College of Health Sciences, Makerere University, Kampala, Uganda; Centre for Tropical Neuroscience, Kampala, Uganda; Centre for Tropical Medicine and Global Health, University of Oxford, Oxford, UK.
College of Health Sciences, Makerere University, Kampala, Uganda; Centre for Tropical Neuroscience, Kampala, Uganda.
Lancet Glob Health. 2024 Jul;12(7):e1149-e1158. doi: 10.1016/S2214-109X(24)00102-5. Epub 2024 May 13.
Nodding syndrome is a poorly understood neurological disorder that predominantly occurs in Africa. We hypothesised that nodding syndrome is a neuroinflammatory disorder, induced by antibodies to Onchocerca volvulus or its Wolbachia symbiont, cross-reacting with host neuronal proteins (HNPs), and that doxycycline can be used as treatment.
In this randomised, double-blind, placebo-controlled, phase 2 trial, we recruited participants from districts affected by nodding syndrome in northern Uganda. We included children and adolescents aged 8-18 years with nodding syndrome, as defined by WHO consensus criteria. Participants were randomly assigned (1:1) to receive either 100 mg doxycycline daily or placebo for 6 weeks via a computer-generated schedule stratified by skin microscopy results, and all parties were masked to group assignment. Diagnoses of O volvulus and antibodies to HNPs were made using luciferase immunoprecipitation system assays and immunohistochemistry. The primary outcome was change in the proportion with antibodies to HNPs, assessed at 24 months. All participants were included in safety analyses, and surviving participants (those with samples at 24 months) were included in primary analyses. Secondary outcomes were: change in concentrations of antibodies to HNPs at 24 months compared with baseline; proportion of participants testing positive for antibodies to O volvulus-specific proteins and concentrations of Ov16 or OVOC3261 antibodies at 24 months compared with baseline; change in seizure burden, proportion achieving seizure freedom, and the proportions with interictal epileptiform discharges on the diagnostic EEG; overall quality of life; disease severity at 24 months; and incidence of all-cause adverse events, serious adverse events, and seizure-related mortality by 24 months. This trial is registered with ClinicalTrials.gov, NCT02850913.
Between Sept 1, 2016, and Aug 31, 2018, 329 children and adolescents were screened, of whom 240 were included in the study. 140 (58%) participants were boys and 100 (42%) were girls. 120 (50%) participants were allocated to receive doxycycline and 120 (50%) to receive placebo. At recruitment, the median duration of symptoms was 9 years (IQR 6-10); 232 (97%) participants had O volvulus-specific antibodies and 157 (65%) had autoantibodies to HNPs. The most common plasma autoantibodies were to human protein deglycase DJ-1 (85 [35%] participants) and leiomodin-1 (77 [32%] participants) and, in cerebrospinal fluid (CSF), to human DJ-1 (27 [11%] participants) and leiomodin-1 (14 [6%] participants). On immunohistochemistry, 46 (19%) participants had CSF autoantibodies to HNPs, including leiomodin-1 (26 [11%]), γ-aminobutyric acid B receptors (two [<1%]), CASPR2 (one [<1%]), or unknown targets (28 [12%]). At 24 months, 161 (72%) of 225 participants had antibodies to HNPs compared with 157 (65%) of 240 at baseline. 6 weeks of doxycycline did not affect the concentration of autoantibodies to HNPs, seizure control, disease severity, or quality of life at the 24-month follow-up but substantially decreased Ov16 antibody concentrations; the median plasma signal-to-noise Ov16 ratio was 16·4 (95% CI 6·4-38·4), compared with 27·9 (8·2-65·8; p=0·033) for placebo. 14 (6%) participants died and, other than one traffic death, all deaths were seizure-related. Acute seizure-related hospitalisations (rate ratio [RR] 0·43 [95% CI 0·20-0·94], p=0·028) and deaths (RR 0·46 [0·24-0·89], p=0·028) were significantly lower in the doxycycline group. At 24 months, 96 (84%) of 114 participants who received doxycycline tested positive for antibodies to Ov16, compared with 97 (87%) of 111 on placebo (p=0·50), and 74 (65%) participants on doxycycline tested positive for antibodies to OVOC3261, compared with 57 (51%) on placebo (p=0·039). Doxycycline was safe; there was no difference in the incidence of grade 3-5 adverse events across the two groups.
Nodding syndrome is strongly associated with O volvulus and the pathogenesis is probably mediated through an O volvulus induced autoantibody response to multiple proteins. Although it did not reverse disease symptoms, doxycycline or another prophylactic antibiotic could be considered as adjunct therapy to antiseizure medication, as it might reduce fatal complications from acute seizures and status epilepticus induced by febrile infections.
Medical Research Council (UK).
