中华实验眼科杂志
中華實驗眼科雜誌
중화실험안과잡지
CHINESE JOURNAL OF EXPERIMENTAL OPHTHALMOLOGY
2015年
8期
705-709
,共5页
肖海%张卉%李涛%吴东%张朝阳%时伟丽%秦利涛%廖世秀
肖海%張卉%李濤%吳東%張朝暘%時偉麗%秦利濤%廖世秀
초해%장훼%리도%오동%장조양%시위려%진리도%료세수
先天性白内障%家系谱%基因突变%DNA测序分析方法%第二代测序%产前诊断
先天性白內障%傢繫譜%基因突變%DNA測序分析方法%第二代測序%產前診斷
선천성백내장%가계보%기인돌변%DNA측서분석방법%제이대측서%산전진단
Cataract/congenital%Pedigree%Mutation%DNA Sequence analysis%Next-generation sequencing%Prenatal diagnosis
背景 某些遗传性疾病具有高度遗传异质性,因此传统的Sanger测序技术已经不能满足医学研究及临床工作的需求.第二代测序(NGS)技术由于具有费用低及检测速度快的优点而得到广泛应用,但在先天性眼病突变基因的检测中的应用效果有待验证.目的 探讨NGS技术对先天性白内障患者进行致病基因诊断和产前诊断的可行性.方法 于2013年1月收集来自河南省洛阳市的一汉族先天性白内障家系,抽取家系中3例患者(Ⅱ2、Ⅲ3、Ⅲ4)和3名表型正常者(Ⅱ3、Ⅲ1、Ⅲ2)的外周血各2 ml,EDTA抗凝,在河南省医学遗传研究所应用NGS技术对先证者进行基因突变位点检测,并采用Sanger测序技术对NGS结果进行验证,然后用Sanger测序技术对该家系其他成员的外周血样本进行突变位点的序列分析,根据确定的致病突变位点对先证者的胎儿进行产前诊断.本研究遵循赫尔辛基宣言,检测方案经河南省人民医院医学伦理委员会批准,所有研究对象均签署知情同意书.结果 该家系4代14位成员中共5例患者,其中男2例,女3例,分布于Ⅰ、Ⅱ、Ⅲ代中,其他家系成员表型正常,符合常染色体显性遗传方式.NGS检测发现先证者Ⅲ3CRYBB1基因第6外显子上存在c.682T>C(p.S228P)杂合突变,Sanger法验证了该点突变.Sanger法检测发现家系中患者均存在CRYBB1基因c.682 T>C突变,而家系中表型正常者CRYBB1基因的c.682位点基因型为T/T野生型.产前诊断结果显示胎儿(Ⅳ1)CRYBB1基因c.682位点基因型为T/T野生型.结论 NGS可用于先天性白内障基因突变的快速检测,该家系致病性基因为CRYBB1基因c.682T>C突变,应用NGS技术结合一代测序技术成功对先证者进行了产前诊断.
揹景 某些遺傳性疾病具有高度遺傳異質性,因此傳統的Sanger測序技術已經不能滿足醫學研究及臨床工作的需求.第二代測序(NGS)技術由于具有費用低及檢測速度快的優點而得到廣汎應用,但在先天性眼病突變基因的檢測中的應用效果有待驗證.目的 探討NGS技術對先天性白內障患者進行緻病基因診斷和產前診斷的可行性.方法 于2013年1月收集來自河南省洛暘市的一漢族先天性白內障傢繫,抽取傢繫中3例患者(Ⅱ2、Ⅲ3、Ⅲ4)和3名錶型正常者(Ⅱ3、Ⅲ1、Ⅲ2)的外週血各2 ml,EDTA抗凝,在河南省醫學遺傳研究所應用NGS技術對先證者進行基因突變位點檢測,併採用Sanger測序技術對NGS結果進行驗證,然後用Sanger測序技術對該傢繫其他成員的外週血樣本進行突變位點的序列分析,根據確定的緻病突變位點對先證者的胎兒進行產前診斷.本研究遵循赫爾辛基宣言,檢測方案經河南省人民醫院醫學倫理委員會批準,所有研究對象均籤署知情同意書.結果 該傢繫4代14位成員中共5例患者,其中男2例,女3例,分佈于Ⅰ、Ⅱ、Ⅲ代中,其他傢繫成員錶型正常,符閤常染色體顯性遺傳方式.NGS檢測髮現先證者Ⅲ3CRYBB1基因第6外顯子上存在c.682T>C(p.S228P)雜閤突變,Sanger法驗證瞭該點突變.Sanger法檢測髮現傢繫中患者均存在CRYBB1基因c.682 T>C突變,而傢繫中錶型正常者CRYBB1基因的c.682位點基因型為T/T野生型.產前診斷結果顯示胎兒(Ⅳ1)CRYBB1基因c.682位點基因型為T/T野生型.結論 NGS可用于先天性白內障基因突變的快速檢測,該傢繫緻病性基因為CRYBB1基因c.682T>C突變,應用NGS技術結閤一代測序技術成功對先證者進行瞭產前診斷.
