中华医学遗传学杂志
中華醫學遺傳學雜誌
중화의학유전학잡지
CHINESE JOURNAL OF MEDICAL GENETICS
2012年
4期
408-412
,共5页
邢娅%季星%肖冰%蒋雯婷%胡琴%胡娟%曹英%陶炯
邢婭%季星%肖冰%蔣雯婷%鬍琴%鬍娟%曹英%陶炯
형아%계성%초빙%장문정%호금%호연%조영%도형
46,XX男性综合征%46,XX睾丸发育不良%SRY基因%X-Y染色体易位%无精症
46,XX男性綜閤徵%46,XX睪汍髮育不良%SRY基因%X-Y染色體易位%無精癥
46,XX남성종합정%46,XX고환발육불량%SRY기인%X-Y염색체역위%무정증
46,XX male syndrome%Testicular dysgenesis%SRY gene%X-Y translocation%Azoospermia
目的 明确6例46,XX男性综合征患者细胞遗传和分子遗传水平的异常,探讨X-Y短臂易位所致46,XX男性综合征的临床特点和发病机制.方法 临床收集6例46,XX男性患者的表型数据,采用染色体核型分析、聚合酶链反应、荧光原位杂交对SRY基因进行检测和定位.结果 6例患者均为SRY阳性XX男性,携带一条由包含SRY区域的Y染色体短臂片段易位至X染色体短臂而构成的异常X染色体.3例患者通过550~700条带染色体核型分析确定了X-Y易位的断裂位点,均位于Xp22.33和Yp11.2;另外3例患者推测其断裂点位于Xp22.32和Yp11.31,或是Xp22.31和Yp11.2,其中Xp22.32、Xp22.31和Yp11.31的断裂位点既往报道较少.不同年龄段SRY阳性46,XX男性临床表现各有特点.4例成年男性患者均因不育而就诊,表现为无精及性发育不良;1例青少年患者以身材矮小和第二性征发育不良为主要特征;1例儿童患者以身材矮小为唯一表现.结论 染色体核型分析、聚合酶链反应和荧光原位杂交等方法的综合运用在46,XX男性综合征的诊断中具有重要意义.高分辨染色体核型分析对于易位导致的XX男性综合征的断裂点机制研究,以及基因型表型关联的深入分析有指导作用.
目的 明確6例46,XX男性綜閤徵患者細胞遺傳和分子遺傳水平的異常,探討X-Y短臂易位所緻46,XX男性綜閤徵的臨床特點和髮病機製.方法 臨床收集6例46,XX男性患者的錶型數據,採用染色體覈型分析、聚閤酶鏈反應、熒光原位雜交對SRY基因進行檢測和定位.結果 6例患者均為SRY暘性XX男性,攜帶一條由包含SRY區域的Y染色體短臂片段易位至X染色體短臂而構成的異常X染色體.3例患者通過550~700條帶染色體覈型分析確定瞭X-Y易位的斷裂位點,均位于Xp22.33和Yp11.2;另外3例患者推測其斷裂點位于Xp22.32和Yp11.31,或是Xp22.31和Yp11.2,其中Xp22.32、Xp22.31和Yp11.31的斷裂位點既往報道較少.不同年齡段SRY暘性46,XX男性臨床錶現各有特點.4例成年男性患者均因不育而就診,錶現為無精及性髮育不良;1例青少年患者以身材矮小和第二性徵髮育不良為主要特徵;1例兒童患者以身材矮小為唯一錶現.結論 染色體覈型分析、聚閤酶鏈反應和熒光原位雜交等方法的綜閤運用在46,XX男性綜閤徵的診斷中具有重要意義.高分辨染色體覈型分析對于易位導緻的XX男性綜閤徵的斷裂點機製研究,以及基因型錶型關聯的深入分析有指導作用.
목적 명학6례46,XX남성종합정환자세포유전화분자유전수평적이상,탐토X-Y단비역위소치46,XX남성종합정적림상특점화발병궤제.방법 림상수집6례46,XX남성환자적표형수거,채용염색체핵형분석、취합매련반응、형광원위잡교대SRY기인진행검측화정위.결과 6례환자균위SRY양성XX남성,휴대일조유포함SRY구역적Y염색체단비편단역위지X염색체단비이구성적이상X염색체.3례환자통과550~700조대염색체핵형분석학정료X-Y역위적단렬위점,균위우Xp22.33화Yp11.2;령외3례환자추측기단렬점위우Xp22.32화Yp11.31,혹시Xp22.31화Yp11.2,기중Xp22.32、Xp22.31화Yp11.31적단렬위점기왕보도교소.불동년령단SRY양성46,XX남성림상표현각유특점.4례성년남성환자균인불육이취진,표현위무정급성발육불량;1례청소년환자이신재왜소화제이성정발육불량위주요특정;1례인동환자이신재왜소위유일표현.결론 염색체핵형분석、취합매련반응화형광원위잡교등방법적종합운용재46,XX남성종합정적진단중구유중요의의.고분변염색체핵형분석대우역위도치적XX남성종합정적단렬점궤제연구,이급기인형표형관련적심입분석유지도작용.
Objective To characterize molecular and cytogenetic abnormalities in six 46,XX males,and to investigate the clinical manifestations and underlying mechanisms in such patients.Methods Clinical data of six XX male patients were collected.Karyotyping,multiple polymerase chain reaction (PCR) and fluorescence in situ hybridization (FISH) were utilized to detect and locate the sex determining region (SRY) gene.Results PCR and FISH showed that all patients were SRY-positive XX males.All patients have their SRY gene located at the tip of derivative X chromosomes,which have resulted from translocation between short arms of X and Y chromosomes. High resolution karyotyping at 550-750 band level has revealed that the translocation breakpoints were at Xp22.33 and Yp11.2 in three patients.In the remaining patients,the breakpoints were either at Xp22.32 and Yp11.31 or Xp22.31 and Yp11.2.The breakpoints at Xp22.32,Xp22.31 and Yp11.31 were rarely reported.Genotype-phenotype correlation analysis indicated that the clinical manifestations were age-specific.Four adult patients have come to clinical attention due to infertility,with typical features including azoospermia and testis dysgenesis,whereas poorly developed secondary sexual characteristics and short stature were main complaints of adolescence patients,and short stature was the sole symptom in a child patient.Conclusion Combined karyotyping,PCR and FISH are important for the analysis of XX males. Particularly,high resolution karyotyping is valuable for the refinement of chromosome breakpoints and detailed analysis of genotype-phenotype correlation.
