Schneider G, Genel M, Bongiovanni A M, Goldman A S, Rosenfield R L
J Clin Invest. 1975 Apr;55(4):681-90. doi: 10.1172/JCI107977.
A partial testicular defect in testosterone secretion has been documented in a pubertal male with a congenital adrenal hyperplasia due to hereditary deficiency of the delta5-isomerase-3beta-hydroxysteroid dehydrogenase enzyme complex (delta5-3beta-HSD). Diagnosis of the enzymatic defect is based on the clinical picture of ambiguous genitalia and salt-losing crisis in infancy, together with high urinary delta5-pregnenetriol and plasma dehydroepiandrosterone when the patient was taken off replacement corticoid treatment. No hormonal response to ACTH or salt deprivation was demonstrable. In addition, in vivo studies revealed a partial enzymatic defect in the testis. Although plasma testosterone was low-normal (250 ng/100 ml), plasma delta5-androstenediol was markedly elevated and rose to a greater extent than testosterone after human chorionic gonadotropin administration. In vitro testicular incubation studies suggested a testicular delta5-3beta-HSD enzyme defect with less delta4 products formed from delta5 precursors than in a control testis. Histochemical studies of the testis were also consistent with this defect. Testicular biopsy revealed spermatogenic arrest, generally diminished Leydig cells, but with focal areas of Leydig cell hyperplasia as well as benign Leydig cell hyperplasia as well as benign Leudig cell nodules within the spermatic cord. In vivo studies of steroid metabolism suggested intact peripheral or hepatic delta5-3beta-HSD activity. These studies imply that delta5-3beta-HSD activity differs in the gonad, adrenal, and peripheral organs. These findings are compatible with the concept that the enzyme complex consists of subunits and/or that enzymes in these organs are under different genetic control.
一名青春期男性因遗传性δ5-异构酶-3β-羟类固醇脱氢酶复合物(δ5-3β-HSD)缺乏导致先天性肾上腺皮质增生,已被证实存在睾丸雄激素分泌部分缺陷。酶缺陷的诊断基于婴儿期外生殖器模糊和失盐危象的临床表现,以及患者停止皮质激素替代治疗时尿中δ5-孕烯三醇水平升高和血浆脱氢表雄酮水平升高。未观察到对促肾上腺皮质激素(ACTH)或限盐的激素反应。此外,体内研究显示睾丸存在部分酶缺陷。尽管血浆睾酮水平处于低正常范围(250 ng/100 ml),但血浆δ5-雄烯二醇水平显著升高,且在给予人绒毛膜促性腺激素后,其升高幅度大于睾酮。体外睾丸孵育研究提示睾丸δ5-3β-HSD酶存在缺陷,与对照睾丸相比,由δ5前体形成的δ4产物减少。睾丸组织化学研究也与该缺陷相符。睾丸活检显示生精停滞,间质细胞总体减少,但存在间质细胞增生灶以及精索内的良性间质细胞增生和良性间质细胞结节。类固醇代谢的体内研究提示外周或肝脏的δ5-3β-HSD活性正常。这些研究表明,δ5-3β-HSD活性在性腺、肾上腺和外周器官中存在差异。这些发现与酶复合物由亚基组成和/或这些器官中的酶受不同基因控制的概念相符。