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Low interleukin-2 concentration favors generation of early memory T cells over effector phenotypes during chimeric antigen receptor T-cell expansion.

Cytotherapy.. 2017-06; 
Kaartinen T,Luostarinen A,Maliniemi P,Keto J,Arvas M,Belt H,Koponen J,Loskog A,Mustjoki S,Porkka K,Ylä-Herttuala S,Korhonen M2
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Abstract

BACKGROUND: Adoptive T-cell therapy offers new options for cancer treatment. Clinical results suggest that T-cell persistence, depending on T-cell memory, improves efficacy. The use of interleukin (IL)-2 for in vitro T-cell expansion is not straightforward because it drives effector T-cell differentiation but does not promote the formation of T-cell memory. We have developed a cost-effective expansion protocol for chimeric antigen receptor (CAR) T cells with an early memory phenotype. METHODS: Lymphocytes were transduced with third-generation lentiviral vectors and expanded using CD3/CD28 microbeads. The effects of altering the IL-2 supplementation (0-300 IU/mL) and length of expansion (10-20 days) on the p... More

Keywords

T-cell expansion; T-cell memory; chimeric antigen receptor T cells; effector function; human; interleukin-2