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脾切除小鼠中的慢性、开放性伯氏疟原虫疟疾

Chronic, patent Plasmodium berghei malaria in splenectomized mice.

作者信息

Eling W M

出版信息

Infect Immun. 1982 Mar;35(3):880-6. doi: 10.1128/iai.35.3.880-886.1982.

Abstract

It was shown that splenectomized mice could develop a certain resistance to Plasmodium berghei but usually no real immunity, since the infection became chronic, often with high parasitemias. A patent infection lasting at least 2 weeks was necessary for the development of this degree of protection. Prolonged suppression to subpatent levels (sulfonamide treatment), rather than radical cure (chloroquine), after 2 weeks of patency yielded a higher proportion of mice resistant to superinfection. An increasing proportion of B10LP, but not C57BL/Rij or BALB/c, mice cleared their chronic infection spontaneously in time. Chronic patent infections were accompanied by anemia, elevated serum glutamate oxaloacetate transaminase levels, indicating liver pathology, and decreased immune reactivity, but the magnitude to these pathological changes was limited compared with changes in primary, lethal infections in intact controls. Parasitemia and pathology did not always develop synchronously.

摘要

研究表明,脾切除的小鼠对伯氏疟原虫可产生一定的抵抗力,但通常不会产生真正的免疫力,因为感染会变成慢性,常常伴有高疟原虫血症。持续至少2周的显性感染是产生这种程度保护作用所必需的。在显性感染2周后,将感染持续抑制到隐性水平(磺胺治疗),而不是彻底治愈(氯喹),会使更多比例的小鼠对再次感染产生抗性。越来越多的B10LP小鼠(但不是C57BL/Rij或BALB/c小鼠)会及时自发清除其慢性感染。慢性显性感染伴有贫血、血清谷氨酸草酰乙酸转氨酶水平升高(表明肝脏病变)以及免疫反应性降低,但与完整对照动物的原发性致死性感染相比,这些病理变化的程度有限。疟原虫血症和病理变化并不总是同步发生。

相似文献

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Plasmodium berghei: selective release of "protective" antigens.
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