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首页> 外文期刊>Psychoneuroendocrinology: An International Journal >Allostatic load in the association of depressive symptoms with incident coronary heart disease: The Jackson Heart Study
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Allostatic load in the association of depressive symptoms with incident coronary heart disease: The Jackson Heart Study

机译:抑郁症状与事件冠心病抑郁症状协会的樟众载荷:杰克逊心脏研究

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African Americans are at heightened risk for coronary heart disease (CHD), with biologic pathways poorly understood. We examined the role of allostatic load (AL) in the association of depressive symptoms with incident CHD among 2,670 African American men and women in the prospective Jackson Heart Study. Depressive symptoms were quantified using the Center for Epidemiologic Studies Depression Scale (CES-D). Incident CHD was ascertained by self-report, death certificate survey, and adjudicated medical record surveillance. Baseline AL was quantified using biologic parameters of metabolic, cardiovascular, immune, and neuroendocrine subsystems and as a combined meta-factor. Sequential models adjusted for demographic, socioeconomic, and behavioral covariates, stratified to examine differences by sex. Greater depressive symptomatology was associated with greater metabolic, cardiovascular, and immune AL (p-values <= 0.036) and AL meta-factor z-scores (p = 0.007), with findings driven by observations among females. Each 1-point increase in baseline depressive symptomatology, and 1-SD increase in metabolic AL, neuroendocrine AL, and AL meta-factor z-scores was associated with 3.3%, 88%, 39%, and 130% increases in CHD risk, respectively (p-values < 0.001). Neuroendocrine AL and AL meta-factor scores predicted incident CHD among males but not females in stratified analyses. Metabolic AL partially mediated the association of depressive symptoms with incident CHD (5.79% mediation, p = 0.044), a finding present among females (p = 0.016) but not males (p = 0.840). Among African American adults, we present novel findings of an association between depressive symptomatology and incident CHD, partially mediated by metabolic AL. These findings appear to be unique to females, an important consideration in the design of targeted interventions for CHD prevention.
机译:非洲裔美国人在冠心病(CHD)的风险上升,生物学途径很差。我们在预期杰克逊心脏研究中的2,670名非洲裔美国男女中,在抑郁症症状与事件CHD中的抑郁症状协会中的作用。使用流行病学研究中心(CES-D)的流行病学研究中心量化抑郁症状。通过自我报告,死亡证明调查和裁决医疗记录监督确定事件CHD。基线Al使用代谢,心血管,免疫和神经内分泌子系统的生物学参数进行量化,并作为组合的荟萃因子。调整人口统计学,社会经济和行为协变量的顺序模型,分层以检查性别的差异。更大的抑郁症状与更高的代谢,心血管和免疫A1(P值<= 0.036)和Al Meta因子Z分数(p = 0.007)相关,具有由女性的观察结果驱动的结果。基线抑郁症状的每1点增加,代谢Al,神经内分泌Al和Al Meta Z分数的1-SD增加与CHD风险的3.3%,88%,39%和130%的增加有关,分别(p值<0.001)。神经内分泌Al和Al Meta因素评分预测了男性中的事件CHD,但在分层分析中不是女性。代谢al部分介导用事件CHD(5.79%调解,P = 0.044),雌性的发现(P = 0.016)但不是男性(P = 0.840)的发现。在非洲裔美国成人中,我们在抑郁症状和事件CHD之间提出了一种关联的新发现,部分介导代谢A1。这些发现对于女性似乎是独一无二的,这是在预防CHD预防的目标干预设计中的重要考虑因素。

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