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暴露于生物反应调节剂后,肺巨噬细胞的一个独特亚群被激活。

Activation of a distinct subpopulation of pulmonary macrophages following exposure to biological response modifiers.

作者信息

Drath D B, Do C, Burd T, Hong L L

机构信息

Department of Biological Science, California State University, Fullerton 92634.

出版信息

Immunol Invest. 1994 Mar;23(2):115-27. doi: 10.3109/08820139409087793.

Abstract

A distinct subpopulation of tissue-associated pulmonary macrophages (TAPM) displayed tumoricidal activity towards syngeneic and xenogeneic targets following in vitro incubation with N-acetylmuramyl-L-alanyl-D-isoglutamine (MDP). This subpopulation, as well as, the predominant population of freely lavagable alveolar macrophages destroyed allogeneic targets following a similar incubation with either 6-0-stearoyl MDP (S-MDP) or recombinant interferon-gamma (IFN-gamma). IFN-gamma-induced in vivo tumoricidal activation of both populations of pulmonary macrophage was most effective when delivered either intravenously or via osmotic minipump infusion and least effective when administered by direct intratracheal instillation. The separate populations also displayed in vivo activation in response to liposome-encapsulated i.v. administered S-MDP. Under comparable conditions, IFN-alpha was not nearly as effective. Metabolic activation of TAPM, assessed by the release of increased levels of superoxide free radicals during phagocytosis, occurred following 24 hr exposure to S-MDP or lipopolysaccharide. Incorporation of these agents into multilamellar vesicle liposomes further augmented the release of superoxide observed at 24 hrs. Our results collectively demonstrated that a subpopulation of lung macrophage, a tissue-associated pulmonary macrophage, may be activated to a tumoricidal state and to release pronounced levels of oxygen free radicals following either in vitro or in situ treatment with several biological response modifiers.

摘要

在与N-乙酰胞壁酰-L-丙氨酰-D-异谷氨酰胺(MDP)进行体外孵育后,一种独特的组织相关肺巨噬细胞(TAPM)亚群对同基因和异种靶标表现出杀肿瘤活性。在与6-O-硬脂酰MDP(S-MDP)或重组干扰素-γ(IFN-γ)进行类似孵育后,该亚群以及可自由灌洗的肺泡巨噬细胞的主要群体均破坏了同种异体靶标。当通过静脉内或渗透微型泵输注给予时,IFN-γ诱导的肺巨噬细胞两种群体的体内杀肿瘤激活最为有效,而通过直接气管内滴注给药时效果最差。这两个独立的群体对脂质体包裹的静脉内给予的S-MDP也表现出体内激活。在可比条件下,IFN-α的效果远不如前者。通过吞噬过程中超氧自由基水平升高的释放来评估,TAPM在暴露于S-MDP或脂多糖24小时后发生代谢激活。将这些试剂掺入多层囊泡脂质体中进一步增强了在24小时观察到的超氧释放。我们的结果共同表明,肺巨噬细胞的一个亚群,即组织相关肺巨噬细胞,在体外或原位用几种生物反应调节剂处理后,可能被激活至杀肿瘤状态并释放大量的氧自由基。

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