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CAR T Cells Generated Using Sleeping Beauty Transposon Vectors and Expanded with an EBV-Transformed Lymphoblastoid Cell Line Display Antitumor Activity In Vitro and In Vivo.

Hum Gene Ther. 2019; 
Chicaybam L,, Abdo L, Carneiro M, Peixoto B, Viegas M, de Sousa P, Fornazin MC, Spago MC, Albertoni Laranjeira AB, de Campos-Lima PO,, Nowill A, Barros LRC, Bonamino MH,.
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Gene Synthesis f Page 5 of 28 5 by gene synthesis in pUC-57 plasmids (Genscript) and cloned into the Sleeping beauty transposon system vector pT3 using AgeI and NotI restriction enzyme sites. Get A Quote

摘要

Chimeric antigen receptor (CAR) T cell immunotherapy for the treatment of cancer is now an approved treatment for B cell malignancies. However, the use of viral vectors to provide long-term CAR expression is associated with high production costs and cumbersome quality controls, impacting the final cost of CAR T cell therapies. Nonviral integrative vectors, such as Sleeping Beauty (SB) transposons, provide an alternative to modify primary T cells. Therefore, we developed a protocol to expand SB-transfected 19BBζ CAR T cells using a lymphoblastoid cell line, and evaluated T cell phenotype as well as function along the T cell expansion. Electroporation of PBMCs with transposon plasmid decreased cell viability on ... More

关键词

CAR; CD19; EBV; LCL; Sleeping Beauty transposon; T lymphocyte