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Pilot & Feasibility Program Application Abstract
Hyperglycemia and white blood cell biology
Ira Goldberg
(New York, NY)
Pilot & Feasibility Program
Several complications of diabetes may be exacerbated by inflammation. Whether this is due to hyperglycemia, defective insulin actions, or other metabolic alterations of diabetes is unknown. In addition, both local tissue inflammation and changes in the biology of circulating white blood cells (WBCs) could lead to pathological changes in organs and vascular tissues. In this regard, we have recently found that loss of WBCs from atherosclerotic mouse lesions is defective in the presence of streptozotocin diabetes. Moreover, we provide Preliminary Results showing that changes in circulating WBCs that occur with diabetes are corrected by glucose reduction using inhibitors to the sodium glucose co-transporter 2 (SGLT2). Thus, the studies proposed will allow us to “understand the possible in vivo efficacy of a promising new therapy for diabetes”, glucose reduction via inhibition of SGLT2. This Pilot application has two aims: Aim 1. To determine if hyperglycemia reduction leads to an alteration in the inflammatory state of circulating monocytes and neutrophils. Aim 2. To determine whether glucose reduction in STZ-treated LDL receptor knockout mice with atherosclerosis will reduce the inflammatory profile of lesional CD68+ cells. Techniques to lower glucose in diabetic mice, isolate circulating monocytes subsets (Lys6-C hi and lo) and granulocytes by FACS, and vascular wall CD68+ cells by laser capture microdissection are in hand. We expect that our studies will clarify the importance of hyperglycemia alone in altering the inflammatory status of circulating and vascular WBCs.
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Please acknowledge all posters, manuscripts or scientific materials that were generated in part or whole using funds from the Diabetic Complications Consortium(DiaComp) using the following text:
Financial support for this work provided by the NIDDK Diabetic Complications Consortium (RRID:SCR_001415, www.diacomp.org), grants DK076169 and DK115255
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