Abstract
Over the past several decades in the United States, incidence of pancreatic cancer (PCa) has increased, with the 5-year survival rate remaining extremely low at 10.8%. Typically, PCa is diagnosed at an advanced stage, with the consequence that there is more tumor heterogeneity and increased probability that more cells are resistant to treatments. Risk factors for PCa can serve as a way to select a high-risk population and develop biomarkers to improve early detection and treatment. We focus on blood-based methylation as an approach to identify a marker set that can be obtained in a minimally invasive way (through peripheral blood) and could be applied to a high-risk subpopulation [those with recent onset type 2 diabetes (DM)]. Blood samples were collected from 30 patients, 15 had been diagnosed with PCa and 15 had been diagnosed with recent onset DM. HumanMethylationEPIC Beadchip (Illumina, CA, United States) was used to quantify methylation of approximately 850,000 methylation sites across the genome and to analyze methylation markers associated with PCa or DM or both. Exploratory analysis conducted to propose importance of top CpG (5′—C—phosphate—G—3′) methylation site associated genes and visualized using boxplots. A methylation-based age predictor was also investigated for ability to distinguish disease groups from controls. No methylation markers were observed to be significantly associated with PCa or new onset diabetes compared with control the respective control groups. In our exploratory analysis, one methylation marker, CpG04969764, found in the Laminin Subunit Alpha 5 (LAMA5) gene region was observed in both PCa and DM Top 100 methylation marker sets. Modification of LAMA5 methylation or LAMA5 gene function may be a way to distinguish those recent DM cases with and without PCa, however, additional studies with larger sample sizes and different study types (e.g., cohort) will be needed to test this hypothesis.
Highlights
Development of effective methods to treat pancreatic cancer (PCa) has eluded investigators
We focus on blood-based methylation in order to identify a marker set that can be obtained in a minimally invasive way and could be used in a high-risk subpopulation
We did not find any methylation markers significantly associated with PCa or new onset diabetes compared with control the respective control groups
Summary
Development of effective methods to treat pancreatic cancer (PCa) has eluded investigators. Risk factors for PCa can serve as a way to select high-risk populations for which biomarkers could be developed to improve early detection and treatment. Recent onset DM (developed within 3 years prior to PCa diagnosis) has been shown to potentially be the result of the presence of the PCa tumor (Aggarwal et al, 2013; Sharma et al, 2018). Another important component of a screening program is trying to make it as minimally invasive to ensure it is acceptable and causes minimal burden to the participant. Biomarkers obtained via peripheral blood would be less invasive than those obtain via tissue from the pancreas
Sign-in/Register to view highlights & summary 
Published Version (
Free)
Talk to us
Join us for a 30 min session where you can share your feedback and ask us any queries you have
Schedule a call