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Organoid cultures recapitulate esophageal adenocarcinoma heterogeneity providing a model for clonality studies and precision therapeutics

机译:类器官培养物概括了食管腺癌的异质性为克隆性研究和精确治疗提供了模型

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摘要

Esophageal adenocarcinoma (EAC) incidence is increasing while 5-year survival rates remain less than 15%. A lack of experimental models has hampered progress. We have generated clinically annotated EAC organoid cultures that recapitulate the morphology, genomic, and transcriptomic landscape of the primary tumor including point mutations, copy number alterations, and mutational signatures. Karyotyping of organoid cultures has confirmed polyclonality reflecting the clonal architecture of the primary tumor. Furthermore, subclones underwent clonal selection associated with driver gene status. Medium throughput drug sensitivity testing demonstrates the potential of targeting receptor tyrosine kinases and downstream mediators. EAC organoid cultures provide a pre-clinical tool for studies of clonal evolution and precision therapeutics.
机译:食道腺癌(EAC)的发病率正在增加,而5年生存率仍不到15%。缺乏实验模型阻碍了进展。我们已经生成了带有临床注释的EAC类器官培养物,该培养物概述了原发肿瘤的形态,基因组和转录组学情况,包括点突变,拷贝数变化和突变特征。类器官培养物的核型分析已证实多克隆性,反映了原发性肿瘤的克隆结构。此外,对亚克隆进行与驱动基因状态相关的克隆选择。中等通量药物敏感性测试证明了靶向受体酪氨酸激酶和下游介质的潜力。 EAC类器官培养物为研究克隆进化和精确疗法提供了临床前工具。

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