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与非致死性鼠疟原虫共感染可抑制伯氏疟原虫NK65引起的发病机制。

Coinfection with nonlethal murine malaria parasites suppresses pathogenesis caused by Plasmodium berghei NK65.

作者信息

Niikura Mamoru, Kamiya Shigeru, Kita Kiyoshi, Kobayashi Fumie

机构信息

Institute of Laboratory Animals, Graduate School of Medicine, Faculty of Medicine, Kyorin University, Tokyo, Japan.

出版信息

J Immunol. 2008 May 15;180(10):6877-84. doi: 10.4049/jimmunol.180.10.6877.

Abstract

Mixed infection with different Plasmodium species is often observed in endemic areas, and the infection with benign malaria parasites such as Plasmodium vivax or P. malariae has been considered to reduce the risk of developing severe pathogenesis caused by P. falciparum. However, it is still unknown how disease severity is reduced in hosts during coinfection. In the present study, we investigated the influence of coinfection with nonlethal parasites, P. berghei XAT (Pb XAT) or P. yoelii 17X (Py 17X), on the outcome of P. berghei NK65 (Pb NK65) lethal infection, which caused high levels of parasitemia and severe pathogenesis in mice. We found that the simultaneous infection with nonlethal Pb XAT or Py 17X suppressed high levels of parasitemia, liver injury, and body weight loss caused by Pb NK65 infection, induced high levels of reticulocytemia, and subsequently prolonged survival of mice. In coinfected mice, the immune response, including the expansion of B220(int)CD11c(+) cells and CD4(+) T cells and expression of IL-10 mRNA, was comparable to that in nonlethal infection. Moreover, the suppression of liver injury and body weight loss by coinfection was reduced in IL-10(-/-) mice, suggesting that IL-10 plays a role for a reduction of severity by coinfection with nonlethal malaria parasites.

摘要

在疟疾流行地区,经常会观察到不同疟原虫物种的混合感染,而感染间日疟原虫或三日疟原虫等良性疟原虫被认为可以降低由恶性疟原虫引起的严重发病风险。然而,目前仍不清楚在混合感染期间宿主的疾病严重程度是如何降低的。在本研究中,我们调查了与非致死性寄生虫伯氏疟原虫XAT(Pb XAT)或约氏疟原虫17X(Py 17X)混合感染对伯氏疟原虫NK65(Pb NK65)致死性感染结果的影响,Pb NK65感染会在小鼠体内导致高水平的寄生虫血症和严重发病。我们发现,同时感染非致死性的Pb XAT或Py 17X可抑制由Pb NK65感染引起的高水平寄生虫血症、肝损伤和体重减轻,诱导高水平的网织红细胞增多症,并随后延长小鼠的存活时间。在混合感染的小鼠中,免疫反应,包括B220(int)CD11c(+)细胞和CD4(+)T细胞的扩增以及IL-10 mRNA的表达,与非致死性感染中的情况相当。此外,在IL-10(-/-)小鼠中,混合感染对肝损伤和体重减轻的抑制作用减弱,这表明IL-10在通过与非致死性疟原虫混合感染降低疾病严重程度方面发挥作用。

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