McIntyre P B, Berkey C S, King S M, Schaad U B, Kilpi T, Kanra G Y, Perez C M
Royal Alexandra Hospital for Children, Sydney, New South Wales, Australia.
JAMA. 1997 Sep 17;278(11):925-31. doi: 10.1001/jama.278.11.925.
To evaluate the effectiveness of dexamethasone in bacterial meningitis in the subcategories of causative organism and timing and nature of antibiotic therapy.
MEDLINE, HEALTHLINE, and AIDSLINE were searched with the Medical Subject Headings "dexamethasone" and "meningitis" in any language. Bibliographies, conference abstracts, and the authors of identified studies were consulted.
Randomized, concurrently controlled trials of dexamethasone therapy in childhood bacterial meningitis published from 1988 to November 1996 were selected. Of 16 studies identified, 5 were not eligible.
Data were extracted by means of standard outcomes in a protocol sent to all principal authors.
Random-effects meta-analysis models were used to obtain summary estimates. As the incidence of severe hearing loss differed significantly by organism among control subjects, organism-specific estimates were used. In Haemophilus influenzae type b meningitis, dexamethasone reduced severe hearing loss overall (combined odds ratio [OR], 0.31; 95% confidence interval [CI], 0.14-0.69). Similar ORs were obtained after studies were stratified by the timing of administration of dexamethasone (before or with antibiotics vs later) or by type of antibiotic (cefuroxime vs other). In pneumococcal meningitis, only studies in which dexamethasone was given early suggested protection, which was significant for severe hearing loss (combined OR, 0.09; 95% CI, 0.0-0.71) and approached significance for any neurological or hearing deficit (combined OR, 0.23; 95% CI, 0.04-1.05). For all organisms combined, the pooled OR suggested protection against neurological deficits other than hearing loss but was not significant (OR, 0.59; 95% CI, 0.34-1.02). Outcomes were similar in studies that used 2 vs more than 2 days of dexamethasone therapy. Adverse effects were not significantly increased with dexamethasone except for secondary fever. The incidence of gastrointestinal tract bleeding increased with longer duration of dexamethasone treatment (0.5% in controls, 0.8% with 2 days of treatment, 3.0% with 4 days of treatment).
The available evidence on adjunctive dexamethasone therapy confirms benefit for H influenzae type b meningitis and, if commenced with or before parenteral antibiotics, suggests benefit for pneumococcal meningitis in childhood. Limiting dexamethasone therapy to 2 days may be optimal.
评估地塞米松在细菌性脑膜炎中针对致病微生物亚类、抗生素治疗时机及性质的有效性。
使用医学主题词“地塞米松”和“脑膜炎”,以任何语言检索MEDLINE、HEALTHLINE和AIDSLINE。查阅了参考文献、会议摘要及已识别研究的作者。
选取1988年至1996年11月发表的关于儿童细菌性脑膜炎地塞米松治疗的随机、同期对照试验。在识别出的16项研究中,5项不符合要求。
通过发送给所有主要作者的方案中的标准结局来提取数据。
使用随机效应荟萃分析模型来获得汇总估计值。由于对照受试者中严重听力损失的发生率因微生物不同而有显著差异,因此使用了针对特定微生物的估计值。在b型流感嗜血杆菌脑膜炎中,地塞米松总体上降低了严重听力损失(合并比值比[OR],0.31;95%置信区间[CI],0.14 - 0.69)。在根据地塞米松给药时间(在抗生素之前或与抗生素同时使用与之后)或抗生素类型(头孢呋辛与其他抗生素)对研究进行分层后,也获得了类似的OR值。在肺炎球菌脑膜炎中,只有早期给予地塞米松的研究显示有保护作用,这对严重听力损失具有显著意义(合并OR,0.09;95% CI,0.0 - 0.71),对任何神经或听力缺陷接近显著意义(合并OR,0.23;95% CI,0.04 - 1.05)。对于所有微生物合并分析,汇总OR表明对除听力损失外的神经缺陷有保护作用,但不显著(OR,0.59;95% CI,0.34 - 1.02)。使用2天与超过2天地塞米松治疗的研究结果相似。除了继发性发热外,地塞米松并未显著增加不良反应。地塞米松治疗时间延长,胃肠道出血的发生率增加(对照组为0.5%,治疗2天为0.8%,治疗4天为3.0%)。
关于辅助使用地塞米松治疗的现有证据证实其对b型流感嗜血杆菌脑膜炎有益,并且如果在静脉注射抗生素之前或同时开始使用,提示对儿童肺炎球菌脑膜炎有益。将地塞米松治疗限制在2天可能是最佳的。
