1988
DOI: 10.1056/nejm198805123181903
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Abnormal Patterns of Insulin Secretion in Non-Insulin-Dependent Diabetes Mellitus

Abstract: To determine whether non-insulin-dependent diabetes is associated with specific alterations in the pattern of insulin secretion, we studied 16 patients with untreated diabetes and 14 matched controls. The rates of insulin secretion were calculated from measurements of peripheral C-peptide in blood samples taken at 15- to 20-minute intervals during a 24-hour period in which the subjects ate three mixed meals. Incremental responses of insulin secretion to meals were significantly lower in the diabetic patients (… Show more

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Cited by 537 publications
(324 citation statements)
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“…19-21 These Ca 2+ oscillations drive pulsatile insulin release 22 – a secretory pattern that enhances hepatic insulin action, 23 protects against insulin resistance, 24 and is lost in T2DM. 25-28 To understand how these Ca 2+ oscillations become defective in T2DM, it is important to first understand how an islet generates and maintains these oscillations.…”
Section: Introductionmentioning
confidence: 99%
“…19-21 These Ca 2+ oscillations drive pulsatile insulin release 22 – a secretory pattern that enhances hepatic insulin action, 23 protects against insulin resistance, 24 and is lost in T2DM. 25-28 To understand how these Ca 2+ oscillations become defective in T2DM, it is important to first understand how an islet generates and maintains these oscillations.…”
Section: Introductionmentioning
confidence: 99%
“…By restoring a more physiologic insulin profile, nateglinide is more effective than repaglinide in controlling prandial glucose excursions with less hyperinsulinaemia. It has been shown convincingly that in Type 2 (noninsulin-dependent) diabetes mellitus [1,2] and even in precursors thereof [3] the kinetics of insulin secretion are disrupted despite the existence of absolute (if not relative) hyperinsulinaemia. The disrupted insulin secretory kinetics can be confirmed by either the absence of the acute insulin response to i.v.…”
Section: Introductionmentioning
confidence: 99%
“…32 In fact, the response time of our modified cells to high glucose challenge closely mimics pancreatic response to a mixed meal challenge in normal human subjects. 33 Furthermore, clinically acceptable glycemic control was achieved in diabetic recipients of pancreas allografts or islet transplants despite abnormal insulin secretion kinetics. 34,35 Indeed, recent data from the NIDDK and JDRF-funded Collaborative Islet Transplant Registry showed that 31-53% of a total of 325 adult recipients of islet transplants suffered severe hypoglycemic episodes.…”
Section: Bone Marrow-derived Insulin Bioimplants Nkf Chen Et Almentioning
confidence: 99%