急性人类 knowlesi 疟原虫感染中以抗炎细胞因子为主导。
Anti-inflammatory cytokines predominate in acute human Plasmodium knowlesi infections.
机构信息
Division of Clinical Sciences, Infection and Immunity Research Centre, St George's University of London, London, United Kingdom.
出版信息
PLoS One. 2011;6(6):e20541. doi: 10.1371/journal.pone.0020541. Epub 2011 Jun 8.
Plasmodium knowlesi has entered the human population of Southeast Asia. Naturally acquired knowlesi malaria is newly described with relatively little available data, including data on the host response to infection. Therefore pre-treatment cytokine and chemokine profiles were determined for 94 P. knowlesi, and for comparison, 20, P. vivax and 22 P. falciparum, patients recruited in Malaysian Borneo. Nine, five and one patient with P. knowlesi, P. falciparum and P. vivax respectively had complicated malaria as defined by World Health Organisation. Patients with uncomplicated P. knowlesi had lower levels of the pro-inflammatory cytokines IL-8 and TNFα than those with complicated disease (both p<0.05, Dunn's post test, DPT). The anti-inflammatory cytokines IL-1ra and IL-10 were detected in all patients in the study. IL-1ra, the most abundant cytokine measured, correlated with parasitaemia in P. knowlesi (r(s) = 0.47, p = <0.0001), P. vivax (r(s) = 0.61, p = 0.0042) and P. falciparum (r(s) = 0.57,p = 0.0054) malaria. IL-10 correlated with parasitaemia in both P. knowlesi (r(s) = 0.54, p = <0.0001) and P. vivax (r(s) = 0.78, p = <0.0001) infections. There were between group differences in soluble markers of macrophage activation (MIP-1β and MCP-1). P. knowlesi patients had significantly lower levels of MIP-1β than P. falciparum (DPT, p = <0.01). Uncomplicated P. knowlesi patients had significantly lower levels of MCP-1 than uncomplicated P. falciparum patients (DPT, p = <0.001). There was no significant difference between complicated and uncomplicated P. knowlesi infections. MCP-1, MIP-1β, IL-8 and TNFα increased in complicated P. knowlesi but decreased in complicated P. falciparum infections. Descriptions of human knowlesi malaria provide a comparative means to discover mediators of pathophysiology in severe P. knowlesi as well as P. falciparum malaria. Crucially, P. knowlesi may be the disease and experimental primate model for severe malaria.
疟原虫 knowlesi 已进入东南亚的人类群体。新描述了自然获得的 knowlesi 疟疾,但其相关数据相对较少,包括宿主对感染的反应数据。因此,对 94 例疟原虫 knowlesi、20 例疟原虫 vivax 和 22 例疟原虫 falciparum 患者进行了治疗前细胞因子和趋化因子谱分析。在研究中,分别有 9、5 和 1 例疟原虫 knowlesi、疟原虫 falciparum 和疟原虫 vivax 患者患有世界卫生组织定义的复杂疟疾。患有无并发症疟原虫 knowlesi 的患者的促炎细胞因子 IL-8 和 TNFα 水平低于患有并发症的患者(均 p<0.05,Dunn 事后检验,DPT)。研究中的所有患者均检测到抗炎细胞因子 IL-1ra 和 IL-10。IL-1ra 是测量到的最丰富的细胞因子,与疟原虫 knowlesi(r(s)=0.47,p<0.0001)、疟原虫 vivax(r(s)=0.61,p=0.0042)和疟原虫 falciparum(r(s)=0.57,p=0.0054)的寄生虫血症相关。IL-10 与疟原虫 knowlesi(r(s)=0.54,p<0.0001)和疟原虫 vivax(r(s)=0.78,p<0.0001)感染的寄生虫血症相关。巨噬细胞活化的可溶性标志物(MIP-1β 和 MCP-1)存在组间差异。疟原虫 knowlesi 患者的 MIP-1β 水平明显低于疟原虫 falciparum(DPT,p<0.01)。无并发症的疟原虫 knowlesi 患者的 MCP-1 水平明显低于无并发症的疟原虫 falciparum 患者(DPT,p<0.001)。复杂和无并发症的疟原虫 knowlesi 感染之间没有显着差异。复杂疟原虫 knowlesi 感染中 MCP-1、MIP-1β、IL-8 和 TNFα 增加,但复杂疟原虫 falciparum 感染中减少。对人类 knowlesi 疟疾的描述为发现严重疟原虫 knowlesi 以及疟原虫 falciparum 疟疾的病理生理学介质提供了一种比较手段。至关重要的是,疟原虫 knowlesi 可能是严重疟疾的疾病和实验灵长类动物模型。
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