Abstract

? PROJECT 2 Cyclin D1 deregulation is observed frequently observed in human cancers especially in esophageal squamous cell carcinoma (ESCC) and esophageal adenocarcinomas (EAC). This deregulation implies that the cyclin D1/CDK4 kinase provides cells with a growth advantage, thereby contributing to cancer development. We have demonstrated that loss of Fbxo4, a component of the E3 ligase, SCFFBXO4, occurs in ESCC and FBXO4 knockout mice are susceptible to tumors. Additional work has revealed that FBXO4 regulates degradation of two distinct oncogenes in ESCC: cyclin D1 and FXR1. Overexpression of cyclin D1 increases mitogen- independent cell proliferation and FXR1 overexpression contributes to bypass of cell senescence and collective tumor initiation. In our new preliminary data, we have discovered that loss of FBXO4 results in cell addiction to Glutamine. In this context, glutamine appears essential due to its metabolic role, wherein it is metabolized to ?-ketoglutarate, an intermediate in the TCA cycle. Cells with mutant FBXO4 quickly undergo apoptosis under conditions of glutamine restriction. Given the generation of inhibitors of glutaminase, this observation provides a potential novel strategy for therapeutic intervention. These exciting discoveries provide critical insights into the mechanisms whereby FBXO4 suppresses neoplastic growth and support the notion that targets of FBXO4 such as FXR1 and cyclin D1/CDK4 activity are key esophageal cancer drivers. The identification of the SCFFBX4 as the cyclin D1 E3 ligase as well as our preliminary studies lead to the overarching hypothesis that the SCFFBX4 E3 ligase maintains threshold levels of the cyclin D1/CDK4 kinase and the FXR1, an RNA binding protein, to maintain esophageal tissue homeostasis. We hypothesize further that cyclin D1 and FXR1 overexpression foster ESCC progression, resulting in cellular vulnerabilities that can be rationally targeted. This hypothesis will be pursued through the following interrelated Specific Aims: (1) To determine the contribution of deregulated cyclin D1 to mutant FBXO4 driven glutamine-dependence in esophageal cancer; (2) To determine the mechanism(s) whereby mutant p53R172H cooperates with cyclin D1T286A to drive ESCC pathogenesis; and (3) To determine the therapeutic potential of targeting glutamine- metabolism in ESCC with dysregulated cyclin D/CDK4. Our collaborative work with Projects 1 and 2, along with support from the Core Facilities, provides new basic and translational perspectives on the cyclin D1/CDK4/CDK6 axis and glutamine metabolism in ESCC.

Public Health Relevance

? PROJECT 2 Cyclin D1 overexpression in human esophageal cancer occurs frequently as a consequence of mutations in the machinery that destroys the cyclin D1 protein. In order to develop effective therapies that counter these events, we have identified the critical component of the machinery, Fbxo4, which directs destruction of the cyclin D1 protein. The experiments in this proposal test the biological properties of Fbxo4 in esophageal cancer and determine the efficacy of therapeutic approaches target therapeutic vulnerabilities associated with cyclin D1/CDK4/CDK6 and glutamine metabolism.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
2P01CA098101-16
Application #
9704630
Study Section
Special Emphasis Panel (ZCA1)
Project Start
2003-08-15
Project End
2024-06-30
Budget Start
2019-04-01
Budget End
2020-03-31
Support Year
16
Fiscal Year
2019
Total Cost
Indirect Cost

  Institution

Name
University of Pennsylvania
Department
Type
DUNS #
042250712
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

Wong, Gabrielle S; Zhou, Jin; Liu, Jie Bin et al. (2018) Targeting wild-type KRAS-amplified gastroesophageal cancer through combined MEK and SHP2 inhibition. Nat Med 24:968-977
Karakasheva, Tatiana A; Dominguez, George A; Hashimoto, Ayumi et al. (2018) CD38+ M-MDSC expansion characterizes a subset of advanced colorectal cancer patients. JCI Insight 3:
Liu, Yang; Sethi, Nilay S; Hinoue, Toshinori et al. (2018) Comparative Molecular Analysis of Gastrointestinal Adenocarcinomas. Cancer Cell 33:721-735.e8
Facompre, Nicole D; Harmeyer, Kayla M; Sahu, Varun et al. (2018) Targeting JARID1B's demethylase activity blocks a subset of its functions in oral cancer. Oncotarget 9:8985-8998
Deng, Jiehui; Wang, Eric S; Jenkins, Russell W et al. (2018) CDK4/6 Inhibition Augments Antitumor Immunity by Enhancing T-cell Activation. Cancer Discov 8:216-233
Karakasheva, Tatiana A; Lin, Eric W; Tang, Qiaosi et al. (2018) IL-6 Mediates Cross-Talk between Tumor Cells and Activated Fibroblasts in the Tumor Microenvironment. Cancer Res 78:4957-4970
Kasagi, Yuta; Chandramouleeswaran, Prasanna M; Whelan, Kelly A et al. (2018) The Esophageal Organoid System Reveals Functional Interplay Between Notch and Cytokines in Reactive Epithelial Changes. Cell Mol Gastroenterol Hepatol 5:333-352
Pectasides, Eirini; Stachler, Matthew D; Derks, Sarah et al. (2018) Genomic Heterogeneity as a Barrier to Precision Medicine in Gastroesophageal Adenocarcinoma. Cancer Discov 8:37-48
Campbell, Joshua D; Yau, Christina; Bowlby, Reanne et al. (2018) Genomic, Pathway Network, and Immunologic Features Distinguishing Squamous Carcinomas. Cell Rep 23:194-212.e6
Whelan, Kelly A; Muir, Amanda B; Nakagawa, Hiroshi (2018) Esophageal 3D Culture Systems as Modeling Tools in Esophageal Epithelial Pathobiology and Personalized Medicine. Cell Mol Gastroenterol Hepatol 5:461-478

Showing the most recent 10 out of 173 publications