AUTHOR=Calviño Cristina , Ceballos Candela , Alfonso Ana , Jauregui Patricia , Calleja-Cervantes Maria E. , San Martin-Uriz Patxi , Rodriguez-Marquez Paula , Martin-Mallo Angel , Iglesias Elena , Abizanda Gloria , Rodriguez-Diaz Saray , Martinez-Turrillas Rebeca , Illarramendi Jorge , Viguria Maria C. , Redondo Margarita , Rifon Jose , Villar Sara , Lasarte Juan J. , Inoges Susana , Lopez-Diaz de Cerio Ascension , Hernaez Mikel , Prosper Felipe , Rodriguez-Madoz Juan R. 

TITLE=Optimization of universal allogeneic CAR-T cells combining CRISPR and transposon-based technologies for treatment of acute myeloid leukemia

JOURNAL=Frontiers in Immunology

VOLUME=14

YEAR=2023

URL=https://www.frontiersin.org/journals/immunology/articles/10.3389/fimmu.2023.1270843

DOI=10.3389/fimmu.2023.1270843

ISSN=1664-3224

ABSTRACT=<p>Despite the potential of CAR-T therapies for hematological malignancies, their efficacy in patients with relapse and refractory Acute Myeloid Leukemia has been limited. The aim of our study has been to develop and manufacture a CAR-T cell product that addresses some of the current limitations. We initially compared the phenotype of T cells from AML patients and healthy young and elderly controls. This analysis showed that T cells from AML patients displayed a predominantly effector phenotype, with increased expression of activation (CD69 and HLA-DR) and exhaustion markers (PD1 and LAG3), in contrast to the enriched memory phenotype observed in healthy donors. This differentiated and more exhausted phenotype was also observed, and corroborated by transcriptomic analyses, in CAR-T cells from AML patients engineered with an optimized CAR construct targeting CD33, resulting in a decreased <italic>in vivo</italic> antitumoral efficacy evaluated in xenograft AML models. To overcome some of these limitations we have combined CRISPR-based genome editing technologies with virus-free gene-transfer strategies using <italic>Sleeping Beauty</italic> transposons, to generate CAR-T cells depleted of HLA-I and TCR complexes (HLA-I<sup>KO</sup>/TCR<sup>KO</sup> CAR-T cells) for allogeneic approaches. Our optimized protocol allows one-step generation of edited CAR-T cells that show a similar phenotypic profile to non-edited CAR-T cells, with equivalent <italic>in vitro</italic> and <italic>in vivo</italic> antitumoral efficacy. Moreover, genomic analysis of edited CAR-T cells revealed a safe integration profile of the vector, with no preferences for specific genomic regions, with highly specific editing of the HLA-I and TCR, without significant off-target sites. Finally, the production of edited CAR-T cells at a larger scale allowed the generation and selection of enough HLA-I<sup>KO</sup>/TCR<sup>KO</sup> CAR-T cells that would be compatible with clinical applications. In summary, our results demonstrate that CAR-T cells from AML patients, although functional, present phenotypic and functional features that could compromise their antitumoral efficacy, compared to CAR-T cells from healthy donors. The combination of CRISPR technologies with transposon-based delivery strategies allows the generation of HLA-I<sup>KO</sup>/TCR<sup>KO</sup> CAR-T cells, compatible with allogeneic approaches, that would represent a promising option for AML treatment.</p>