Label-Free Proteomics of the Fetal Pancreas Identifies Deficits in the Peroxisome in Rats with Intrauterine Growth Restriction.

Xiaomei Liu Yanyan Guo Jun Wang Linlin Gao Caixia Liu

Published in: Oxidative medicine and cellular longevity (2019)

The present study identified DEPs in the fetal pancreas of IUGR rats by proteomic analysis. Downregulation of pancreas peroxins and dysregulation of enzymes involved in peroxisomal FAO may impair the biogenesis and function of the peroxisome and may underlie the development of T2 diabetes mellitus in adult IUGR rats. Disorders of cell cycle regulators may induce cell division arrest and lead to smaller islets. The present data provide new insight into the role of the peroxisome in the development of the pancreas and may be valuable in furthering our understanding of the pathogenesis of IUGR-induced diabetes.

Keyphrases

cell cycle
label free
cell proliferation
type diabetes
traumatic brain injury
mass spectrometry
signaling pathway
genome wide
cell therapy
stem cells
high glucose
gene expression
transcription factor
dna methylation
big data
bone marrow
machine learning
insulin resistance
childhood cancer