Comunián-Carrasco Gabriella, Peña-Martí Guiomar E, Martí-Carvajal Arturo J
Departamento de Obstetricia y Ginecología, Universidad de Carabobo, Urbanización Fundación Mendoza calle 19, 5ta etapa N° 22-40, Valencia, Estado Carabobo, Venezuela, 2001.
Cochrane Database Syst Rev. 2018 Feb 21;2(2):CD011167. doi: 10.1002/14651858.CD011167.pub2.
Gonorrhoea is a sexually transmitted infection that is caused by Neisseria gonorrhoeae, and is a major public health challenge today. N gonorrhoeae can be transmitted from the mother's genital tract to the newborn during birth, and can cause gonococcal ophthalmia neonatorum as well as systemic neonatal infections. It can also cause endometritis and pelvic sepsis in the mother. This review updates and replaces an earlier Cochrane Review on antibiotics for treating this infectious condition.
To assess the clinical effectiveness and harms of antibiotics for treating gonorrhoea in pregnant women.
We searched the Cochrane Pregnancy and Childbirth Group's Trials Register (31 May 2017), LILACS database (1982 to April 5, 2017), the WHO International Clinical Trials Registry Platform (ICTRP; April 5, 2017), ClinicalTrials.gov (April 5, 2017), the ISRCTN Registry (April 5, 2017), and Epistemonikos (April 5, 2017). We also searched reference lists of all retrieved articles.
We included randomised controlled trials (RCTs) comparing the use of antibiotics for treating gonorrhoea in pregnancy. The antibiotics could have been used alone or in combination, were administered parenterally, orally, or both, and were compared with another antibiotic.We included RCTs regardless of their publication status (published, unpublished, published as an article, an abstract, or a letter), language, or country. We applied no limits on the length of follow-up.We excluded RCTs using a cluster- or cross-over design, or quasi-RCTs.
Three review authors independently assessed trials for inclusion and risk of bias, extracted data, and checked them for accuracy.
We included two RCTs, that randomised 514 pregnant women (347 women analysed) at a mean gestational age of 22 weeks. Both trials were conducted in the outpatient department of the same two hospitals in the USA between 1993 and 2001, and had a follow-up of 14 days. One of the trials was sponsored by a drug company. We considered both trials to be at a high risk of bias.One trial compared ceftriaxone (125 mg, intramuscular) with cefixime (400 mg, oral); the other trial had three arms, and assessed ceftriaxone (250 mg, intramuscular) versus either amoxicillin (3 g, oral) plus probenecid (1 g, oral) or spectinomycin (2 g, intramuscular). We did not include the spectinomycin data because this medication is no longer produced. We were unable to conduct meta-analysis because the trials compared different medications.We found inconclusive evidence that there were clear differences in the cure of gonococcal infections (genital, extragenital, or both) between intramuscular ceftriaxone versus oral amoxicillin plus oral probenecid (risk ratio (RR) 1.07, 95% confidence interval (CI) 0.98 to 1.16; one RCT; 168 women; very low-quality evidence) or intramuscular ceftriaxone versus oral cefixime (RR 0.99, 95% CI 0.91 to 1.08; one RCT; 95 women; very low-quality evidence).Neither of the trials reported on two of this review's primary maternal outcomes: incidence of obstetric complications (miscarriage, premature rupture of membranes, preterm delivery, or fetal death), or disseminated gonococcal infection, or on the incidence of neonatorum ophthalmia in the neonates.One trial reported one case of vomiting in the oral amoxacillin plus probenecid group. Trials reported pain at the injection sites, but did not quantify it. Hyperberbilurrubinemia was more frequent in neonates whose mothers were exposed to ceftriaxone. There were no clear differences between groups for neonatal malformation.
AUTHORS' CONCLUSIONS: This Cochrane Review found high levels of cure of gonococcal infections in pregnancy with the given antibiotic regimens. However, the evidence in this review is inconclusive as it does not support one particular regimen over another. This conclusion was based on very low-quality evidence (downgraded for poor trial design, imprecision) from two trials (involving 514 women), which we assessed to be at a high risk of bias for a number of domains. The harm profiles of the antibiotic regimes featured in this review remain unknown.High-quality RCTs are needed, with sufficient power to assess the clinical effectiveness and potential harms of antibiotics in pregnant women with gonorrhoea. These should be planned according to Standard Protocol Items: Recommendations for Interventional Trials (SPIRIT),conducted following CONSORT recommendations, and based on Patient-Centered Outcomes Research Institute (PCORI) outcomes.
