检测胎儿纤连蛋白以降低早产风险。
Fetal fibronectin testing for reducing the risk of preterm birth.
作者信息
Berghella Vincenzo, Saccone Gabriele
机构信息
Division of Maternal Fetal Medicine, Department of Obstetrics and Gynecology, Thomas Jefferson University, 833 Chestnut Street, Level 1, Philadelphia, Pennsylvania, USA, PA 19107.
出版信息
Cochrane Database Syst Rev. 2019 Jul 29;7(7):CD006843. doi: 10.1002/14651858.CD006843.pub3.
BACKGROUND
Fetal fibronectin (FFN) is an extracellular matrix glycoprotein localized at the maternal-fetal interface of the amniotic membranes, between chorion and decidua, where it is concentrated in this area between decidua and trophoblast. In normal conditions, FFN is found at very low levels in cervicovaginal secretions. Levels greater than or equal to 50 ng/mL at or after 22 weeks have been associated with an increased risk of spontaneous preterm birth. In fact, FFN is one of the best predictors of preterm birth in all populations studied so far, and can help in selecting which women are at significant risk for preterm birth. This is an update of a review first published in 2008.
OBJECTIVES
To assess the effectiveness of management based on knowledge of FFN testing results for preventing preterm birth.
SEARCH METHODS
For this update, we searched Cochrane Pregnancy and Childbirth's Trials Register (7 September 2018), ClinicalTrials.gov, the WHO International Clinical Trials Registry Platform (ICTRP) (7 September 2018), and reference lists of retrieved studies.
SELECTION CRITERIA
Randomized controlled trials of pregnant women screened with FFN for risk of preterm birth. Studies included are based exclusively on knowledge of FFN results versus no such knowledge, and we have excluded studies including women with only positive or only negative FFN results.
DATA COLLECTION AND ANALYSIS
Two review authors independently assessed trials for inclusion and risk of bias, extracted data, and checked them for accuracy. The quality of the evidence was assessed using the GRADE approach.
MAIN RESULTS
We identified 16 trials, of which six were eligible for inclusion. The six included studies randomized 546 women with singleton gestations and threatened preterm labor (PTL) at 23 0/7 to 34 6/7 weeks. A total of 277 women were randomized to knowledge and 269 to no knowledge of FFN. No trials were identified on asymptomatic women or multiple gestations.The risk of bias of included studies was mixed. For selected important outcomes, preterm birth before 37, 34, and 32 weeks, and maternal hospitalization, we graded the quality of the evidence and created a 'Summary of findings' table. For these outcomes, the evidence was graded as mainly low quality due to the imprecision of effect estimates.Management based on knowledge of FFN results may reduce preterm birth before 37 weeks (21.6%) versus controls without such knowledge (29.2%) (risk ratio (RR) 0.72, 95% confidence interval (CI) 0.52 to 1.01; 4 trials; 357 women; low-quality evidence). However, management based on knowledge of FFN results may make little or no difference to preterm birth before 34 (RR 1.09, 95% CI 0.54 to 2.18; 4 trials; 357 women; low-quality evidence) or maternal hospitalization (RR 1.06, 95% CI 0.79 to 1.43; 5 trials; 441 women; low-quality evidence). The evidence for preterm birth before 32 weeks is uncertain because the quality was found to be very low (average RR 0.79, 95% CI 0.16 to 3.96; 4 trials; 357 women; very low-quality evidence).For all other outcomes, for which there were available data (preterm birth less than 28 weeks; gestational age at delivery (weeks); birthweight less than 2500 g; perinatal death; tocolysis; steroids for fetal lung maturity; time to evaluate; respiratory distress syndrome; neonatal intensive care unit (NICU) admission; and NICU days), knowledge of FFN results may make little or no difference to the outcomes.
