3个遗传性出血性毛细血管扩张症家系临床和基因诊断研究被引量：1

Clinical characteristics and molecular mechanisms of hereditary hemorrhagic telangiectasis( HHT) in 3 families

导出

摘要目的对遗传性出血性毛细血管扩张症(HHT)家系做临床诊断并探索其分子发病机制。方法收集3个疑似HHT患者的病史、临床表型和家族史等基本资料,对患者凝血功能相关指标做实验室检测,排除凝血系统异常。采用直接测序法对HHT相关基因ENG和ACVRL1做序列分析,寻找致病突变;将所发现的突变重新扩增PCR产物反向测序以证实。比对新的基因突变,筛查100个正常人、单核苷酸多态性数据库、人类基因突变数据库和HHT基因变异数据库以排除多态性。结果 3个家系中均存在出血、毛细血管扩张、阳性家族史等HHT典型临床特点,凝血功能均未发现异常。基因测序显示突变均存在于ACVRL1基因上,3个家系携带的突变分别是g.18349C>A,p.Ser462X、g.12876G>T,p.Glu281X和g.12079G>T,p.Val228Phe,其中g.18349C>A,p.Ser462X和g.12079G>T,p.Val228Phe为新发致病突变。在100个正常人和数据库中均未发现相关突变;3个突变均导致ACVRL1基因编码的ALK-1蛋白激酶功能区内的氨基酸发生改变。结论在这3个有典型HHT表现的家系中,发生在ALK-1蛋白激酶功能区内氨基酸的改变是其分子水平的致病原因。 Objective To disclose the molecular mechanisms of hereditary hemorrhagic telangiectasis（ HHT）. Methods The medical history,clinical information and family history of 3 suspected HHT families were collected after informed consent. Laboratory inspection was performed to exclude other possible pathogenesis related to coagulation abnormalities. All the exons and flanking sequence of the 2 HHT related genes,ENG and ACVRL1,respectively,were amplified and sequenced directly. Reverse sequencing was employed to justify the mutations we found. Comparing with 100 normal people,database of SNP,the human gene mutation database and HHT mutation database,we excluded polymorphism and determined whether the mutations were novel. Results The typical clinical characteristics of HHT such as bleeding,telangiectasis and positive family history existed in all 3 families. Abnormalities of coagulation system were found in none of the patients. The results of sequencing found 3 mutations（ g. 18349C A,p. Ser462X,g. 12876G T,p. Glu281X and g. 12079G T,p. Val228Phe） of ACVRL1 in the 3 families. Of the mutations,g. 18349C A,p. Ser462X and g. 12079G T,p. Val228Phe were novel. None of the 3 mutations were polymorphism after blasting with 100 normal people and related database. All the 3 mutations led to amino acid alterations in the protein kinase region of ALK-1 coded by ACVRL1. Conclusion Amino acid alterations in protein kinase region of ALK-1 led to typical HHT in 3 families.

作者迟昆姜林林陆晔玲戴菁丁秋兰王学锋王鸿利

机构地区上海交通大学医学院附属瑞金医院上海交通大学医学院附属瑞金医院临床检验科

出处《中国输血杂志》 CAS CSCD 北大核心 2013年第12期1193-1197,共5页 Chinese Journal of Blood Transfusion

基金上海市重点学科建设计划(12GWZX0202)

关键词出血性毛细血管扩张症遗传性 ACVRL1基因突变激酶功能区 hereditary hemorrhagic telangiectasis ACVRL1 gene mutation protein kinase region

分类号 R554.9 [医药卫生—血液循环系统疾病] R446.112 [医药卫生—诊断学]

引文网络
相关文献

参考文献20

1Faughnan ME, Palda VA, Garcia-Tsao G, et al. International guide- lines for the diagnosis and management of hereditary haemorrhagic telangiectasia. J Med Genet, 2011,48 ( 2 ) : 73-87.
2Dakeishi M, Shioya T, Wada Y, et al. Genetic epidemiology of he- reditary hemorrhagic telangieetasia in a local community in the northern part of Japan. Hum Mui, 2002,19 ( 2 ) : 140 -148.
3Heutink P, Haitjema T, Breedveld G, et al. Linkage of hereditary haemorrbagic telangiectasia to chromosome 9q34 and evidence fir locus heterogeneity. J Medl Genet,1994,31 (12) :933-936.
4Johnson DW, Berg JN, Gallione CJ ,et al. A second locus for hered- itary hemorrhagic telangiectasia maps to chromosome 12. Genome Res, 1995,5( 1 ) :21-28.
5Gallione C J, Repetto GM, Legius E, et ',ft. A combined syndrome of juvenile polyposis and hereditary haemorrhagic telangiectasia asso- ciated ith mutations in MADH4 ( SMAD 4 ). "Lancet, 2004,363 (9412) :852-859.
6Bayrak-Toydemir.P, McDonald J, Akarsu N ,et al. A fourth locus for hereditary hemorrhagic telangiectasia maps to chromosome 7. Am J Med Genet Part A,2006,140(20):2155-2162.
7Schulte C, Geisthoff U, Lux A, et al. High frequency of ENG and ALK1/ACVRLI mutations in German HHT patients. Hum Mut, 2005,25 ( 6 ) :595-595.
8Shovlin CL, Guttmacher AE, Buscarini E, et al. Diagnostic criteriafor hereditary hemorrhagic telangiectasia ( Rendu-Osler-Veber syn- dnme). Am J Med GeJlet,2000,91 ( 1 ) :66-67.
9Richards-Yulz J, Grant K, Chao EC, et al. Update on molecular di- agnosis of hereditary hemorrhagic telangiectasia. Hum Genet, 2010,128( 1 ) :61-77.
10Govani I"S, Shovlin CL: Hereditary haemorrhagic telangiecta.'ia: a clinical and scientific review. Eur J Hum Genet ,2009,17 (7) :860- 871.

