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溶组织内阿米巴:长期维持的无菌培养物毒力降低的机制

Entamoeba histolytica: mechanism of decrease of virulence of axenic cultures maintained for prolonged periods.

作者信息

Olivos Alfonso, Ramos Espiridión, Nequiz Mario, Barba Carlos, Tello Eusebio, Castañón Guadalupe, González Augusto, Martínez Rubén D, Montfort Irmgard, Pérez-Tamayo Ruy

机构信息

Department of Experimental Medicine, National Autonomous University of México Medical School, Mexico.

出版信息

Exp Parasitol. 2005 Jul;110(3):309-12. doi: 10.1016/j.exppara.2005.03.020. Epub 2005 Apr 19.

Abstract

Intraportal injection of non-virulent E. histolytica (derived from prolonged axenic culture of virulent E. histolytica) strain HM1-IMSS in normal hamsters results in no liver lesions and disappearance of the parasites 48-72 h after injection. Viability of non-virulent E. histolytica after 2 h of in vitro incubation in either fresh or decomplemented hamster serum is the same as control virulent E. histolytica (50-90%). In hamsters made leukopenic, or both leukopenic+hypocomplementemic, or hypocomplementemic+sephadex microspheres (to produce focal liver ischemia) intraportally injected non-virulent E. histolytica cause no lesions and disappear after 24 h. In addition, neither hypocomplementemia nor immunosuppression with cyclosporin A prolonged the survival of non-virulent E. histolytica. Methyl prednisolone treatment of hamsters resulted in survival of large numbers of non-virulent E. histolytica in the liver, with little inflammation and minimal tissue damage, for up to 7 days. Inflammatory cells (macrophages) would appear to be chiefly responsible for elimination of non-virulent E. histolytica. Parallel experiments with E. dispar suggest a different mechanism for its non-pathogenicity.

摘要

在正常仓鼠门静脉内注射无毒力的溶组织内阿米巴(源自有毒力的溶组织内阿米巴的长期单菌培养)菌株HM1-IMSS,不会导致肝脏损伤,且注射后48 - 72小时寄生虫消失。无毒力的溶组织内阿米巴在新鲜或去补体的仓鼠血清中体外孵育2小时后的活力与对照有毒力的溶组织内阿米巴相同(50 - 90%)。在造成白细胞减少的仓鼠中,或同时造成白细胞减少+补体减少的仓鼠中,或补体减少+葡聚糖微球(以产生局灶性肝缺血)的仓鼠中,门静脉内注射无毒力的溶组织内阿米巴不会引起病变,且24小时后消失。此外,补体减少或用环孢素A进行免疫抑制均未延长无毒力的溶组织内阿米巴的存活时间。用甲基强的松龙治疗仓鼠,导致大量无毒力的溶组织内阿米巴在肝脏内存活,炎症轻微,组织损伤最小,长达7天。炎性细胞(巨噬细胞)似乎是清除无毒力的溶组织内阿米巴的主要原因。用迪斯帕内阿米巴进行的平行实验提示了其非致病性的不同机制。

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