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An IL-2-grafted antibody immunotherapy with potent efficacy against metastatic cancer.


ABSTRACT: Modified interleukin-2 (IL-2) formulations are being tested in cancer patients. However, IL-2 immunotherapy damages IL-2 receptor (IL-2R)-positive endothelial cells and stimulates IL-2R? (CD25)-expressing lymphocytes that curtail anti-tumor responses. A first generation of IL-2R? (CD122)-biased IL-2s addressed some of these drawbacks. Here, we present a second-generation CD122-biased IL-2, developed by splitting and permanently grafting unmutated human IL-2 (hIL-2) to its antigen-binding groove on the anti-hIL-2 monoclonal antibody NARA1, thereby generating NARA1leukin. In comparison to hIL-2/NARA1 complexes, NARA1leukin shows a longer in vivo half-life, completely avoids association with CD25, and more potently stimulates CD8+ T and natural killer cells. These effects result in strong anti-tumor responses in various pre-clinical cancer models, whereby NARA1leukin consistently surpasses the efficacy of hIL-2/NARA1 complexes in controlling metastatic disease. Collectively, NARA1leukin is a CD122-biased single-molecule construct based on unmutated hIL-2 with potent efficacy against advanced malignancies.

SUBMITTER: Sahin D 

PROVIDER: S-EPMC7755894 | biostudies-literature | 2020 Dec

REPOSITORIES: biostudies-literature

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An IL-2-grafted antibody immunotherapy with potent efficacy against metastatic cancer.

Sahin Dilara D   Arenas-Ramirez Natalia N   Rath Matthias M   Karakus Ufuk U   Hümbelin Monika M   van Gogh Merel M   Borsig Lubor L   Boyman Onur O  

Nature communications 20201222 1


Modified interleukin-2 (IL-2) formulations are being tested in cancer patients. However, IL-2 immunotherapy damages IL-2 receptor (IL-2R)-positive endothelial cells and stimulates IL-2Rα (CD25)-expressing lymphocytes that curtail anti-tumor responses. A first generation of IL-2Rβ (CD122)-biased IL-2s addressed some of these drawbacks. Here, we present a second-generation CD122-biased IL-2, developed by splitting and permanently grafting unmutated human IL-2 (hIL-2) to its antigen-binding groove  ...[more]

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