Herrera C, Holberton J, Davis P
Pediatrics, Duke University Medical Center, DUMC 3179, Durham, North Carolina 27710, USA.
Cochrane Database Syst Rev. 2004(1):CD003480. doi: 10.1002/14651858.CD003480.pub2.
Indomethacin is a prostaglandin inhibitor used to treat patent ductus arteriosus (PDA) in preterm infants. Although indomethacin produces ductal closure in the majority of cases, it is ineffective in up to 40% of patients. Furthermore, the ductus will re-open in up to 35% of infants who initially respond to the drug. A more prolonged course of indomethacin has been studied regarding the potential to achieve higher rates of ductal closure.
To determine if a prolonged course of indomethacin (compared to a short course) reduces the rate of treatment failure in preterm infants with PDA without unwanted side-effects.
The search included review of personal files, abstracts of conferences, and the following electronic databases: MEDLINE (1966 to April 2003), EMBASE (1974 to April 2003), and Oxford Database of Perinatal Trials, Cochrane Central Register of Controlled Trials (The Cochrane Library, Issue 3, 2003). No language restrictions were applied.
The three reviewers independently abstracted data from each study. Relative risk (RR) and Risk Difference (RD) with 95% confidence intervals (CI) using the fixed effect model for meta-analysis are reported. When a statistically significant RD was found, the number needed to treat (NNT) or number needed to harm (NNH) was also calculated with 95% CIs. A chi-square test was used to test for heterogeneity of results among included trials.
Prolonged indomethacin treatment when compared to the short course resulted in a borderline statistically significant difference in PDA re-opening rate favoring the prolonged course [RR 0.54 (95% CI 0.3, 0.99); RD -0.12 (95% CI -0.24, -0.01); NNT = 8 (4, 100). There was no statistically significant treatment effect on PDA closure, re-treatment, or ligation rates. The prolonged course was associated with a decreased incidence of severe IVH [RR 0.49 (95% CI 0.25, 0.98); RD -0.12 (95% CI -0.24, -0.01); NNT 8 (4, 100)] and renal function impairment, as evidenced by a lower proportion of infants having an increased creatinine level [RR 0.52 (95% CI 0.34, 0.81); RD -0.20 (95% CI -0.33, -0.08); NNT 5 (3, 13)]. However, there was a trend for the prolonged course to increase the proportion of infants with CLD in the one trial reporting this outcome [RR 2.24 (95% CI 0.98, 5.12); RD 0.24 (95% CI 0.01, 0.47)].
Prolonged as compared to short course of indomethacin for the treatment of PDA in preterm infants has a borderline effect on reducing the rate of PDA re-opening and it may be associated with an increased risk for CLD. However, prolonged course of indomethacin appears to reduce the risk of severe intracranial hemorrhage and renal impairment in this population. Definitive recommendations about the preferred duration of indomethacin therapy, i.e. prolonged versus short course, for the treatment of PDA in premature infants cannot be made based on the current findings of this review.
There is a paucity of data on optimal duration of indomethacin therapy for the treatment of PDA, in particular for ELBW premature infants. Future randomized clinical trials should include this high risk population and investigate the premature infants. Future randomized clinical trials should include this high risk population and investigate the possibility of tailoring duration of therapy (prolonged versus short) to individual response in terms of echocardiographic findings and/or prostaglandin levels, focusing on clinically significant outcomes and potential complications associated with either strategy. In addition, factors which may influence treatment effect need to be taken into account when designing such studies.
吲哚美辛是一种前列腺素抑制剂,用于治疗早产儿动脉导管未闭(PDA)。尽管吲哚美辛在大多数情况下能使导管闭合,但在高达40%的患者中无效。此外,在最初对该药物有反应的婴儿中,高达35%的婴儿动脉导管会重新开放。关于延长吲哚美辛疗程以实现更高导管闭合率的可能性已进行了研究。
确定延长吲哚美辛疗程(与短疗程相比)是否能降低PDA早产儿的治疗失败率且无不良副作用。
检索包括查阅个人档案、会议摘要以及以下电子数据库:MEDLINE(1966年至2003年4月)、EMBASE(1974年至2003年4月)以及牛津围产期试验数据库、Cochrane对照试验中央注册库(Cochrane图书馆,2003年第3期)。未设语言限制。
1)设计与人群:随机或半随机对照试验,纳入经临床和/或超声心动图检查诊断为PDA的早产儿。2)干预措施:通过任何途径给予吲哚美辛治疗,长疗程(四剂或更多剂)与短疗程(三剂或更少剂)。3)结局指标:报告以下至少一项结局:PDA未闭合、需再次治疗、PDA重新开放、PDA结扎、死亡率、辅助通气时间、慢性肺病(CLD)、依赖补充氧气时间、脑室内出血(IVH)(全部及重度)、尿量减少、血清肌酐升高、坏死性小肠结肠炎(NEC)、出血倾向、早产儿视网膜病变(ROP)以及住院时间。
三位审阅者独立从每项研究中提取数据。采用固定效应模型进行荟萃分析,报告相对风险(RR)和风险差(RD)及95%置信区间(CI)。当发现具有统计学意义的RD时,还计算了治疗所需人数(NNT)或伤害所需人数(NNH)及95%CI。采用卡方检验来检验纳入试验结果的异质性。
与短疗程相比,延长吲哚美辛疗程在PDA重新开放率方面有边缘统计学显著差异,倾向于延长疗程[RR 0.54(95%CI 0.3,0.99);RD -0.12(95%CI -0.24,-0.01);NNT = 8(4,100)]。在PDA闭合、再次治疗或结扎率方面无统计学显著治疗效果。延长疗程与重度IVH发生率降低相关[RR 0.49(95%CI 0.25,0.98);RD -0.12(95%CI -0.24,-0.01);NNT 8(4,100)]以及肾功能损害相关,表现为肌酐水平升高的婴儿比例较低[RR 0.52(95%CI 0.34,0.81);RD -0.20(95%CI -0.33,-0.08);NNT 5(3,13)]。然而,在一项报告此结局的试验中,延长疗程有使CLD婴儿比例增加的趋势[RR 2.24(95%CI 0.98,5.12);RD 0.24(95%CI 0.01,0.47)]。
与短疗程相比,延长吲哚美辛疗程治疗早产儿PDA在降低PDA重新开放率方面有边缘效果,且可能与CLD风险增加相关。然而,延长吲哚美辛疗程似乎可降低该人群中重度颅内出血和肾功能损害的风险。基于本综述的当前结果,无法就治疗早产儿PDA时吲哚美辛治疗的首选疗程(即延长疗程与短疗程)给出明确建议。
关于吲哚美辛治疗PDA的最佳疗程,尤其是超低出生体重早产儿的数据匮乏。未来的随机临床试验应纳入这一高危人群并进行研究。未来的随机临床试验应纳入这一高危人群,并根据超声心动图结果和/或前列腺素水平针对个体反应研究调整治疗疗程(延长与短疗程)的可能性,重点关注临床显著结局以及与两种策略相关的潜在并发症。此外,设计此类研究时需考虑可能影响治疗效果的因素。
