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首页> 外文期刊>Infection and immunity >Effects of Concomitant Schistosoma haematobium Infection on the Serum Cytokine Levels Elicited by Acute Plasmodium falciparum Malaria Infection in Malian Children
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Effects of Concomitant Schistosoma haematobium Infection on the Serum Cytokine Levels Elicited by Acute Plasmodium falciparum Malaria Infection in Malian Children

机译:伴随性血吸虫血吸虫感染对马里儿童急性恶性疟原虫疟疾感染引起的血清细胞因子水平的影响

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Polyparasitism is common in the developing world, and interactions that alter disease severity may occur. We previously demonstrated that infection with Schistosoma hematobium was associated with protection against Plasmodium falciparum infection in children who were 4 to 8 years old. In this study, we determined whether underlying helminth infections affected the cytokine responses to acute falciparum malaria. A total of 338 schistosomiasis-positive [Sch(+)] children who were 4 to 14 years old were matched by age, residence, and sex with 338 schistosomiasis-negative [Sch(?)] children and monitored for a malaria transmission season (25 weeks). Serologic cytokine levels were measured at the time of the first clinical malaria episode and in children who did not contract malaria. Elevated background levels of interleukin-6 (IL-6) (37.1 pg/ml versus 10.9 pg/ml [P = 0.04]), IL-4 (27.7 pg/ml versus 6.9 pg/ml [P = 0.02]), IL-10 (18.2 pg/ml versus 7.2 pg/ml [P < 0.001]), and gamma interferon (18.2 pg/ml versus 4.7 pg/ml [P = 0.006]) were noted in Sch(+) children compared to Sch(?) children without malaria. IL-6 and IL-10 levels were elevated in association with acute malaria, but the levels appeared to be blunted in Sch(+) children compared to Sch(?) children who were 4 to 8 years old (for IL-6, 96.2 pg/ml versus 137.2 pg/ml [P = 0.08]; for IL-10, 195.9 pg/ml versus 282.2 pg/ml [P = 0.06]). The level of IL-10 was similarly lower in Sch(+) children than in Sch(?) children who were 9 to 14 years old (91.2 pg/ml versus 141.2 pg/ml [P = 0.03]). IL-4 levels were inversely correlated with the time until the first malaria infection in both the Sch(+) children (P < 0.001) and the Sch(?) children (P < 0.001) who were 4 to 8 years old. We postulate that the Th2-enriched environment induced by schistosomiasis protects against malaria and alters the cytokine milieu during an actual infection.
机译:多寄生性疾病在发展中国家很普遍,并且可能发生改变疾病严重程度的相互作用。先前我们证明,血吸虫血吸虫感染与4至8岁儿童预防恶性疟原虫感染有关。在这项研究中,我们确定潜在的蠕虫感染是否影响对急性恶性疟疾的细胞因子反应。总共338名4至14岁的血吸虫病呈阳性[Sch(+)]儿童按年龄,居住地和性别与338名血吸虫病呈阴性[Sch(+)]儿童进行匹配,并监测了疟疾传播季节( 25周)。在首次临床疟疾发作时和未感染疟疾的儿童中测量血清细胞因子水平。白细胞介素6(IL-6)(37.1 pg / ml与10.9 pg / ml [ P = 0.04]),IL-4(27.7 pg / ml与6.9 pg / ml [ P = 0.02],IL-10(18.2 pg / ml与7.2 pg / ml [ P <0.001])和伽玛干扰素(18.2 pg / ml与4.7) pg / ml [ P = 0.006])在Sch(+)儿童中与没有疟疾的Sch(?)儿童相比。与急性疟疾相关的IL-6和IL-10水平升高,但与4至8岁的Sch(?)儿童相比,Sch(+)儿童的水平似乎减弱了(IL-6为96.2 pg / ml与137.2 pg / ml [ P = 0.08];对于IL-10,则为195.9 pg / ml与282.2 pg / ml [ P = 0.06])。 Sch(+)儿童的IL-10水平也比9至14岁的Sch(?)儿童低(91.2 pg / ml对141.2 pg / ml [ P = 0.03 ])。 IL-4水平与Sch(+)儿童( P <0.001)和Sch(?)儿童( P <0.001),年龄在4至8岁之间。我们假设由血吸虫病诱导的富含Th2的环境可预防疟疾并在实际感染期间改变细胞因子的环境。

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