4.7 Article

Imaging Memory T-Cells Stratifies Response to Adjuvant Metformin Combined with αPD-1 Therapy

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出版社

MDPI
DOI: 10.3390/ijms232112892

关键词

immune checkpoint inhibitors (ICI); positron emission tomography (PET); potassium channels; metformin

资金

  1. Institute of Bioengineering and Bioimaging (IBB), Agency for Science, Technology and Research (A*STAR)

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Studies suggest that using metformin as an adjuvant therapy can enhance the immunological memory response in cancer treatment with immune checkpoint inhibitors (ICI). However, some combination therapies may exacerbate the immune response and lead to adverse immune-related events.
The low response rates associated with immune checkpoint inhibitor (ICI) use has led to a surge in research investigating adjuvant combination strategies in an attempt to enhance efficacy. Repurposing existing drugs as adjuvants accelerates the pace of cancer immune therapy research; however, many combinations exacerbate the immunogenic response elicited by ICIs and can lead to adverse immune-related events. Metformin, a widely used type 2 diabetes drug is an ideal candidate to repurpose as it has a good safety profile and studies suggest that metformin can modulate the tumour microenvironment, promoting a favourable environment for T cell activation but has no direct action on T cell activation on its own. In the current study we used PET imaging with [F-18]AlF-NOTA-KCNA3P, a radiopharmaceutical specifically targeting K(V)1.3 the potassium channel over-expressed on active effector memory T-cells, to determine whether combining PD1 with metformin leads to an enhanced immunological memory response in a preclinical colorectal cancer model. Flow cytometry was used to assess which immune cell populations infiltrate the tumours in response to the treatment combination. Imaging with [F-18]AlF-NOTA-KCNA3P demonstrated that adjuvant metformin significantly improved anti-PD1 efficacy and led to a robust anti-tumour immunological memory response in a syngeneic colon cancer model through changes in tumour infiltrating effector memory T-cells.

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