幼年利什曼原虫感染犬单核细胞杀伤、超氧阴离子和一氧化氮生成的评价。

Cytobios Pub Date : 1998-01-01
M A Panaro, S Lisi, V Mitolo, A Acquafredda, A Fasanella, M G Carelli, O Brandonisio
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引用次数: 0

摘要

利什曼原虫属的原生动物感染几种哺乳动物的网状内皮细胞,包括狗,它们经常引起一种慢性的、不能自愈的内脏疾病。犬外周血单核细胞对利什曼原虫的杀虫机制尚未得到详细的研究。因此,使用以下参数评估健康犬感染婴儿利什曼原虫的单核细胞培养:(1)吞噬和杀伤能力;(2)氧化爆发,就超氧阴离子(O2-)释放而言;(3)一氧化氮(NO)活性,就亚硝酸盐(NO2-)产生而言,在NO合成酶抑制剂ng -单甲基- l-精氨酸(NGMMLA)存在或不存在的情况下。平行实验用豆豆蛋白a激活的PBMC上清液刺激单核细胞和未刺激的单核细胞。用于单核细胞活化的PBMC上清液中ifn - γ的量是通过犬Madin Darby细胞系的生物测定来确定的。结果表明,与未受刺激的细胞相比,受上清液刺激的单核细胞的吞噬能力、杀伤能力和O2生成显著增加。在单核细胞活化的PBMC上清液中,杀伤能力、O2生成和ifn - γ的量呈正相关。在未刺激和刺激的培养物之间,或者在有和没有NGMMLA的相同培养物之间,一氧化氮的产生没有显著差异。最后,在NGMMLA存在或不存在的情况下,杀伤百分比相似,表明在该实验模型中,外周血犬单核细胞缺乏no介导的杀伤。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Evaluation of killing, superoxide anion and nitric oxide production by Leishmania infantum-infected dog monocytes.

Protozoa of the genus Leishmania infect reticuloendothelial cells of several mammalian species, including dogs, in which they often give rise to a chronic, not self-healing visceral disease. The parasitocidal mechanism of peripheral blood monocytes towards Leishmania in the dog has not been investigated in detail. Consequently, Leishmania infantum-infected monocyte cultures of healthy dogs were evaluated using the following parameters: (1) phagocytosis and killing capacities; (2) oxidative burst, in terms of superoxide anion (O2-) release, and (3) nitric oxide (NO) activity, in terms of nitrite (NO2-) production in the presence or absence of the NO synthase inhibitor NG-monomethyl-L-arginine (NGMMLA). Parallel experiments were performed on monocytes stimulated with supernatants of concanavalin A-activated PBMC and on unstimulated monocytes. The amount of IFN-gamma in PBMC supernatants used for monocyte activation was determined by a biological assay on a canine Madin Darby cell line. Results demonstrated that phagocytosis, killing capacity and O2- production significantly increased in monocytes stimulated with supernatants, in comparison with unstimulated cells. A positive correlation was observed between the killing capacity, the O2- production and the amount of IFN-gamma in PBMC supernatants employed for monocyte activation. No significant differences were observed in NO production between unstimulated and stimulated cultures, or between the same cultures with and without NGMMLA. Finally, the killing percentage was similar in the presence or absence of NGMMLA, suggesting that in this experimental model peripheral blood dog monocytes lack NO-mediated killing.

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