队列简介:通过早期检测改善妊娠结局(改善),一个国际多中心前瞻性队列

Gillian M. Maher, Louise C. Kenny, Kate Navaratnam, Zarko Alfirevic, Darina Sheehan, Philip N. Baker, Christian Gluud, Robin Tuytten, Marius Kublickas, Boel Niklasson, Johannes J. Duvekot, Caroline B. van den Berg, Pensee Wu, Karolina Kublickiene, Fergus P. McCarthy, Ali S. Khashan
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引用次数: 0

摘要

背景:通过早期检测改善妊娠结局(Improved)是一项多中心、欧洲IIa期临床研究。改进的主要目的是使基于新兴生物标志物技术的创新原型子痫前期风险评估测试能够进行评估和改进。在这里,我们描述了改进的概况,并邀请研究人员进行合作。方法在2013年11月至2017年8月期间,从爱尔兰(N= 1501)、英国(N= 1108)、荷兰(N=810)和瑞典(N=619)的产科单位招募4038例低风险无产单胎妊娠。参与者在妊娠~11周(可选访问)、~15周、~20周、~34周(可选访问)和产后(分娩后72小时内)由一名研究助产士进行访谈。临床数据包括妊娠~15周时收集的产妇社会人口学、病史和生活方式因素信息,以及每次研究访问时收集的产妇测量数据。生物库样本包括在所有单位妊娠期间每次研究访问时收集的血液、尿液和头发,以及在爱尔兰和瑞典出生时收集的脐带/血液样本。74.0% (N= 2922)为无并发症妊娠,3.1% (N=122)为子痫前期,3.6% (N=143)为自发性早产,10.5% (N=416)为小于胎龄儿。我们在妊娠15周和20周时对一组代谢物生物标志物和一组蛋白质生物标志物进行了子痫前期风险评估。由于技术问题和测试要求的变化,商业实体将其转化为临床应用的测试受到阻碍。蛋白质小组的工作被放弃,而使用代谢物生物标志物进行子痫前期风险评估的工作仍在进行中。根据改进研究的最初目标,数据和生物库现在可用于国际合作,以对不良妊娠结局的原因和预防进行高质量的研究。
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Cohort profile: Improved Pregnancy Outcomes via Early Detection (IMPROvED), an International Multicentre Prospective Cohort
Background Improved Pregnancy Outcomes via Early Detection (IMPROvED) is a multi-centre, European phase IIa clinical study. The primary aim of IMPROvED is to enable the assessment and refinement of innovative prototype preeclampsia risk assessment tests based on emerging biomarker technologies. Here we describe IMPROvED’s profile and invite researchers to collaborate. Methods A total of 4,038 low-risk nulliparous singleton pregnancies were recruited from maternity units in Ireland (N=1,501), United Kingdom (N=1,108), The Netherlands (N=810), and Sweden (N=619) between November 2013 to August 2017. Participants were interviewed by a research midwife at ~11 weeks (optional visit), ~15 weeks, ~20 weeks, ~34 weeks’ gestation (optional visit), and postpartum (within 72-hours following delivery). Findings to date Clinical data included information on maternal sociodemographic, medical history, and lifestyle factors collected at ~15 weeks’ gestation, and maternal measurements, collected at each study visit. Biobank samples included blood, urine, and hair collected at each study visit throughout pregnancy in all units plus umbilical cord/blood samples collected at birth in Ireland and Sweden. A total of 74.0% (N=2,922) had an uncomplicated pregnancy, 3.1% (N=122) developed preeclampsia, 3.6% (N=143) had a spontaneous preterm birth, and 10.5% (N=416) had a small for gestational age baby. We evaluated a panel of metabolite biomarkers and a panel of protein biomarkers at 15 weeks and 20 weeks’ gestation for preeclampsia risk assessment. Their translation into tests with clinical application, as conducted by commercial entities, was hampered by technical issues and changes in test requirements. Work on the panel of proteins was abandoned, while work on the use of metabolite biomarkers for preeclampsia risk assessment is ongoing. Future plans In accordance with the original goals of the IMPROvED study, the data and biobank are now available for international collaboration to conduct high quality research into the cause and prevention of adverse pregnancy outcomes.
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