The pharmacology of second-generation chimeric antigen receptors

SJC Van Der Stegen, M Hamieh… - Nature reviews Drug …, 2015 - nature.com
Nature reviews Drug discovery, 2015nature.com
Second-generation chimeric antigen receptors (CARs) retarget and reprogramme T cells to
augment their antitumour efficacy. The combined activating and co-stimulatory domains
incorporated in these CARs critically determine the function, differentiation, metabolism and
persistence of engineered T cells. CD19-targeted CARs that incorporate CD28 or 4-1BB
signalling domains are the best known to date. Both have shown remarkable complete
remission rates in patients with refractory B cell malignancies. Recent data indicate that …
Abstract
Second-generation chimeric antigen receptors (CARs) retarget and reprogramme T cells to augment their antitumour efficacy. The combined activating and co-stimulatory domains incorporated in these CARs critically determine the function, differentiation, metabolism and persistence of engineered T cells. CD19-targeted CARs that incorporate CD28 or 4-1BB signalling domains are the best known to date. Both have shown remarkable complete remission rates in patients with refractory B cell malignancies. Recent data indicate that CD28-based CARs direct a brisk proliferative response and boost effector functions, whereas 4-1BB-based CARs induce a more progressive T cell accumulation that may compensate for less immediate potency. These distinct kinetic features can be exploited to further develop CAR-based T cell therapies for a variety of cancers. A new field of immunopharmacology is emerging.
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