Martens J W, Geller D H, Arlt W, Auchus R J, Ossovskaya V S, Rodriguez H, Dunaif A, Miller W L
Department of Pediatrics, University of California, San Francisco 94143-0978, USA.
J Clin Endocrinol Metab. 2000 Nov;85(11):4338-46. doi: 10.1210/jcem.85.11.6971.
Polycystic ovary syndrome (PCOS) is a common endocrine disorder affecting approximately 5-10% of women of reproductive age. The clinical features of PCOS include oligo/anovulation, hyperandrogenemia, and hyperinsulinemia. Because P450c17 is the single enzyme catalyzing both 17alpha-hydroxylase and 17,20-lyase activities in the ovary and adrenal, some have suggested that defects in P450c17 may cause the hyperandrogenism of PCOS. Previous studies have shown that serine hyperphosphorylation of P450c17 increases the enzyme's 17,20-lyase activity, thereby favoring androgen production, and that serine phosphorylation of the insulin receptor beta-chain (IR-beta) inhibits IR-beta tyrosine phosphorylation, causing insulin resistance in vitro. We previously suggested that a gain of function mutation in a single serine kinase might cause the hyperandrogenism and insulin resistance observed in PCOS patients by excessive phosphorylation of both P450c17 and IR-beta. To test this hypothesis, we obtained fibroblasts from nine previously studied patients: three controls, three PCOS patients with normal levels of IR-beta serine phosphorylation, and three PCOS patients with increased levels of IR-beta serine phosphorylation. Initial studies showed that such skin fibroblasts could not be transfected effectively by calcium phosphate, diethylaminoethyl-dextran, lipofection or adenovirus procedures. Therefore, we employed a retroviral infection system to stably express human P450c17 in the primary cultures of fibroblast cells from the PCOS patients and controls and measured the resulting 17alpha-hydroxylase and 17,20-lyase activity. The cells were analyzed in a blinded fashion until the study was complete. The 17alpha-hydroxylase and 17,20-lyase activities in each cell line correlated well with the amount of P450c17 protein expressed, but there was no correlation between either enzymatic activity (or their ratio) with the clinical phenotype of the cells' donors even when results were corrected for the number of P450c17 complementary DNA inserts per cell line. Overnight incubation with 1 micromol/L insulin also did not affect enzymatic activity. Thus, we were unable to find evidence for the hypothesis that in PCOS a single abnormal kinase hyperphosphorylates both IR-beta, causing insulin resistance, and P450c17, causing hyperandrogenism. However, because fibroblasts do not normally express either P450c17 or the accessory proteins needed for its optimal activity, these results cannot exclude a role for serine phosphorylation in the hyperandrogenism and insulin resistance of PCOS.
多囊卵巢综合征(PCOS)是一种常见的内分泌紊乱疾病,影响着约5%-10%的育龄女性。PCOS的临床特征包括少排卵/无排卵、高雄激素血症和高胰岛素血症。由于P450c17是卵巢和肾上腺中唯一催化17α-羟化酶和17,20-裂解酶活性的酶,因此有人认为P450c17缺陷可能导致PCOS的高雄激素血症。先前的研究表明,P450c17的丝氨酸过度磷酸化会增加该酶的17,20-裂解酶活性,从而有利于雄激素的产生,并且胰岛素受体β链(IR-β)的丝氨酸磷酸化会抑制IR-β酪氨酸磷酸化,在体外导致胰岛素抵抗。我们先前曾提出,单一丝氨酸激酶的功能获得性突变可能通过P450c17和IR-β的过度磷酸化导致PCOS患者出现高雄激素血症和胰岛素抵抗。为了验证这一假设,我们从9名先前研究过的患者身上获取了成纤维细胞:3名对照者、3名IR-β丝氨酸磷酸化水平正常的PCOS患者以及3名IR-β丝氨酸磷酸化水平升高的PCOS患者。初步研究表明,通过磷酸钙、二乙氨基乙基葡聚糖、脂质转染或腺病毒方法无法有效地转染此类皮肤成纤维细胞。因此,我们采用逆转录病毒感染系统在PCOS患者和对照者的成纤维细胞原代培养物中稳定表达人P450c17,并测量由此产生的17α-羟化酶和17,20-裂解酶活性。在研究完成之前,对细胞进行盲法分析。每个细胞系中的17α-羟化酶和17,20-裂解酶活性与所表达的P450c17蛋白量密切相关,但即使对每个细胞系中P450c17互补DNA插入片段的数量进行校正后,酶活性(或其比值)与细胞供体的临床表型之间也没有相关性。用1μmol/L胰岛素过夜孵育也不影响酶活性。因此,我们无法找到证据支持以下假设:在PCOS中,单一异常激酶会使IR-β过度磷酸化导致胰岛素抵抗,同时使P450c17过度磷酸化导致高雄激素血症。然而,由于成纤维细胞通常不表达P450c17或其最佳活性所需的辅助蛋白,这些结果不能排除丝氨酸磷酸化在PCOS的高雄激素血症和胰岛素抵抗中的作用。
