Journal
INTERNIST
Volume 48, Issue 7, Pages 698-+Publisher
SPRINGER HEIDELBERG
DOI: 10.1007/s00108-007-1876-z
Keywords
diabetes mellitus type 2; diabetes therapy; endocannabinoid receptor blockers; GLP 1 analogues/incretin mimetics; DPP 4 inhibitor
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The development of a variety of new substances will considerably expand the therapeutic choices in the treatment of type 2 diabetes. In 2006, the endocannabinoid receptor blocker Rimonabant has been approved for the treatment of type 2 diabetes in Germany. This compound has led to significant reductions of body weight along with improvements of HbA1c levels and lipid profiles, but the lack of health insurance coverage limits its large scale use in germany. In April 2007, the first members of the GLP 1 analogues/ incretin mimetics (exenatide, Byetta((R)) ) and DPP 4 inhbitors (sitagliptin, Januvia((R))) have become available for the treatment of type 2 diabetes in Germany. Both drugs have significantly lowered HbA1c levels in clinical studies. In addition, the incretin mimetics have caused a progressive reduction of body weight, while the DPP 4 inhibitors have been rather weight neutral. Sitagliptin can be administered orally, whereas exenatide has to be injected subcutaneously. Neither the DPP 4 inhibitors, nor the incretin mimetics have led to the development of hypoglycaemia, unless combined with sulfonylureas. Overall, the introduction of these new drug classes will certainly broaden our therapeutic choices in the management of type 2 diabetes. The long-term effects of these drugs on the development of diabetic complications in long-term trials remains to be awaited.
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