4.6 Article

A novel membrane-bound interleukin-2 promotes NK-92 cell persistence and anti-tumor activity

Journal

ONCOIMMUNOLOGY
Volume 11, Issue 1, Pages -

Publisher

TAYLOR & FRANCIS INC
DOI: 10.1080/2162402X.2022.2127282

Keywords

IL-2; IL-2R alpha; natural killer cells; NK cells persistence; cancer; immunotherapy; NKG2D

Funding

  1. West China Hospital, Sichuan University [ZYGD20003]
  2. National Natural Science Foundation of China [81902918]

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A novel membrane-bound IL-2 was constructed to improve the persistence and enhance the anti-tumor activity of NK-92 cells. This technology has potential significance for clinical development.
A major challenge in natural killer (NK) cell immunotherapy is the limited persistence of NK cells in vivo. However, the proliferation of NK cells is dependent on cytokines such as interleukin-2 (IL-2). Although IL-2 is a critical cytokine for NK cell activation and survival, IL-2 administration in adoptive NK cell therapy can induce adverse toxicities. To improve the persistence of NK cells and attenuate the systemic toxicity of IL-2, we constructed a cell-restricted artificial IL-2, named membrane-bound IL-2 (mbIL-2), comprising human IL-2 and human IL-2R alpha joined by a classic linker. We found that mbIL-2-activated NK-92 cells can survive and proliferate in vitro and in vivo, independent of exogenous IL-2, while mbIL-2-expressing NK-92 cells do not support bystander cell survival or proliferation. Additionally, mbIL-2 enhanced NK-92 cell-mediated antitumor activity by tuning the IL-2 receptor downstream signals and NK cell receptor repertoire expression. To conclude, our novel mbIL-2 improves NK-92 cell persistence and enhances NK-92 cell-mediated antitumor activity. NK-92 cells genetically modified to express the novel mbIL-2 with potential significance for clinical development.

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