Development of novel avenues to overcome challenges facing CAR T cells.

Translational Research(2017)

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摘要
There has been dramatic success in treating patients with adoptive transfer of autologous T cells genetically modified to express a chimeric antigen receptor redirecting them to the antigen CD19. Despite this success, the application of chimeric antigen receptor T-cell therapy in solid malignancies has encountered many challenges that need to be overcome if similar success across other cancers is to become a reality. These challenges can be classified into 6 categories: the heterogeneity of tumor cell clones and tumor-associated antigen expression; poor T-cell trafficking into the tumor site; poor T-cell survival and persistence; the presence of suppressive immune cells; the secretion of suppressive soluble factors in the tumor microenvironment; and the upregulation of T-cell intrinsic inhibitory pathways. We outline specific representative hurdles in each of these categories and summarize the progress made in understanding them and developing strategies to overcome them.
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AICD,AMP,APC,ATP,CAFs,CAR,CEA,CTLA4,DAG,DGK,HIF,IDO,IRs,MDSCs,NKTs,PD-1,PGE2,SCID,TAAs,TAMs,TANs,TCR,TGF-β,TILs,TME,Tregs,TRUCK,TSA,VEGF
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