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Abrogating Cbl-b in effector CD8(+) T cells improves the efficacy of adoptive therapy of leukemia in mice.

J Clin Invest. 2010; 
Stromnes IM, Blattman JN, Tan X, Jeevanjee S, Gu H, Greenberg PD.
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Gene Synthesis Putative Cbl-b siRNA sequences (21-nt long, initial aa motif, ~50% GC) homologous between human and mouse were predict- ed and synthesized by Genscript and cloned into the pQCXIH retroviral construct (Clontech). Get A Quote

摘要

The clinical use of adoptive immunotherapy with tumor-reactive T cells to treat established cancers is limited in part by the poor in vivo survival and function of the transferred T cells. Although administration of exogenous cytokines such as IL-2 can promote T cell survival, such strategies have many nonspecific activities and are often associated with toxicity. We show here that abrogating expression of Casitas B-lineage lymphoma b (Cbl-b), a negative regulator of lymphocyte activation, in tumor-reactive CD8(+) T cells expanded ex vivo increased the efficacy of adoptive immunotherapy of disseminated leukemia in mice. Mechanistically, Cbl-b abrogation bypassed the requirement for exogenous IL-2 administration... More

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