| Literature DB >> 14988246 |
Shaoping Deng1, Marko Vatamaniuk, Xiaolun Huang, Nicolai Doliba, Moh-Moh Lian, Adam Frank, Ergun Velidedeoglu, Niraj M Desai, Brigitte Koeberlein, Bryan Wolf, Clyde F Barker, Ali Naji, Franz M Matschinsky, James F Markmann.
Abstract
Type 2 diabetic subjects manifest both disordered insulin action and abnormalities in their pancreatic islet cells. Whether the latter represents a primary defect or is a consequence of the former is unknown. To examine the beta-cell mass and function of islets from type 2 diabetic patients directly, we isolated islets from pancreata of type 2 diabetic cadaveric donors (n = 14) and compared them with islets from normal donors (n = 14) matched for age, BMI, and cold ischemia time. The total recovered islet mass from type 2 diabetic pancreata was significantly less than that from nondiabetic control subjects (256,260 islet equivalents [2,588 IEq/g pancreas] versus 597,569 islet equivalents [6,037 IEq/g pancreas]). Type 2 diabetic islets were also noted to be smaller on average, and histologically, islets from diabetic patients contained a higher proportion of glucagon-producing alpha-cells. In vitro study of islet function from diabetic patients revealed an abnormal glucose-stimulated insulin release response in perifusion assays. In addition, in comparison with normal islets, an equivalent number of type 2 diabetic islets failed to reverse hyperglycemia when transplanted to immunodeficient diabetic mice. These results provide direct evidence for abnormalities in the islets of type 2 diabetic patients that may contribute to the pathogenesis of the disease.Entities:
Mesh:
Year: 2004 PMID: 14988246 DOI: 10.2337/diabetes.53.3.624
Source DB: PubMed Journal: Diabetes ISSN: 0012-1797 Impact factor: 9.461