Single-cell transcriptome analysis reveals dynamic changes of the preclinical A549 cancer models, and the mechanism of dacomitinib

转录组 A549电池 生物 癌症研究 体外 细胞生物学 药理学 化学 基因表达 基因 遗传学
作者
Xiaoyan Chen,Yangziwei Yu,Haoyang Zheng,Yang Ming,Chuqiao Wang,Qianqian Cai,Weiguo Zhang,Feixiang Jiang,Zhu YanMei,Hedi Yang,Tianbiao Zhang,Zhaoli Zhou
出处
期刊:European Journal of Pharmacology [Elsevier]
卷期号:960: 176046-176046
标识
DOI:10.1016/j.ejphar.2023.176046
摘要

The in vitro A549 cells, and A549 xenografts in nude mouse, were two commonly used models for anti-cancer drug discovery. However, the biological and molecular characteristics of these two classic models, and also the dynamic transcriptome changes after dacomitinib exposure remains elusive. We performed single-cell RNA sequencing to define the transcriptome profile at single-cell resolution, and processed tumor samples for bulk RNA and protein analysis to validate the differently expressed genes. Transcriptome profiling revealed that the in vitro A549 cells are heterogeneous. The minimal subpopulation of the in vitro A549 cells, which were characterized by the signature of response to unfolded protein, became the overriding subpopulation of the xenografts. The EGFR non-activating A549 cells were resistant to dacomitinib in vitro, while A549 xenografts were comparatively sensitive as EGFR-activating HCC827 xenografts. Dacomitinib inhibited MAPK signaling pathway, and increased the immune response in the A549 xenografts. A phagocytosis checkpoint stanniocalcin-1 (STC1) was significantly inhibited in dacomitinib-treated xenografts. So here our study gives the first insight of the heterogeneity of the two classic models, and the translational potential of dacomitinib being used into a broader patient population rather than EGFR common activating mutation.
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