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首页> 外文期刊>The journal of immunology >Macrophage Activation for Tumor Cytotoxicity: Induction of Tumoricidal Macrophages by Supernatants of PPD-Stimulated Bacillus Calmette-Guérin-Immune Spleen Cell Cultures
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Macrophage Activation for Tumor Cytotoxicity: Induction of Tumoricidal Macrophages by Supernatants of PPD-Stimulated Bacillus Calmette-Guérin-Immune Spleen Cell Cultures

机译:巨噬细胞激活的肿瘤细胞毒性:PPD刺激的卡介苗-Guérin-免疫脾细胞培养物上清液诱导的杀肿瘤性巨噬细胞。

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Resident peritoneal macrophages from normal mice were activated for tumor cytotoxicity in vitro by co-cultivation with BCG[1][1]-immune spleen cells and PPD and by incubation with supernatants of PPD-stimulated BCG-immune spleen cell cultures (lymphokine supernatants). Lymphokine activation of macrophages occurred in unfractionated PC suspensions as well as in macrophage monolayers depleted of nonadherent PC. Tumor cytotoxicity by lymphokine-activated macrophages was evident by 3 to 4 hr of culture in active supernatants, reached maximal levels by 8 to 12 hr, and was absent by 20 hr. Continued incubation in lymphokines or even re-exposure after washing did not maintain macrophage cytotoxicity. The capacity of normal resident macrophages to be activated by lymphokines in vitro progressively decreased and was absent by 20 hr in culture. This decrease did not necessarily reflect cell death; macrophage viability as estimated by exclusion of trypan blue or by phagocytic responses did not change over the 20-hr culture period. The short lived nature of both macrophage tumoricidal capacity and capacity of precursor cells to be activated by lymphokines may function as negative feedback mechanisms in immune reactions. [1]: #fn-1
机译:通过与BCG [1] [1]-免疫脾细胞和PPD共培养,并与PPD刺激的BCG-免疫脾细胞培养物上清液(淋巴因子上清液)一起孵育,可激活正常小鼠的腹膜巨噬细胞体外的肿瘤细胞毒性。 。巨噬细胞的淋巴因子激活发生在未分级的PC悬浮液中以及未粘附PC耗尽的巨噬细胞单层中。淋巴因子激活的巨噬细胞在活动上清液中培养3到4 hr时具有明显的肿瘤细胞毒性,在8到12 hr时达到最大水平,在20 hr时不存在。继续在淋巴因子中孵育,甚至在清洗后再次接触也不能保持巨噬细胞的细胞毒性。正常驻留巨噬细胞在体外被淋巴因子激活的能力逐渐降低,并且在培养20小时后消失。这种下降并不一定反映出细胞死亡。通过排除锥虫蓝或通过吞噬反应评估的巨噬细胞生存力在20小时的培养期内未发生变化。巨噬细胞杀伤能力和被淋巴因子激活的前体细胞的能力的短暂寿命可能在免疫反应中充当负反馈机制。 [1]:#fn-1

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