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用人/鼠嵌合重组白细胞介素-12(rIL-12)在体内增强γ干扰素:对小鼠和大鼠体内感染因子的多效性作用

In vivo augmentation of IFN-gamma with a rIL-12 human/mouse chimera: pleiotropic effects against infectious agents in mice and rats.

作者信息

Gladue R P, Laquerre A M, Magna H A, Carroll L A, O'Donnell M, Changelian P S, Franke A E

机构信息

Central Research Division, Pfizer, Inc., Groton, CT 06340.

出版信息

Cytokine. 1994 May;6(3):318-28. doi: 10.1016/1043-4666(94)90029-9.

Abstract

A heterodimer containing the mouse 35 kDa and human 40 kDa subunit of IL-12 was expressed in COS cells (cIL-12). Administration of 25-200 U of the cIL-12-COS supernatant to mice twice daily for 2 days augmented spleen cell IFN-gamma production in response to IL-2 and peritoneal macrophage activity (superoxide and nitrites) as compared to animals receiving mock transfected supernatants. cIL-12 also increased levels of IFN-gamma in serum but most dramatically following an LPS injection (50-fold over controls). Animals pretreated with cIL-12 suffered enhanced mortality following challenge with the Gram negative organism E. coli but enhanced survival or clearance following infection with the Gram positive organisms L. monocytogenes and S. aureus. Although daily treatment of mice with cIL-12 following an intranasal influenza A infection elevated levels of IFN-gamma in the bronchioalveolar lavage fluid three-fold over controls, neither prophylactic or therapeutic treatment with the same dose level decreased viral titres in the lung. In addition, no effect was observed in animals infected with encephalomyocarditis virus or respiratory syncytial virus. Therefore, cIL-12 is a potent in vivo augmentor of IFN-gamma production. It has differential effects on infectious disease depending on the invading organism and time of administration; being efficacious for intracellular bacteria but ineffective at the same dose levels against viral diseases.

摘要

一种包含小鼠IL-12的35 kDa亚基和人IL-12的40 kDa亚基的异二聚体在COS细胞中表达(cIL-12)。与接受mock转染上清液的动物相比,每天给小鼠两次注射25 - 200 U的cIL-12 - COS上清液,持续2天,可增强脾细胞对IL-2的IFN-γ产生以及腹腔巨噬细胞活性(超氧化物和亚硝酸盐)。cIL-12还可增加血清中IFN-γ的水平,但在注射LPS后最为显著(比对照组高50倍)。用cIL-12预处理的动物在用革兰氏阴性菌大肠杆菌攻击后死亡率增加,但在用革兰氏阳性菌单核细胞增生李斯特菌和金黄色葡萄球菌感染后存活率提高或清除加快。尽管在甲型流感病毒鼻内感染后每天用cIL-12治疗小鼠可使支气管肺泡灌洗液中IFN-γ水平比对照组提高三倍,但相同剂量水平的预防性或治疗性治疗均未降低肺内病毒滴度。此外,在感染脑心肌炎病毒或呼吸道合胞病毒的动物中未观察到任何效果。因此,cIL-12是一种体内有效的IFN-γ产生增强剂。它对传染病的影响因入侵生物体和给药时间而异;对细胞内细菌有效,但相同剂量水平对病毒性疾病无效。

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