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多发性硬化症中与病毒性上呼吸道感染相关的临床复发及磁共振成像显示的疾病活动情况。

Clinical relapses and disease activity on magnetic resonance imaging associated with viral upper respiratory tract infections in multiple sclerosis.

作者信息

Edwards S, Zvartau M, Clarke H, Irving W, Blumhardt L D

机构信息

Department of Virology, University Hospital, Nottingham, UK.

出版信息

J Neurol Neurosurg Psychiatry. 1998 Jun;64(6):736-41. doi: 10.1136/jnnp.64.6.736.

Abstract

BACKGROUND

Although the risk of clinical attacks of multiple sclerosis seems to be significantly increased with viral upper respiratory tract infections (URTI), serological evidence for the reported association remains controversial. In addition, although MRI is six to 10 times more sensitive than clinical exacerbations in indexing disease activity, any possible association between URTI and MRI activity has yet to be investigated.

OBJECTIVES

To examine the relation between URTI and disease activity, in multiple sclerosis patients participating in a placebo controlled trial of interferon beta-1a, as indexed both by clinical exacerbation rate and by the number and volume of gadolinium-diethylenetriaminepentaacetic acid (Gd-DTPA) enhancing lesions on MRI. "At risk" periods were defined around symptomatic URTI, with or without serological confirmation.

RESULTS

The relative risk of clinical relapse for serologically unconfirmed symptomatic URTI was 2.1 (p=0.004). Raised antiviral antibody titres conferred a relative risk of multiple sclerosis exacerbations that was 3.4 times higher than the "not at risk" periods (annual attack rates of 5.7 v 1.6, respectively, p=0.006). There was no definite relation between the number or the volume of active lesions on MRI and either symptomatic or serologically defined at risk periods.

CONCLUSIONS

These results confirm the previously reported association between viral infections and multiple sclerosis exacerbations and indicate that the relative risk may be even higher when viral infection is serologically confirmed. However, the results, perhaps because of the confounding effects of interferon beta-1a, do not provide convincing evidence of increased blood-brain barrier breakdown or inflammation during periods of virally induced immune stimulation.

摘要

背景

尽管多发性硬化临床发作的风险似乎会因病毒性上呼吸道感染(URTI)而显著增加,但关于所报道关联的血清学证据仍存在争议。此外,尽管磁共振成像(MRI)在反映疾病活动方面比临床病情加重敏感6至10倍,但URTI与MRI活动之间的任何可能关联尚未得到研究。

目的

在参与干扰素β-1a安慰剂对照试验的多发性硬化患者中,以临床病情加重率以及MRI上钆喷酸葡胺(Gd-DTPA)强化病灶的数量和体积为指标,研究URTI与疾病活动之间的关系。“风险期”定义为有症状的URTI前后,无论有无血清学确认。

结果

血清学未确认的有症状URTI导致临床复发的相对风险为2.1(p = 0.004)。抗病毒抗体滴度升高使多发性硬化病情加重的相对风险比“非风险期”高3.4倍(年发作率分别为5.7和1.6,p = 0.006)。MRI上活动性病灶的数量或体积与有症状或血清学定义的风险期之间没有明确关系。

结论

这些结果证实了先前报道的病毒感染与多发性硬化病情加重之间的关联,并表明病毒感染经血清学确认时相对风险可能更高。然而,这些结果可能由于干扰素β-1a的混杂作用,没有提供令人信服的证据表明在病毒诱导的免疫刺激期间血脑屏障破坏或炎症增加。

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