For the Luo translation of the abstract see Supplementary Materials section.
点头综合征是一种尚未完全了解的神经紊乱疾病,主要发生在非洲。我们假设点头综合征是一种神经炎症性疾病,由针对旋毛虫或其沃尔巴克氏体共生体的抗体引起,这些抗体与宿主神经元蛋白(HNPs)发生交叉反应,而强力霉素可用作治疗药物。
在这项随机、双盲、安慰剂对照、2 期试验中,我们从乌干达北部受点头综合征影响的地区招募了参与者。我们纳入了符合世界卫生组织共识标准的年龄在 8-18 岁之间的点头综合征儿童和青少年。参与者按皮肤显微镜检查结果进行分层,以 1:1 的比例随机分配接受每日 100mg 强力霉素或安慰剂治疗,为期 6 周,所有参与者均对分组情况进行了盲法处理。使用荧光素酶免疫沉淀系统检测和免疫组织化学检测来确定 O 旋毛虫和针对 HNP 的抗体。主要结局是在 24 个月时针对 HNP 的抗体比例的变化。所有参与者均进行安全性分析,在 24 个月时仍存活且有样本的参与者纳入主要分析。次要结局包括:24 个月时针对 HNP 的抗体浓度与基线相比的变化;24 个月时针对 O 旋毛虫特异性蛋白的抗体阳性比例以及 Ov16 或 OVOC3261 抗体浓度与基线相比的变化;癫痫发作负担的变化、达到无癫痫发作的比例以及诊断性 EEG 上的局灶性癫痫样放电比例;整体生活质量;24 个月时的疾病严重程度;以及 24 个月时的全因不良事件、严重不良事件和与癫痫发作相关的死亡率发生率。本试验在 ClinicalTrials.gov 注册,编号为 NCT02850913。
2016 年 9 月 1 日至 2018 年 8 月 31 日期间,共有 329 名儿童和青少年接受了筛查,其中 240 名符合研究条件。140 名(58%)参与者为男性,100 名(42%)为女性。120 名(50%)参与者被分配接受强力霉素治疗,120 名(50%)接受安慰剂治疗。在入组时,症状持续时间的中位数为 9 年(IQR 6-10);232 名(97%)参与者有 O 旋毛虫特异性抗体,157 名(65%)有针对 HNP 的自身抗体。最常见的血浆自身抗体是针对人蛋白去糖基酶 DJ-1(85[35%]名参与者)和雷米定-1(77[32%]名参与者),而在脑脊液(CSF)中,针对人 DJ-1(27[11%]名参与者)和雷米定-1(14[6%]名参与者)。免疫组织化学检测显示,46 名(19%)参与者的 CSF 中有针对 HNP 的自身抗体,包括雷米定-1(26[11%])、γ-氨基丁酸 B 受体(两个[<1%])、CASPR2(一个[<1%])或未知靶标(28[12%])。在 24 个月时,225 名参与者中有 161 名(72%)有针对 HNP 的抗体,而 240 名参与者中有 157 名(65%)在基线时有针对 HNP 的抗体。6 周的强力霉素治疗并未影响针对 HNP 的抗体浓度、癫痫发作控制、疾病严重程度或 24 个月时的生活质量,但显著降低了 Ov16 抗体浓度;Ov16 血浆信号噪声比值的中位数为 16.4(95%CI 6.4-38.4),而安慰剂组为 27.9(8.2-65.8;p=0.033)。14 名(6%)参与者死亡,除了一起交通事故死亡外,所有死亡均与癫痫发作有关。癫痫相关急性住院率(率比[RR]0.43[95%CI 0.20-0.94],p=0.028)和死亡率(RR 0.46[0.24-0.89],p=0.028)在强力霉素组显著降低。在 24 个月时,接受强力霉素治疗的 114 名参与者中有 96 名(84%)针对 Ov16 的抗体检测呈阳性,而安慰剂组的 111 名参与者中有 97 名(87%)呈阳性(p=0.50),接受强力霉素治疗的 74 名参与者中有 57 名(51%)针对 OVOC3261 的抗体检测呈阳性,而安慰剂组的 57 名参与者中有 57 名(51%)呈阳性(p=0.039)。强力霉素是安全的;两组之间 3-5 级不良事件的发生率没有差异。
点头综合征与 O 旋毛虫密切相关,其发病机制可能是由 O 旋毛虫诱导的针对多种蛋白质的自身抗体反应介导的。虽然它没有逆转疾病症状,但强力霉素或其他预防性抗生素可考虑作为抗癫痫药物的辅助治疗,因为它可能降低因发热性感染引起的急性癫痫发作和癫痫持续状态的致命并发症。
医学研究委员会(英国)。
