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mRNA and protein levels of rat pancreas specific protein disulphide isomerase are downregulated during hyperglycemia
R GUPTA, K BHAR, N SEN, D BHOWMICK, S MUKHOPADHYAY, , A SIDDHANTA,
Published in National Institute of Science Communication
2016
PMID: 26934777
Volume: 54
   
Issue: 2
Pages: 100 - 107
Abstract
Diabetes (Type I and Type II) which affects nearly every organ in the body is a multi-factorial non-communicable disorder. Hyperglycemia is the most characteristic feature of this disease. Loss of beta cells is common in both types of diabetes whose detailed cellular and molecular mechanisms are yet to be elucidated. As this disease is complex, identification of specific biomarkers for its early detection, management and devising new therapies is challenging. Based on the fact that functionally defective proteins provide the biochemical basis for many diseases, in this study, we tried to identify differentially expressed proteins during hyperglycemia. For that, hyperglycemia was induced in overnight fasted rats by intra-peritoneal injection of streptozotocin (STZ). The pancreas was isolated from control and treated rats for subsequent analyses. The 2D-gel electrophoresis followed by MALDI-TOF-MS-MS analyses revealed several up- and down- regulated proteins in hyperglycemic rat pancreas including the downregulation of a pancreas specific isoform of protein disulphide isomerase a2 (Pdia2).This observation was validated by western blot. Quantitative PCR experiments showed that the level of Pdia2 mRNA is also proportionally reduced in hyperglycemic pancreas. © 2016, National Institute of Science Communication. All right reserved.
About the journal
JournalIndian Journal of Experimental Biology
PublisherNational Institute of Science Communication
ISSN0019-5189
Open AccessNo