中华儿科杂志
中華兒科雜誌
중화인과잡지
Chinese Journal of Pediatrics
2014年
7期
488-493
,共6页
赵锋%余自华%杨勇辉%聂晓晶%黄隽%王承峰%夏桂枝%陈光明
趙鋒%餘自華%楊勇輝%聶曉晶%黃雋%王承峰%夏桂枝%陳光明
조봉%여자화%양용휘%섭효정%황준%왕승봉%하계지%진광명
肾病综合征%激素耐药%MYO1E基因%突变%汉族
腎病綜閤徵%激素耐藥%MYO1E基因%突變%漢族
신병종합정%격소내약%MYO1E기인%돌변%한족
Nephrotic syndrome%Steroid-resistant%MYO1E%Mutation%Chinese Han ethnic group
目的 分析中国汉族散发性激素耐药型肾病综合征(SRNS)儿童MYO1E基因突变及其特点.方法 研究对象为54例中国汉族散发性SRNS患儿,对照人群为59名尿检正常的健康志愿者.取所有研究对象外周静脉血3 ml,提取基因组DNA; PCR扩增MYO1E基因全部28个外显子及其周围的部分内含子;应用DNA直接测序法、限制性酶切片段分析法进行MYO1E基因突变分析.结果 在54例散发性SRNS病例中共发现MYO1E基因51个变异.其中有10个变异IVS1-11T>C、IVS2-86T>A、279T> C(D93D)、IVS6-181G>A、718C> T(L240F)、1678A> G(T560A)、IVS16-35A>G、IVS18 +48T>A、IVS19+ 38G>A和IVS25+13C>T在59名正常对照人群未检出,表明它们是MYO1E基因突变;另41个变异在美国国立生物技术信息中心(NCBI)的单核苷酸多态性(SNP)数据库中已公布,属于MYO1E基因多态性.上述新发现的10个MYO1E基因突变呈单杂合状态.结论 MYO1E基因突变不是本研究中国汉族散发性SRNS患儿的主要致病原因.
目的 分析中國漢族散髮性激素耐藥型腎病綜閤徵(SRNS)兒童MYO1E基因突變及其特點.方法 研究對象為54例中國漢族散髮性SRNS患兒,對照人群為59名尿檢正常的健康誌願者.取所有研究對象外週靜脈血3 ml,提取基因組DNA; PCR擴增MYO1E基因全部28箇外顯子及其週圍的部分內含子;應用DNA直接測序法、限製性酶切片段分析法進行MYO1E基因突變分析.結果 在54例散髮性SRNS病例中共髮現MYO1E基因51箇變異.其中有10箇變異IVS1-11T>C、IVS2-86T>A、279T> C(D93D)、IVS6-181G>A、718C> T(L240F)、1678A> G(T560A)、IVS16-35A>G、IVS18 +48T>A、IVS19+ 38G>A和IVS25+13C>T在59名正常對照人群未檢齣,錶明它們是MYO1E基因突變;另41箇變異在美國國立生物技術信息中心(NCBI)的單覈苷痠多態性(SNP)數據庫中已公佈,屬于MYO1E基因多態性.上述新髮現的10箇MYO1E基因突變呈單雜閤狀態.結論 MYO1E基因突變不是本研究中國漢族散髮性SRNS患兒的主要緻病原因.
목적 분석중국한족산발성격소내약형신병종합정(SRNS)인동MYO1E기인돌변급기특점.방법 연구대상위54례중국한족산발성SRNS환인,대조인군위59명뇨검정상적건강지원자.취소유연구대상외주정맥혈3 ml,제취기인조DNA; PCR확증MYO1E기인전부28개외현자급기주위적부분내함자;응용DNA직접측서법、한제성매절편단분석법진행MYO1E기인돌변분석.결과 재54례산발성SRNS병례중공발현MYO1E기인51개변이.기중유10개변이IVS1-11T>C、IVS2-86T>A、279T> C(D93D)、IVS6-181G>A、718C> T(L240F)、1678A> G(T560A)、IVS16-35A>G、IVS18 +48T>A、IVS19+ 38G>A화IVS25+13C>T재59명정상대조인군미검출,표명타문시MYO1E기인돌변;령41개변이재미국국립생물기술신식중심(NCBI)적단핵감산다태성(SNP)수거고중이공포,속우MYO1E기인다태성.상술신발현적10개MYO1E기인돌변정단잡합상태.결론 MYO1E기인돌변불시본연구중국한족산발성SRNS환인적주요치병원인.
Objective Previous studies have demonstrated that two homozygous missense MYO1E mutations are associated with childhood autosomal recessive focal segmental glomerulosclerosis in steroidresistant nephrotic syndrome (SRNS) families from Italy and Turkey.Non-disease-causing heterozygous MYO1E variants were also found in other SRNS patient cohorts.However,the role of MYO1E mutations in Chinese sporadic SRNS has not been established.Method Peripheral blood samples were collected for genetic analysis from 54 children with sporadic SRNS in Chinese Han ethnic group and a normal control group of 59 healthy adult volunteers.None of the patients carried mutations in NPHS2 or WT1.Genomic DNA was extracted from peripheral blood leukocytes.Twenty-eight exons and exon-intron boundaries of the MYO1E gene were amplified by polymerase chain reaction.Mutational analysis was performed by direct DNA sequencing and restriction endonuclease digestion.Result Fifty-one variants in the MYO1E gene were identified in 54 children with sporadic SRNS.Among them,10 MYO1E mutations of IVS1-11T > C,IVS2-86T > A,279T > C (D93D),IVS6-181G > A,718C > T (L240F),1678A > G (T560A),IVS16-35A > G,IVS18 + 48T > A,IVS19 + 38G > A and IVS25 + 13C > T were detected in 11 patients,whereas they were absent in the 59 normal Chinese controls.Forty-one variants in MYO1E were identified and all of them were published in single nucleotide polymorphism database from national center for biotechnology information.Furthermore,all the 10 MYO1E mutations were in heterozygous states.Conclusion MYO1E mutations are not a major cause of Chinese children with sporadic SRNS in the study.