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孕早期不良妊娠结局的预测因素。

First trimester predictors of adverse pregnancy outcomes.

作者信息

Brameld Kate J, Dickinson Jan E, O'Leary Peter, Bower Carol, Goldblatt Jack, Hewitt Beverley, Murch Ashleigh, Stock Rosanne

机构信息

Office of Population Health Genomics, Department of Health, East Perth, Western Australia, Australia.

出版信息

Aust N Z J Obstet Gynaecol. 2008 Dec;48(6):529-35. doi: 10.1111/j.1479-828X.2008.00912.x.

Abstract

AIM

To identify first trimester indicators of adverse pregnancy outcomes.

METHOD

Data were obtained from the statewide evaluation of first trimester screening for Down syndrome in Western Australia which included 22,695 pregnancies screened between August 2001 and October 2003. Screening data were linked with pregnancy outcome information from the Hospital Morbidity Database and the Birth Defects Registry. The odds ratios (OR) of adverse outcomes were analysed for combined risk incorporating maternal age, nuchal translucency (NT) and biochemical parameters and then separately for each parameter (pregnancy-associated plasma protein-A (PAPP-A), free beta human chorionic gonadotropin (beta-hCG) and NT).

RESULTS

Risk assessments for first trimester combined screening are derived from maternal age, ultrasound measurement of fetal NT, maternal serum free beta-hCG and PAPP-A. Increased combined risk for Down syndrome was significantly (P < 0.01) associated with spontaneous loss at or before 24 weeks gestation (OR 13.51), birth defects (OR 6.58) and preterm birth at or before 32 weeks gestation (OR 3.2). Maternal serum PAPP-A below the 5th centile was associated with Down syndrome (OR 8.43), spontaneous loss before 24 weeks (OR 5.04) and later than 24 weeks (OR 4.50), preterm delivery before 32 weeks (OR 3.11) and before 37 weeks (OR 2.24). NT above the 95th centile was associated with Down syndrome (OR 43.91), birth defects (OR 4.02) and spontaneous loss before 24 weeks (OR 6.24). Low levels of free beta-hCG and increased NT were less consistently associated with adverse outcomes and high levels of free beta-hCG showed limited use as an indicator. The detection rates for all outcomes other than Down syndrome were less than 40%.

CONCLUSION

Biochemical indicators and NT that are measured during first trimester screening for Down syndrome show a number of associations with adverse outcomes, but do not show appropriate performance characteristics for screening tests. These data are consistent with the view that the individual components, specifically low PAPP-A levels alone, do not provide an effective screening tool for adverse pregnancy outcomes.

摘要

目的

确定孕早期不良妊娠结局的指标。

方法

数据来自西澳大利亚州对孕早期唐氏综合征筛查的全州评估,其中包括2001年8月至2003年10月期间筛查的22,695例妊娠。筛查数据与医院发病率数据库和出生缺陷登记处的妊娠结局信息相关联。分析了合并风险(包括孕妇年龄、颈项透明层(NT)和生化参数)的不良结局的比值比(OR),然后分别分析每个参数(妊娠相关血浆蛋白-A(PAPP-A)、游离β人绒毛膜促性腺激素(β-hCG)和NT)的比值比。

结果

孕早期联合筛查的风险评估源自孕妇年龄、胎儿NT的超声测量、孕妇血清游离β-hCG和PAPP-A。唐氏综合征合并风险增加与妊娠24周及以前的自然流产(OR 13.51)、出生缺陷(OR 6.58)以及妊娠32周及以前的早产(OR 3.2)显著相关(P < 0.01)。孕妇血清PAPP-A低于第5百分位数与唐氏综合征(OR 8.43)、24周前自然流产(OR 5.04)和24周后自然流产(OR 4.50)、32周前早产(OR 3.11)和37周前早产(OR 2.24)相关。NT高于第95百分位数与唐氏综合征(OR 43.91)、出生缺陷(OR 4.02)和24周前自然流产(OR 6.24)相关。游离β-hCG水平低和NT增加与不良结局的相关性不太一致,游离β-hCG水平高作为指标的用途有限。除唐氏综合征外,所有结局的检出率均低于40%。

结论

孕早期唐氏综合征筛查期间测量的生化指标和NT与不良结局存在多种关联,但不具备筛查试验的合适性能特征。这些数据与以下观点一致,即单独的各个成分,特别是单独的低PAPP-A水平,不能为不良妊娠结局提供有效的筛查工具。

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