赞比亚农村儿童因热性癫痫发作的复发率

E. Chomba, T. Taylor, W. Hauser, C. Wasterlain, N. Organek, G. Birbeck
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引用次数: 8

摘要

背景:非洲儿童发热性癫痫发作后的长期结果尚未得到很好的描述,但疟疾相关的癫痫发作是癫痫的一个危险因素。设计/方法:107例连续入院的发热性惊厥患儿(FS组)与同时入院的发热性疾病无惊厥或仅发热性疾病(FIO)患儿年龄匹配。每季度的后续评估可以阻止中期癫痫发作和发展结果。结果:214名儿童入组,平均随访20.4个月(中位24个月,模式27个月)。最常见的诊断是临床疟疾。在随访期间,FS组的儿童更容易出现反复的热性惊厥(29.9比11.3%;RR1.27;CI 1.10-1.46),非诱发性癫痫发作(27.1 vs 1.9%;RR 1.35;CI 1.20-1.52)和癫痫(11.2 vs. 0.9;RR 1.16;可信区间1.04 - -1.20)。随访期间非诱发性癫痫发作的危险因素包括入组时年龄较小(25.5 vs. 34.6个月,p=0.04)和指标疾病前发育迟缓(33.3 vs. 13.1%, p=0.009)。在FS组中,入组时有局灶性癫痫发作的儿童更有可能出现非诱发性癫痫发作(52.9 vs. 20%, p=0.007)和癫痫(41.7 vs. 7.8%, p=0.03)。结论:在赞比亚农村,因热性癫痫发作入院的儿童继发癫痫的风险很高。需要进一步研究以确定特定的感染性病因(如疟疾)是否与此类儿童的癫痫发展有关。在获得医疗保健服务有限的地方,热性癫痫发作入院也可能是预先存在的后期癫痫倾向的标志。无论如何,随访是必要的,以促进早期开始治疗,如果复发,无因性癫痫发作发生。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Seizure Recurrence in Rural Zambian Children Admitted with Febrile Seizures
Background: Long-term outcomes following febrile seizures in African children are not well described, but ma- laria-associated seizures are a risk factor for epilepsy. Design/Methods: 107 consecutive children admitted with febrile seizures (FS group) were age-matched to concurrently admitted children with febrile illness and no seizure, or febrile illness only (FIO). Quarterly follow-up assessments deter- mined interim seizures and developmental outcomes. Results: 214 children were enrolled and followed for mean 20.4 months (median 24, mode 27). The most common diag- nosis was clinical malaria. During follow-up, children in the FS group were more likely to have recurrent febrile seizures (29.9 vs. 11.3%; RR1.27; CI 1.10-1.46), an unprovoked seizure (27.1 vs. 1.9%; RR 1.35; CI 1.20-1.52) and epilepsy (11.2 vs. 0.9; RR 1.16; CI 1.04-1.20). Risk factors for unprovoked seizures during follow-up included younger age at enroll- ment (25.5 v. 34.6 months, p=0.04) and developmental delay preceding the index illness (33.3 vs. 13.1%, p=0.009). Within the FS group, children with focal seizures at enrollment were more likely to experience unprovoked seizures (52.9 vs. 20%, p=0.007) and epilepsy (41.7 vs. 7.8%, p=0.03). Conclusions: Children admitted with febrile seizures in rural Zambia have a high risk of subsequent epilepsy. Further re- search is needed to determine if specific infectious etiologies (e.g. malaria) are associated with epilepsy development in such children. Where access to healthcare services are limited, febrile seizure admission may also be a marker for a pre- existing propensity toward later epilepsy. Regardless, follow- up is warranted to facilitate early initiation of treatment if recurrent, unprovoked seizures occur.
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