V gamma 1 gamma-delta T cells steer airway macrophages towards a pro-fibrotic response in an autochthonous lung cancer mouse model [scRNA-Seq]
收藏NIAID Data Ecosystem2026-05-10 收录
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https://www.ncbi.nlm.nih.gov/sra/SRP618406
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Gamma-delta T cells are important for host defence at the respiratory mucosa, acting directly or through interactions with other cells. However, how Gamma-Delta T cells influence other immune cells in the lung remains unclear. Using a genetically engineered mouse model of lung cancer, we show that tumours drive expansion of both CD27+ and CD27â Gamma-Delta T cells. Advanced microscopy techniques indicated that CD27â Gamma-Delta T cells are enriched in tumours, while CD27+ Gamma-Delta T cells are more prone to interact with macrophages in tumour-associated adventitial cuffs. SiglecFlow pro-fibrotic airway macrophages were more prevalent in lung tumour-bearing mice than tumour-free mice. This pro-fibrotic subset was reduced in lungs when the cancer model was crossed to Tcrd knockout mice or treated with V Gamma1-depleting antibodies, but not in TcrgV4/6 knockout mice. Thus, our findings implicate V Gamma1 Gamma-Delta T cells in driving tumour-associated airway macrophage functional imprinting. Determining the translatability to human health may offer new avenues for refining patient management and immunotherapeutic strategies. Overall design: Lung tissue from Mus musculus was extracted, and three distinct regions were sampled: tumour tissue, tumour-distant tissue, and normal tissue. Macrophages were isolated from each sample using flow cytometry. The sorted cell populations were then sequenced using the 10X Genomics Chromium Single Cell 3' protocol.
创建时间:
2026-02-06



