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Targeting of the tumor microenvironment by curcumin

Xiao FuCollege of Basic Medicine Shaoyang University Shaoyang ChinaYingni HeCollege of Basic Medicine Shaoyang University Shaoyang ChinaMu LiCollege of Basic Medicine Shaoyang University Shaoyang ChinaZezhi HuangShaoyang Key Laboratory of Molecular Biology Diagnosis Shaoyang ChinaMasoud NajafiMedical Technology Research Center Institute of Health Technology, Kermanshah University of Medical Sciences Kermanshah Iran
2021en
ABI

Аннотация

The tumor microenvironment (TME) is made up of several cells and molecules that affect the survival of cancer cells. Indeed, certain (immunosuppressive) cells which promote tumors can promote the growth of tumors by stimulating the proliferation of cancer cells and promoting angiogenesis. During tumor growth, antitumoral immunity includes natural killer cells and CD8+ T cells cannot overcome immunosuppressive responses and cancer cell proliferation. In order to achieve the appropriate therapeutic response, we must kill cancer cells and suppress the release of immunosuppressive molecules. The balance between anti-tumor immunity and immunosuppressive cells, such as regulatory T cells (Tregs), cancer-associated fibroblasts, tumor-associated macrophages, and myeloid-derived suppressor cells plays a key role in the suppression or promotion of cancer cells. Curcumin is a plant-derived agent that has shown interesting properties for cancer therapy. It has shown that not only directly inhibit the growth of cancer cells, but can also modulate the growth and activity of immunosuppressant and tumor-promoting cells. In this review, we explain how curcumin modulates interactions within TME in favor of tumor treatment. The potential modulating effects of curcumin on the responses of cancer cells to treatment modalities such as immunotherapy will also be discussed.

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