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Historical perspective

The area of diabetes research is rapidly evolving, and various directions are being pursued based on emerging insights into glucose regulation. In recent years, scientific attention has been directed to incretin hormones and their role in glycemic control. Incretins are intestinal hormones released in response to ingestion of food that, at physiologic levels, increase the insulin response in a glucose-dependent manner. 50,51 Interest in incretins as a basis for therapy has grown in recent years and has led to the discovery of additional approaches for treating type 2 diabetes.

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1902: First Observation of an Intestinal Effect on Pancreatic Response

Bayliss and Starling made the first observation that a factor produced by the intestine could stimulate secretion from the pancreas. 50,52

1932: Incretin First Defined

La Barre introduced the term incretin to describe hormonal activity deriving from the gut that was able to increase the endocrine secretion from the pancreas. 53

1964: Oral vs IV Infusion of Glucose (the Incretin Effect Demonstrated)

Two independent research teams (McIntyre, Elrick) simultaneously communicated the discovery that oral administration
of glucose 42,50,54 induced a greater insulin response than IV infusion of glucose. This difference was called the
incretin effect. 50

1973: GIP Demonstrated to Be a Human Incretin

The insulin stimulatory role of GIP, initially called gastric inhibitory peptide, could be demonstrated in humans. Thus, GIP became the first identified incretin hormone and was renamed glucose-dependent insulinotropic polypeptide. 50

1986: Incretin Effect Demonstrated to Be Reduced in Patients With Type 2 Diabetes

Nauck et al observed a reduced incretin effect in type 2 diabetes. 43

1987: GLP-1 Demonstrated to Be a Human lncretin

The glucose-dependent incretin effect of a second intestinal peptide hormone, glucagon-like peptide 1 (GLP-1) (7-36), was demonstrated in humans. 44

1995: DPP-4 Enzyme Degrades GLP-1 and GIP

The finding that GLP-1 and GIP are degraded by the enzyme dipeptidyl peptidase-4 (DPP-4) 27,39,55 initiated the development of agents for the treatment of type 2 diabetes.

2000 and Beyond: DPP-4 Inhibitors and Incretin Mimetics

Ongoing research and investigation.