PO.MCB08.02 · 分子与细胞生物学

Genomic analyses of patient-derived xenografts reveal novel molecular subsets of PDAC and their association with clinical features

海报缩略图:Genomic analyses of patient-derived xenografts reveal novel molecular subsets of PDAC and their association with clinical features
编号 1982 展板 8 时间 4/20 09:00–12:00 区域 Section 23 主讲 Chani Stossel
分会场 Genomic Drivers of Cancer Pathogenesis
查看完整资料 下载 PDF 登录后可访问当前开放资料 AACR 官方页面 ↗

作者与单位

Chani Stossel1, Rotem Tal2, Rouven Hoefflin2, Maria Raitses-Gurevich1, Dikla Atias1, Yulia Glick Gorman1, Gali Altman1, Tamar Beller1, Talia Golan1, Itay Tirosh2

1Sheba Medical Center, Tel Hashomer, Israel,2Weizmann Institute of Science, Rechovot, Israel

摘要 Abstract

Pancreatic ductal adenocarcinoma (PDAC) is a dismal disease with limited therapeutic options. We have established a large-scale RNA-seq dataset comprised of >120 PDAC patient-derived xenograft (PDX) models and >300 bulk RNA-seq specimens (when counting biological replicates). This cohort includes diverse PDAC clinical manifestations, such as patients with particularly low survival (<8 weeks) that are under-represented in other large-scale efforts (e.g. TCGA). Our analysis identified two transcriptional programs with a highly heterogeneous expression among the basal-like models: a unique partial-Epithelial-to-Mesenchymal program (Basal-Mesenchymal) and an epithelial senescence-associated program (Basal-EpiSen), reminiscent of the pan-cancer epithelial senescence-associated program that we recently described in other epithelial malignancies. Notably, high expression of the Basal- Mesenchymal program is strongly associated with low-survival and with models established from patient's tumors at terminal stage. Next, we compared representative Basal- Mesenchymal and Basal-EpiSen PDAC cell lines across the comprehensive Cancer Cell Line Encyclopedia (CCLE) drug response dataset. Our initial results show differential drug sensitivity and gene dependencies between the Basal- Mesenchymal and Basal-EpiSen subsets, highlighting their potential clinical significance. We show that the Basal-like subtype diverges into two distinct clinically-relevant subsets. Taken together, our work provides an unprecedented resource towards improving PDAC molecular classification, an essential step for PDAC precision medicine.
利益披露 Disclosure
C. Stossel, None.. R. Tal, None.. R. Hoefflin, None.. M. Raitses-Gurevich, None.. D. Atias, None.. Y. Glick Gorman, None.. G. Altman, None.. T. Beller, None. T. Golan, CuResponse Stock Option, consultant. Astra Zeneca ). Abbvie ), Receipt of honoraria or consultation fees; Receipt of speakers bureau. MSD Merck Receipt of honoraria or consultation fees. ClearNoteHealth Receipt of speakers bureau. I. Tirosh, None.

在会议检索中打开