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首页> 外文期刊>Journal of Leukocyte Biology: An Official Publication of the Reticuloendothelial Society >Quantifying NK cell growth and survival changes in response to cytokines and regulatory checkpoint blockade helps identify optimal culture and expansion conditions
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Quantifying NK cell growth and survival changes in response to cytokines and regulatory checkpoint blockade helps identify optimal culture and expansion conditions

机译:量化NK细胞生长和存活变化响应细胞因子和监管检查点封闭有助于确定最佳的培养和膨胀条件

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摘要

Abstract NK cells are innate lymphocytes critical for immune surveillance, particularly in eradication of metastatic cancer cells and acute antiviral responses. In contrast to T cells, NK cell‐mediated immunity is rapid, with spontaneous cytotoxicity and cytokine/chemokine production upon pathogen detection. The renaissance in cancer immunology has cast NK cell biology back into the spotlight with an urgent need for deeper understanding of the regulatory networks that govern NK cell antitumor activity. To this end, we have adapted and refined a series of quantitative cellular calculus methods, previously applied to T and B lymphocytes, to dissect the biologic outcomes of NK cells following stimulation with cytokines (IL‐15, IL‐12, IL‐18) or deletion of genes that regulate NK cell proliferation ( Cish ), survival ( Bcl2l11 ), and activation‐induced‐cell‐death (AICD; Fas). Our methodology is well suited to delineate effects on division rate, intrinsic apoptosis, and AICD, permitting variables such as population half‐life, rate of cell division, and their combined influence on population numbers in response to stimuli to be accurately measured and modelled. Changes in these variables that result from gene deletion, concentration of stimuli, time, and cell density give insight into the dynamics of NK cell responses and serve as a platform to dissect the mechanism of action of putative checkpoints in NK cell activation and novel NK cell immunotherapy agents.
机译:摘要NK细胞是对免疫监测至关重要的先天淋巴细胞,特别是在根除转移性癌细胞和急性抗病毒反应中。与T细胞相比,NK细胞介导的免疫力是快速的,自发细胞毒性和细胞因子/趋化因子产生在病原体检测中。癌症免疫学中的文艺复兴使NK细胞生物学恢复到聚光灯中,迫切需要更深入地了解管理NK细胞抗肿瘤活动的监管网络。为此,我们已经改编和精制了一系列的一系列定量细胞微积分方法,以前施用于T和B淋巴细胞,将刺激细胞因子(IL-15,IL-12,IL-18)进行筛选后的NK细胞的生物学结果或缺失调节NK细胞增殖(CISH),存活(BCL2L11)和活化诱导细胞死亡(AICD; FAS)的基因。我们的方法非常适合划分对分裂率,内在细胞凋亡和AICD的影响,允许诸如人口半衰期,细胞分裂率的变量,以及它们对响应刺激和建模的刺激而对人口数的综合影响。由基因缺失,刺激浓度,时间和细胞密度导致的这些变量的变化,并用作NK细胞反应的动态,并用作解剖拟给性检查点在NK细胞活化和新型NK细胞中的作用机制的平台免疫治疗剂。

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