淋病是一种由淋病奈瑟菌引起的性传播感染,是当今主要的公共卫生挑战。淋病奈瑟菌可在分娩时从母亲的生殖道传播给新生儿,可导致新生儿淋菌性眼炎以及全身性新生儿感染。它还可引起母亲的子宫内膜炎和盆腔败血症。本综述更新并取代了之前关于治疗这种感染性疾病的抗生素的Cochrane综述。
评估抗生素治疗孕妇淋病的临床有效性和危害。
我们检索了Cochrane妊娠与分娩组试验注册库(2017年5月31日)、拉丁美洲和加勒比卫生科学数据库(1982年至2017年4月5日)、世界卫生组织国际临床试验注册平台(ICTRP;2017年4月5日)、ClinicalTrials.gov(2017年4月5日)、ISRCTN注册库(2017年4月5日)和Epistemonikos(2017年4月5日)。我们还检索了所有检索到的文章的参考文献列表。
我们纳入了比较孕期使用抗生素治疗淋病的随机对照试验(RCT)。抗生素可以单独使用或联合使用,通过肌肉注射、口服或两者兼用,并与另一种抗生素进行比较。我们纳入了RCT,无论其发表状态(已发表、未发表、以文章、摘要或信函形式发表)、语言或国家。我们对随访时间长度没有限制。我们排除了采用整群或交叉设计的RCT或半随机对照试验。
三位综述作者独立评估试验是否纳入以及偏倚风险,提取数据并检查其准确性。
我们纳入了两项RCT,共随机分配了514名平均孕周为22周的孕妇(分析了347名妇女)。两项试验均于1993年至2001年在美国同一两家医院的门诊进行,随访时间为14天。其中一项试验由一家制药公司赞助。我们认为这两项试验都存在较高的偏倚风险。一项试验比较了头孢曲松(125mg,肌肉注射)与头孢克肟(400mg,口服);另一项试验有三个组,评估了头孢曲松(250mg,肌肉注射)与阿莫西林(3g,口服)加丙磺舒(1g,口服)或大观霉素(2g,肌肉注射)。我们未纳入大观霉素的数据,因为这种药物已不再生产。由于试验比较的是不同药物,我们无法进行荟萃分析。我们发现证据不确凿,即肌肉注射头孢曲松与口服阿莫西林加口服丙磺舒之间(风险比(RR)1.07,95%置信区间(CI)0.98至1.16;一项RCT;168名妇女;极低质量证据)或肌肉注射头孢曲松与口服头孢克肟之间(RR 0.99,95%CI 0.91至1.08;一项RCT;95名妇女;极低质量证据)在淋病感染(生殖器、生殖器外或两者)的治愈方面没有明显差异。两项试验均未报告本综述的两个主要产妇结局:产科并发症(流产、胎膜早破、早产或胎儿死亡)或播散性淋病感染的发生率,也未报告新生儿淋菌性眼炎的发生率。一项试验报告口服阿莫西林加丙磺舒组有1例呕吐。试验报告了注射部位疼痛,但未进行量化。母亲使用头孢曲松的新生儿中高胆红素血症更常见。两组在新生儿畸形方面没有明显差异。
本Cochrane综述发现,使用给定的抗生素方案治疗孕期淋病的治愈率较高。然而,本综述中的证据不确凿,因为它不支持一种特定方案优于另一种方案。这一结论基于两项试验(涉及五百一十四名妇女)的极低质量证据(因试验设计不佳、不精确而降级),我们评估这两项试验在多个领域存在较高的偏倚风险。本综述中所涉及的抗生素方案的危害情况仍不清楚。需要高质量的RCT,有足够的效力来评估抗生素对患有淋病的孕妇的临床有效性和潜在危害。这些试验应根据标准方案项目:干预试验建议(SPIRIT)进行规划,按照CONSORT建议开展,并基于以患者为中心的结局研究所(PCORI)的结局。
