Project description:Biliary tract cancers (BTCs) are lethal malignancies, including intrahepatic and extrahepatic cholangiocarcinoma, gallbladder carcinoma, and ampullary carcinoma. Through multi-omics profiling and CRISPR screens of 63 BTC cell lines, we identify widespread EGFR dependency and subtype-specific vulnerabilities with predictive markers. Strategies to overcome targeted therapy resistance include EGFR inhibition potentiating mutant-KRAS and FGFR inhibition, while SHP2 inhibition counters FGFR inhibitor resistance. Clustering by gene/protein expression and dependencies reveals functional subtypes ductal, squamous, and bi-lineage each with distinct survival dependencies. Transcriptional analysis of patient samples highlights the prognostic value of this classification. This BTC cell line atlas uncovers therapeutic targets, defines disease subtypes, and serves as a critical resource for BTC research. Multiplexed proteomics was performed using TMT tags (TMT1 to TMT12) and TMTpro tags (TMT13 to TMT17) and the SPS3 method on an Orbitrap Fusion Lumos instrument. Sample key is as follows: CCLP (ICCL_TMT2:129c, ICCL_TMT6:127n), CCSW1(ICCL_TMT2:128c, ICCL_TMT7:130c), AOVC1 (ICCL_TMT9:129n, ICCL_TMT10:129c), EGI1(ICCL_TMT16:126, ICCL_TMT16:127n), ETK1 (ICCL_TMT16:127c, ICCL_TMT16:128n), G415 (ICCL_TMT11:129c, ICCLTMT12:130n), GB2 (ICCL_TMT1:127n, ICCL_TMT5:128n), HKGZCC (ICCL_TMT4:129n, ICCL_TMT8:128c), HUCCT1 (ICCL_TMT1:127c, ICCL_TMT6:129n), HUH28 (ICCL_TMT4:130n, ICCL_TMT8:128n), GB3 (ICCL_TMT3:131n, ICCL_TMT7:131n), ICC10 (ICCL_TMT1:128c, ICCL_TMT7:126), ICC10-6 (ICCL_TMT4:128n, ICCL_TMT7:127n), ICC10-8 (ICCL_TMT2:131n, ICCL_TMT7:127c), ICC11 (ICCL_TMT4:128c, ICCL_TMT5:129n), ICC12 (ICCL_TMT4:130c, ICCL_TMT6:129c), ICC13-7 (ICCL_TMT2:126, ICCL_TMT8:127c, ICCL_TMT11:129n, ICCL_TMT12:131n), ECC3 (ICCL_TMT1:128n, ICCL_TMT5:127c), ICC16 (ICCL_TMT11:128n, ICCL_TMT12:128c), ICC17 (ICCL_TMT3:129c, ICCL_TMT7:129n), ICC18 (ICCL_TMT13:127c, ICCL_TMT13:128n), ICC19 (ICCL_TMT11:128c, ICCL_TMT12:127c), ICC2 (ICCL_TMT4:127c, ICCL_TMT5:126), ICC20 (ICCL_TMT13:128c, ICCL_TMT13:129n), ICC21 (ICCL_TMT14:131n, ICCL_TMT14:131c), ICC24 (ICCL_TMT13:129c, ICCL_TMT13:130n), ICC25 (ICCL_TMT13:130c, ICCL_TMT13:131n), ICC26 (ICCL_TMT15:128c, ICCL_TMT15:129n), ECC4 (ICCL_TMT4:127n, ICCL_TMT6:131n, ICCL_TMT13:126, ICCL_TMT13:127n), ICC4 (ICCL_TMT9:128n, ICCL_TMT10:130n), ICC5 (ICCL_TMT3:127c, ICCL_TMT6:130n), ICC8 (ICCL_TMT2:127n, ICCL_TMT7:129c), ICC9 (ICCL_TMT2:127c, ICCL_TMT7:128c), KKU100 (ICCL_TMT9:127n, ICCL_TMT10:131n), KKU312 (ICCL_TMT9:129c, ICCL_TMT10:127n), GB4 (ICCL_TMT15:127n, ICCL_TMT15:128n), NOZ (ICCL_TMT16:132c, ICCL_TMT16:133n), OCUG1 (ICCL_TMT16:129n), RBE (ICCL_TMT1:126, ICCL_TMT7:128n), SG231 (ICCL_TMT9:126, ICCL_TMT10:127c), SNU1079 (ICCL_TMT9:130c, ICCL_TMT10:128n), SNU1196 (ICCL_TMT1:130n, ICCL_TMT8:130n), SNU245 (ICCL_TMT17:128n, ICCL_TMT17:129c), SNU308 (ICCL_TMT4:131n, ICCL_TMT8:131n), SNU478 (ICCL_TMT2:128n, ICCL_TMT6:130c), SNU869 (ICCL_TMT4:129c, ICCL_TMT5:130n), SSP25 (ICCL_TMT2:130c, ICCL_TMT5, 131n), TFK1 (ICCL_TMT17:126, ICCL_TMT17:130c) TGC1TKB (ICCL_TMT17:127c, ICCL_TMT17:129n), TGBC52TKB (ICCL_TMT11:130c, ICCL_TMT12:128n), TKKK (ICCL_TMT9:128c, ICCL_TTM10:129n), YSCCC (ICCL_TMT9:127c, ICCL_TMT10:126), ICC7 (ICCL_TMT3:128c, ICCL_TMT5:129c), OZ (ICCL_TMT11:127n, ICCL_TMT12:129n), KMCH1 (ICCL_TMT1:129n, ICCL_TMT8:129c), KKU055 (ICCL_TMT16:131c), ICC28 (ICCL_TMT2:132n, ICCL_TMT3:126), TGBC14TKB (ICCL_TMT11:131n, ICCL_TMT12:130c), PLCPRF5 (ICCL_TMT14:129n, ICCL_TMT14:129c) TONG (ICCL_TMT14:127n, ICCL_TMT14:127c), HUH7 (ICCL_TMT15:129c, ICCL_TMT14:130n, ICCL_TMT14:130c), SNU449 (ICCL_TMT15:131n), SNU387 (ICCL_TMT17:126, ICCL_TMT17:128c), JHH7 (ICCL_TMT15:130n, ICCL_TMT1:130c), SNU475 (ICCL_TMT17:130n, ICCL_TMT17:132n), HEPG2 (ICCL_TMT13:131c, ICCL_TMT13:132n), SNU423 (ICCL_TMT17:131n, ICC_TMT17:131c)

