{beta}-Cell Failure in Diabetes and Preservation by Clinical Treatment

doi:10.1210/10.1210/er.2006-0038

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ß-Cell Failure in Diabetes and Preservation by Clinical Treatment

Bernardo L. Wajchenberg

Endocrine Service and Diabetes and Heart Center of The Heart Institute, Hospital das Clinicas of The University of São Paulo Medical School, São Paulo, SP 05403-000, Brazil

Correspondence: Address all correspondence to: Bernardo L. Wajchenberg, Diabetes and Heart Center of The Heart Institute, Hospital das Clinicas of The University of São Paulo Medical School, Av. Eneas C. Aguiar 44, Bloco II, AB São Paulo, SP 05403-000, Brazil. E-mail: bernarwaj{at}globo.com.

There is a progressive deterioration in ß-cell functionand mass in type 2 diabetics. It was found that islet functionwas about 50% of normal at the time of diagnosis, and a reductionin ß-cell mass of about 60% was shown at necropsy.The reduction of ß-cell mass is attributable to acceleratedapoptosis. The major factors for progressive loss of ß-cellfunction and mass are glucotoxicity, lipotoxicity, proinflammatorycytokines, leptin, and islet cell amyloid. Impaired ß-cellfunction and possibly ß-cell mass appear to be reversible,particularly at early stages of the disease where the limitingthreshold for reversibility of decreased ß-cell masshas probably not been passed.

Among the interventions to preserve or "rejuvenate" ß-cells,short-term intensive insulin therapy of newly diagnosed type2 diabetes will improve ß-cell function, usually leadingto a temporary remission time. Another intervention is the inductionof ß-cell "rest" by selective activation of ATP-sensitiveK+ (K_ATP) channels, using drugs such as diazoxide.

A third type of intervention is the use of antiapoptotic drugs,such as the thiazolidinediones (TZDs), and incretin mimeticsand enhancers, which have demonstrated significant clinicalevidence of effects on human ß-cell function.

The TZDs improve insulin secretory capacity, decrease ß-cellapoptosis, and reduce islet cell amyloid with maintenance ofneogenesis. The TZDs have indirect effects on ß-cellsby being insulin sensitizers. The direct effects are via peroxisomeproliferator-activated receptor ${gamma}$ activation in pancreatic islets,with TZDs consistently improving basal ß-cell function.These beneficial effects are sustained in some individuals withtime. There are several trials on prevention of diabetes withTZDs.

Incretin hormones, which are released from the gastrointestinaltract in response to nutrient ingestion to enhance glucose-dependentinsulin secretion from the pancreas, aid the overall maintenanceof glucose homeostasis through slowing of gastric emptying,inhibition of glucagon secretion, and control of body weight.From the two major incretins, glucagon-like peptide-1 (GLP-1)and glucose-dependent insulinotropic polypeptide (GIP), onlythe first one or its mimetics or enhancers can be used for treatmentbecause the diabetic ß-cell is resistant to GIP action.Because of the rapid inactivation of GLP-1 by dipeptidyl peptidase(DPP)-IV, several incretin analogs were developed: GLP-1 receptoragonists (incretin mimetics) exenatide (synthetic exendin-4)and liraglutide, by conjugation of GLP-1 to circulating albumin.The acute effect of GLP-1 and GLP-1 receptor agonists on ß-cellsis stimulation of glucose-dependent insulin release, followedby enhancement of insulin biosynthesis and stimulation of insulingene transcription. The chronic action is stimulating ß-cellproliferation, induction of islet neogenesis, and inhibitionof ß-cell apoptosis, thus promoting expansion of ß-cellmass, as observed in rodent diabetes and in cultured ß-cells.Exenatide and liraglutide enhanced postprandial ß-cellfunction.

The inhibition of the activity of the DPP-IV enzyme enhancesendogenous GLP-1 action in vivo, mediated not only by GLP-1but also by other mediators. In preclinical studies, oral activeDPP-IV inhibitors (sitagliptin and vildagliptin) also promotedß-cell proliferation, neogenesis, and inhibition ofapoptosis in rodents. Meal tolerance tests showed improvementin postprandial ß-cell function.

Obviously, it is difficult to estimate the protective effectsof incretin mimetics and enhancers on ß-cells in humans,and there is no clinical evidence that these drugs really haveprotective effects on ß-cells.

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