Loss of beta cell function as fasting glucose increases in the non-diabetic range

Godsland, Ian F.; Jeffs, J. A. R.; Johnston, Desmond G.

doi:10.1007/s00125-004-1454-z

Cited by 116 publications

(105 citation statements)

References 57 publications

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“…Indeed, fasting hyperinsulinaemia, known to reflect decreased insulin sensitivity, and decreased insulin secretion together constitute the strongest independent predictor of type 2 diabetes [10]. Furthermore, decreased beta cell function may exist already at normal fasting plasma glucose levels [11]. Thus, detailed information on the pathogenesis of disturbed glucose regulation in AMI patients may pave the way for novel treatments aimed at improving cardiovascular outcome and delaying the onset of clinical diabetes and typical diabetes complications.…”

Section: Introductionmentioning

confidence: 99%

Beta cell dysfunction in patients with acute myocardial infarction but without previously known type 2 diabetes: a report from the GAMI study

et al. 2005

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Aims/hypothesis: Patients with acute myocardial infarction (AMI) but without previously known type 2 diabetes have a high prevalence of undiagnosed IGT and type 2 diabetes. Such perturbations have dismal prognostic implications. The aim of this study was to characterise AMI patients in terms of insulin resistance and beta cell function. Methods: A total of 168 consecutive AMI patients were classified by means of an OGTT before hospital discharge as having NGT, IGTor type 2 diabetes. The homeostasis model assessment (HOMA-IR) was used to estimate insulin resistance. Beta cell responsiveness was quantified as insulinogenic index (IGI) at 30 min (ΔI 30 /ΔG 30 (r=−0.218, p=0.010) and to the area under the curve for glucose (r=−0.475, p<0.001). Conclusions/interpretation: Glucose abnormalities are very common in patients with AMI but without previously known type 2 diabetes. To a significant extent, this seems to be related to impaired beta cell function and implies that dysglycaemia immediately after an infarction is not a stress epiphenomenon but reflects stable disturbances of glucose regulation preceding the AMI. Early beta cell dysfunction may have important pathophysiological implications and may serve as a future target for treatment strategies.

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Section: Introductionmentioning

confidence: 99%

Beta cell dysfunction in patients with acute myocardial infarction but without previously known type 2 diabetes: a report from the GAMI study

et al. 2005

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“…In normal rats, small (0.89 mmol/l or 16 mg/dl) increments in mean daylong FPG have been shown to completely abolish first-phase insulin secretion [7]. Such an effect in humans could explain the results observed by Godsland et al [1]. Moreover, in animal studies, correction of chronic hyperglycaemia with phlorizin restores first-phase insulin secretion, indicating that the reduction in first-phase insulin secretion is the result of chronic hyperglycaemia rather than the cause in this animal model [6].…”

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confidence: 84%

To: Godsland IF, Jeffs JA, Johnston DG (2004) Loss of beta cell function as fasting glucose increases in the non-diabetic range. Diabetologia 47:1157–1166

