New therapeutic strategies based on biasing IL-2 mutants for cancers and autoimmune diseases

•IL-2 is the key cytokine to maintain Treg and Teff cell functions.•Engineering IL-2 with biased effecacies on cancer or autoimmune diseases.•New therapeutic strategies including IL-2 mutants, IL-2/mAb complexes, IL-2 fusion proteins.•These methods extends half-life, reduces toxicity, and increases...

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Veröffentlicht in:International immunopharmacology 2022-09, Vol.110, p.108935-108935, Article 108935
Hauptverfasser: Jin, Dongfu, Jiang, Yaxin, Chang, Lu, Wei, Jing, Sun, Jian
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Sprache:eng
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Zusammenfassung:•IL-2 is the key cytokine to maintain Treg and Teff cell functions.•Engineering IL-2 with biased effecacies on cancer or autoimmune diseases.•New therapeutic strategies including IL-2 mutants, IL-2/mAb complexes, IL-2 fusion proteins.•These methods extends half-life, reduces toxicity, and increases specificity of IL-2. Interleukin-2 (IL-2) is an immunomodulatory multifunctional cytokine. High-dose IL-2 was first approved by the U.S. Food and Drug Administration (FDA) in the 1990s for the treatment of metastatic renal cell carcinoma and metastatic melanoma. However, the short half-life of IL-2 and its toxicity caused by high-dose IL-2 limit the clinical use of IL-2. Recently, the development of cell-type-selective engineered IL-2 products become a hot research filed, mainly because IL-2 stimulates both regulatory T cells (Treg) and effector T cells (Teff) in vivo. The selective effect of IL-2 on Treg and Teff can be improved by designing biased IL-2 mutants, which showed reduced toxicity while being more effective in stimulating anti-tumor effector immunity or ameliorating autoimmune diseases. In this review we summarize the biological properties of IL-2 mutants reported so far. The design process and principle of IL-2 mutants, IL-2 mutant antibody complexes and IL-2 fusion proteins were discussed, which provided research basis for the design and application of IL-2 mutants in the future.
ISSN:1567-5769
1878-1705
DOI:10.1016/j.intimp.2022.108935