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Effectiveness of Intrapleural Tissue Plasminogen Activator and Dornase Alfa vs Tissue Plasminogen Activator Alone in Children with Pleural Empyema A Randomized Clinical Trial

机译:胸腔内纤溶酶原激活剂和DORNASE ALFA对组织纤溶酶原单独服用胸腔脓肿性临床试验的儿童组织纤溶酶原素活化剂的有效性

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摘要

Importance Clinical guidelines recommend that children with pleural empyema be treated with chest tube insertion and intrapleural fibrinolytics. The addition of dornase alfa (DNase) has been reported to improve outcomes in adults but remains unproven in children. Objective To determine if intrapleural tissue plasminogen activator (tPA) and DNase is more effective than tPA and placebo at reducing hospital length of stay in children with pleural empyema. Design, Setting, and Participants This multicenter, parallel-group, placebo-controlled, superiority randomized clinical trial included children diagnosed as having pleural empyema requiring drainage aged 6 months to 18 years treated at 6 tertiary Canadian children's hospitals. A total of 379 children were assessed for eligibility; 281 were excluded and 98 were randomized. One child was excluded after randomization for not meeting the inclusion criteria. Data were collected from March 4, 2013, to December 13, 2017. Interventions Participants underwent chest tube insertion and 3 daily administrations of intrapleural tPA, 4 mg, followed by DNase, 5 mg (intervention group), or 5 mL of normal saline (placebo; control group). Participants, families, clinical staff, and members of the study team were blinded to allocation. Main Outcomes and Measures The primary outcome was hospital length of stay from chest tube insertion to discharge. Secondary outcomes included time to meeting discharge criteria, time to chest tube removal, mean fever duration, additional pleural drainage procedures, hospital readmissions, and total health care cost. Results Of the 97 analyzed children with pleural empyema, 52 (54%) were male, and the mean (SD) age was 5.1 (3.6) years. A total of 49 children were randomized to tPA and DNase and 48 were randomized to tPA and placebo. Treatment with tPA and DNase was not associated with decreased hospital length of stay compared with tPA and placebo (mean [SD] length of stay, 9.0 [4.9] vs 9.1 [5.3] days; mean difference, -0.1 days; 95% CI, -2.0 to 2.1; P = .96). Similarly, no significant differences were observed for any of the secondary outcomes. Of the 14 adverse events in the tPA and DNase group, 6 (43%) were serious; of the 21 adverse events in the tPA and placebo group, 8 (38%) were serious. There were no deaths. Conclusions and Relevance The addition of DNase to intrapleural tPA for children with pleural empyema had no effect on hospital length of stay or other outcomes compared with tPA with placebo. Clinical practice guidelines should continue to support the use of chest tube insertion and intrapleural fibrinolytics alone as first-line treatment for pediatric empyema.
机译:重要性临床指南建议使用胸膜脓胸的儿童用胸管插入和骨膜纤维蛋白溶解剂进行处理。据报道,添加了Dornase Alfa(DNase)以改善成人的结果,但儿童仍未治疗。目的探讨胎儿组织纤溶酶原激活剂(TPA)和DNase是否比TPA和安慰剂在减少胸膜脓肿儿童的患者的留学期间更有效。设计,设定和参与者该多中心,并行组,安慰剂控制,优势随机临床试验包括诊断为患有6个月的胸膜脓胸胸膜脓肿,以6个月为18岁,在6岁的加拿大儿童医院治疗18岁。共有379名儿童评估资格;被排除在外,98例随机排除。随机化后,一个孩子被排除在不符合纳入标准之后。从2013年3月4日收集数据,到2017年12月13日。干预参与者接受了胸管插入和3日每日腹膜TPA,4毫克,其次是DNase,5毫克(干预组)或5ml的生理盐水(安慰剂;对照组)。参与者,家庭,临床人员和研究团队的成员被蒙蔽了分配。主要结果和措施主要结果是医院避免从胸管插入放电。次要结果包括在履行排放标准时,胸管去除时间,平均发烧持续时间,额外的胸腔引流程序,医院入伍和全面保健成本。 97分析胸膜脓肿儿童的结果,52(54%)是男性,平均(SD)年龄为5.1(3.6)年。将49名儿童随机分配给TPA,DNase和48被随机化为TPA和安慰剂。与TPA和安慰剂相比,用TPA和DNase治疗与医院的住院减少无关(平均停留时间,9.0 [4.9] Vs 9.1 [5.3];平均差异,-0.1天; 95%CI, -2.0至2.1; p = .96)。类似地,对于任何次要结果没有观察到显着差异。在TPA和DNase组的14例不良事件中,6(43%)严重;在TPA和安慰剂组中的21例不良事件中,8(38%)严重。没有死亡。结论和相关性与胸膜脓肿儿童的DNA酶添加到胸膜内TPA对与安慰剂的TPA相比,对医院的住宿或其他结果没有影响。临床实践指南应继续支持使用胸管插入和胸膜内纤维蛋白溶解,单独作为小儿脓胸的一线治疗。

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  • 来源
    《JAMA pediatrics》 |2020年第4期|共9页
  • 作者单位

    McMaster Univ McMaster Childrens Hosp Hamilton ON Canada;

    Univ Toronto Hosp Sick Children Dept Pediat 555 Univ Ave Toronto ON M5G 1X8 Canada;

    Univ Toronto Hosp Sick Children Dept Diagnost Imaging Image Guided Therapy Toronto ON Canada;

    Univ Ottawa Childrens Hosp Eastern Ontario Ottawa ON Canada;

    Univ Montreal Ctr Hosp Univ St Justine Montreal PQ Canada;

    McMaster Univ McMaster Childrens Hosp Hamilton ON Canada;

    Univ British Columbia British Columbias Childrens Hosp Dept Pediat Div Resp Med Vancouver BC;

    Univ British Columbia British Columbias Childrens Hosp Dept Pediat Div Resp Med Vancouver BC;

    Hlth Sci Ctr Winnipeg MB Canada;

    Univ Calgary Alberta Childrens Hosp Calgary AB Canada;

    Univ Calgary Alberta Childrens Hosp Calgary AB Canada;

    Univ Calgary Alberta Childrens Hosp Calgary AB Canada;

    McMaster Univ McMaster Childrens Hosp Hamilton ON Canada;

    Univ Toronto Dalla Lana Sch Publ Hlth Toronto ON Canada;

    Univ Toronto St Michaels Hosp Li Ka Shing Knowledge Inst Appl Hlth Res Ctr Toronto ON Canada;

    Univ Toronto St Michaels Hosp Li Ka Shing Knowledge Inst Appl Hlth Res Ctr Toronto ON Canada;

    Univ Toronto St Michaels Hosp Li Ka Shing Ctr Healthcare Analyt Res &

    Training Toronto ON;

    Univ Toronto Hosp Sick Children Dept Pediat 555 Univ Ave Toronto ON M5G 1X8 Canada;

    St Michaels Hosp Ctr Excellence Econ Anal Res CLEAR HUB Hlth Res Solut Toronto ON Canada;

    Univ Toronto Dalla Lana Sch Publ Hlth Toronto ON Canada;

    Univ Toronto Hosp Sick Children Dept Pediat 555 Univ Ave Toronto ON M5G 1X8 Canada;

    Univ Toronto Hosp Sick Children Dept Pediat 555 Univ Ave Toronto ON M5G 1X8 Canada;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 儿科学;
  • 关键词

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