同被引文献5

1殷建团,邱跃灵.肺动静脉瘘1例并文献复习[J].临床肺科杂志,2012,17(7):1202-1203. 被引量：1
2董祥军,周国锋,梁斌,李林,郑传胜,梁惠民,冯敢生.肺动静脉畸形的影像诊断及介入治疗分析[J].临床放射学杂志,2016,35(1):131-134. 被引量：11
3孙葳,杨敏,要雅君,邢海英,彭清,舒俊龙,门茜,刘冉,许珂,邹英华,黄一宁.肺动静脉畸形右向左分流的对比增强经颅多普勒超声检测特点[J].中华神经科杂志,2017,50(3):195-200. 被引量：5
4杨秀军,肖婷婷.小儿肺动静脉畸形的影像诊断与介入治疗一例[J].中华介入放射学电子杂志,2017,5(4):241-243. 被引量：3
5陈巍文,吴盛迪,蒋炜.肝肺综合征研究进展[J].中国临床医学,2018,25(5):810-814. 被引量：5

引证文献1

1李凤芝,王东,张倩.高龄肺动静脉瘘一例报告[J].北京医学,2020,42(3):268-270.

1陆恩祥.罕见多脏器受累的遗传性及出血性毛细血管扩张症一例[J].中华医学超声杂志（电子版）,2009,6(3):79-80.
2张治红,罗江琳.垂体后叶素停用致尿崩症的观察及护理[J].中国社区医师（医学专业）,2008,10(24):84-85.
3刘畅,吕垠遐,杨小东,黄燕花,罗翼,易群.遗传性出血性毛细血管扩张症基因突变分析[J].中华医学遗传学杂志,2013,30(2):176-179. 被引量：2
4徐万峰,刘玖琴,李凯.累及肺、肝脏的遗传性出血性毛细血管扩张症(附3例报告并文献复习)[J].医学影像学杂志,2009,19(11):1463-1465. 被引量：4
5骆杰伟,陈慧,杨柳青,朱爱兰,伍严安,李建卫.一个遗传性出血性毛细血管扩张症家系患者的ACVRL1基因突变分析[J].中华医学遗传学杂志,2008,25(3):308-310. 被引量：2
6刘畅,吕垠遐,石朝利,易群.遗传性出血性毛细血管扩张症ENG、ACVRL1和SMAD4基因筛查突变阴性1例报告[J].四川大学学报（医学版）,2014,45(5):882-882.
7陈胜江,白东峰,夏明钰,秦玲,张周龙,陈梅.超声在遗传性出血性毛细血管扩张症肝受累中的应用价值[J].中国超声医学杂志,2007,23(3):233-235. 被引量：7
8陈纪平,陈家铎.遗传性出血性毛细血管扩张症家族9例报告[J].中国罕少见病杂志,1995,2(1):38-38.
9王俊华,刘彩云,梁慧.遗传性出血性毛细血管扩张症6例围术期护理[J].齐鲁护理杂志（下半月刊）（外科护理）,2010,16(9):60-61.
10李群,郭争捷,王卫民,陈腾.遗传性、出血性毛细血管扩张症的超声诊断[J].中国超声诊断杂志,2003,4(6):422-423. 被引量：4

中国输血杂志

2013年第12期

浏览历史

内容加载中请稍等...

3个遗传性出血性毛细血管扩张症家系临床和基因诊断研究被引量：1

参考文献20

同被引文献5

引证文献1

相关作者

相关机构

相关主题

浏览历史

3个遗传性出血性毛细血管扩张症家系临床和基因诊断研究 被引量：1

参考文献20

同被引文献5

引证文献1

相关作者

相关机构

相关主题

浏览历史

3个遗传性出血性毛细血管扩张症家系临床和基因诊断研究被引量：1