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首页> 外文期刊>British Journal of Cancer >Microenvironmental arginine depletion by macrophages in vivo
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Microenvironmental arginine depletion by macrophages in vivo

机译:体内巨噬细胞耗竭的微环境精氨酸

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Since the tumour-selective cytotoxic activity of activated macrophages in vitro can be attributed to depletion of the culture medium of L-arginine by macrophage arginase, a series of experiments was designed to determine whether such a mechanism could operate in vivo. Extracellular fluid obtained from Gullino chambers within established tumours contained high levels of arginase, no detectable arginine and high levels of ornithine. When tumours were disaggregated into single-cell suspensions, arginase was readily detected within tumour macrophages but not within malignant cells. Inflammatory ascites induced in mice by Corynebacterium parvum was rich in arginase, depleted of L-arginine and cytotoxic in vitro to L5178Y and V79 cells. High levels of arginase in the ascites fluid were associated with resistance to challenge with syngeneic L5178Y cells. Lymph collected from the cisterna chyli in rats bearing a macrophage-rich sarcoma on the small bowel contained elevated levels of arginase, was depleted of arginine and contained increased concentrations of ornithine. We conclude that in sites of macrophage infiltration there is microenvironmental arginine depletion due to the action of arginase, and that arginase release could represent an important macrophage effector mechanism against a variety of targets, including malignant cells, virus-infected cells, fungi and parasites.
机译:由于活化的巨噬细胞在体外的肿瘤选择性细胞毒活性可归因于巨噬细胞精氨酸酶消耗L-精氨酸的培养基,因此设计了一系列实验来确定这种机制是否可以在体内起作用。从已确诊的肿瘤中的古利诺小室获得的细胞外液含有高水平的精氨酸酶,无可检测的精氨酸和高水平的鸟氨酸。当将肿瘤分解成单细胞悬液时,在肿瘤巨噬细胞中很容易检测到精氨酸酶,而在恶性细胞中却没有检测到。细小棒状杆菌诱导的小鼠炎症性腹水富含精氨酸酶,缺乏L-精氨酸并在体外对L5178Y和V79细胞具有细胞毒性。腹水中高水平的精氨酸酶与同型L5178Y细胞对攻击的抗性相关。从大鼠小肠乳糜池收集的淋巴在小肠上富含巨噬细胞肉瘤,其精氨酸酶水平升高,精氨酸消耗减少,鸟氨酸浓度升高。我们得出的结论是,由于精氨酸酶的作用,在巨噬细胞浸润部位存在微环境中的精氨酸消耗,精氨酸酶的释放可能代表针对多种靶标的重要的巨噬细胞效应子机制,包括恶性细胞,病毒感染的细胞,真菌和寄生虫。

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