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Insulin receptor based lymphocyte trafficking in the progression of type 1 diabetes.

Citation
Morran, M. P., et al. “Insulin Receptor Based Lymphocyte Trafficking In The Progression Of Type 1 Diabetes.”. Journal Of Biological Methods.
Center University of Michigan
Author Michael P Morran, Ali G Al-Dieri, Andrea L Nestor-Kalinoski, Richard K Jordan, Nirdesh K Gupta, Marcia F McInerney
Keywords Cre-recombinase, chemotaxis, diabetes, Insulin receptor, insulitis
Abstract

The insulin receptor (IR) is a transmembrane receptor which recognizes and binds the hormone insulin. We describe two models that were devised to explore the role of IR over-expression on T-lymphocytes and their chemotactic motility in the progression of type 1 diabetes. FVB/NJ-CD3-3×FLAG-mIR/MFM mice were generated to selectively over-express 3×FLAG tagged murine IR in T-lymphocytes an engineered CD3 enhancer and promoter construct. Insertion of the 3×FLAG-mIR transgene into FVB/NJ mice, a known non-autoimmune prone strain, lead to a minor population of detectable 3×FLAG-mIR tagged T-lymphocytes in peripheral blood and the presence of a few lymphocytes in the pancreas of the Tg+/- compared to age matched Tg-/- control mice. In order to induce stronger murine IR over-expression then what was observed with the CD3 enhancer promoter construct, a second system utilizing the strong CAG viral promoter was generated. This system induces cell specific IR over-expression upon Cre-Lox recombination to afford functional 3×FLAG tagged murine IR with an internal eGFP reporter. The pPNTlox2-3×FLAG-mIR plasmid was constructed and validated in HEK-Cre-RFP cells to ensure selective Cre recombinase based 3×FLAG-mIR expression, receptor ligand affinity towards insulin, and functional initiation of signal transduction upon insulin stimulation.

Year of Publication
2018
Journal
Journal of biological methods
Volume
5
Issue
1
Date Published
12/2018
ISSN Number
2326-9901
DOI
10.14440/jbm.2018.209
Alternate Journal
J Biol Methods
PMID
29862308
PMCID
PMC5983036
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