Center for Human Reproduction, New York, NY 10021, USA.
Reprod Biol Endocrinol. 2013 Jun 27;11:58. doi: 10.1186/1477-7827-11-58.
Low functional ovarian reserve (FOR) is at all ages associated with low testosterone (T) levels. Causes are, however, unknown. We, therefore, investigate whether androgens with low FOR are associated with non-specific immune system activation.
322 infertile women with low and normal FOR (controls) were assessed with a broadly based immune profile, which in previous studies has proven effective in differentiating infertile patients with and without immune system activation. Patients were either immune-positive (greater than or equal to one positive tested parameter) or immune negative (no positive test). 135 suffered from prematurely diminished FOR (POA/OPOI; < age 38), 155 from physiologic diminished FOR due to age (DOR; > age 40), and 32 were controls (< age 38 with normal age-specific FOR). Prevalence of immune-positive vs. negative was assessed in all 3 patient groups.
Women with immune abnormalities, overall, demonstrated higher total T (TT, P = 0.004) and free T (FT, P < 0.001) levels than those without. The three clinical and two immunologic-defined patient groups demonstrated significant statistical interaction in mean TT (P = 0.008), with mean TT and FT in women with positive immune findings being significantly higher in control than in POA/OPOI and physiologic DOR patients (all 4 differences P < 0.001). No such differences between the three groups were seen in women without immune abnormalities.
In this study we used a definition of immune-positivity, which favors sensitivity over specificity, resulting in significant numbers of false-positives but likely only few false-negatives. The study allows suggesting the possibility of an immune system-derived androgen-production factor (APF), which maintains normal androgen levels but is deficient in women with low FOR and immune system inactivity. Existence of such an APF would suggest the presence of a still unknown functional adrenal autoimmune system.
低卵巢储备功能(FOR)在各个年龄段均与低睾酮(T)水平相关。然而,其病因尚不清楚。因此,我们研究了低 FOR 女性的雄激素是否与非特异性免疫系统激活有关。
322 名低 FOR 和正常 FOR(对照组)的不孕女性接受了广泛的免疫谱评估,该评估在之前的研究中已被证明可有效区分有无免疫系统激活的不孕患者。患者要么为免疫阳性(一项或多项检测指标阳性),要么为免疫阴性(无阳性检测结果)。135 名患者为过早 FOR 降低(POA/OPOI;<38 岁),155 名患者为因年龄导致的生理性 FOR 降低(DOR;>40 岁),32 名患者为对照组(<38 岁,年龄特异性 FOR 正常)。评估了所有 3 组患者中免疫阳性与免疫阴性的发生率。
总体而言,有免疫异常的女性的总 T(TT,P = 0.004)和游离 T(FT,P < 0.001)水平均高于无免疫异常的女性。3 个临床和 2 个免疫定义的患者组在 TT 的平均水平上表现出显著的统计学交互作用(P = 0.008),有阳性免疫发现的女性的 TT 和 FT 平均值显著高于 POA/OPOI 和生理性 DOR 患者(所有 4 个差异 P < 0.001)。在无免疫异常的女性中,这 3 组之间没有发现这种差异。
在本研究中,我们使用了一种免疫阳性的定义,这种定义有利于提高敏感性而不是特异性,因此产生了大量的假阳性结果,但可能只有少数假阴性结果。该研究提示可能存在一种源于免疫系统的雄激素产生因子(APF),该因子可维持正常的雄激素水平,但在低 FOR 和免疫系统不活跃的女性中却缺乏。这种 APF 的存在表明存在一个未知的功能性肾上腺自身免疫系统。