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Cytokine Profile in Early Infection by Leptospira interrogans in A/J Mice

机译:leptospira interrogans在a / J小鼠早期感染的细胞因子概况

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Leptospirosis is considered a neglected disease with an estimated more than one million cases every year. Since rodents are at the same time the main reservoir and generally asymptomatic to Leptospira infection, understanding why some animal species are resistant and others are susceptible to this infection would shed some light in how to control this important zoonosis. The innate immune response against Leptospira is mainly dependent on phagocytosis and activation of the Complement System. In this context, cytokines may drive the early control of infection and the adaptive response. Since the Complement System is important to eliminate leptospires in vivo, we investigated if Complement C5 in A/J mice would modulate the cytokine production during infection by Leptospira interrogans serovar Kennewicki type Pomona Fromm (LPF). Thus, our aim was to investigate the systemic levels of pro- and anti-inflammatory cytokines during Leptospira infection in the blood, liver, lung, and kidney on the third and sixth days of infection in A/J C5+/+ and A/J C5-/- mice. Blood levels of TNF-α, IL-6, IFN-γ, and MCP-1 reached a peak on the third day. Although both mouse strains developed splenomegaly, similar histopathological alterations in the liver and the lung, levels of pro- and anti-inflammatory cytokines were different. A/J C5+/+ mice had higher levels of liver IL-10, IL-1β, IL-12p40, and IL-12p70 and kidney IL-1β, IL-12p40, and IL-12p70 on the sixth day of infection when compared to A/J C5-/- mice. Our results showed that in A/J genetic background, the Complement component C5 modulates a cytokine profile in the liver and kidney of infected mice, which may play a role in the control of disease progression.
机译:钩端螺旋体病被认为是一种被忽视的疾病,每年估计超过一百万例。由于啮齿动物同时,主要储层和百分之然无症状的leptospira感染,了解为什么一些动物物种是抗性的,其他人易受这种感染的影响会揭示如何控制这种重要的动物病。对leptospira的先天免疫应答主要依赖于吞噬作用和补体系统的激活。在这种情况下,细胞因子可以推动感染的早期控制和适应性反应。由于补体系是在体内消除百分之叶片的重要性,我们研究了A / J小鼠中的补体C5是否会通过Lepterospira Interrogans Serovar Kennewicki型Pomona(LPF)调节细胞因子产生。因此,我们的目的是在A / J C5 + / +和A / J中的第三和第六天感染血液,肝脏,肺和肾脏在血液,肝脏,肺和肾脏中的乳酸骨膜感染过程中的全身水平C5 - / - 小鼠。 TNF-α,IL-6,IFN-γ和MCP-1的血液水平在第三天达到了峰值。虽然两种小鼠菌株发育脾肿大,但肝脏和肺部的类似组织病理学改变,促炎细胞因子的水平不同。 A / J C5 + / +小鼠在比较时具有更高水平的肝脏IL-10,IL-1β,IL-12P40和IL-12P70和肾IL-1β,IL-12P40和IL-12P70比较到A / J C5 - / - 小鼠。我们的研究结果表明,在A / J遗传背景下,补体组分C5调节感染小鼠的肝脏和肾脏中的细胞因子谱,这可能在疾病进展的控制中发挥作用。

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