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Development of CAR-T Cell Therapy for B-ALL Using a Point-of-Care Approach

biorxiv. 2019; 
Luiza de Macedo Abdo,  Luciana Rodrigues Carvalho Barros,  Mariana Saldanha Viegas,  Luisa Vieira Codeço Marques,  Priscila de Sousa Ferreira,  Leonardo Chicaybam,  Martín Hernán Bonamino
Products/Services Used Details Operation
Peptide Synthesis The 19BBz CAR sequence was supplied by Dr. Dario Campana (St Jude Children’s Research Hospital, Memphis, TN). The sequence was codon optimized and synthesized by Genscript (Piscataway, NJ) and a myc-tag was added between CD8α signal peptide and scFv to allow flow cytometry-based detection as described elsewhere (15). The transgene was cloned using AgeI/NotI sites in the transposon vector pT3 provided by Dr. Richard Morgan (NIH). The SB100x transposase which is encoded by plasmid pCMV-SB100x was provided by Dr Sang Won Han (Federal University of São Paulo [UNIFESP], Brazil). Get A Quote

摘要

Recently approved by the FDA and European Medicines Agency, CAR-T cell therapy is a new treatment option for B-cell malignancies. Currently, CAR-T cells are manufactured in centralized facilities and face bottlenecks like complex scaling up, high costs and logistic operations. These difficulties are mainly related to the use of viral vectors and the requirement to expand CAR-T cells to reach the therapeutic dose. In this paper, by using Sleeping Beauty-mediated genetic modification delivered by electroporation, we show that CAR-T cells can be generated and used without the need for ex vivoactivation and expansion, consistent with a point-of-care (POC) approach. Our results show that minimally manipulated CAR-T... More

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