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小鼠和兔接种减毒克鲁斯锥虫肝脏疫苗的副作用。

Side effects of immunization with liver attenuated Trypanosoma cruzi in mice and rabbits.

作者信息

Basombrío M A, Besuschio S, Cossio P M

出版信息

Infect Immun. 1982 Apr;36(1):342-50. doi: 10.1128/iai.36.1.342-350.1982.

DOI:10.1128/iai.36.1.342-350.1982
PMID:6804389
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC351224/
Abstract

Immunity against lethal, bloodstream forms of Trypanosoma cruzi was achieved in mice by preinoculation of approximately equal to 10(5) culture epimastigotes of an attenuated T. cruzi strain (TCC). The risks of TCC inoculation in terms of pathogenicity or eventual increase in virulence of TCC progeny were evaluated. No pathogenic parasites could be selected from TCC progeny by either mouse, triatome, or culture passages. Immunizing doses of live TCC did not induce in adult mice alterations resembling chronic Chagas' disease, as judged by patterns of mortality, tissue damage, autoantibodies, or parasite recovery. On the basis of the same criteria, However, a remarkable similarity could be established between the disease caused in mice by inoculation of low numbers (10(2)) of pathogenic trypomastigotes and human chronic Chagas' disease. Although patent parasitemias were never revealed in fresh blood mounts obtained from TCC-inoculated mice, a few hemocultures and xenodiagnoses gave positive results, particularly soon after inoculations at birth. The parasites recovered by either method remained in the attenuated, epimastigote stage. In rabbits, no local lesions, fever, weight loss, or histopathological alterations were detected after subcutaneous inoculation of 10(7) TCC organisms, although one fifth of the animals yielded positive hemocultures of epimastigotes. The contrasting host response to cultured epimastigotes as compared with blood trypomastigotes indicates that, in experimental Chagas' disease, immunoprotection is not necessarily associated with immunopathology.

摘要

通过预先接种约10⁵个减毒克氏锥虫株(TCC)的培养型前鞭毛体,小鼠获得了针对克氏锥虫致死性血流型的免疫力。评估了接种TCC在致病性或TCC后代毒力最终增加方面的风险。无论是通过小鼠传代、锥蝽传代还是培养传代,均无法从TCC后代中筛选出致病寄生虫。根据死亡率、组织损伤、自身抗体或寄生虫回收情况判断,成年小鼠接种活TCC的免疫剂量并未诱发类似慢性恰加斯病的改变。然而,基于相同标准,接种少量(10²)致病性锥鞭毛体在小鼠中引发的疾病与人类慢性恰加斯病之间可确立显著相似性。尽管从接种TCC的小鼠新鲜血涂片从未发现明显的寄生虫血症,但一些血液培养和虫媒诊断呈阳性结果,尤其是在出生后接种后不久。通过任何一种方法回收的寄生虫均处于减毒的前鞭毛体阶段。在兔子中,皮下接种10⁷个TCC生物体后,未检测到局部病变、发热、体重减轻或组织病理学改变,尽管五分之一的动物血液培养前鞭毛体呈阳性。与血液中的锥鞭毛体相比,宿主对培养型前鞭毛体的反应截然不同,这表明在实验性恰加斯病中,免疫保护不一定与免疫病理学相关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/11c5/351224/65af9b4559d2/iai00151-0356-b.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/11c5/351224/8c4ca568693f/iai00151-0356-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/11c5/351224/65af9b4559d2/iai00151-0356-b.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/11c5/351224/8c4ca568693f/iai00151-0356-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/11c5/351224/65af9b4559d2/iai00151-0356-b.jpg

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本文引用的文献

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