배경 모사유전성질병구유고도유전이질성,인차전통적Sanger측서기술이경불능만족의학연구급림상공작적수구.제이대측서(NGS)기술유우구유비용저급검측속도쾌적우점이득도엄범응용,단재선천성안병돌변기인적검측중적응용효과유대험증.목적 탐토NGS기술대선천성백내장환자진행치병기인진단화산전진단적가행성.방법 우2013년1월수집래자하남성락양시적일한족선천성백내장가계,추취가계중3례환자(Ⅱ2、Ⅲ3、Ⅲ4)화3명표형정상자(Ⅱ3、Ⅲ1、Ⅲ2)적외주혈각2 ml,EDTA항응,재하남성의학유전연구소응용NGS기술대선증자진행기인돌변위점검측,병채용Sanger측서기술대NGS결과진행험증,연후용Sanger측서기술대해가계기타성원적외주혈양본진행돌변위점적서렬분석,근거학정적치병돌변위점대선증자적태인진행산전진단.본연구준순혁이신기선언,검측방안경하남성인민의원의학윤리위원회비준,소유연구대상균첨서지정동의서.결과 해가계4대14위성원중공5례환자,기중남2례,녀3례,분포우Ⅰ、Ⅱ、Ⅲ대중,기타가계성원표형정상,부합상염색체현성유전방식.NGS검측발현선증자Ⅲ3CRYBB1기인제6외현자상존재c.682T>C(p.S228P)잡합돌변,Sanger법험증료해점돌변.Sanger법검측발현가계중환자균존재CRYBB1기인c.682 T>C돌변,이가계중표형정상자CRYBB1기인적c.682위점기인형위T/T야생형.산전진단결과현시태인(Ⅳ1)CRYBB1기인c.682위점기인형위T/T야생형.결론 NGS가용우선천성백내장기인돌변적쾌속검측,해가계치병성기인위CRYBB1기인c.682T>C돌변,응용NGS기술결합일대측서기술성공대선증자진행료산전진단.
Background Due to the genetic heterogeneity of many diseases,the Sanger sequencing technology is far from satisfying the needs of scientific research and clinical applications.The next-generation sequencing (NGS) technology is being widely used in relevant studies because of its lower cost and much higher throughput.Objective This study was to explore the feasibility of NGS technology for the detection of genetic cause of congenital cataract.Methods A Chinese congenital cataract pedigree was collected from Luoyang city in Medical Genetic Institute of Henan Province in January,2013.The peripheral blood of 2 ml was obtained from each 3 patients with congenital cataract (Ⅱ 2,Ⅲ 3,Ⅲ 4) and 3 subjects with normal phenotype (Ⅱ 3,Ⅲ 1,Ⅲ 2) in this pedigree respectively using EDTA anticoagulant tube.The mutant gene of proband was detected by NGS,and the result was verified by Sanger sequencing.Sanger sequencing was employed to determine the mutation sites of other subjects in this pedigree and further to perform the prenatal diagnosis.The research followed the Declaration of Helsinki,and the protocol was approved by the Medical Ethics Committee of Henan Provincial People's Hospital.Written informed consent was obtained from each subject prior to any medical examination.Results Total 5 patients were found in 14 family members of 4 generations in this pedigree,including 2 males and 3 females in generation of Ⅰ,Ⅱ,Ⅲ,and the other family members showed normal phenotype,which followed autosomal dominant inheritance pattern.NGS revealed that the proband occurred a heterozygous mutation of c.682 (p.S228P) in the exon 6 of CRYYB1 gene,and the outcome was further confirmed by Sanger sequencing.In addition,this heterozygous mutant gene was also found in other patients of this pedigree.However,the genotype of c.682 in the exon 6 of CRYYB1 gene was T/T wild type in the subjects with normal phenotype in this pedigree.The genotype of CRYYB1 gene was T/T wild type in the fetus (Ⅳ 1) by prenatal diagnosis.Conclusions NGS is a useful tool for the detection of mutant gene in congenital cataractous pedigree.The heterozygous mutation of c.682T>C (p.S228P) in the exon 6 of CRYYB1 gene is the causative mutation in this pedigree.NGS combined with Sanger sequencing enables prenatal diagnosis of the disease.
