Literature DB >> 17968971

Why insulin sensitizers but not secretagogues should be retained when initiating insulin in type 2 diabetes.

Philip Raskin1.   

Abstract

The stringent targets set for HbA(1c) levels in type 2 diabetes are currently achieved by fewer than half the patients in the United States. Failure to manage hyperglycaemia in the early stages of disease results in progressive loss of beta-cell function, which ultimately necessitates the initiation of insulin therapy. At this point, choices have to be made on whether to continue oral anti-diabetic drug therapy and, if so, with which agent(s). Historically, sulfonylureas have been the mainstay of oral anti-diabetic drug therapy; however, their long-term efficacy in patients with depleted beta-cell capacity is doubtful, and other classes of oral anti-diabetic drugs, notably the insulin sensitizers, may prove more reliable. These agents (metformin and thiazolidinediones) appear to provide various benefits over and above sustained glycaemic control, which may variably include reduced loss of beta-cell function as well as improvements to cardiovascular risk factors, morbidity, and mortality. Metformin also limits weight gain associated with insulin therapy. This manuscript presents the case that when insulin therapy is initiated it should be tailored to individual needs through combination with one or more insulin sensitizers rather than a secretagogue. 2007 John Wiley & Sons, Ltd

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Year:  2008        PMID: 17968971     DOI: 10.1002/dmrr.783

Source DB:  PubMed          Journal:  Diabetes Metab Res Rev        ISSN: 1520-7552            Impact factor:   4.876


  9 in total

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6.  Use of non-insulin diabetes medicines after insulin initiation: A retrospective cohort study.

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8.  Calcium-dependent ultrasound stimulation of secretory events from pancreatic beta cells.

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  9 in total

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