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首页> 外文期刊>The Journal of Experomental Medicine >Immunological regulation of experimental cutaneous leishmaniasis. IV. Prophylactic effect of sublethal irradiation as a result of abrogation of suppressor T cell generation in mice genetically susceptible to leishmania tropica
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Immunological regulation of experimental cutaneous leishmaniasis. IV. Prophylactic effect of sublethal irradiation as a result of abrogation of suppressor T cell generation in mice genetically susceptible to leishmania tropica

机译:实验性皮肤利什曼病的免疫学调节。 IV。废除抑制性T细胞在遗传易感热带利什曼原虫中的小鼠产生的致死作用的预防作用

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摘要

The overwhelming susceptibility of BALB/c mice to infection with Leishmania tropica can be substantially reversed by immediately prior sub-lethal irradiation. This is related to radiation dosage, and at 550 rad, causes 60 percent complete cures and only 19 percent (instead of 100 percent) incidence of progressive disease. Irradiation 10 d before infection is only weakly prophylactic, whereas 10 d after is without effect. Control of lesion development is only apparent after the first 30 d, coincident with the analogous onset previously found in resistant strains and adult thymectomized, x-irradiated, bone marrow-reconstituted BALB/c mice. Instead of the specific suppression of DTH characteristic of L. tropica infection in the BALB/c strain, healed irradiated mice express strong anti-leishmanial DTH reactivity and resistance to reinfection. T cells from these mice transfer DTH reactivity which is suppressed by admixture with cells from nonhealed, nonreactive donors. Irradiated BALB/c mice again develop inexorable disease progression, after its transient arrest, when they are reconstituted with normal T cells. When the T cells are derived from uncontrollably-infected donors, the susceptibility regained is indistinguishable from that of normal mice. B cells do not modify the prophylactic effect of 550 rad, whereas T cells from healed mice confer strong protective immunity throughout the initial phase. Regression or progression of disease correlates completely with DTH reactivity in all these groups. Although BALB/c mice express an extreme level of genetic susceptibility to L. tropica infection, they are nevertheless capable of mounting a curative cell mediated immune response. That this is ineffective during pathogenesis of the disease was previously associated correlatively with potent specific suppressor T cell generation, which is now shown to be preventable by prior irradiation. Most important, however, a causal role for these cells in vivo has been demonstrated directly by reconstitution.
机译:BALB / c小鼠对热带利什曼原虫感染的压倒性敏感性可以通过之前的亚致死辐射基本逆转。这与辐射剂量有关,在550 rad时可导致60%的完全治愈,而仅进行进展性疾病的发生率为19%(而不是100%)。感染前10 d辐照仅具有较弱的预防作用,而感染10 d后无效果。病变发展的控制仅在头30天后才明显,与先前在抗性品系和经胸腺切除,X射线照射,骨髓重组BALB / c小鼠中发现的类似发作相吻合。在BALB / c株中,热带病菌感染DTH的特性不会受到特异的抑制,经辐照的小鼠表现出很强的抗Leishmanial DTH反应性和对再感染的抵抗力。这些小鼠的T细胞转移了DTH反应性,而DTH反应性则与未愈合,非反应性供体的细胞混合而受到抑制。辐射的BALB / c小鼠短暂停滞后,当它们被正常T细胞重建时,其疾病发展仍不可避免。当T细胞来自不受控制的感染供体时,恢复的敏感性与正常小鼠没有区别。 B细胞不会改变550 rad的预防作用,而治愈小鼠的T细胞在整个初始阶段均具有强大的保护性免疫力。在所有这些组中,疾病的恶化或进展与DTH反应性完全相关。尽管BALB / c小鼠对热带L.感染表现出极高的遗传易感性,但它们仍能够进行治愈性细胞介导的免疫反应。在疾病的发病过程中这是无效的,以前与有效的特异性抑制性T细胞的产生相关,现在证明可以通过事先的照射来预防。然而,最重要的是,通过重建直接证明了这些细胞在体内的起因作用。

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