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Interleukin 12 induction of interferon gamma-dependent protection against malaria.

机译:白介素12诱导干扰素对疟疾的伽马依赖性保护。

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摘要

Intraperitoneal injection of recombinant Interleukin 12 (rIL-12) at 30 ng/day for 5 days beginning 1 to 2 days before sporozoite challenge or administration of a single dose of 150 ng of rIL-122 days before challenge protected 100% of BALB/c mice against challenge with 10(2) Plasmodium yoelii sporozoites. rIL-12-induced protection was eliminated in all mice by administration of a monoclonal antibody against interferon gamma and in 50% of mice by administration of NG-monomethyl-L-arginine, a competitive inhibitor of nitric oxide synthase. rIL-12 protected BALB/c mice treated with cytotoxic anti-CD4 and anti-CD8 monoclonal antibodies, as well as T-cell- and B-cell-deficient severe combined immunodeficiency mice. These data suggest that rIL-12 stimulates non-B, non-T cells to produce interferon gamma that kills intrahepatic parasites by stimulating nitric oxide production. If rIL-12 proves to be well tolerated by humans, our findings support consideration of rIL-12 as an immunoprophylactic against malaria.
机译:在子孢子攻击前1到2天以30 ng /天腹腔注射重组白介素12(rIL-12)5天,或在攻击前单剂量注射150 ng rIL-122天保护100%的BALB / c小鼠对抗10(2)约氏疟原虫子孢子的攻击。通过给予针对干扰素γ的单克隆抗体,在所有小鼠中消除了rIL-12诱导的保护,并且通过给予竞争性一氧化氮合酶抑制剂NG-单甲基-L-精氨酸,在50%的小鼠中消除了rIL-12诱导的保护。 rIL-12保护了用细胞毒性抗CD4和抗CD8单克隆抗体治疗的BALB / c小鼠,以及T细胞和B细胞缺陷的严重联合免疫缺陷小鼠。这些数据表明,rIL-12刺激非B非T细胞产生干扰素γ,该干扰素通过刺激一氧化氮的产生杀死肝内寄生虫。如果证明rIL-12被人类很好地耐受,则我们的发现支持将rIL-12视为针对疟疾的免疫预防剂。

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