UCL Cancer Institute, University College London, London, United Kingdom; and.
Department of Pediatrics, Centro di Ricerca Matilde Tettamanti, University of Milano-Bicocca, Milan, Italy.
Blood. 2014 Aug 21;124(8):1277-87. doi: 10.1182/blood-2014-01-545020. Epub 2014 Jun 26.
A compact marker/suicide gene that utilizes established clinical-grade reagents and pharmaceuticals would be of considerable practical utility to T-cell cancer gene therapy. Marker genes enable measurement of transduction and allow selection of transduced cells, whereas suicide genes allow selective deletion of administered T cells in the face of toxicity. We have created a highly compact marker/suicide gene for T cells combining target epitopes from both CD34 and CD20 antigens (RQR8). This construct allows selection with the clinically approved CliniMACS CD34 system (Miltenyi). Further, the construct binds the widely used pharmaceutical antibody rituximab, resulting in selective deletion of transgene-expressing cells. We have tested the functionality of RQR8 in vitro and in vivo as well as in combination with T-cell engineering components. We predict that RQR8 will make T-cell gene therapy both safer and cheaper.
一种利用既定临床级试剂和药物的紧凑型标记/自杀基因,对于 T 细胞癌症基因治疗具有重要的实际应用价值。标记基因可用于测量转导,并允许选择转导细胞,而自杀基因则允许在面对毒性时选择性删除给予的 T 细胞。我们已经为 T 细胞创建了一个非常紧凑的标记/自杀基因,该基因结合了 CD34 和 CD20 抗原的靶表位(RQR8)。该构建体允许使用临床批准的 CliniMACS CD34 系统(Miltenyi)进行选择。此外,该构建体与广泛使用的药物抗体利妥昔单抗结合,导致表达转基因的细胞选择性删除。我们已经在体外和体内以及与 T 细胞工程组件结合的情况下测试了 RQR8 的功能。我们预测 RQR8 将使 T 细胞基因治疗更加安全和廉价。
