46,XX男性综合征与47,XXY克氏综合征患者相比的临床、内分泌和表观遗传学特征。
Clinical, endocrinological, and epigenetic features of the 46,XX male syndrome, compared with 47,XXY Klinefelter patients.
作者信息
Vorona Elena, Zitzmann Michael, Gromoll Jörg, Schüring Andreas N, Nieschlag Eberhard
机构信息
Institute of Reproductive Medicine, University Clinics of Münster, D-48129 Münster, Germany.
出版信息
J Clin Endocrinol Metab. 2007 Sep;92(9):3458-65. doi: 10.1210/jc.2007-0447. Epub 2007 Jun 19.
CONTEXT
The 46,XX male syndrome represents a rare, poorly characterized form of male hypogonadism.
OBJECTIVE
The objective of the study was to distinguish the 46,XX male syndrome from the more frequent 47,XXY-Klinefelter syndrome in regard to clinical, hormonal, and epigenetic features.
DESIGN
This was a case-control study.
SETTING
The study was conducted at a university-based reproductive medicine and andrology institution.
PATIENTS
Eleven SRY-positive 46,XX males were compared with age-matched controls: 101 47,XXY Klinefelter patients, 78 healthy men, and 157 healthy women [latter all heterozygous for androgen receptor (AR) alleles].
INTERVENTIONS
There were no interventions.
MAIN OUTCOME MEASURES
There was a comparison of phenotype, endocrine profiles, and X-chromosomal inactivation patterns of AR alleles.
RESULTS
The 46,XX males were significantly smaller than Klinefelter patients or healthy men, resembling female controls in height and weight. The incidence of maldescended testes was significantly higher than that in Klinefelter patients and controls. Gynecomastia was more frequent in comparison with controls, whereas there was a nonsignificant trend in comparison with Klinefelter patients. All XX males were infertile and most were hypogonadal. The inactivation patterns of AR alleles in XX males were significantly more skewed than in Klinefelter patients and women. Seven of 10 heterozygous XX male patients displayed an extreme skewing of more than 80% with no preference toward the shorter or longer AR allele. The length of the AR CAG repeat polymorphism was positively related to traits of hypogonadism.
CONCLUSIONS
XX males are distinctly different from Klinefelter patients in terms of clinical and epigenetic features. Nonrandom X chromosome inactivation ratios are common in XX males, possibly due to the translocated SRY gene. The existence of a Y-chromosomal, growth-related gene is discussed.
背景
46,XX男性综合征是一种罕见的、特征不明的男性性腺功能减退形式。
目的
本研究的目的是在临床、激素和表观遗传特征方面,将46,XX男性综合征与更常见的47,XXY-克兰费尔特综合征区分开来。
设计
这是一项病例对照研究。
地点
该研究在一家大学附属生殖医学与男科机构进行。
患者
11名SRY阳性的46,XX男性与年龄匹配的对照组进行比较:101名47,XXY克兰费尔特患者、78名健康男性和157名健康女性[后者均为雄激素受体(AR)等位基因杂合子]。
干预措施
无干预措施。
主要观察指标
比较表型、内分泌谱和AR等位基因的X染色体失活模式。
结果
46,XX男性明显比克兰费尔特患者或健康男性矮小,身高和体重与女性对照组相似。隐睾发生率显著高于克兰费尔特患者和对照组。与对照组相比,男性乳房发育更为常见,而与克兰费尔特患者相比则有不显著的趋势。所有XX男性均不育,大多数性腺功能减退。XX男性中AR等位基因的失活模式比克兰费尔特患者和女性明显更偏斜。10名杂合子XX男性患者中有7名表现出超过80%的极端偏斜,对较短或较长的AR等位基因无偏好。AR CAG重复多态性的长度与性腺功能减退特征呈正相关。
结论
XX男性在临床和表观遗传特征方面与克兰费尔特患者明显不同。非随机的X染色体失活比例在XX男性中很常见,可能是由于SRY基因易位所致。讨论了Y染色体上与生长相关基因的存在。
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