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局限性前列腺肿瘤的多重成像显示微环境中雄激素受体(AR)阳性细胞的空间组织发生改变。

Multiplex imaging of localized prostate tumors reveals altered spatial organization of AR-positive cells in the microenvironment.

作者信息

Ak Çiğdem, Sayar Zeynep, Thibault Guillaume, Burlingame Erik A, Kuykendall M J, Eng Jennifer, Chitsazan Alex, Chin Koei, Adey Andrew C, Boniface Christopher, Spellman Paul T, Thomas George V, Kopp Ryan P, Demir Emek, Chang Young Hwan, Stavrinides Vasilis, Eksi Sebnem Ece

机构信息

Cancer Early Detection Advanced Research (CEDAR), Knight Cancer Institute, OHSU, Portland, OR 97239, USA.

Department of Biomedical Engineering, School of Medicine, OHSU, Portland, OR 97209, USA.

出版信息

iScience. 2024 Aug 3;27(9):110668. doi: 10.1016/j.isci.2024.110668. eCollection 2024 Sep 20.

Abstract

Mapping the spatial interactions of cancer, immune, and stromal cell states presents novel opportunities for patient stratification and for advancing immunotherapy. While single-cell studies revealed significant molecular heterogeneity in prostate cancer cells, the impact of spatial stromal cell heterogeneity remains poorly understood. Here, we used cyclic immunofluorescent imaging on whole-tissue sections to uncover novel spatial associations between cancer and stromal cells in low- and high-grade prostate tumors and tumor-adjacent normal tissues. Our results provide a spatial map of single cells and recurrent cellular neighborhoods in the prostate tumor microenvironment of treatment-naive patients. We report unique populations of mast cells that show distinct spatial associations with M2 macrophages and regulatory T cells. Our results show disease-specific neighborhoods that are primarily driven by androgen receptor-positive (AR+) stromal cells and identify inflammatory gene networks active in AR+ prostate stroma.

摘要

绘制癌症、免疫和基质细胞状态的空间相互作用图为患者分层和推进免疫治疗提供了新的机会。虽然单细胞研究揭示了前列腺癌细胞中显著的分子异质性,但空间基质细胞异质性的影响仍知之甚少。在这里,我们对全组织切片进行循环免疫荧光成像,以揭示低级别和高级别前列腺肿瘤以及肿瘤邻近正常组织中癌症与基质细胞之间新的空间关联。我们的结果提供了未经治疗患者前列腺肿瘤微环境中单细胞和反复出现的细胞邻域的空间图谱。我们报告了独特的肥大细胞群体,它们与M2巨噬细胞和调节性T细胞表现出不同的空间关联。我们的结果显示了主要由雄激素受体阳性(AR+)基质细胞驱动的疾病特异性邻域,并确定了在AR+前列腺基质中活跃的炎症基因网络。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4fff/11379676/7813076b8f7b/fx1.jpg

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