AUTHORS' CONCLUSIONS: The evidence from this review suggests that management based on knowledge of FFN results may reduce preterm birth before 37 weeks. However, our confidence in this result is limited as the evidence was found to be of low quality. Effects on other substantive outcomes are uncertain due to serious concerns in study design, inconsistency, and imprecision of effect estimates. No trials were identified on asymptomatic women, or multiple gestations.Future studies are needed that include specific populations (e.g. singleton gestations with symptoms of preterm labor), a study group managed with a protocol based on the FFN results, and that report not only maternal but also important perinatal outcomes. Cost-effectiveness analyses are also needed.
背景
胎儿纤连蛋白(FFN)是一种细胞外基质糖蛋白,定位于羊膜的母胎界面,在绒毛膜和蜕膜之间,在蜕膜和滋养层之间的这个区域富集。在正常情况下,宫颈阴道分泌物中FFN水平非常低。22周及以后FFN水平大于或等于50 ng/mL与自发性早产风险增加相关。事实上,FFN是迄今为止所有研究人群中早产的最佳预测指标之一,有助于筛选出哪些女性有早产的显著风险。这是2008年首次发表的一篇综述的更新。
目的
评估基于FFN检测结果的管理措施预防早产的有效性。
检索方法
本次更新,我们检索了Cochrane妊娠与分娩试验注册库(2018年9月7日)、ClinicalTrials.gov、世界卫生组织国际临床试验注册平台(ICTRP)(2018年9月7日)以及检索到的研究的参考文献列表。
选择标准
对孕妇进行FFN筛查早产风险的随机对照试验。纳入的研究仅基于FFN结果的知晓情况与无此类知晓情况的对比,我们排除了仅纳入FFN结果为阳性或仅为阴性的女性的研究。
数据收集与分析
两位综述作者独立评估试验是否纳入及偏倚风险,提取数据并检查其准确性。使用GRADE方法评估证据质量。
主要结果
我们识别出16项试验,其中6项符合纳入标准。这6项纳入研究将546名单胎妊娠且有先兆早产(PTL)的女性随机分组,孕周为23⁰/₇至34⁶/₇周。共277名女性被随机分配至知晓FFN结果组,269名被分配至不知晓组。未识别出关于无症状女性或多胎妊娠的试验。纳入研究的偏倚风险各异。对于选定的重要结局,即37周前、34周前和32周前早产以及产妇住院情况,我们对证据质量进行了分级并创建了“结果总结”表。对于这些结局,由于效应估计不精确,证据主要被分级为低质量。基于FFN结果知晓情况的管理措施可能会降低37周前早产的发生率(21.6%),与不知晓FFN结果的对照组(29.2%)相比(风险比(RR)0.72,95%置信区间(CI)0.52至1.01;4项试验;357名女性;低质量证据)。然而,基于FFN结果知晓情况的管理措施对34周前早产(RR 1.09,95% CI 0.54至2.18;4项试验;357名女性;低质量证据)或产妇住院情况(RR 1.06,95% CI 0.79至1.43;5项试验;441名女性;低质量证据)可能影响很小或无影响。32周前早产的证据不确定,因为发现质量非常低(平均RR 0.79,95% CI 0.16至3.96;4项试验;357名女性;极低质量证据)。对于所有其他有可用数据的结局(小于28周早产;分娩孕周(周);出生体重小于2500 g;围产期死亡;宫缩抑制剂使用;促胎儿肺成熟的类固醇使用;评估时间;呼吸窘迫综合征;新生儿重症监护病房(NICU)入住;以及NICU住院天数),FFN结果的知晓情况对这些结局可能影响很小或无影响。
作者结论
本综述的证据表明,基于FFN结果知晓情况的管理措施可能会降低37周前早产的发生率。然而,我们对这一结果的信心有限,因为证据质量被发现较低。由于对研究设计、不一致性和效应估计不精确存在严重担忧,对其他实质性结局的影响尚不确定。未识别出关于无症状女性或多胎妊娠的试验。未来需要开展包括特定人群(如具有先兆早产症状的单胎妊娠)的研究,一个基于FFN结果的方案进行管理的研究组,并且不仅报告产妇结局,还报告重要的围产期结局。还需要进行成本效益分析。
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