Zhu Y S, Katz M D, Imperato-McGinley J
Department of Medicine, Cornell University Medical College, New York, NY 10021, USA.
Baillieres Clin Endocrinol Metab. 1998 Apr;12(1):83-113. doi: 10.1016/s0950-351x(98)80478-3.
Male pseudohermaphroditism due to 17 beta-hydroxysteroid dehydrogenase-3 (17 beta-HSD-3) deficiency and 5 alpha-reductase-2 (5 alpha-RD-2) deficiency provides natural human genetic models to elucidate androgen actions. To date, five 17 beta-HSD isozymes have been cloned that catalyse the oxidoreduction of androstenedione and testosterone and dihydrotestosterone (DHT), oestrone and oestradiol. Mutations in the isozyme 17 beta-HSD-3 gene are responsible for male pseudohermaphroditism due to 17 beta-HSD deficiency. The type 3 isozyme preferentially catalyses the reduction of androstenedione to testosterone and is primarily expressed in the testes. Fourteen mutations in the 17 beta-HSD-3 gene have been identified from different ethnic groups. Affected males with the 17 beta-HSD-3 gene defect have normal wolffian structures but ambiguous external genitalia at birth. Many are raised as girls but virilize at the time of puberty and adopt a male gender role. Some develop gynaecomastia at puberty, which appears to be related to the testosterone/oestradiol ratio. Two 5 alpha-reductase (5 alpha-RD) isozymes, types 1 and 2, have been identified, which convert testosterone to the more potent androgen DHT. Mutations in the 5 alpha-RD-2 gene cause male pseudohermaphroditism, and 31 mutations in the 5 alpha-RD-2 gene have been reported from various ethnic groups. Such individuals also have normal wolffian structure but ambiguous external genitalia at birth and are raised as girls. Virilization occurs at puberty, often with a gender role change. The prostate remains infantile and facial hair is decreased. Balding has not been reported.
由于17β-羟基类固醇脱氢酶-3(17β-HSD-3)缺乏和5α-还原酶-2(5α-RD-2)缺乏导致的男性假两性畸形为阐明雄激素的作用提供了天然的人类遗传模型。迄今为止,已克隆出五种17β-HSD同工酶,它们催化雄烯二酮与睾酮、双氢睾酮(DHT)、雌酮与雌二醇之间的氧化还原反应。17β-HSD-3基因的同工酶突变是导致17β-HSD缺乏所致男性假两性畸形的原因。3型同工酶优先催化雄烯二酮还原为睾酮,主要在睾丸中表达。已从不同种族群体中鉴定出17β-HSD-3基因的14种突变。患有17β-HSD-3基因缺陷的男性出生时中肾结构正常,但外生殖器模糊不清。许多人从小被当作女孩抚养,但在青春期会出现男性化,并转变为男性性别角色。有些人在青春期会出现乳腺增生,这似乎与睾酮/雌二醇的比例有关。已鉴定出两种5α-还原酶(5α-RD)同工酶,即1型和2型,它们将睾酮转化为活性更强的雄激素双氢睾酮。5α-RD-2基因的突变会导致男性假两性畸形,不同种族群体已报告了5α-RD-2基因的31种突变。这些个体出生时中肾结构也正常,但外生殖器模糊不清,从小被当作女孩抚养。青春期会出现男性化,通常伴有性别角色的转变。前列腺仍处于幼稚状态,面部毛发减少。尚未有脱发的报道。
