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首页> 外文期刊>The Journal of Experomental Medicine >Immunological regulation of experimental cutaneous leishmaniasis. III. Nature and significance of specific suppression of cell-mediated immunity in mice highly susceptible to Leishmania tropica.
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Immunological regulation of experimental cutaneous leishmaniasis. III. Nature and significance of specific suppression of cell-mediated immunity in mice highly susceptible to Leishmania tropica.

机译:实验性皮肤利什曼病的免疫学调节。三,在高度易患热带利什曼原虫的小鼠中特异性抑制细胞介导的免疫的性质和意义。

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摘要

BALB/c mice have been an exceptional susceptibility to Leishmania tropica infection such that cutaneous lesions grow without restraint in all cases leading to fatal metastasis and visceralization in normal and x-irradiated, bone-marrow reconstituted (XBM) animals. Adult thymectomized, x-irradiated, bone marrow-reconstituted (ATxXBM) BALB/c mice, however, show pronounced retardation of lesion growth leading to some survival and even cures. A similar trend was also found in moderately susceptible (BALB/c X C57BL/6)F1 mice, in contrast with the "resistant" CBA strain, in which, as previously known, ATxXBM animals showed impairment of normal, spontaneous self-healing. These convere effects are paralleled by respective leishmania-specific delayed-type hypersensitivity (DTH) reactivities, prior thymectomy leading to diminution in CBA and augmentation in BALB/c and (BALB/c X C57BL/6)F1. Anti-leishmanial DTH responses, amplfiable by cyclophosphamide pretreatment, can be detected in BALB/c mice within 10 d of infection with 2 X 10(7) promastigotes, but becomes near-totally suppressed by day 25-35. No such suppressin is found in CBA, C57BL/6, or (BALB/c X C57BL/6)F1 mice together with varying degrees of immune control of lesion development or regression. Suppression of DTH in BALB/c mice is leishmania specific and does not extent to 2,4-dinitrofluorobenzene (DNFB) or sheep erythrocytes specificities. Spleen cells from suppressed L. tropica-infected mice when transferred to normal BALB/c mice impaired the induction of DTH to leishmanial antigen. This property resided in the T cell-enriched fraction and not in the T cell-depleted fraction. It is concluded that a major component of the striking inability of BALB/c mice to control L. tropica infection involves profound impairment of a potentially curative cell-mediated immune response by suppressor T cell generation. The possibility is discussed that this may be secondary to rapid amastigote (antigen) accumulation in macrophages expressing the primary genetic "defect."
机译:BALB / c小鼠对热带利什曼原虫(Leishmania tropica)感染具有特殊的易感性,因此在所有情况下皮肤病变均可不受限制地生长,导致正常和X射线骨髓重建(XBM)动物的致命转移和内脏化。然而,成年的经胸腺切除,X射线照射,骨髓重建(ATxXBM)的BALB / c小鼠表现出明显的病灶生长迟缓,导致某些存活甚至治愈。在中度敏感的(BALB / c X C57BL / 6)F1小鼠中也发现了类似的趋势,这与“抗性” CBA品系相反,在该品系中,如先前所知,ATxXBM动物表现出正常的自发性自我修复功能受损。这些令人信服的效果与相应的利什曼原虫特异性延迟型超敏反应(DTH)反应性,胸腺切除术导致CBA减少,BALB / c和(BALB / c X C57BL / 6)F1增加同时发生。可以在BALB / c小鼠中感染2 X 10(7)前鞭毛体后10天内在BALB / c小鼠中检测出抗环磷酰胺DTH反应,可通过环磷酰胺预处理对其进行扩增,但在第25-35天时几乎被完全抑制。在CBA,C57BL / 6或(BALB / c X C57BL / 6)F1小鼠中未发现这种抑制素,并且对病变的发展或消退有不同程度的免疫控制。 BALB / c小鼠中DTH的抑制是利什曼原虫特异性的,并且不属于2,4-二硝基氟苯(DNFB)或绵羊红细胞的特异性。来自抑制的热带气旋病感染小鼠的脾细胞,当转移到正常的BALB / c小鼠时,会破坏DTH对利什曼原虫抗原的诱导。该性质存在于富含T细胞的部分中,而不存在于贫T细胞的部分中。结论是,BALB / c小鼠无法控制热带骆驼感染的惊人能力的主要组成部分涉及抑制性T细胞的产生,对潜在的治愈性细胞介导的免疫反应的严重损害。讨论了这种可能性可能与继发鞭毛体(抗原)在表达主要遗传“缺陷”的巨噬细胞中的积累有关。

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