首页> 外文期刊>Antimicrobial agents and chemotherapy. >Intranasal Interleukin-12 Treatment Promotes Antimicrobial Clearance and Survival in Pulmonary Francisella tularensis subsp. novicida Infection.
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Intranasal Interleukin-12 Treatment Promotes Antimicrobial Clearance and Survival in Pulmonary Francisella tularensis subsp. novicida Infection.

机译:鼻内白细胞介素12治疗可促进土弗朗西丝菌亚种的抗菌清除和存活。 novicida感染。

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摘要

Francisella tularensis is a highly virulent facultative intracellular bacterium and is considered a potential biological warfare agent. Inhalation tularemia can lead to the development of bronchopneumonia, which is frequently fatal without medical intervention. Treatment strategies that directly target the respiratory mucosa may extend the efficacy of therapy, particularly for the medical management of acute aerosol exposure. To this end, we describe an intranasal (i.n.) strategy for the treatment of pulmonary Francisella infection in mice that uses a combinatorial approach with the conventional antibiotic gentamicin and interleukin 12 (IL-12). The i.n. administration of IL-12 alone promoted bacterial clearance and extended the time to death but did not prevent mortality against lethal pulmonary challenge with Francisella tularensis subsp. novicida. However, i.n. treatment with gentamicin and IL-12 therapeutically at 8 and 24 h after challenge markedly enhanced the rate of survival (70 to 100%) againstpulmonary infection compared to the rates of survival for animals treated with antibiotic alone (17%) or IL-12 alone (0%). A delay in combinatorial therapy over a span of 4 days progressively decreased the efficacy of this treatment regimen. This combinatorial treatment was shown to be highly dependent upon the induction of endogenous gamma interferon and may also involve the activation of natural killer cells. Together, these findings suggest that IL-12 may be a potent adjunct for chemotherapy to enhance drug effectiveness against pulmonary Francisella infection.
机译:图拉弗朗西斯菌是一种高毒力兼性细胞内细菌,被认为是一种潜在的生物战剂。吸入性吐拉血血症可导致支气管肺炎的发展,如果不进行医学干预,通常会致命。直接针对呼吸道粘膜的治疗策略可能会扩大治疗效果,尤其是对于急性气雾剂暴露的医学管理。为此,我们描述了一种鼻内(i.n.)策略,该策略用于小鼠的肺弗朗西斯菌感染,该策略采用与常规抗生素庆大霉素和白介素12(IL-12)结合使用的方法。 i.n.单独使用IL-12可以促进细菌清除并延长死亡时间,但不能防止因土拉弗朗西斯菌引起的致命性肺部攻击而导致死亡。 Novicida。但是,与仅单独使用抗生素(17%)或单独使用IL-12治疗的动物的存活率相比,在激发后8和24 h用庆大霉素和IL-12进行治疗可显着提高抗肺部感染的存活率(70至100%) (0%)。组合治疗的延迟超过4天逐渐降低了该治疗方案的疗效。已表明这种组合治疗高度依赖于内源性γ干扰素的诱导,并且还可能涉及天然杀伤细胞的激活。在一起,这些发现表明IL-12可能是化学疗法的有效辅助手段,以增强抗肺弗朗西斯菌感染的药效。

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