Project description:Oncogenic mutations in the EGFR gene account for 15-20% of lung adenocarcinoma (LUAD) cases. However, the mechanism for EGFR driven tumor development and growth is not fully understood. Here, using a mRNA expression profiling-based approach we identified betacellulin (BTC) as one the gene upregulated by oncogenic EGFR in a MAP kinase-dependent manner. BTC protein expression was markedly increased in LUAD patient samples compared to normal lung tissue, with higher expression in EGFR-mutant LUAD. BTC was sufficient to transform immortalized mouse cells, initiate tumor development in mice, and promote the survival of immortalized human lung epithelial cells. Conversely, knockdown of BTC inhibited the growth of EGFR-mutant human LUAD cells in culture and their tumor-forming ability in mice. Mechanistically, BTC knockdown resulted in attenuated EGFR signaling and apoptosis induction. Collectively, these results demonstrate a key role of BTC in EGFR-mutant LUAD, with potential therapeutic implications in LUAD and other EGFR-mutant cancers.

Project description:Biliary tract carcinoma (BTC) has a poor prognosis due to limited treatment options. There is therefore urgent need to identify new targets and to design innovative therapeutic approaches. Among potential candidate molecules, we evaluated the non-receptor tyrosine kinase Src, observing promising antitumor effects of its small molecule inhibitor Saracatinib in BTC preclinical models. The presence of an active Src protein was investigated by immunohistochemistry in 19 surgical samples from BTC patients. Upon Saracatinib treatment, the phosphorylation of Src and of its downstream transducers was evaluated in the BTC cell lines TFK-1, EGI-1, HuH28 and TGBC1-TKB. The effect of Saracatinib on proliferation and migration was analyzed in these same cell lines, and its antitumor activity was essayed in EGI-1 mouse xenografts. Saracatinib-modulated transcriptome was profiled in EGI-1 cells and in tumor samples of the xenograft model. Src was activated in about 80% of the human BTC samples. In cultured BTC cell lines, low-dose Saracatinib counteracted the activation of Src and of its downstream effectors, increased the fraction of cells in G0/G1 phase, and inhibited cell migration. At high concentrations (median dose from 2.26 to 6.99 µM), Saracatinib was also capable of inhibiting BTC cell proliferation. In vivo, Saracatinib treatment resulted in delayed tumor growth, associated with an impaired vascular network. We here provide a demonstration that the targeted inhibition of Src kinase by Saracatinib is of therapeutic benefit in preclinical models of BTC. We propose our results as a basis for the design of Saracatinib-based clinical applications. EGI-1 cell line treated with Saracatinib at the dose of 10 µM vs EGI-1 cell line untreated; EGI-1 xenograft treated with Saracatinib at the dose of 25 mg/Kg/die vs EGI-1 xenograft untreated Transcriptional alteration mediated by Saracatinib in vitro and in vivo

