| Literature DB >> 26511507 |
Ee W Su1, Caitlin J Moore1, Samantha Suriano1, Christopher Bryce Johnson1, Neizel Songalia1, Alicia Patterson1, Daniel J Neitzke1, Kristina Andrijauskaite1, Elizabeth Garrett-Mayer2, Shikhar Mehrotra1, Chrystal M Paulos3, Andrew L Doedens4, Ananda W Goldrath4, Zihai Li3, David J Cole1, Mark P Rubinstein5.
Abstract
Interleukin-2 (IL-2) is a lymphocyte growth factor that is an important component of many immune-based cancer therapies. The efficacy of IL-2 is thought to be limited by the expansion of T regulatory cells, which express the high-affinity IL-2 receptor subunit IL-2Rα. IL-15 is under investigation as an alternative to IL-2. Although both cytokines signal through IL-2Rβγ, IL-15 does not bind IL-2Rα and therefore induces less T regulatory cell expansion. However, we found that transferred effector CD8(+) T cells induced curative responses in lymphoreplete mice only with IL-2-based therapy. Although conventional in vitro assays showed similar effector T cell responsiveness to IL-2 and IL-15, upon removal of free cytokine, IL-2 mediated sustained signaling dependent on IL-2Rα. Mechanistically, IL-2Rα sustained signaling by promoting a cell surface IL-2 reservoir and recycling of IL-2 back to the cell surface. Our results demonstrate that IL-2Rα endows T cells with the ability to compete temporally for limited IL-2 via mechanisms beyond ligand affinity. These results suggest that strategies to enhance IL-2Rα expression on tumor-reactive lymphocytes may facilitate the development of more effective IL-2-based therapies.Entities:
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Year: 2015 PMID: 26511507 PMCID: PMC4805116 DOI: 10.1126/scitranslmed.aac8155
Source DB: PubMed Journal: Sci Transl Med ISSN: 1946-6234 Impact factor: 17.956