Dynamic Responses of Circulating T Cells After Stereotactic Body Radiation Therapy for Bone Metastasis in Patients With Breast Cancer.

Int J Radiat Oncol Biol Phys

Department of Radiation Oncology, Seoul National University Bundang Hospital, Seongnam, Republic of Korea; Department of Radiation Oncology, Seoul National University College of Medicine, Seoul, Republic of Korea; Medical Science Research Institute, Seoul National University Bundang Hospital, Seongnam, Republic of Korea; Department of Tumor Biology and Cancer Research Institute, Seoul National University, Seoul, Republic of Korea; Integrated Major in Innovative Medical Science, Seoul National University Graduate School, Seoul, Republic of Korea. Electronic address:

Published: March 2024

Purpose: Preclinical studies have shown that radiation therapy modulates antitumor immune responses. However, circulating T-cell responses after radiation therapy in patients with cancer have been poorly characterized. This study aims to explore the changes in circulating T cells after stereotactic body radiation therapy (SBRT).

Methods And Materials: Peripheral blood samples of 30 patients with breast cancer who underwent SBRT for bone metastasis were analyzed using multicolor flow cytometry. Phenotypes of PD-1 CD8 T cells and regulatory T (T) cells were examined. Additionally, plasma protein levels were analyzed using a bead-based immunoassay.

Results: Circulating PD-1 CD8 T cells, which are enriched for tumor-specific clonotypes, were activated at 1 week after SBRT. However, circulating T cells were also activated after SBRT; this pattern was also evident among effector Foxp3CD45RA T cells. We observed no difference in T-cell responses according to the fraction size and number. Notably, activation of T cells was more prominent in patients who experienced greater activation of PD-1 CD8 T cells. Plasma level changes in TGF-β1, soluble CTLA-4, and soluble 4-1BB at 1 week after SBRT were associated with PD-1 CD8 T-cell responses. Activation of T cells at 1 week after SBRT was associated with worse progression-free survival. Clinical factors including molecular subtype were not associated with the T-cell responses.

Conclusions: SBRT induced activation of both potentially tumor-specific CD8 T cells and T cells, which were tightly associated with each other. These results may support the use of T cell-modulating strategies with SBRT to improve the antitumor immune response.

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http://dx.doi.org/10.1016/j.ijrobp.2023.09.020DOI Listing

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