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Changes in the tumor immune microenvironment in resected recurrent soft tissue sarcomas

  
@article{ATM28500,
	author = {Biqiang Zheng and Jian Wang and Weiluo Cai and Iweng Lao and Yingqiang Shi and Xiaoying Luo and Wangjun Yan},
	title = {Changes in the tumor immune microenvironment in resected recurrent soft tissue sarcomas},
	journal = {Annals of Translational Medicine},
	volume = {7},
	number = {16},
	year = {2019},
	keywords = {},
	abstract = {Background: Little is known about how the tumor immune microenvironment (TIME) is modulated in recurrent soft tissue sarcomas (STS).
Methods: We evaluated CD8+ T cells, CD20+ B cells, Foxp3+ regulatory T cells (Tregs), and programmed cell death ligand 1 (PD-L1) in 72 paired pre-recurrent (1st resected) versus post-recurrent (2nd resected) STS by immunohistochemistry. Correlations with time to recurrence and prognosis were determined.
Results: We found that CD8, PD-L1, CD20, and Foxp3-positive cell counts changed in post-recurrent STS. PD-L1-positive tumor cell and lymphocyte counts increased in post-recurrent STS, whereas CD8+ T cell counts decreased. Changes in CD8+ T cell, CD20+ B cell, and PD-L1+ lymphocyte counts were associated with the time interval between surgeries. At admission, fewer CD8+ T cells were detected in patients with relapse than in newly diagnosed patients. Furthermore, post-recurrent STS with fewer CD8+ T cells compared with pre-recurrent STS were more likely to exhibit re-recurrence. The change in CD8+ T cells was positively associated with overall survival. In multivariate analyses, a decrease in CD8+ T cell counts in post-recurrent STS was an independent unfavorable prognostic factor.
Conclusions: The TIME differs between pre-recurrent STS and post-recurrent STS. The variation in CD8+ T cells and PD-L1 positivity may have essential roles during tumor relapse and provides a basis for determining therapeutic strategies.},
	issn = {2305-5847},	url = {https://atm.amegroups.org/article/view/28500}
}