Stagnaro-Green A, Roman S H, Cobin R H, el-Harazy E, Wallenstein S, Davies T F
Department of Medicine, Mount Sinai School of Medicine, New York, New York 10029.
J Clin Endocrinol Metab. 1992 Mar;74(3):645-53. doi: 10.1210/jcem.74.3.1740500.
Immune function in normal pregnancy and the postpartum period remains poorly defined. We hypothesized that a comparative study between pregnant women with normal and abnormal immune function would further our understanding of the immune mechanisms of pregnancy. We chose to study a cohort of pregnant women at risk for the development of postpartum thyroid dysfunction (PPTD) as well as a group of normal controls. We chose PPTD as the model for abnormal immune function because of the relative ease of monitoring disease development and the relatively high prevalence for PPTD reported in earlier studies. Five hundred and fifty-two women were screened for the presence of thyroid autoantibodies in the first trimester of pregnancy. Thirty-three thyroid autoantibody-positive women and 28 thyroid autoantibody-negative women were followed prospectively throughout pregnancy and 6 months into the postpartum period. Lymphocyte subset analyses, thyroid function tests, and thyroid autoantibodies (antihuman thyroglobulin and antithyroid peroxidase) were performed at defined intervals. All patients were HLA serotyped. Normal pregnancy was principally characterized by decreased CD4+ T-cells and increasing CD8+ T-cells, causing a significant fall in the CD4+/CD8+ ratio in late pregnancy and into the postpartum period. Women who developed PPTD had 1) a higher CD4+/CD8+ ratio (P = 0.04), 2) activation of T-cells in the postpartum period (P = 0.02), and 3) significantly higher thyroid autoantibody titers (antihuman thyroglobulin, P = 0.02; antithyroid peroxidase, P = 0.0018). We found an overall incidence for PPTD of 8.8%. These data demonstrated that women who were thyroid autoantibody positive in the first trimester of pregnancy had a one in three chance of developing PPTD. We observed a significant fall in the T-cell helper/suppressor ratio in normal pregnant women, which was associated with distinct T-cell subset changes. This pregnancy-initiated T-cell regulation reflected an overall suppression of immune function. The development of PPTD was a frequent postpartum event in our population and was associated with a triad of immune markers: a reduction in the normal immune suppression of pregnancy (as indicated by higher T-cell helper/suppressor ratios), enhanced postpartum T-cell activation, and elevated thyroid autoantibodies. The reduction in the degree of immune suppression was, therefore, a major factor in the development of PPTD. Our results define immunological changes that occur in normal pregnancy and distinct immunological abnormalities necessary for the development of PPTD.
正常妊娠及产后时期的免疫功能仍未明确界定。我们假设,对免疫功能正常和异常的孕妇进行比较研究,将有助于我们进一步了解妊娠的免疫机制。我们选择研究一组有产后甲状腺功能障碍(PPTD)发生风险的孕妇以及一组正常对照。我们选择PPTD作为免疫功能异常的模型,是因为监测疾病发展相对容易,且早期研究报道的PPTD患病率相对较高。在妊娠早期对552名女性进行甲状腺自身抗体筛查。33名甲状腺自身抗体阳性女性和28名甲状腺自身抗体阴性女性在整个孕期及产后6个月进行前瞻性随访。在规定时间进行淋巴细胞亚群分析、甲状腺功能测试以及甲状腺自身抗体(抗人甲状腺球蛋白和抗甲状腺过氧化物酶)检测。所有患者进行了HLA分型。正常妊娠的主要特征是CD4+ T细胞减少,CD8+ T细胞增加,导致妊娠晚期及产后CD4+/CD8+比值显著下降。发生PPTD的女性有以下情况:1)CD4+/CD8+比值较高(P = 0.04);2)产后T细胞激活(P = 0.02);3)甲状腺自身抗体滴度显著更高(抗人甲状腺球蛋白,P = 0.02;抗甲状腺过氧化物酶,P = 0.0018)。我们发现PPTD的总体发生率为8.8%。这些数据表明,妊娠早期甲状腺自身抗体阳性的女性有三分之一的几率发生PPTD。我们观察到正常孕妇的T细胞辅助/抑制比值显著下降,这与不同的T细胞亚群变化有关。这种由妊娠引发的T细胞调节反映了免疫功能的总体抑制。在我们的研究人群中,PPTD的发生是常见的产后事件,并且与一组免疫标志物相关:妊娠正常免疫抑制的降低(以较高的T细胞辅助/抑制比值表示)、产后T细胞激活增强以及甲状腺自身抗体升高。因此,免疫抑制程度的降低是PPTD发生的主要因素。我们的结果明确了正常妊娠期间发生的免疫变化以及PPTD发生所必需的明显免疫异常。
