中华泌尿外科杂志
中華泌尿外科雜誌
중화비뇨외과잡지
CHINESE JOURNAL OF UROLOGY
2011年
3期
160-163
,共4页
胡七一%费前进%蔡健%翁志梁%林礼彰%黄学锋%李澄棣
鬍七一%費前進%蔡健%翁誌樑%林禮彰%黃學鋒%李澄棣
호칠일%비전진%채건%옹지량%림례창%황학봉%리징체
不育,男性%染色体障碍%Y染色体微缺失
不育,男性%染色體障礙%Y染色體微缺失
불육,남성%염색체장애%Y염색체미결실
Infertility,male%Chromosome disorders%Y chromosome microdeletions
目的 探讨男性不育症与染色体畸变及Y染色体微缺失之间的关系.方法临床诊断男性不育患者1975例,采集外周血淋巴细胞常规培养,Giemsa染色,镜下观察并分析染色体核型;选取Y染色体特异性序列标签点(STS),应用PCR技术对无精子症及少精子症患者进行Y染色体微缺失检测.结果 1975例患者中,染色体核型异常305例(15.44%),其中常染色体异常101例(5.11%),患者主要表现为少精子症、畸形精子症;性染色体异常204例(10.33%),主要表现以克氏征(5.62%)为主.728例无精子症或少精子症患者中,Y染色体微缺失109例(14.97%),其中AZFa区缺失3例(2.75%),均表现为无精子症;AZFb区缺失5例(4.59%),表现为无精子症2例、严重少精子症2例,精液正常1例;AZFc区缺失者68例(62.39%),患者主要表现为无精子症和严重少精子症;AZFa区和AZFc区均缺失者5例(4.59%),均表现为无精子症;AZFb区和AZFc区均缺失者15例(13.76%),患者以无精子症表现为主;AZFa区、AZFb区和AZFc区均缺失者6例(5.50%),均表现为无精子症.结论染色体异常及Y染色体微缺失均为男性不育的重要病因.
目的 探討男性不育癥與染色體畸變及Y染色體微缺失之間的關繫.方法臨床診斷男性不育患者1975例,採集外週血淋巴細胞常規培養,Giemsa染色,鏡下觀察併分析染色體覈型;選取Y染色體特異性序列標籤點(STS),應用PCR技術對無精子癥及少精子癥患者進行Y染色體微缺失檢測.結果 1975例患者中,染色體覈型異常305例(15.44%),其中常染色體異常101例(5.11%),患者主要錶現為少精子癥、畸形精子癥;性染色體異常204例(10.33%),主要錶現以剋氏徵(5.62%)為主.728例無精子癥或少精子癥患者中,Y染色體微缺失109例(14.97%),其中AZFa區缺失3例(2.75%),均錶現為無精子癥;AZFb區缺失5例(4.59%),錶現為無精子癥2例、嚴重少精子癥2例,精液正常1例;AZFc區缺失者68例(62.39%),患者主要錶現為無精子癥和嚴重少精子癥;AZFa區和AZFc區均缺失者5例(4.59%),均錶現為無精子癥;AZFb區和AZFc區均缺失者15例(13.76%),患者以無精子癥錶現為主;AZFa區、AZFb區和AZFc區均缺失者6例(5.50%),均錶現為無精子癥.結論染色體異常及Y染色體微缺失均為男性不育的重要病因.
목적 탐토남성불육증여염색체기변급Y염색체미결실지간적관계.방법림상진단남성불육환자1975례,채집외주혈림파세포상규배양,Giemsa염색,경하관찰병분석염색체핵형;선취Y염색체특이성서렬표첨점(STS),응용PCR기술대무정자증급소정자증환자진행Y염색체미결실검측.결과 1975례환자중,염색체핵형이상305례(15.44%),기중상염색체이상101례(5.11%),환자주요표현위소정자증、기형정자증;성염색체이상204례(10.33%),주요표현이극씨정(5.62%)위주.728례무정자증혹소정자증환자중,Y염색체미결실109례(14.97%),기중AZFa구결실3례(2.75%),균표현위무정자증;AZFb구결실5례(4.59%),표현위무정자증2례、엄중소정자증2례,정액정상1례;AZFc구결실자68례(62.39%),환자주요표현위무정자증화엄중소정자증;AZFa구화AZFc구균결실자5례(4.59%),균표현위무정자증;AZFb구화AZFc구균결실자15례(13.76%),환자이무정자증표현위주;AZFa구、AZFb구화AZFc구균결실자6례(5.50%),균표현위무정자증.결론염색체이상급Y염색체미결실균위남성불육적중요병인.
Objective To study the relationship between chromosomal abnormality and Y chromosome microdeletions and male infertility. Methods Lymphocytes were cultured from peripheral blood of 1975 male infertility patients and stained with Giemsa. The chromosomes were analyzed under microscope. Y chromosome specific sequence tags (STS) were selected, then the Y chromosome microdeletions in AZF regions were screened by polymerase chain reaction (PCR) in azoospermia and oligozoospermia patients. Results There were 305 cases of detected chromosomal abnormalities (15.44%) in the 1975 cases. There were 101 cases (5.11 %) with autosome abnormalities which clinically manifested as oligozoospermia and teratospermia. There were 204 cases (10. 33%) of sexual chromosome abnormalities and the patients were mainly characterized with Klinefelter's syndrome. Y chromosome microdeletions were detected in 109 (14.97 %) of the 728 cases of azoospermia or oligozoospermia. The most common microdeletion of Y chromosome was AZFc (62.39%) and these patients were characterized with azoospermia and oligozoospermia. Five patients (4. 59%) who suffered Y chromosome microdeletion in AZFa region and AZFb region were characterized with azoospermia. Fifteen cases (13.76%) with microdeletion in AZFb region and AZFc region were mainly characterized with azoospermia. There were 6 cases (5. 50 % ) of microdeletion in AZFa, AZFb and AZFc regions,these patients were all characterized with azoospermia. Conclusions Both Chromosome abnormalities and Y chromosome microdeletions are important causes for male infertility.
