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新西兰黑鼠对高剂量墨西哥利什曼原虫感染具有免疫抗性,但对低剂量感染则不然。

New Zealand black mice are immunologically resistant to high-dose, but not low-dose Leishmania mexicana infection.

作者信息

Dorea R C, Alexander J, Gallagher G

机构信息

Immunology Research Group, University of Strathclyde, Glasgow, Scotland.

出版信息

Clin Exp Immunol. 1991 Aug;85(2):231-5. doi: 10.1111/j.1365-2249.1991.tb05710.x.

Abstract

The course of infection following s.c. inoculation of a wide dose range of L. mexicana stationary-phase promastigotes (SPP) was examined in sexually mature and immature NZB mice of both sexes. Infection with a high dose (greater than 10(7) SPP) was able to induce a protective in vivo response, which could be adoptively transferred with parasite-immune T cells, into naive, syngeneic recipients. In contrast, s.c. infection with a low dose (less than 10(7) SPP) induced non-healing lesions; disease susceptibility could also be transferred into naive animals with T cells from non-immune donors. When the ability to mount a delayed-type hypersensitivity (DTH) reaction was tested in these two groups, the high-parasite dose group gave a significantly higher response. The in vivo protection and high DTH response were reflected in the ability of cells derived from the high-dose resistant (but not low-dose susceptible) mice to mount an antigen-specific T cell response in vitro. The possible immunological effector mechanisms underlying high-dose resistance and low-dose susceptibility are discussed.

摘要

在性成熟和未成熟的雌雄新西兰黑鼠(NZB)中,研究了皮下接种不同剂量范围的墨西哥利什曼原虫静止期前鞭毛体(SPP)后的感染过程。高剂量(大于10⁷个SPP)感染能够诱导体内保护性反应,这种反应可通过寄生虫免疫T细胞传递给同基因的未感染的受体。相比之下,低剂量(小于10⁷个SPP)皮下感染会导致不愈合的损伤;疾病易感性也可通过来自非免疫供体的T细胞传递给未感染的动物。当检测这两组动物产生迟发型超敏反应(DTH)的能力时,高寄生虫剂量组的反应明显更高。体内保护和高DTH反应反映在来自高剂量抗性(而非低剂量易感)小鼠的细胞在体外产生抗原特异性T细胞反应的能力上。文中讨论了高剂量抗性和低剂量易感性潜在的免疫效应机制。

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