4.7 Article

Mesenchymal stromal cells as carriers of IL-12 reduce primary and metastatic tumors of murine melanoma

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SCIENTIFIC REPORTS
卷 11, 期 1, 页码 -

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NATURE PORTFOLIO
DOI: 10.1038/s41598-021-97435-9

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  1. National Science Centre, Poland [UMO-2015/17/N/NZ4/02738]

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The study demonstrated that MSC are effective carriers of IL-12 cytokine, showing anti-tumor effects in primary and metastatic melanoma models. The use of MSC as carriers allowed for intravenous administration of IL-12 without toxic side effects, resulting in reduced tumor growth and metastases, decreased vascular density, and increased immune response in treated mice. Therapeutic properties of IL-12 cytokine were successfully exerted by modified MSC without inducing toxicity.
Due to immunosuppressive properties and confirmed tropism towards cancer cells mesenchymal stromal cells (MSC) have been used in many trials. In our study we used these cells as carriers of IL-12 in the treatment of mice with primary and metastatic B16-F10 melanomas. IL-12 has confirmed anti-cancer activity, induces a strong immune response against cancer cells and acts as an anti-angiogenic agent. A major limitation of the use of IL-12 in therapy is its systemic toxicity. The aim of the work was to develop a system in which cytokine may be administered intravenously without toxic side effects. In this study MSC were used as carriers of the IL-12. We confirmed antitumor effectiveness of the cells secreting IL-12 (MSC/IL-12) in primary and metastatic murine melanoma models. We observed inhibition of tumor growth and a significant reduction in the number of metastases in mice after MSC/IL-12 administration. MSC/IL-12 decreased vascular density and increased the number of anticancer M1 macrophages and CD8(+) cytotoxic T lymphocytes in tumors of treated mice. To summarize, we showed that MSC are an effective, safe carrier of IL-12 cytokine. Administered systemically they exert therapeutic properties of IL-12 cytokine without toxicity. Therapeutic effect may be a result of pleiotropic (proinflammatory and anti-angiogenic) properties of IL-12 released by modified MSC.

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