP法检测先天性巨结肠酪氨酸激酶受体基因突变[J].中华实验外科杂志,1999,16(3):195-196.
4詹江华,牛军,胡博,戴春娟,尹娟,胡晓丽,谷继卿,汪帕.应用DHPLC筛查先天性巨结肠RET基因突变研究[J].天津医药,2006,34(8):519-521. 被引量：6
5黄春伟,殷勤,吴建胜.成人门静脉海绵样变的相关疾病分析[J].实用医学杂志,2009,25(21):3649-3651. 被引量：2
6牛会忠,王丽亚,耿建磊.先天性巨结肠与RET基因突变相关性研究[J].河北医药,2013,35(1):53-54.
7詹江华,房志勤,谷继卿.先天性巨结肠RET基因转录水平的研究[J].中华小儿外科杂志,1999,20(1):5-6. 被引量：12
8麻宏伟,王,姜梅,赵颇,宓真,高红.一种简便、快速筛查软骨发育不全FGFR3基因G380R突变的检测方法[J].中国医科大学学报,1999,28(4):316-316.
9杨圣能.先天性肛门闭锁一期手术治疗8例[J].浙江中西医结合杂志,2007,17(11):706-707.
10李爱武,张文同,栾怡,段祥升,冯进波,王凤英.先天性巨结肠层粘连蛋白基因与RET基因表达的关系[J].中华普通外科杂志,2006,21(8):607-608. 被引量：1

临床儿科杂志

2001年第4期

浏览历史

内容加载中请稍等...

先天性巨结肠RET基因突变及相关疾病分析

参考文献10

相关作者

相关机构

相关主题

浏览历史