Project description:Adenocarcinomas of the ampulla of Vater are classified as biliary cancers, though the exact epithelium of origin for these cancers is not known. We sought to molecularly classify ampullary adenocarcinomas in comparison to known adenocarcinomas of the pancreas, extrahepatic bile duct, and duodenum by gene expression analysis. We analyzed 32 fresh-frozen resected, untreated periampullary adenocarcinomas (8 pancreatic, 2 extrahepatic biliary, 8 duodenal, and 14 ampullary) using the Affymetrix U133 Plus 2.0 genome array.

Project description:Purpose: Biliary tract cancers (BTCs) carry a very poor prognosis and have no approved targeted therapies. Recent genomic profiling of primary BTCs identified a number of potentially actionable drug targets, however accurate model systems to evaluate these targets are currently lacking. The purpose of this study was to compare the genomic landscape of commonly used BTC cell lines to primary BTCs, and to utilize these models for drug target evaluation. Design: Twenty BTC cell lines were profiled by RNA-seq analysis. Results: Transcriptomic profiling of BTC cell lines identified two subtypes, enriched for epithelial and mesenchymal genes respectively, which were also identified in primary BTC. Conclusions: Cell lines harbor similar genomic alterations to primary BTCs. Integration of cell line and primary cancer data identify novel molecular subsets, and highlight specific molecular vulnerabilities in BTC.

Project description:Biliary tract carcinoma (BTC) has a poor prognosis due to limited treatment options. There is therefore urgent need to identify new targets and to design innovative therapeutic approaches. Among potential candidate molecules, we evaluated the non-receptor tyrosine kinase Src, observing promising antitumor effects of its small molecule inhibitor Saracatinib in BTC preclinical models. The presence of an active Src protein was investigated by immunohistochemistry in 19 surgical samples from BTC patients. Upon Saracatinib treatment, the phosphorylation of Src and of its downstream transducers was evaluated in the BTC cell lines TFK-1, EGI-1, HuH28 and TGBC1-TKB. The effect of Saracatinib on proliferation and migration was analyzed in these same cell lines, and its antitumor activity was essayed in EGI-1 mouse xenografts. Saracatinib-modulated transcriptome was profiled in EGI-1 cells and in tumor samples of the xenograft model. Src was activated in about 80% of the human BTC samples. In cultured BTC cell lines, low-dose Saracatinib counteracted the activation of Src and of its downstream effectors, increased the fraction of cells in G0/G1 phase, and inhibited cell migration. At high concentrations (median dose from 2.26 to 6.99 µM), Saracatinib was also capable of inhibiting BTC cell proliferation. In vivo, Saracatinib treatment resulted in delayed tumor growth, associated with an impaired vascular network. We here provide a demonstration that the targeted inhibition of Src kinase by Saracatinib is of therapeutic benefit in preclinical models of BTC. We propose our results as a basis for the design of Saracatinib-based clinical applications.

Project description:Identifying the spectrum of genes required for cancer cell survival can reveal essential cancer circuitry and therapeutic targets, but such a map remains incomplete for many cancer types. We apply genome-scale CRISPR-Cas9 loss-of-function screens to map the landscape of selectively essential genes in chordoma, a bone cancer with few validated targets. This approach confirms a known chordoma dependency, TBXT (T; brachyury), and identifies a range of additional dependencies, including PTPN11, ADAR, PRKRA, LUC7L2, SRRM2, SLC2A1, SLC7A5, FANCM, and THAP1. CDK6, SOX9, and EGFR, genes previously implicated in chordoma biology, are also recovered. We find genomic and transcriptomic features that predict specific dependencies, including interferon-stimulated gene expression, which correlates with ADAR dependence and is elevated in chordoma. Validating the therapeutic relevance of dependencies, small-molecule inhibitors of SHP2, encoded by PTPN11, have potent preclinical efficacy against chordoma. Our results generate an emerging map of chordoma dependencies to enable biological and therapeutic hypotheses.

Project description:To uncover the full repertoire of genetic and transcriptomic landscape of biliary tract cancer (BTC), we molecularly characterized BTC based on genetic and transcriptomic alteration profiles.

Project description:Mutational signatures define immune and Wnt-associated subtypes of ampullary carcinoma

Project description:Gene expression profiling of ampullary carcinomas classifies ampullary carcinomas into biliary-like and intestinal-like subtypes that are prognostic of outcome