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单纯疱疹病毒性脑炎

Herpes simplex encephalitis.

作者信息

Sköldenberg B

机构信息

Karolinska Institute, Department of Infectious Diseases, Danderyd Hospital, Sweden.

出版信息

Scand J Infect Dis Suppl. 1991;80:40-6.

PMID:1666445
Abstract

Diagnostic and therapeutic advances in the management of herpes simplex encephalitis (HSE) have been significant over the last decade. Serological analysis of simultaneously drawn CSF and serum samples allows reliable diagnostics of HSE, but not until after 3-10 days following the onset of neurological symptoms. Polymerase chain reaction (PCR) assay with two nested primer pairs, being developed for the amplication of HSV DNA in CSF, was applied to 151 CSF samples from 43 consecutive patients with HSE. As controls, 87 CSF samples from 60 patients with acute febrile focal encephalopathy (initially suspected to be HSE but excluded by the absence of intrathecal HSV antibody synthesis) were tested. PCR detected HSV DNA in 42/43 patients and remained positive up to 27 days after the onset of neurological symptoms. By a combination of PCR and serological analysis of intrathecal HSV antibody synthesis, aetiological diagnosis of HSE can be made by one or both methods from early disease and up to 15 years after the onset of HSE. In one Swedish and one American trial of acyclovir versus vidarabine in HSE, acyclovir 10 mg/kg 8-hourly for 10 days significantly decreased mortality as well as morbidity in the survivors. Early start of acyclovir treatment is necessary in HSE; the prognosis is correlated to age and stage of consciousness and neurological involvement at start of the therapy. Data has shown the need of neuropsychological assessment in final determination of the level of disability after HSE. The profiles and dynamics of the inflammatory cascade of cytokines from lymphocytes and other brain cells, provoked by the intracerebral HSV infection, needs to be characterized to enable understanding of the pathogenic process in HSE and hence its adequate antiinflammatory treatment.

摘要

在过去十年中,单纯疱疹病毒性脑炎(HSE)的诊断和治疗取得了重大进展。同时采集脑脊液和血清样本进行血清学分析可实现HSE的可靠诊断,但要在神经症状出现3 - 10天后才能实现。为扩增脑脊液中的HSV DNA而开发的带有两对巢式引物的聚合酶链反应(PCR)检测法,应用于43例连续HSE患者的151份脑脊液样本。作为对照,检测了60例急性发热性局灶性脑病患者(最初怀疑为HSE,但因鞘内HSV抗体合成缺失而排除)的87份脑脊液样本。PCR在42/43例患者中检测到HSV DNA,并且在神经症状出现后长达27天仍呈阳性。通过PCR和鞘内HSV抗体合成的血清学分析相结合,从疾病早期到HSE发病后15年,可通过一种或两种方法进行HSE的病因诊断。在一项瑞典和一项美国关于阿昔洛韦与阿糖腺苷治疗HSE的试验中,阿昔洛韦10mg/kg每8小时一次,共10天,显著降低了死亡率以及幸存者的发病率。HSE患者必须尽早开始阿昔洛韦治疗;预后与年龄、意识状态以及治疗开始时的神经受累情况相关。数据表明,在最终确定HSE后的残疾程度时需要进行神经心理学评估。需要对由脑内HSV感染引发的淋巴细胞和其他脑细胞炎症级联反应中细胞因子的特征和动态进行表征,以便了解HSE的致病过程,从而进行适当的抗炎治疗。

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