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An intra-tumoral niche maintains and differentiates stem-like CD8 T cells

机译:肿瘤内生态位维持并分化干细胞样CD8 T细胞

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摘要

Tumour-infiltrating lymphocytes are associated with a survival benefit in several tumour types and with the response to immunotherapy(1-8). However, the reason some tumours have high CD8 T cell infiltration while others do not remains unclear. Here we investigate the requirements for maintaining a CD8 T cell response against human cancer. We find that CD8 T cells within tumours consist of distinct populations of terminally differentiated and stem-like cells. On proliferation, stem-like CD8 T cells give rise to more terminally differentiated, effector-molecule-expressing daughter cells. For many T cells to infiltrate the tumour, it is critical that this effector differentiation process occur. In addition, we show that these stem-like T cells reside in dense antigen-presenting-cell niches within the tumour, and that tumours that fail to form these structures are not extensively infiltrated by T cells. Patients with progressive disease lack these immune niches, suggesting that niche breakdown may be a key mechanism of immune escape.
机译:肿瘤浸润淋巴细胞与多种肿瘤类型的生存获益以及对免疫疗法的反应有关(1-8)。但是,尚不清楚某些肿瘤具有高CD8 T细胞浸润性的原因。在这里,我们研究了维持针对人类癌症的CD8 T细胞反应的要求。我们发现,肿瘤内的CD8 T细胞由不同的终末分化和干细胞样细胞组成。增殖时,干细胞样CD8 T细胞产生更多末端分化的表达效应分子的子细胞。对于许多T细胞浸润肿瘤而言,至关重要的是发生这种效应物分化过程。此外,我们显示这些干样T细胞驻留在肿瘤内的致密抗原呈递细胞壁ches中,未能形成这些结构的肿瘤不会被T细胞广泛浸润。进行性疾病的患者缺乏这些免疫功能,这表明小生境破坏可能是免疫逃逸的关键机制。

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