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[地塞米松对细菌性脑膜脑炎的支持性(抗炎)治疗]

[Supportive (antiinflammatory) treatment of bacterial meningoencephalitis with dexamethasone].

作者信息

Szychowska Z

机构信息

Kliniki Chorób Zakaźnych Wieku Dzieciecego Akademii Medycznej im. Piastów Slaskich we Wrocławiu.

出版信息

Pol Merkur Lekarski. 1997 Apr;2(10):291-4.

PMID:9377671
Abstract

With improved understanding of the pathophysiology of bacterial meningitis, a number of points in the deleterious inflammatory cascade have been identified as possible sites for modulation. Dexamethasone attenuates tissue injury by inhibiting host mediators at several steps in the inflammatory process. Animal and clinical trials have demonstrated that adjunctive corticosteroid therapy reduces the production of cytokines in the CSF. This results in decreased severity of the inflammatory process and fewer neurologic sequelae. However, routine use of steroids adjunctive treatment of bacterial meningitis remains controversial. Data support the use of adjunctive corticosteroid therapy in children with S. pneumoniae and H. influenzae type b meningitis. There is not sufficient evidence supporting the use of adjunctive corticosteroid therapy in patients with meningitis caused by N. meningitidis, which is the main cause of purulent meningitis in Poland. Also, the routine use of the dexamethasone in children and adult meningitis in Poland cannot presently be recommended. When using dexamethasone timing and dosage seems to be crucial. Administration before or with antibiotics is optimal for attenuating the subarachnoid space inflammatory response. The host's inflammatory response can be accompanied by the neuroendocrine response which is complex and its mediators are not well understood. Data indicate that the large component of the neuroendocrine response (e.g. inadequate secretion of ADH and large adrenocortical stress response) adversely affects the outcome from bacterial meningitis. So, the modulating effect of dexamethasone on both inflammatory and neuroendocrine response may be beneficial in bacterial meningitis and can probably be, achieved with sufficiently high dose of dexamethasone w has not yet been specified. Based on present pathophysiological and pharmacokinetic data, and to achieve maximum benefits and minimum complications, dexamethasone therapy started 10 min before the first dose of antibiotic and given every 12 h for only 2 days in a dose 0.8 mg/kg/day is suggested. Future studies of the pathogenesis and pathophysiology of bacterial meningitis may lead to the development of other adjunctive treatment strategies, improving the outcome of this serious disease.

摘要

随着对细菌性脑膜炎病理生理学认识的提高,有害炎症级联反应中的一些环节已被确定为可能的调节位点。地塞米松通过在炎症过程的多个步骤抑制宿主介质来减轻组织损伤。动物和临床试验表明,辅助性皮质类固醇治疗可减少脑脊液中细胞因子的产生。这导致炎症过程的严重程度降低和神经后遗症减少。然而,细菌性脑膜炎辅助使用类固醇的常规治疗仍存在争议。数据支持在患有肺炎链球菌和b型流感嗜血杆菌脑膜炎的儿童中使用辅助性皮质类固醇治疗。没有足够的证据支持在由脑膜炎奈瑟菌引起的脑膜炎患者中使用辅助性皮质类固醇治疗,脑膜炎奈瑟菌是波兰化脓性脑膜炎的主要病因。此外,目前不建议在波兰儿童和成人脑膜炎中常规使用地塞米松。使用地塞米松时,时机和剂量似乎至关重要。在使用抗生素之前或同时给药最有利于减轻蛛网膜下腔炎症反应。宿主的炎症反应可能伴有复杂的神经内分泌反应,其介质尚未完全了解。数据表明,神经内分泌反应的很大一部分(例如抗利尿激素分泌不足和肾上腺皮质应激反应过大)对细菌性脑膜炎的预后产生不利影响。因此,地塞米松对炎症和神经内分泌反应的调节作用可能对细菌性脑膜炎有益,并且可能通过尚未确定的足够高剂量的地塞米松来实现。根据目前的病理生理学和药代动力学数据,为了实现最大益处和最小并发症,建议在第一剂抗生素前10分钟开始使用地塞米松治疗,每12小时给药一次,仅持续2天,剂量为0.8mg/kg/天。未来对细菌性脑膜炎发病机制和病理生理学的研究可能会导致开发其他辅助治疗策略,改善这种严重疾病的预后。

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