Abstract

Effective cancer prevention depends on distinguishing between indolent and progressive pre-malignant neoplasms, so that the cost and risks of interventions can be focused on patients likely to progress to cancer, while patients at low risk of progression can be reassured and removed from frequent surveillance. Because neoplastic progression is a process of clonal evolution, we are developing a novel class of biomarkers that directly measure the evolutionary process. We have previously shown that measures of clonal diversity in Barrett's esophagus predict progression to esophageal adenocarcinoma. However, those methods depended on detecting distinct clones by taking multiple, spatially separated biopsies from each neoplasm. This is not feasible for many neoplasms. In order to generalize the use of genetic diversity as a biomarker of progression to other neoplasms, we propose to develop a genetic fingerprinting technique for measuring genetic heterogeneity at the single cell, or single crypt, level. We will flow sort single cells into a 96 well plate and use fluorescent inter-simple sequence repeat PCR (FISSR-PCR) to detect insertions, deletions and translocations in each cell's genome. If single cell assays prove unreliable, we can isolate single whole epithelial crypts into separate wells to characterize genetic diversity at the crypt level. We will test this assay on Barrett's esophagus biopsies from 19 genetically mapped esophagectomy specimens to determine if p53 wildtype epithelium is less genetically diverse than epithelium with p53 loss of heterozygosity, which in turn is less diverse than aneuploid or tetraploid epithelium. This will determine if the molecular events that characterize Barrett's neoplastic progression are associated with increasing genetic diversity at the single cell level. The success of this project will open up three important future studies: 1) Tests of whether genetic diversity in a variety of intraepithelial neoplasms is associated with progression to malignancy. 2) Tests of whether genetic diversity is associated with the evolution of resistance to cancer prevention interventions or therapy. 3) Tests of the genetic diversity of pre-clinical models of neoplastic progression so that we can develop models that faithfully recapitulate the genetic diversity of sporadic human neoplasms. Such models will be important for estimating the likelihood that resistance will develop to cancer prevention agents and provide tools for studying the management and prevention of such resistance. To address these problems we utilize expertise in caner biology, evolutionary biology and computational biology, as well as access to a tissue bank of biopsies from a Barrett's esophagus cohort that has been collected prospectively since 1989. This provides an opportunity to rapidly translate credentialed biomarkers into phase IV biomarker studies and from there into the clinic.

Public Health Relevance

Only a small fraction of benign tumors become malignant, but once they do, they are very difficult to cure. Thus, attention has turned to preventing cancer. However, most cancer prevention drugs have some toxicity or pose some risk to the patient. We need methods to distinguish between truly benign tumors and those likely to become malignant so that both surveillance and interventions can be focused on patients at the highest risk, and we can reassure patients who are unlikely to develop cancer. We found that by measuring the number of different mutant cells in a benign esophageal tumor, we could identify patients at high and low risk for developing esophageal cancer. We are proposing to develop a method to measure the number of different mutant cells in any tumor, not just esophageal tumors.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Small Research Grants (R03)
Project #
5R03CA137811-02
Application #
7688488
Study Section
Special Emphasis Panel (ZCA1-SRLB-F (O1))
Program Officer
Richmond, Ellen S
Project Start
2008-09-17
Project End
2010-08-31
Budget Start
2009-09-01
Budget End
2010-08-31
Support Year
2
Fiscal Year
2009
Total Cost
$59,228
Indirect Cost

  Institution

Name
Wistar Institute
Department
Type
DUNS #
075524595
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

Kostadinov, Rumen L; Kuhner, Mary K; Li, Xiaohong et al. (2013) NSAIDs modulate clonal evolution in Barrett's esophagus. PLoS Genet 9:e1003553
Aktipis, C Athena; Maley, Carlo C; Pepper, John W (2012) Dispersal evolution in neoplasms: the role of disregulated metabolism in the evolution of cell motility. Cancer Prev Res (Phila) 5:266-75
Kosoff, Rachelle E; Gardiner, Kristin L; Merlo, Lauren M F et al. (2012) Development and characterization of an organotypic model of Barrett's esophagus. J Cell Physiol 227:2654-9
Merlo, Lauren M F; Kosoff, Rachelle E; Gardiner, Kristin L et al. (2011) An in vitro co-culture model of esophageal cells identifies ascorbic acid as a modulator of cell competition. BMC Cancer 11:461
Chen, Jun; Sprouffske, Kathleen; Huang, Qihong et al. (2011) Solving the puzzle of metastasis: the evolution of cell migration in neoplasms. PLoS One 6:e17933
Sprouffske, Kathleen; Pepper, John W; Maley, Carlo C (2011) Accurate reconstruction of the temporal order of mutations in neoplastic progression. Cancer Prev Res (Phila) 4:1135-44
Reid, Brian J; Kostadinov, Rumen; Maley, Carlo C (2011) New strategies in Barrett's esophagus: integrating clonal evolutionary theory with clinical management. Clin Cancer Res 17:3512-9
Caulin, Aleah F; Maley, Carlo C (2011) Peto's Paradox: evolution's prescription for cancer prevention. Trends Ecol Evol 26:175-82
Aktipis, C Athena; Kwan, Virginia S Y; Johnson, Kathryn A et al. (2011) Overlooking evolution: a systematic analysis of cancer relapse and therapeutic resistance research. PLoS One 6:e26100
Merlo, Lauren M F; Maley, Carlo C (2010) The role of genetic diversity in cancer. J Clin Invest 120:401-3

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