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类风湿关节炎中下丘脑-垂体-性腺轴及肾上腺雄激素功能的紊乱:激素与该疾病关系的探索历程。

Perturbations of hypothalamic-pituitary-gonadal axis and adrenal androgen functions in rheumatoid arthritis: an odyssey of hormonal relationships to the disease.

作者信息

Masi A T, Chatterton R T, Aldag J C

机构信息

Department of Medicine, University of Illinois College of Medicine at Peoria 61656-1649, USA.

出版信息

Ann N Y Acad Sci. 1999 Jun 22;876:53-62; discussion 62-3. doi: 10.1111/j.1749-6632.1999.tb07622.x.

Abstract

Rheumatoid arthritis (RA) is a heterogeneous disease with a diverse spectrum of manifestations and course of illness. Multiple factors are believed to contribute to its etiology. Nevertheless, consistent features are observed across populations, which include (1) increased familial or immunogenetic risk in younger-onset disease; (2) female predisposition, particularly during child-bearing ages; (3) predictable clinical improvement during pregnancy and worsening postpartum; and (4) increased incidence with aging, which suggest that hormonal factors influence the disease. In 1974, serum was prospectively obtained from pre-RA cases, 4 to 20 (mean = 12.0) years prior to onset of disease and concurrently from controls (CN) matched (4 CN per 1 RA) on age (+/- 2 years), race (all Caucasians), and entry menopausal status (EMS). CN have no known rheumatic disease. Pre-RA were divided into subgroups, according to EMS, i.e., premenopausal vs. non-premenopausal (peri- or post-menopausal), and either age at entry in 1974 or age at onset of RA. For example, one 3-way subgrouping includes: I. Entry premenopausal and RA onset < age 50 years; II. Entry premenopausal and RA onset age 50+ years, and III. Entry postmenopausal. The 11 youngest pre-RA (I) had a mean entry age of 29 years and RA onset of 41 years. An alternative 4-way subgrouping (a, b, c, d) divided the female subjects into premenopausal (last menstrual period [LMP], 0-31 days) and non-premenopausal major groups, as well as younger vs. older subgroups within the major EMS categories. The younger premenopausal women in each subgrouping system, that is, I or a, overlap almost entirely. Assays (RIA) of the major sex hormones were performed, e.g., luteinizing hormone (LH); follicle stimulating (FSH); estradiol (E2); progesterone (P4); and total testosterone (T); as well as adrenal hormones, including androstenendione (A4); dehydroepiandrosterone (DHEA); its sulfate (DHEAS); and cortisol (C). A significantly lower entry mean serum DHEAS level (mumol/L) was found in the pre-RA subgroup I, than in the 43 CN (2.14 +/- 0.47 vs. 3.62 +/- 0.37, respectively, (p = 0.033). The 25 older pre-RA and 100 CN (subgroups II and III) showed close mean DHEAS levels (1.89 +/- 0.30 and 1.94 +/- 0.14, respectively, p = 0.45). The serum DHEAS levels in pre-RA vs. CN subgroups were validated in a second reference laboratory. Also, the youngest pre-RA subgroup (I) showed a significant dissociation between entry serum DHEAS and cortisol levels (r = -0.660, p = 0.027), which differed (p = 0.017) from its matched CN, and from the older pre-RA (p = 0.004). Analyses of results based upon subgroupings by EMS and entry age (a, b, c, d) showed similar results. No significant differences were found between pre-RA and CN groups in levels of serum cortisol, other adrenal steroids, or the sex hormones assayed. In a sample of younger premenopausal women, significantly low serum DHEAS levels were found 4 to 20 years prior to onset of RA. Dissociation of serum cortisol and DHEAS levels was also found in the youngest, but not older, pre-RA subjects. The data suggest that subtle adrenal cortical dysfunction, manifested mainly by adrenal androgen (AA) deficiency, may either predispose to younger-onset RA or be a long-term marker in a minority subgroup of women.

摘要

类风湿关节炎(RA)是一种具有多种临床表现和病程的异质性疾病。多种因素被认为与它的病因有关。然而,在不同人群中观察到一些一致的特征,包括:(1)年轻发病型疾病的家族或免疫遗传风险增加;(2)女性易感性,尤其是在生育年龄;(3)孕期临床症状可预测性改善,产后病情恶化;(4)发病率随年龄增长而增加,这表明激素因素影响该疾病。1974年,前瞻性地采集了RA发病前4至20年(平均 = 12.0年)的病例血清,并同时采集了年龄(±2岁)、种族(均为白种人)和进入绝经状态(EMS)匹配(每1例RA对应4例对照)的对照(CN)血清。CN无已知的风湿性疾病。根据EMS将RA发病前病例分为亚组,即绝经前与非绝经前(围绝经期或绝经后),以及1974年进入研究时的年龄或RA发病年龄。例如,一种三分法亚组包括:I. 进入研究时绝经前且RA发病年龄 < 50岁;II. 进入研究时绝经前且RA发病年龄≥50岁;III. 进入研究时绝经后。11例最年轻的RA发病前病例(I组)进入研究时的平均年龄为29岁,RA发病年龄为41岁。另一种四分法亚组(a、b、c、d)将女性受试者分为绝经前(末次月经[LMP],0 - 31天)和非绝经前两大组,以及在主要EMS类别中的年轻与年长亚组。每个亚组系统中较年轻的绝经前女性,即I组或a组,几乎完全重叠。对主要性激素进行了放射免疫分析(RIA),例如促黄体生成素(LH);促卵泡生成素(FSH);雌二醇(E2);孕酮(P4);以及总睾酮(T);还有肾上腺激素,包括雄烯二酮(A4);脱氢表雄酮(DHEA);其硫酸盐(DHEAS);以及皮质醇(C)。发现RA发病前病例I组进入研究时的血清DHEAS平均水平(μmol/L)显著低于43例对照(分别为2.14 ± 0.47与3.62 ± 0.37,(p = 0.033)。25例年龄较大的RA发病前病例和100例对照(II组和III组)的DHEAS平均水平相近(分别为1.89 ± 0.30和1.94 ± 0.14,p = 0.45)。RA发病前病例与对照亚组的血清DHEAS水平在第二个参考实验室得到验证。此外,最年轻的RA发病前病例亚组(I组)进入研究时的血清DHEAS与皮质醇水平之间存在显著分离(r = -0.660,p = 0.027),这与匹配的对照不同(p = 0.017),也与年龄较大的RA发病前病例不同(p = 0.004)。基于EMS和进入研究时年龄的亚组分析(a、b、c、d)结果相似。在血清皮质醇、其他肾上腺类固醇或所检测的性激素水平方面,RA发病前病例组与对照组之间未发现显著差异。在一组较年轻的绝经前女性样本中,发现RA发病前4至20年血清DHEAS水平显著降低。在最年轻而非年龄较大的RA发病前受试者中也发现了血清皮质醇与DHEAS水平的分离。数据表明,主要表现为肾上腺雄激素(AA)缺乏的轻微肾上腺皮质功能障碍,可能要么使患者易患年轻发病型RA,要么是少数女性亚组中的一个长期标志物。

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