Advanced & Cell Therapy Services, Banc de Sang i Teixits (Blood and Tissue Bank, BST), Barcelona, Spain; Transfusional Medicine Group, Vall d'Hebron Research Institute, Universitat Autònoma de Barcelona (VHIR-UAB), Barcelona, Spain.
Advanced & Cell Therapy Services, Banc de Sang i Teixits (Blood and Tissue Bank, BST), Barcelona, Spain; Transfusional Medicine Group, Vall d'Hebron Research Institute, Universitat Autònoma de Barcelona (VHIR-UAB), Barcelona, Spain.
Transplant Cell Ther. 2023 Sep;29(9):572.e1-572.e13. doi: 10.1016/j.jtct.2023.06.001. Epub 2023 Jun 6.
During the first outbreak of an emergent virus, methods need to be developed to rapidly establish suitable therapies for patients with high risk of severe disease caused by the pathogen. Considering the importance of the T-cell response in controlling viral infections, adoptive cell therapy with virus-specific T cells has been used as a safe and effective antiviral prophylaxis and treatment for immunocompromised patients. The main objective of this study was to establish an effective and safe method to cryostore whole blood as starting material and to adapt a T-cell activation and expansion protocol to generate an off-the-shelf antiviral therapeutic option. Additionally, we studied how memory T-cell phenotype, clonality based on T-cell receptor, and antigen specificity could condition characteristics of the final expanded T-cell product. Twenty-nine healthy blood donors were selected from a database of convalescent plasma donors with a confirmed history of SARS-CoV-2 infection. Blood was processed using a fully automated, clinical-grade, and 2-step closed system. Eight cryopreserved bags were advanced to the second phase of the protocol to obtain purified mononucleated cells. We adapted the T-cell activation and expansion protocol, without specialized antigen-presenting cells or presenting molecular structures, in a G-Rex culture system with IL-2, IL-7, and IL-15 cytokine stimulation. The adapted protocol successfully activated and expanded virus-specific T cells to generate a T-cell therapeutic product. We observed no major impact of post-symptom onset time of donation on the initial memory T-cell phenotype or clonotypes resulting in minor differences in the final expanded T-cell product. We showed that antigen competition in the expansion of T-cell clones affected the T-cell clonality based on the T-cell receptor β repertoire. We demonstrated that good manufacturing practice of blood preprocessing and cryopreserving is a successful procedure to obtain an initial cell source able to activate and expand without a specialized antigen-presenting agent. Our 2-step blood processing allowed recruitment of the cell donors independently of the expansion cell protocol timing, facilitating donor, staff, and facility needs. Moreover, the resulting virus-specific T cells could be also banked for further use, notably maintaining viability and antigen specificity after cryopreservation.
在新发传染病疫情暴发的初期,需要制定方案为高危重症患者迅速建立适宜的治疗方法。鉴于 T 细胞反应在控制病毒感染中的重要性,采用病毒特异性 T 细胞过继细胞疗法,已经被用于免疫功能低下患者的安全有效的抗病毒预防和治疗。本研究的主要目的是建立一种有效和安全的方法,以冷冻保存全血作为起始材料,并适应 T 细胞激活和扩增方案,以生成现成的抗病毒治疗选择。此外,我们研究了记忆 T 细胞表型、基于 T 细胞受体的克隆性以及抗原特异性如何影响最终扩增的 T 细胞产品的特征。从 SARS-CoV-2 感染确诊史的恢复期血浆供体数据库中选择了 29 名健康献血者。使用全自动、临床级、两步封闭系统处理血液。将 8 个冷冻保存袋推进到方案的第二阶段,以获得纯化的单核细胞。我们在 G-Rex 培养系统中,使用 IL-2、IL-7 和 IL-15 细胞因子刺激,适应了无需专门抗原呈递细胞或呈递分子结构的 T 细胞激活和扩增方案。该方案成功地激活和扩增了病毒特异性 T 细胞,生成了 T 细胞治疗产品。我们观察到,供体发病后时间对初始记忆 T 细胞表型或导致最终扩增的 T 细胞产品产生微小差异的克隆型没有重大影响。我们表明,在 T 细胞克隆的扩增过程中,抗原竞争会影响基于 T 细胞受体β库的 T 细胞克隆性。我们证明了血液预处理和冷冻保存的良好生产规范是获得初始细胞源的成功程序,无需专门的抗原呈递剂即可激活和扩增。我们的两步血液处理允许独立于细胞扩增方案时间招募供体,方便了供体、工作人员和设施的需求。此外,获得的病毒特异性 T 细胞也可以储存以备进一步使用,特别是在冷冻保存后保持活力和抗原特异性。
