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Dietary γ-mangostin triggers immunogenic cell death and activates cGAS signaling in acute myeloid leukemia

Pharmacological Research, ISSN: 1043-6618, Vol: 197, Page: 106973
2023
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Sun Yat-sen University Researchers Detail Findings in Acute Myeloid Leukemia (Dietary g-mangostin triggers immunogenic cell death and activates cGAS signaling in acute myeloid leukemia)

2023 NOV 30 (NewsRx) -- By a News Reporter-Staff News Editor at NewsRx Hematology Daily -- New research on acute myeloid leukemia is the subject

Article Description

Immunogenic cell death (ICD), one of cell-death types through release of damage-associated molecular patterns from dying tumor cells, activates tumor-specific immune response and elicits anti-tumor immunity by traditional radiotherapy and chemotherapy. However, whether natural products could induce ICD in leukemia is not elucidated. Here, we report dietary γ-mangostin eradicates murine primary leukemic cells and prolongs the survival of leukemic mice. As well, it restrains primary leukemic cells and CD34 + leukemic progenitor cells from leukemia patients. Strikingly, γ-mangostin attenuates leukemic cells by inducing ICD as characterized by expression of HSP90B1, ANXA1 and IL1B. Additionally, γ-mangostin accelerates cytoplasmic chromatin fragments generation, promoting DNA damage response, and enhances cGAS activation, leading to up-regulation of chemokines. Meanwhile, it induces HDAC4 degradation and acetylated histone H3 accumulation, which promotes chemokines transcription. Ultimately, CD8 + T cell is activated and recruited by γ-mangostin-induced chemokines in the microenvironment. Our study identifies γ-mangostin triggers ICD and activates cGAS signaling through DNA damage response and epigenetic modification. Therefore, dietary γ-mangostin would act as a potential agent to provoke anti-tumor immunity in the prevention and treatment of leukemia.

Bibliographic Details

Long, Zi-Jie; Wang, Jun-Dan; Qiu, Sheng-Xiang; Zhang, Yi; Wu, Si-Jin; Lei, Xin-Xing; Huang, Ze-Wei; Chen, Jia-Jie; Yang, Yong-Liang; Zhang, Xiang-Zhong; Liu, Quentin

Elsevier BV

Pharmacology, Toxicology and Pharmaceutics

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