Abstract

Extracellular RNA (exRNA) is an emerging paradigm as endocrine signals in cellular communication, biomarker development, therapeutic applications and systemic physiology. This UH2/UH3 project is to test the hypothesis that salivary extracellular RNA (exRNA) can be developed for the clinical detection of human diseases. Our laboratory first reported the existence of a transcriptome and microRNA profile in cell free saliva followed by its scientific characterizations and clinical utilities including biomarker development for molecular oncology applications. Most recently we have performed RNA-sequencing in cell free saliva and reported three major types of RNA in saliva (mRNA, miRNA and snoRNA). This UH2/UH3 application is to test the hypothesis that salivary exRNA can be developed to detect gastric cancer by performing a biomarker development study to definitively validate salivary exRNA biomarkers for the detection of gastric cancer. We are selecting gastric cancer to be the human disease indication because of an ongoing productive collaboration with the Samsung Medical Center where we have already procured saliva from 500 gastric cancer patients and 2250 non-gastric cancer controls. This will permit the UH2 phase for exRNA biomarker discovery to begin immediately. Additional clinical samples will be procured in the UH3 phase, 375 cases and 375 non-gastric cancer match controls each year for two years. These clinical samples for discovery and validation will allow us to definitively validate if salivary exRNA can be used to detect gastrc cancer in a defined clinical setting (Context of Use). There are four Specific Aims in the UH2 phase of the project.
Aim 1 is to randomly select saliva from 100 gastric cancer and 100 non-gastric cancer controls to be used in Aim 2 which is to perform comprehensive RNA-sequencing to comprehensively profile salivary exRNA to the nucleotide level.
Aim 3 is to perform data and statistical analysis of the profiled salivary mRNA, miRNA, and snoRNA to select the top 20 salivary ex- mRNA, ex-miRNA and ex-snoRNA.
Aim 4 is to verify the candidate exRNA biomarkers in the original discovery cohort. Only verified candidate salivary exRNA will be advanced to the UH3 phase. In the UH3 phase, Aim 5 is to enroll and procure saliva from an additional 750 gastric cancer patients and 750 non-gastric cancer controls.
Aim 6 will use 500 of the gastric cancer saliva and 500 matched control subjects from Aim 4 to individually validate the verified candidate salivary exRNA biomarkers and configure a panel of validate exRNA biomarkers with highest performance using logistic regression analysis. The panel will be validated in Aim 7 using saliva from an independent cohort of 250 gastric cancer and 250 non-gastric cancer controls. The goals of this UH2/UH3 application are to demonstrate the clinical utility of salivary exRNA by the discovering and definitively validating salivary exRNA biomarkers for the detection of a human disease condition.

Public Health Relevance

Extracellular RNA (exRNA) is an emerging paradigm in cellular communication, biomarker development, therapeutic applications and systemic physiology. This UH2/UH3 project is to test the hypothesis that salivary exRNA biomarker can be developed for the detection of a human disease condition, gastric cancer. The discovered salivary exRNA biomarkers will be determined if they can be definitively validated. The definitive validation of the salivary exRNA for gastric cancer detection will credential the clinical utility of salivary exRNA for biomarker development for human disease detection.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Center for Advancing Translational Sciences (NCATS)
Type
Exploratory/Developmental Cooperative Agreement Phase II (UH3)
Project #
4UH3TR000923-03
Application #
8962182
Study Section
Special Emphasis Panel (ZRG1-GGG-R (51))
Program Officer
Tagle, Danilo A
Project Start
2013-08-01
Project End
2018-07-31
Budget Start
2013-08-01
Budget End
2016-07-31
Support Year
3
Fiscal Year
2015
Total Cost
$985,293
Indirect Cost
$316,175

  Institution

Name
University of California Los Angeles
Department
Dentistry
Type
Schools of Dentistry
DUNS #
092530369
City
Los Angeles
State
CA
Country
United States
Zip Code
90095

  Publications

He, X; Li, F; Bor, B et al. (2018) Human tRNA-Derived Small RNAs Modulate Host-Oral Microbial Interactions. J Dent Res 97:1236-1243
Wei, Fang; Strom, Charles M; Cheng, Jordan et al. (2018) Electric Field-Induced Release and Measurement Liquid Biopsy for Noninvasive Early Lung Cancer Assessment. J Mol Diagn 20:738-742
Kaczor-Urbanowicz, Karolina E; Trivedi, Harsh M; Lima, Patricia O et al. (2018) Salivary exRNA biomarkers to detect gingivitis and monitor disease regression. J Clin Periodontol 45:806-817
Nonaka, T; Wong, D T W (2018) Liquid Biopsy in Head and Neck Cancer: Promises and Challenges. J Dent Res 97:701-708
Kaczor-Urbanowicz, Karolina Elzbieta; Kim, Yong; Li, Feng et al. (2018) Novel approaches for bioinformatic analysis of salivary RNA sequencing data for development. Bioinformatics 34:1-8
Katsiougiannis, Stergios; Chia, David; Kim, Yong et al. (2017) Saliva exosomes from pancreatic tumor-bearing mice modulate NK cell phenotype and antitumor cytotoxicity. FASEB J 31:998-1010
Kaczor-Urbanowicz, Karolina El?bieta; Martin Carreras-Presas, Carmen; Aro, Katri et al. (2017) Saliva diagnostics - Current views and directions. Exp Biol Med (Maywood) 242:459-472
Nonaka, Taichiro; Wong, David T W (2017) Saliva-Exosomics in Cancer: Molecular Characterization of Cancer-Derived Exosomes in Saliva. Enzymes 42:125-151
Wang, Xiaoqian; Kaczor-Urbanowicz, Karolina El?bieta; Wong, David T W (2017) Salivary biomarkers in cancer detection. Med Oncol 34:7
Majem, Blanca; Li, Feng; Sun, Jie et al. (2017) RNA Sequencing Analysis of Salivary Extracellular RNA. Methods Mol Biol 1537:17-36

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