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Late pregnancy thyroid-binding globulin predicts perinatal depression

机译:妊娠晚期甲状腺结合球蛋白可预测围产期抑郁

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Previously we found that late pregnancy total and free thyroxine (TT4, FT4) concentrations were negatively related to greater pre and/or postpartum depressive symptoms. In a much larger cohort, the current study examined whether these thyroid indices measured earlier in the third trimester (31-33 weeks) predict subsequent perinatal depression and anxiety ratings as well as syndromal depression. Thyroid-binding globulin (TBG) concentrations increase markedly during pregnancy and may be an index of sensitivity to elevated estrogen levels. TBG was examined in this study because prior findings suggest that postpartum depression is related to sensitivity to mood destabilization by elevated sex hormone concentrations during pregnancy. Our cohort was 199 euthyroid women recruited from a public health obstetrics clinic (63.8% Hispanic, 21.6% Black). After screening and blood draws for hormone measures at pregnancy weeks 31-33, subjects were evaluated during home visits at pregnancy weeks 35-36 as well as postpartum weeks 6 and 12. Evaluations included psychiatric interviews for current and life-time DSM-IV psychiatric history (M.I.N.I.-Plus), subject self-ratings and interviewer ratings for depression and anxiety (Edinburgh Postnatal Depression Scale, Montgomery-Asberg Depression Rating Scale; Spiel-berger State-Trait Anxiety Inventory, Hamilton Anxiety Inventory), as well as a standardized interview to obtain life-time trauma history. Numerous covariates were included in all regression analyses. Trauma and major depression history were robustly significant predictors of depression and anxiety ratings over the study period when these variables were analyzed individually or in a combined model including FT4 or TBG (p < .001). When analyzed alone, FT4 levels were a less strong but still significant predictor of all depression and anxiety ratings (p < .05) while TBG levels was a significant or nearly significant predictor of most ratings. FT4, TBG and trauma history, but not major depression history, were significant individual predictors of syndromal depression during the study period (p < .05) in single predictor models. In models combining each with trauma and major depression history, FT4 and TBG generally were not significantly predictive of depression or anxiety ratings, and FT4 was also not a significant predictor of syndromal depression: however, in the combined model TBG was a particularly strong predictor of perinatal syndromal depression (p = .005) and trauma history was also significant (p = .016). Further study of the interactions among TBG, FT4, sex hormones, trauma history and perinatal depression may provide insights into the pathophysiological basis of individual variance in vulnerability to mood destabilization by the hormone conditions of pregnancy. Published by Elsevier Ltd.
机译:以前我们发现妊娠后期总和游离甲状腺素(TT4,FT4)浓度与产前和/或产后抑郁症状加重负相关。在一个更大的队列中,当前的研究检查了在孕晚期(31-33周)较早测量的这些甲状腺指数是否可以预测随后的围产期抑郁和焦虑等级以及综合症抑郁。甲状腺结合球蛋白(TBG)的浓度在怀孕期间显着增加,可能是对雌激素水平升高的敏感性指标。在这项研究中检查了TBG,因为先前的发现表明,产后抑郁与怀孕期间性激素浓度升高对情绪不稳定的敏感性有关。我们的队列是从公共卫生产科诊所招募的199名甲状腺功能正常的女性(西班牙裔63.8%,黑人21.6%)。在妊娠第31-33周进行筛查和抽血以测定激素水平之后,在妊娠35-36周以及产后第6和12周对家访进行评估,评估包括对当前和终生DSM-IV精神病学的精神病学访谈。历史(MINI-Plus),受试者对抑郁和焦虑的自我评估和访问者评估(爱丁堡产后抑郁量表,蒙哥马利-阿斯伯格抑郁量表;斯皮尔-伯杰州特质焦虑量表,汉密尔顿焦虑量表),以及标准化的采访以获取终生创伤史。所有回归分析中都包含许多协变量。当这些变量被单独或在包括FT4或TBG在内的组合模型中进行分析时,在研究期内,创伤和重度抑郁史是抑郁和焦虑等级的有力预测指标(p <.001)。单独分析时,FT4水平不是所有抑郁和焦虑评分的强力指标,但仍是重要指标(p <.05),而TBG水平是大多数抑郁指标或重要指标的重要指标。在单一预测模型中,FT4,TBG和创伤史,但不是严重的抑郁史,是研究期间综合征抑郁的重要个体预测因子(p <.05)。在将创伤和严重抑郁史结合起来的模型中,FT4和TBG通常不能显着预测抑郁或焦虑程度,而FT4也不是综合征抑郁的重要预测因子;但是,在合并模型中,TBG尤其是对抑郁症的强烈预测围产期综合征(p = .005)和创伤史也很明显(p = .016)。进一步研究TBG,FT4,性激素,创伤史和围生期抑郁症之间的相互作用可能为洞悉因妊娠激素状况而导致情绪不稳定的个体差异的病理生理基础提供见解。由Elsevier Ltd.发布

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