Abstract

A major mechanism by which tumors survive from both chemotoxic and targeted therapies is hypothesized to be the result intra-tumoral heterogeneity. Tumor heterogeneity have been postulated to contribute to tumor evolution and therapy evasion through different mechanisms: generation of resistant subclones, cooperation between minor subclonal populations, minor subclones generating stromal signaling that favors tumor progression, etc. The genetic and epigenetic diversity that underlies tumor heterogeneity is siystematially missed by traditional genomic approaches. The overall goal of this project is to develop approaches to characterize functional dependencies and specific transcriptional programs in distinct tumor subpopulations, using single cell molecular profiling and analysis, with specific emphasis on clones and niches inducing relapse or progression.
The first aim (1) of this project is to develop and implement new methods to capture tumor clonal representation and to integrate large-scale expression and mutational analysis in single cells. This will be done by conducting deep exome and RNA sequencing together with single-cell profiling to identify point mutations, indels, and gene fusions in tumor cells.
The second aim of this project (2) is to identify epigenetically distinct cell niches with identical mutational spectra that either escape treatment or can regenerate the tumor. Clonally expanded tumor cells may be genetically identical with respect to the mutations identified in (1) but represent distinct epigenetic states, characterized by distinct gene expression signatures. The methods developed in (1) will be applied to residual tumor cells following therapy in PDX models to elucidate the drivers of drug resistance in epigenetically distinct cells. Finally the third aim (3) is to identify the molecular interactions that implement cell-cell communication processes, within a heterogenous tumor- microenviroment milieu. This will be achieved by developing novel information theoretic methodologies for the prioritization of specific ligands and receptors that mediate single cell communication and interaction. These methodologies will be specifically applied to elucidate novel tumor checkpoint inhibitors and other mechanisms that are relevant to immunotherapy applications.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Specialized Center--Cooperative Agreements (U54)
Project #
5U54CA209997-05
Application #
9976486
Study Section
Special Emphasis Panel (ZCA1)
Project Start
Project End
Budget Start
2020-08-01
Budget End
2021-07-31
Support Year
5
Fiscal Year
2020
Total Cost
Indirect Cost

  Institution

Name
Columbia University (N.Y.)
Department
Type
DUNS #
621889815
City
New York
State
NY
Country
United States
Zip Code
10032

  Publications

Chiu, Hua-Sheng; Martínez, María Rodríguez; Komissarova, Elena V et al. (2018) The number of titrated microRNA species dictates ceRNA regulation. Nucleic Acids Res 46:4354-4369
Ding, Hongxu; Wang, Wanxin; Califano, Andrea (2018) iterClust: a statistical framework for iterative clustering analysis. Bioinformatics 34:2865-2866
Giudice, I Del; Rigolin, G M; Raponi, S et al. (2018) Refined karyotype-based prognostic stratification of chronic lymphocytic leukemia with a low- and very-low-risk genetic profile. Leukemia 32:543-546
Thorsson, Vésteinn; Gibbs, David L; Brown, Scott D et al. (2018) The Immune Landscape of Cancer. Immunity 48:812-830.e14
Arnes, Luis; Liu, Zhaoqi; Wang, Jiguang et al. (2018) Comprehensive characterisation of compartment-specific long non-coding RNAs associated with pancreatic ductal adenocarcinoma. Gut :
Risom, Tyler; Langer, Ellen M; Chapman, Margaret P et al. (2018) Differentiation-state plasticity is a targetable resistance mechanism in basal-like breast cancer. Nat Commun 9:3815
Ding, Hongxu; Douglass Jr, Eugene F; Sonabend, Adam M et al. (2018) Quantitative assessment of protein activity in orphan tissues and single cells using the metaVIPER algorithm. Nat Commun 9:1471
Rajbhandari, Presha; Lopez, Gonzalo; Capdevila, Claudia et al. (2018) Cross-Cohort Analysis Identifies a TEAD4-MYCN Positive Feedback Loop as the Core Regulatory Element of High-Risk Neuroblastoma. Cancer Discov 8:582-599
Cesana, Marcella; Guo, Michael H; Cacchiarelli, Davide et al. (2018) A CLK3-HMGA2 Alternative Splicing Axis Impacts Human Hematopoietic Stem Cell Molecular Identity throughout Development. Cell Stem Cell 22:575-588.e7
Yuan, Jinzhou; Levitin, Hanna Mendes; Frattini, Veronique et al. (2018) Single-cell transcriptome analysis of lineage diversity in high-grade glioma. Genome Med 10:57

Showing the most recent 10 out of 27 publications