AUTHOR=Yip Linda , Fuhlbrigge Rebecca , Alkhataybeh Reem , Fathman C. Garrison 

TITLE=Gene Expression Analysis of the Pre-Diabetic Pancreas to Identify Pathogenic Mechanisms and Biomarkers of Type 1 Diabetes

JOURNAL=Frontiers in Endocrinology

VOLUME=11

YEAR=2020

URL=https://www.frontiersin.org/journals/endocrinology/articles/10.3389/fendo.2020.609271

DOI=10.3389/fendo.2020.609271

ISSN=1664-2392

ABSTRACT=<p>Type 1 Diabetes (T1D) occurs as a result of the autoimmune destruction of pancreatic β-cells by self-reactive T cells. The etiology of this disease is complex and difficult to study due to a lack of disease-relevant tissues from pre-diabetic individuals. In this study, we performed gene expression analysis on human pancreas tissues obtained from the Network of Pancreatic Organ Donors with Diabetes (nPOD), and showed that 155 genes were differentially expressed by ≥2-fold in the pancreata of autoantibody-positive (AA+) at-risk individuals compared to healthy controls. Only 48 of these genes remained changed by ≥2-fold in the pancreata of established T1D patients. Pathway analysis of these genes showed a significant association with various immune pathways. We were able to validate the differential expression of eight disease-relevant genes by QPCR analysis: A significant upregulation of <italic>CADM2</italic>, and downregulation of <italic>TRPM5, CRH, PDK4, ANGPL4, CLEC4D, RSG16</italic>, and <italic>FCGR2B</italic> was confirmed in the pancreata of AA+ individuals versus controls. Studies have already implicated <italic>FCGR2B</italic> in the pathogenesis of disease in non-obese diabetic (NOD) mice. Here we showed that <italic>CADM2, TRPM5, PDK4</italic>, and <italic>ANGPL4</italic> were similarly changed in the pancreata of pre-diabetic 12-week-old NOD mice compared to NOD.B10 controls, suggesting a possible role for these genes in the pathogenesis of both T1D and NOD disease. The loss of the leukocyte-specific gene, <italic>FCGR2B</italic>, in the pancreata of AA+ individuals, is particularly interesting, as it may serve as a potential whole blood biomarker of disease progression. To test this, we quantified <italic>FCGR2B</italic> expression in peripheral blood samples of T1D patients, and AA+ and AA- first-degree relatives of T1D patients enrolled in the TrialNet Pathway to Prevention study. We showed that <italic>FCGR2B</italic> was significantly reduced in the peripheral blood of AA+ individuals compared to AA- controls. Together, these findings demonstrate that gene expression analysis of pancreatic tissue and peripheral blood samples can be used to identify disease-relevant genes and pathways and potential biomarkers of disease progression in T1D.</p>