Abdul‐Ghani

DeFronzo

2005

Diabetologia

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Godsland and colleagues [1], the investigators report a significant decline in beta cell function, which begins within the normal range of fasting plasma glucose (FPG) concentrations. Using the IVGTT in 553 non-diabetic men with an FPG<7.0 mmol/l, they observed a marked decline in first-phase insulin secretion, beginning at an FPG well within the normal range, without any change in insulin sensitivity. These results suggest that the decline in insulin secretion is the primary event and is unrelated to changes in insulin sensitivity. A similar observation has been reported in children [2], although most previous studies have demonstrated a decrease in insulin sensitivity in adults with an FPG >6.1 mmol/l (110 mg/dl) [3,4]. The defect in first-phase insulin secretion is reminiscent of the decline in insulin secretion observed in normal glucose-tolerant subjects with 2-h plasma glucose concentrations well within the normal range, reported by Gasteldelli and colleagues [5]. Both observations [1,5] suggest that the current cut-off values that define normal glucose tolerance do not correspond to plasma glucose levels that identify the presence of physiological alterations in insulin secretion in vivo. In their interpretation of the association between the decline in first-phase insulin secretion and the rise in FPG in response to intravenous glucose, Godsland et al. suggest that loss of pancreatic beta cell function in the first phase is, therefore, the critical factor in declining glucose homeostasis in the non-diabetic range of FPG [1]. Although we agree that impaired beta cell function occurs in individuals with FPG concentrations that are considered to be within the normal range [5], we are concerned about the authors' interpretation of their results. The decline in first-phase insulin secretion that accompanies the rise in FPG does not necessarily indicate a causal relationship. One could argue that the increase in FPG, secondary to excess hepatic glucose production or insulin resistance in peripheral tissues, is the primary event and that chronic, sustained modest hyperglycaemia leads to impaired insulin secretion, i.e. glucotoxicity. A 'glucotoxic' effect of hyperglycaemia has been demonstrated in vivo, both in humans and animals, and in vitro in cell culture systems [6][7][8]. In normal rats, small (0.89 mmol/l or 16 mg/dl) increments in mean daylong FPG have been shown to completely abolish first-phase insulin secretion [7]. Such an effect in humans could explain the results observed by Godsland et al. [1]. Moreover, in animal studies, correction of chronic hyperglycaemia with phlorizin restores first-phase insulin secretion, indicating that the reduction in first-phase insulin secretion is the result of chronic hyperglycaemia rather than the cause in this animal model [6]. Although a similar study in man is needed to establish that hyperglycaemia is the primary disturbance and leads to impaired insulin secretion, indirect evidence supports this scenario. First, correction of hyperglycaemia improves insulin ...

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“…Returning to the work of Godsland and co-workers [1], I believe that it may serve not only to challenge the definition of normal glycaemic values, but also to support the reassessment of the concept of prediabetes, i.e. that there is a non-hyperglycaemic stage of diabetes-just as diabetologists such as Rolf Luft and Stefan Fajans suggested almost 50 years ago.…”

mentioning

confidence: 97%

“…The data of Godsland et al [1] provide convincing evidence in support of the ADA initiative and offer both evidence and logic for lowering the upper normal limits for fasting plasma glucose, which Schriger and Lorber [4] question aggressively in their paper on the Expert Committee's proposal. The anxiety of these two researchers derives from the calculation that, due to the changes proposed by the Expert Committee, the number of patients with impaired fasting glucose in the USA will rise from 10 to 35 million, thus affecting 22.5% of the adult population.…”

mentioning

confidence: 99%

“…To the Editor For more than two decades I have awaited data such as those published by Godsland and co-workers [1] in the July issue of your journal. Although they focused primarily on the identification of the early disturbances that occur in the natural history of type 2 diabetes (the progressive loss of the first, and then of the second phase of insulin response), it seems of great importance to me that these changes occur at blood glucose levels between 5.0 and 5.4 mmol/l.…”

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confidence: 99%

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Comment on: Godsland IF, Jeffs JAR, Johnston DG (2004) Loss of beta cell function as fasting glucose increases in the non-diabetic range. Diabetologia 47:1157–1166

Ionescu-Tîrgovişte¹

2004

Diabetologia

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Loss of beta cell function as fasting glucose increases in the non-diabetic range

Cited by 116 publications

References 57 publications

Beta cell dysfunction in patients with acute myocardial infarction but without previously known type 2 diabetes: a report from the GAMI study

Beta cell dysfunction in patients with acute myocardial infarction but without previously known type 2 diabetes: a report from the GAMI study

To: Godsland IF, Jeffs JA, Johnston DG (2004) Loss of beta cell function as fasting glucose increases in the non-diabetic range. Diabetologia 47:1157–1166

Comment on: Godsland IF, Jeffs JAR, Johnston DG (2004) Loss of beta cell function as fasting glucose increases in the non-diabetic range. Diabetologia 47:1157–1166

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