利用细胞因子分泌快速产生多病毒特异性T细胞用于过继性免疫治疗。
Exploiting cytokine secretion to rapidly produce multivirus-specific T cells for adoptive immunotherapy.
作者信息
Fujita Yuriko, Leen Ann M, Sun Jiali, Nakazawa Yozo, Yvon Eric, Heslop Helen E, Brenner Malcolm K, Rooney Cliona M
机构信息
Center for Cell and Gene Therapy, Baylor College of Medicine, the Methodist Hospital, Texas Children's Hospital, Houston, TX 77030, USA.
出版信息
J Immunother. 2008 Sep;31(7):665-74. doi: 10.1097/CJI.0b013e318181b4bd.
Abstract
Viral infections remain a major cause of morbidity and mortality after hematopoietic stem cell transplantation (HSCT), and conventional small-molecule therapeutics often have modest benefit, high cost, and adverse effects. Adoptive transfer of donor-derived virus-specific T cells has proved feasible and safe after HSCT and to reconstitute immunity against cytomegalovirus, Epstein-Barr virus, and adenovirus. Current protocols to generate these cytotoxic T cell lines are lengthy, taking up to 12 weeks. As viral infections often occur <30 days after HSCT, speedy production of virus-specific cytotoxic T cells lacking alloreactivity is highly desirable. We now describe a modified rapid selection method for production and characterization of CD4 and CD8 T cells specific for cytomegalovirus, Epstein-Barr virus, and adenovirus in a single infusate. We use Ad5f35-pp65/latent membrane protein 2 vectors in a single procedure over a 48-hour time period and manufacture a product suited for clinical use. By simultaneously expanding a portion of the selected product, we can characterize phenotype and function of the infused product and link them with subsequent in vivo outcome.
摘要
病毒感染仍然是造血干细胞移植(HSCT)后发病和死亡的主要原因,传统小分子疗法往往疗效有限、成本高昂且有不良反应。供体来源的病毒特异性T细胞过继性转移在HSCT后已证明是可行且安全的,能够重建针对巨细胞病毒、爱泼斯坦-巴尔病毒和腺病毒的免疫力。目前生成这些细胞毒性T细胞系的方案耗时漫长,长达12周。由于病毒感染常在HSCT后<30天发生,因此非常需要快速生产出无同种异体反应性的病毒特异性细胞毒性T细胞。我们现在描述一种改良的快速筛选方法,用于在单一输注液中生产和鉴定针对巨细胞病毒、爱泼斯坦-巴尔病毒和腺病毒的CD4和CD8 T细胞。我们在48小时的单一过程中使用Ad5f35-pp65/潜伏膜蛋白2载体,并制造出适合临床使用的产品。通过同时扩增所选产品的一部分,我们可以鉴定输注产品的表型和功能,并将它们与随后的体内结果联系起来。
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