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γ-干扰素对疟原虫红细胞外期发育的抑制作用。

Inhibition of development of exoerythrocytic forms of malaria parasites by gamma-interferon.

作者信息

Ferreira A, Schofield L, Enea V, Schellekens H, van der Meide P, Collins W E, Nussenzweig R S, Nussenzweig V

出版信息

Science. 1986 May 16;232(4752):881-4. doi: 10.1126/science.3085218.

DOI:10.1126/science.3085218
PMID:3085218
Abstract

A specific DNA probe was used to study the effect of recombinant rat, mouse, and human gamma-interferon (gamma-IFN) on the course of sporozoite-induced malaria infections. In mice and rats infected with sporozoites of Plasmodium berghei, mouse and rat gamma-IFN's strongly inhibited the development of the exoerythrocytic forms in the liver liver cells of the hosts, but not the development of the erythrocytic stages. The degree of inhibition of the exoerythrocytic forms was proportional to the dose of gamma-IFN administered, but was independent of the number of sporozoites used for challenge. A 30 percent reduction in the development of exoerythrocytic forms in rat liver was achieved when 150 units (about 15 nanograms of protein) of rat gamma-IFN were injected a few hours before sporozoite challenge; the reduction was 90 percent or more with higher doses of gamma-IFN. The effect was less pronounced if the gamma-IFN was administered 18 hours before or a few hours after challenge. Human gamma-IFN also diminished the parasitemia in chimpanzees infected with sporozoites of the human malaria parasite Plasmodium vivax. The target of gamma-IFN activity may be the infected hepatocytes themselves, as shown by in vitro experiments in which small doses of the human lymphokine inhibited the development of exoerythrocytic forms of Plasmodium berghei in a human hepatoma cell line. These results suggest that immunologically induced interferon may be involved in controlling malaria infection under natural conditions.

摘要

一种特异性DNA探针被用于研究重组大鼠、小鼠和人γ干扰素(γ-IFN)对子孢子诱导的疟疾感染进程的影响。在用伯氏疟原虫子孢子感染的小鼠和大鼠中,小鼠和大鼠γ-IFN强烈抑制宿主肝细胞内的红细胞外期发育,但不影响红细胞内期的发育。红细胞外期的抑制程度与所给予的γ-IFN剂量成正比,但与用于攻击的子孢子数量无关。在子孢子攻击前数小时注射150单位(约15纳克蛋白质)的大鼠γ-IFN,可使大鼠肝脏中红细胞外期发育减少30%;给予更高剂量的γ-IFN时,减少幅度可达90%或更多。如果在攻击前18小时或攻击后数小时给予γ-IFN,效果则不太明显。人γ-IFN也可降低感染人疟原虫间日疟子孢子的黑猩猩的寄生虫血症。γ-IFN活性的靶标可能是被感染的肝细胞本身,体外实验表明,小剂量的人淋巴因子可抑制人肝癌细胞系中伯氏疟原虫红细胞外期的发育。这些结果提示,免疫诱导的干扰素可能在自然条件下参与控制疟疾感染。

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