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中国男性Y染色体微缺失与特发性无精子症和严重少精子症患者的关系

Relationship between microdeletion on Y chromosome and patients with idiopathic azoospermia and severe oligozoospermia in the Chinese.

作者信息

Fu Junjiang, Li Luyun, Lu Guangxiu

机构信息

Laboratory of Human Reproductive Engineering, Central South University Xiangya Medical College, Changsha 410078, China.

出版信息

Chin Med J (Engl). 2002 Jan;115(1):72-5.

Abstract

OBJECTIVES

To evaluate the relationship between microdeletion or mutation on the Y chromosome and Chinese patients with idiopathic azoospermia and severe oligozoospermia and to establish a molecular detection method.

METHODS

Microdeletion or mutation detection at the AZFa (sY84 and USP9Y), AZFb, AZFc/DAZ and SRY regions of the Y chromosome. Seventy-three azoospermia and 28 severe oligozoospermia patients were evaluated using PCR and PCR-SSCP techniques.

RESULTS

Twelve of 101 patients (12%) with the AZFc/DAZ microdeletion were found, including 8 with azoospermia (11%) and 4 with severe oligozoospermia (14.3%), and 1 patient had a AZFb and AZFc/DAZ double deletion. No deletions in the AZFa or SRY regions were found. No deletions in AZFa, AZFb, AZFc/DAZ or SRY regions were found in 60 normal men who had produced one or more children.

CONCLUSIONS

Microdeletion on the Y chromosome, especially at its AZFc/DAZ regions, may be a major cause of azoospermia and severe oligozoospermia leading to male infertility in China. It is recommended that patients have genetic counseling and microdeletion detection on the Y chromosome before intracytoplasmic sperm injection.

摘要

目的

评估Y染色体微缺失或突变与中国特发性无精子症和严重少精子症患者之间的关系,并建立一种分子检测方法。

方法

对Y染色体的AZFa(sY84和USP9Y)、AZFb、AZFc/DAZ和SRY区域进行微缺失或突变检测。采用聚合酶链反应(PCR)和PCR-单链构象多态性(PCR-SSCP)技术对73例无精子症患者和28例严重少精子症患者进行评估。

结果

在101例患者中发现12例(12%)存在AZFc/DAZ微缺失,其中8例无精子症患者(11%),4例严重少精子症患者(14.3%),1例患者存在AZFb和AZFc/DAZ双重缺失。未发现AZFa或SRY区域的缺失。在60例有一个或多个孩子的正常男性中,未发现AZFa、AZFb、AZFc/DAZ或SRY区域的缺失。

结论

Y染色体微缺失,尤其是AZFc/DAZ区域的微缺失,可能是导致中国男性不育的无精子症和严重少精子症的主要原因。建议患者在进行卵胞浆内单精子注射前进行遗传咨询和Y染色体微缺失检测。

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