Department of Endocrinology & Metabolism, All India Institute of Medical Sciences, New Delhi 29, India.
Steroids. 2013 Dec 11;78(12-13):1159-63. doi: 10.1016/j.steroids.2013.08.010. Epub 2013 Sep 4.
T is converted to a more potent androgen, DHT by the action of microsomal membrane enzyme 5α reductase 2. Defects in 5α reductase 2 isozyme results in incomplete virilisation of external male genitalia. Mutations in SRD5A2 gene leads to diminished enzyme activity, thus hampering DHT synthesis from T. We describe two unrelated patients from India with 5αRD2 due to novel insertion of nucleotides in the exon 1 of SRD5A2 gene that lead to premature termination of protein. Master S (case 1; III.8) was 3 years old at initial evaluation, had perineoscrotal hypospadias, microphallus and both testes were palpable in the inguinal region. Master P (case 2; III.9) was born as normal full term baby. He had primary complaint of microphallus, penoscrotal hypospadias and gonads in the inguinal region. Diagnosis of 5αRD2 was made, as T/DHT ratio in the two cases was 41 and 131.2 respectively. Sequence analysis of SRD5A2 gene showed an insertion of nucleotides TA in exon 1 (c.188_189). This resulted in premature termination of the protein due to stop codon at amino acid position 7. The protein formed is drastically truncated and inadequate protein synthesized explains the phenotypic characteristics of our patients.
T 会被微粒体膜酶 5α 还原酶 2 转化为更有效的雄激素 DHT。5α 还原酶 2 同工酶的缺陷导致外部男性生殖器不完全男性化。SRD5A2 基因的突变导致酶活性降低,从而阻碍了 T 向 DHT 的合成。我们描述了来自印度的两名无关患者,他们的 5αRD2 是由于 SRD5A2 基因外显子 1 中的核苷酸插入导致蛋白质提前终止。Master S(病例 1;III.8)在最初评估时 3 岁,具有会阴阴囊性尿道下裂、小阴茎,并且两个睾丸都可在腹股沟区域触及。Master P(病例 2;III.9)出生时是正常的足月婴儿。他主要抱怨小阴茎、阴茎阴囊性尿道下裂和腹股沟区域的性腺。5αRD2 的诊断是通过两个病例中的 T/DHT 比值分别为 41 和 131.2 得出的。SRD5A2 基因的序列分析显示外显子 1 中有核苷酸 TA 的插入(c.188_189)。这导致了氨基酸位置 7 的终止密码子,从而导致蛋白质提前终止。形成的蛋白质明显截短,合成的蛋白质不足解释了我们患者的表型特征。
