首页> 外文期刊>Journal of immunotherapy >The impact of ex vivo clinical grade activation protocols on human T-cell phenotype and function for the generation of genetically modified cells for adoptive cell transfer therapy.
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The impact of ex vivo clinical grade activation protocols on human T-cell phenotype and function for the generation of genetically modified cells for adoptive cell transfer therapy.

机译:离体临床等级激活方案对人类T细胞表型和功能的影响,用于产生过继细胞转移疗法的基因修饰细胞。

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摘要

Optimized conditions for the ex vivo activation, genetic manipulation, and expansion of human lymphocytes for adoptive cell therapy may lead to protocols that maximize their in vivo function. We analyzed the effects of 4 clinical grade activation and expansion protocols over 3 weeks on cell proliferative rate, immunophenotype, cell metabolism, and transduction efficiency of human peripheral blood mononuclear cells (PBMCs). Peak lentiviral transduction efficiency was early (days 2 to 4), at a time when cells showed a larger size, maximal uptake of metabolic substrates, and the highest level of proximal T-cell receptor signaling engagement. Anti-CD2/3/28 activation beads induced greater proliferation rate and skewed PBMCs early on to a CD4 phenotype when compared with the cells cultured in OKT3. Multicolor surface phenotyping demonstrated that changes in T-cell surface markers that define T-cell functional phenotypes were dependent on the time spent in culture as opposed to the particular activation protocol. In conclusion, ex vivo activation of human PBMCs for adoptive cell therapy demonstrate defined immunophenotypic and functional signatures over time, with cells early on showing larger sizes, higher transduction efficiency, maximal metabolic activity, and zeta-chain-associated protein-70 activation.
机译:用于过继细胞疗法的人类淋巴细胞的离体激活,基因操作和扩增的最佳条件可能会导致其体内功能最大化的方案。我们分析了3个星期内4种临床级别的激活和扩展方案对人外周血单核细胞(PBMC)的细胞增殖率,免疫表型,细胞代谢和转导效率的影响。慢病毒的最高转导效率是早期的(第2至4天),此时细胞显示出较大的大小,代谢底物的最大吸收以及近端T细胞受体信号传导参与的最高水平。与在OKT3中培养的细胞相比,抗CD2 / 3/28激活珠可诱导更高的增殖速率,并使PBMC早期偏向CD4表型。多色表面表型表明,定义T细胞功能表型的T细胞表面标志物的变化取决于培养所花费的时间,而不是特定的激活方案。总之,用于过继细胞治疗的人PBMC的离体激活随着时间的推移显示出明确的免疫表型和功能性特征,早期细胞显示出更大的尺寸,更高的转导效率,最大的代谢活性以及与zeta链相关的70蛋白活化。

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