KRT17high/CXCL8+ Tumor Cells Display Both Classical and Basal Features and Regulate Myeloid Infiltration in the Pancreatic Cancer Microenvironment

肿瘤微环境 胰腺癌 白细胞介素8 癌症研究 生物 人口 髓样 细胞因子 癌症 免疫学 医学 免疫系统 内科学 环境卫生
作者
Eileen S. Carpenter,Padma Kadiyala,Ahmed M. Elhossiny,Samantha B. Kemp,Jay Li,Nina G. Steele,Rémy Nicolle,Zeribe C. Nwosu,Julia Freeman,Henry Dai,Daniel Paglia,Wenting Du,Katelyn L. Donahue,Jacqueline Morales,Paola I Medina-Cabrera,Monica E. Bonilla,Lindsey Harris,Stephanie The,Valerie Gunchick,Nicole Peterson,Kristee Brown,Michael Mattea,Carlos Espinoza,Jake McGue,Sarah M Kabala,Rachel K Baliira,Nur M Renollet,Ann Mooney,Jianhua Liu,Sean Bhalla,Jeremy P. Farida,Christopher Ko,Jorge D. Machicado,Richard S. Kwon,Erik–Jan Wamsteker,Allison R. Schulman,M ANDERSON,Ryan Law,Anoop Prabhu,Pierre A. Coulombe,Arvind Rao,Timothy L. Frankel,Filip Bednar,Jiaqi Shi,Vaibhav Sahai,Marina Pasca di Magliano
出处
期刊:Clinical Cancer Research [American Association for Cancer Research]
卷期号:: OF1-OF17 被引量:1
标识
DOI:10.1158/1078-0432.ccr-23-1421
摘要

Pancreatic ductal adenocarcinoma (PDAC) is generally divided in two subtypes, classical and basal. Recently, single cell RNA sequencing has uncovered the co-existence of basal and classical cancer cells, as well as intermediary cancer cells, in individual tumors. The latter remains poorly understood; here, we sought to characterize them using a multimodal approach.We performed subtyping on a single cell RNA sequencing dataset containing 18 human PDAC samples to identify multiple intermediary subtypes. We generated patient-derived PDAC organoids for functional studies. We compared single cell profiling of matched blood and tumor samples to measure changes in the local and systemic immune microenvironment. We then leveraged longitudinally patient-matched blood to follow individual patients over the course of chemotherapy.We identified a cluster of KRT17-high intermediary cancer cells that uniquely express high levels of CXCL8 and other cytokines. The proportion of KRT17High/CXCL8+ cells in patient tumors correlated with intra-tumoral myeloid abundance, and, interestingly, high pro-tumor peripheral blood granulocytes, implicating local and systemic roles. Patient-derived organoids maintained KRT17High/CXCL8+cells and induced myeloid cell migration in an CXCL8-dependent manner. In our longitudinal studies, plasma CXCL8 decreased following chemotherapy in responsive patients, while CXCL8 persistence portended worse prognosis.Through single cell analysis of PDAC samples we identified KRT17High/CXCL8+ cancer cells as an intermediary subtype, marked by a unique cytokine profile and capable of influencing myeloid cells in the tumor microenvironment and systemically. The abundance of this cell population should be considered for patient stratification in precision immunotherapy.
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