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Optimizing a photoallodepletion protocol for adoptive immunotherapy after haploidentical SCT

机译:优化单相SCT后的过继免疫疗法的光脱氧方案

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In adults, one-haplotype-mismatched haematopoietic SCT (haploidentical HSCT) is associated with slow immune recovery due to decaying thymic function and extensive T-cell depletion of the graft. Although essential for preventing GVHD, T-cell depletion underlies the major reasons for transplant failure: leukemia relapse and infections, with infection-related mortality accounting for about 40% of non-leukemic deaths. Adoptive T-cell therapy would be helpful for these patients but to administer it without causing GVHD, alloreactive T cells need to be eliminated from donor T lymphocytes before infusion. In a preclinical study, to address this problem, we determined the efficacy of photodynamic purging of alloreactive T cells, by investigating combinations of parameters in order to achieve maximum allodepletion, preservation of T-regulatory cells and of pathogen and leukemia-specific T-cell responses in donor-vs-recipient MLR. We also needed to identify an optimal method to quantify the Ag-specific T-cell repertoires. Optimal procedures were identified. In particular, we compared limiting-dilution analyses (LDA) of proliferating T cells with H 3 -thymidine incorporation by bulk T cells and with flow cytometry CD25 expression, which is accepted as a T-cell activation marker. This study demonstrated that LDA is a reliable, predictable and sensitive method for measuring alloreactive, pathogen- and leukemia-specific T-cell frequencies.
机译:在成年人中,由于胸腺功能下降和移植物广泛的T细胞耗竭,单倍型不匹配的造血SCT(单倍型HSCT)与缓慢的免疫恢复有关。尽管对于预防GVHD至关重要,但T细胞耗竭是移植失败的主要原因:白血病复发和感染,与感染相关的死亡率约占非白血病死亡的40%。过继性T细胞疗法对这些患者有帮助,但要在不引起GVHD的情况下进行治疗,则必须在输注前从供体T淋巴细胞中清除同种反应性T细胞。在临床前研究中,为了解决此问题,我们通过研究参数组合以实现最大的去内质,维持T调节细胞以及病原体和白血病特异性T细胞的参数组合,确定了光动力学清除同种反应性T细胞的功效。供体与受体的MLR反应。我们还需要找到一种最佳方法来量化Ag特异的T细胞库。确定了最佳程序。特别是,我们比较了通过大量T细胞掺入H 3-胸苷和流式细胞术CD25表达(其被认为是T细胞活化标记物)对增殖T细胞的有限稀释分析(LDA)。这项研究表明,LDA是测量同种反应性,病原体和白血病特异性T细胞频率的可靠,可预测和敏感的方法。

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