Persistence of adoptively transferred T cells with a kinetically engineered IL-2 receptor agonist

Author:

Parisi Giulia,Saco Justin D.,Salazar Felix B.,Tsoi Jennifer,Krystofinski Paige,Puig-Saus Cristina,Zhang Ruixue,Zhou Jing,Cheung-Lau Gardenia C.,Garcia Alejandro J.,Grasso Catherine S.,Tavaré Richard,Hu-Lieskovan Siwen,Mackay Sean,Zalevsky Jonathan,Bernatchez Chantale,Diab Adi,Wu Anna M.ORCID,Comin-Anduix Begoña,Charych Deborah,Ribas AntoniORCID

Abstract

AbstractInterleukin-2 (IL-2) is a component of most protocols of adoptive cell transfer (ACT) therapy for cancer, but is limited by short exposure and high toxicities. NKTR-214 is a kinetically-engineered IL-2 receptor βγ (IL-2Rβγ)-biased agonist consisting of IL-2 conjugated to multiple releasable polyethylene glycol chains resulting in sustained signaling through IL-2Rβγ. We report that ACT supported by NKTR-214 increases the proliferation, homing and persistence of anti-tumor T cells compared to ACT with IL-2, resulting in superior antitumor activity in a B16-F10 murine melanoma model. The use of NKTR-214 increases the number of polyfunctional T cells in murine spleens and tumors compared to IL-2, and enhances the polyfunctionality of T and NK cells in the peripheral blood of patients receiving NKTR-214 in a phase 1 trial. In conclusion, NKTR-214 may have the potential to improve the antitumor activity of ACT in humans through increased in vivo expansion and polyfunctionality of the adoptively transferred T cells.

Funder

Foundation for the National Institutes of Health

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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