首页> 美国卫生研究院文献>Infection and Immunity >Enhancement of Experimental Cutaneous Leishmaniasis by Leishmania Molecules Is Dependent on Interleukin-4 Serine Protease/Esterase Activity and Parasite and Host Genetic Backgrounds
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Enhancement of Experimental Cutaneous Leishmaniasis by Leishmania Molecules Is Dependent on Interleukin-4 Serine Protease/Esterase Activity and Parasite and Host Genetic Backgrounds

机译:利什曼原虫分子增强实验性皮肤利什曼原虫病取决于白细胞介素-4丝氨酸蛋白酶/酯酶活性以及寄生虫和宿主遗传背景

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摘要

Most inbred strains of mice, like the BALB/c strain, are susceptible to Leishmania amazonensis infections and resistant to Leishmania braziliensis infections. This parasite-related difference could result from the activity of an L. amazonensis-specific virulence factor. In agreement with this hypothesis, it is shown here that the intravenous injection of BALB/c mice with L. amazonensis amastigote extract (LaE) but not the L. braziliensis extract confers susceptibility to L. braziliensis infection. This effect was associated with high circulating levels of IgG1 anti-L. amazonensis antibodies and with an increase in interleukin-4 (IL-4) production and a decrease in gamma interferon production by draining lymph node cells. Moreover, the effect was absent in IL-4-knockout mice. The biological activity in the LaE was not mediated by amphiphilic molecules and was inhibited by pretreatment of the extract with irreversible serine protease inhibitors. These findings indicate that the LaE contains a virulence-related factor that (i) enhances the Leishmania infection by promoting Th2-type immune responses, (ii) is not one of the immunomodulatory Leishmania molecules described so far, and (iii) is either a serine protease or has an effect that depends on that protease activity. In addition to being Leishmania species specific, the infection-enhancing activity was also shown to depend on the host genetic makeup, as LaE injections did not affect the susceptibility of C57BL/6 mice to L. braziliensis infection. The identification of Leishmania molecules with infection-enhancing activity could be important for the development of a vaccine, since the up- or downmodulation of the immune response against a virulence factor could well contribute to controlling the infection.
机译:大多数自交系小鼠,如BALB / c株,都对亚马逊利什曼原虫敏感,并对巴西利什曼原虫感染具有抗性。这种与寄生虫相关的差异可能是由于亚马逊乳杆菌特异性毒力因子的活性所致。与此假设相符,此处显示了用亚马逊乳杆菌鞭毛虫提取物(LaE)静脉注射BALB / c小鼠,但巴西乳杆菌提取物却不具有对巴西乳杆菌感染的易感性。这种作用与高水平的IgG1抗L循环水平有关。通过排空淋巴结细胞而产生的Amazonensis抗体和白介素4(IL-4)产生的增加和γ干扰素产生的减少。而且,在IL-4敲除小鼠中没有这种作用。 LaE中的生物活性不是由两亲性分子介导的,而是通过用不可逆的丝氨酸蛋白酶抑制剂预处理提取物而抑制的。这些发现表明,LaE包含一种与毒力相关的因子,该因子(i)通过促进Th2型免疫应答来增强利什曼原虫感染,(ii)并非到目前为止描述的免疫调节利什曼原虫分子之一,并且(iii)是丝氨酸蛋白酶或具有取决于该蛋白酶活性的作用。除了特定的利什曼原虫物种外,还显示出增强感染的活性还取决于宿主的基因组成,因为LaE注射并不影响C57BL / 6小鼠对巴西乳杆菌的易感性。具有增强感染活性的利什曼原虫分子的鉴定对于疫苗的开发可能很重要,因为针对毒力因子的免疫应答的上调或下调可以很好地有助于控制感染。

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