中华实验眼科杂志
中華實驗眼科雜誌
중화실험안과잡지
CHINESE JOURNAL OF EXPERIMENTAL OPHTHALMOLOGY
2012年
9期
819-823
,共5页
张素华%张晓慧%张哲%刘杰为%江琳%刘建亭%董慧%郭彩虹
張素華%張曉慧%張哲%劉傑為%江琳%劉建亭%董慧%郭綵虹
장소화%장효혜%장철%류걸위%강림%류건정%동혜%곽채홍
先天性白内障%微卫星标记%等位基因共享分析%基因测序
先天性白內障%微衛星標記%等位基因共享分析%基因測序
선천성백내장%미위성표기%등위기인공향분석%기인측서
Congenital cataract%Microsatellite marker%Alleles sharing analysis%Gene sequencing
背景 遗传因素是先天性白内障的主要致病因素之一,致病基因的筛查是研究先天性白内障发病分子机制的重要步骤. 目的 明确一结晶样晶状体混浊的先天性常染色体显性遗传白内障(ADCC)家系的致病基因. 方法 收集山西省榆社县一个四代先天性结晶样混浊白内障家系22名成员,其中患者10例.在获得知情同意后,该家系成员进行家系调查以确定遗传方式.经裂隙灯显微镜检查和常规眼科临床检查确定表型.采集其中17例家系成员的外周静脉血5 ml并提取DNA,ADCC的17个已知致病基因周围选取22个荧光标记的微卫星,通过对微卫星标志物的扩增和基因型分析对该家系进行基因两点连锁分析,并计算对数优势评分(LOD)值.对筛选的候选基因进行直接测序分析. 结果 该家系患者晶状体混浊表型非常类似,家系分析表明为四代垂直遗传,符合单基因ADCC的特点.基因连锁分析提示,该家系与微卫星D2S325位点和D2S2358位点连锁,最大LOD值分别为1.20(θ=0)和0.22(θ=0),位于此区域内的CR YGD基因测序后发现一个已经报道的错义突变c.C70A(p.P23T). 结论 CRYGD基因P23T突变是该家系结晶样晶状体混浊的致病原因.
揹景 遺傳因素是先天性白內障的主要緻病因素之一,緻病基因的篩查是研究先天性白內障髮病分子機製的重要步驟. 目的 明確一結晶樣晶狀體混濁的先天性常染色體顯性遺傳白內障(ADCC)傢繫的緻病基因. 方法 收集山西省榆社縣一箇四代先天性結晶樣混濁白內障傢繫22名成員,其中患者10例.在穫得知情同意後,該傢繫成員進行傢繫調查以確定遺傳方式.經裂隙燈顯微鏡檢查和常規眼科臨床檢查確定錶型.採集其中17例傢繫成員的外週靜脈血5 ml併提取DNA,ADCC的17箇已知緻病基因週圍選取22箇熒光標記的微衛星,通過對微衛星標誌物的擴增和基因型分析對該傢繫進行基因兩點連鎖分析,併計算對數優勢評分(LOD)值.對篩選的候選基因進行直接測序分析. 結果 該傢繫患者晶狀體混濁錶型非常類似,傢繫分析錶明為四代垂直遺傳,符閤單基因ADCC的特點.基因連鎖分析提示,該傢繫與微衛星D2S325位點和D2S2358位點連鎖,最大LOD值分彆為1.20(θ=0)和0.22(θ=0),位于此區域內的CR YGD基因測序後髮現一箇已經報道的錯義突變c.C70A(p.P23T). 結論 CRYGD基因P23T突變是該傢繫結晶樣晶狀體混濁的緻病原因.
배경 유전인소시선천성백내장적주요치병인소지일,치병기인적사사시연구선천성백내장발병분자궤제적중요보취. 목적 명학일결정양정상체혼탁적선천성상염색체현성유전백내장(ADCC)가계적치병기인. 방법 수집산서성유사현일개사대선천성결정양혼탁백내장가계22명성원,기중환자10례.재획득지정동의후,해가계성원진행가계조사이학정유전방식.경렬극등현미경검사화상규안과림상검사학정표형.채집기중17례가계성원적외주정맥혈5 ml병제취DNA,ADCC적17개이지치병기인주위선취22개형광표기적미위성,통과대미위성표지물적확증화기인형분석대해가계진행기인량점련쇄분석,병계산대수우세평분(LOD)치.대사선적후선기인진행직접측서분석. 결과 해가계환자정상체혼탁표형비상유사,가계분석표명위사대수직유전,부합단기인ADCC적특점.기인련쇄분석제시,해가계여미위성D2S325위점화D2S2358위점련쇄,최대LOD치분별위1.20(θ=0)화0.22(θ=0),위우차구역내적CR YGD기인측서후발현일개이경보도적착의돌변c.C70A(p.P23T). 결론 CRYGD기인P23T돌변시해가계결정양정상체혼탁적치병원인.
Background Inheritance is one of main causing-disease factors in congenital cataract.So the screen of causing-disease gene in congenital cataract patients is a critical step.Objective This survey was to investigate the molecular characteristics of a Chinese pedigree with a special crystalline autosomal dominant congenital cataract(ADCC) in Shanxi province.Methods This study was approved by Ethic Commission of Shanxi Eye Hospital.Informed consent was obtained from each subject before any medical examination.Twenty-two families from a pedigree with special crystalline were included in this study.The family members received regular ophthalmologic and general examinations to rule out any concomitant disorders.Blood samples were obtained to extract the DNA from all the subjects.Twenty-two fluorescent labeled microsatellites were selected from 17 causing genes of ADCC and amplified and screened for the linkage analysis.LOD was calculated and the candidate gene was directly sequenced.Results Ten individuals with congenital cataract were found in the family with the similar phenotype.The inheritance mode complied with the autosomal dominant pattern.Linkage analysis indicated a gene chain at D2S325 and D2S2358 with the LOD value 1.20(θ =0) and 0.22(θ =0).A known c.C70A(p.P23T) missence mutation at the coding region of CRYGD gene was detected by direct sequence.Conclusions A missense mutation P23T of the CRYGD gene cause the autosomal dominant congenital nuclear cataract with the special phenotype.
