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苏拉明对人和鼠细胞中自然杀伤细胞及单核细胞介导的细胞毒性的调节作用。

Modulation by suramin of NK and monocytic cell-mediated cytotoxicity in human and murine cells.

作者信息

Zhang H X, Sozzani S, D'Alessandro F, Luini W, Vecchi A, Spreafico F

机构信息

Istituto di Ricerche Farmacologiche Mario Negri, Milan, Italy.

出版信息

Int J Immunopharmacol. 1988;10(6):695-707. doi: 10.1016/0192-0561(88)90023-9.

Abstract

The in vitro effects of suramin, a compound recently tested in AIDS treatment, were investigated on human and murine NK and monocyte macrophage cytotoxicity and monocyte migratory ability. In a short-term, TNF-dependent assay, pre-exposure (4-18 h) to 100-400 micrograms/ml suramin was associated with a markedly increased cytotoxicity by human monocytes and murine-elicited peritoneal macrophages, paralleled by a greater cytotoxic capacity in the supernates of these effectors. Preincubation with the same pharmacological suramin concentrations also resulted in enhanced spontaneous and directed migration in monocytic cells. Suramin-preincubated human PBL and murine splenocytes were unchanged in their basal NK cytotoxicity but exhibited a deficient response to IFN. Pre- and post-incubations with suramin resulted in increased macrophagic cytotoxicity for TNF-insensitive targets. Conversely, postincubation of effectors with the drug at 100-400 micrograms/ml was associated with profound decreases in both NK and TNF-mediated macrophagic cytotoxicities, and prior exposure to suramin of macrophagic supernates resulted in reduced cytotoxic activity. The mechanisms involved in the complex modulatory activity of suramin for monocyte macrophages and NK cells and the possible therapeutic implications of these findings are discussed.

摘要

苏拉明是最近在艾滋病治疗中进行测试的一种化合物,研究了其对人和小鼠自然杀伤细胞(NK)及单核细胞巨噬细胞的细胞毒性和单核细胞迁移能力的体外作用。在一项短期的、肿瘤坏死因子(TNF)依赖性试验中,预先暴露(4 - 18小时)于100 - 400微克/毫升的苏拉明会使人类单核细胞和小鼠诱导的腹腔巨噬细胞的细胞毒性显著增加,同时这些效应细胞的上清液中的细胞毒性能力也更强。用相同药理浓度的苏拉明进行预孵育还会导致单核细胞的自发迁移和定向迁移增强。预先用苏拉明孵育的人类外周血淋巴细胞(PBL)和小鼠脾细胞的基础NK细胞毒性没有变化,但对干扰素(IFN)的反应不足。用苏拉明进行预孵育和后孵育会使巨噬细胞对TNF不敏感的靶标的细胞毒性增加。相反,效应细胞在100 - 400微克/毫升的药物浓度下进行后孵育会导致NK和TNF介导的巨噬细胞细胞毒性都显著降低,并且预先将巨噬细胞上清液暴露于苏拉明会导致细胞毒性活性降低。文中讨论了苏拉明对单核细胞巨噬细胞和NK细胞复杂调节活性所涉及的机制以及这些发现可能的治疗意义。

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