Kramer M S, Goulet L, Lydon J, Séguin L, McNamara H, Dassa C, Platt R W, Chen M F, Gauthier H, Genest J, Kahn S, Libman M, Rozen R, Masse A, Miner L, Asselin G, Benjamin A, Klein J, Koren G
Department of Pediatrics, McGill University, 1020 Pine Avenue West, Montreal, Quebec, Canada H3A 1A2.
Paediatr Perinat Epidemiol. 2001 Jul;15 Suppl 2:104-23. doi: 10.1046/j.1365-3016.2001.00012.x.
Preterm birth is the leading cause of infant mortality in industrialised societies. Its incidence is greatly increased among the socially disadvantaged, but the reasons for this excess are unclear and have been relatively unexplored. We hypothesise two distinct sets of causal pathways and mechanisms that may explain social disparities in preterm birth. The first set involves chronic and acute psychosocial stressors, psychological distress caused by those stressors, increased secretion of placental corticotropin releasing hormone (CRH), changes in sexual behaviours or enhanced susceptibility to bacterial vaginosis and chorioamnionitis, cigarette smoking or cocaine use, and decidual vasculopathy. The second hypothesised pathway is a gene-environment interaction based on a highly prevalent mutation in the gene for methylenetetrahydrofolate reductase (MTHFR), combined with low folate intake from the diet and from prenatal vitamin supplements, consequent hyperhomocysteinemia, and decidual vasculopathy. We propose to test these hypothesised pathways and mechanisms in a nested case-control study within a prospectively recruited and followed cohort of pregnant women with singleton pregnancies who deliver at one of four Montreal hospitals that serve an ethnically and socio-economically diverse population. Following recruitment during the late first or early second trimester, participating women are seen at 24-26 weeks, when a research nurse obtains a detailed medical and obstetric history; administers several scales to assess chronic and acute stressors and psychological function; obtains blood samples for CRH, red blood cell and plasma folate, homocysteine, and DNA for the MTHFR mutation; and performs a digital and speculum examination to measure cervical length and vaginal pH and to obtain swabs for bacterial vaginosis and fetal fibronectin. After delivery, each case (delivery at < 37 completed weeks following spontaneous onset of labour or prelabour rupture of membranes) and two controls are selected for placental pathological examination, hair analysis of cotinine, cocaine, and benzoylecgonine, and analysis of stored blood and vaginal specimens. Statistical analysis will be based on multiple logistic regression and structural equation modelling, with sequential construction of models of potential aetiological determinants and covariates to test the hypothesised causal pathways and mechanisms. The research we propose should improve understanding of the factors and processes that mediate social disparities in preterm birth. This improved understanding should help not only in developing strategies to reduce the disparities but also in suggesting preventive interventions applicable across the entire socio-economic spectrum.
早产是工业化社会中婴儿死亡的主要原因。在社会弱势群体中,早产的发生率大幅上升,但这种差异的原因尚不清楚,且相对未得到充分研究。我们假设了两组不同的因果途径和机制,它们可能解释早产中的社会差异。第一组涉及慢性和急性心理社会应激源、这些应激源引起的心理困扰、胎盘促肾上腺皮质激素释放激素(CRH)分泌增加、性行为改变或对细菌性阴道病和绒毛膜羊膜炎易感性增强、吸烟或使用可卡因以及蜕膜血管病变。第二个假设途径是基于亚甲基四氢叶酸还原酶(MTHFR)基因中一种高度普遍的突变与饮食和产前维生素补充剂中低叶酸摄入相结合的基因 - 环境相互作用,随之产生的高同型半胱氨酸血症以及蜕膜血管病变。我们建议在一项巢式病例对照研究中检验这些假设的途径和机制,该研究在一个前瞻性招募并随访的单胎妊娠孕妇队列中进行,这些孕妇在蒙特利尔的四家医院之一分娩,这些医院服务于种族和社会经济背景多样的人群。在孕早期晚期或孕中期早期招募后,参与研究的女性在孕24 - 26周时接受检查,届时研究护士会获取详细的医疗和产科病史;使用多个量表评估慢性和急性应激源以及心理功能;采集血液样本检测CRH、红细胞和血浆叶酸、同型半胱氨酸以及用于检测MTHFR突变的DNA;进行指诊和窥器检查以测量宫颈长度和阴道pH值,并获取用于检测细菌性阴道病和胎儿纤连蛋白的拭子。分娩后,为进行胎盘病理检查、毛发中可替宁、可卡因和苯甲酰爱康宁分析以及储存血液和阴道标本分析,选取每例病例(在自发宫缩或胎膜早破后<37足周分娩)和两名对照。统计分析将基于多元逻辑回归和结构方程模型,通过依次构建潜在病因决定因素和协变量模型来检验假设的因果途径和机制。我们提议的这项研究应能增进对介导早产社会差异的因素和过程的理解。这种增进的理解不仅有助于制定减少差异的策略,还能为整个社会经济层面提出适用的预防干预措施提供建议。
