Adaptive β-Cell Neogenesis in the Adult Mouse in Response to Glucocorticoid-Induced Insulin Resistance

Courty, Émilie; Besseiche, A.; Huong, Thi Thu; Liboz, Alexandrine; Aguid, Fatima Mohamed; Quilichini, Evans; Buscato, Mélissa; Gourdy, Pierre; Gautier, Jean‐François; Riveline, Jean‐Pierre; Haumaitre, Cécile; Buyse, Marion; Fève, Bruno; Guillemain, Ghislaine; Blondeau, B.

doi:10.2337/db17-1314

Cited by 27 publications

(33 citation statements)

References 62 publications

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“…Any abnormality in the epigenetic regulatory mechanism will affect chromatin structure and gene expression, leading to the occurrence of a variety of diseases (Nilsson et al, 2018 ; Li S. et al, 2019 ; Perez and Lehner, 2019 ). Epigenetic changes are important regulatory mechanisms of islet β cell function and play irreplaceable roles in the normal physiological function of pancreatic β cells and insulin-secreting cells and apoptosis (Courty et al, 2019 ; Gong and Jiang, 2020 ; Makkar et al, 2020 ). There is no doubt that epigenetics research already becomes the focus of the study of pancreatic β cells in recent years.…”

Section: Introductionmentioning

confidence: 99%

RETRACTED: Roles of Epigenetic Modifications in the Differentiation and Function of Pancreatic β-Cells

Liu

et al. 2020

Front. Cell Dev. Biol.

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Diabetes, a metabolic disease with multiple causes characterized by high blood sugar, has become a public health problem. Hyperglycaemia is caused by deficiencies in insulin secretion, impairment of insulin function, or both. The insulin secreted by pancreatic β cells is the only hormone in the body that lowers blood glucose levels and plays vital roles in maintaining glucose homeostasis. Therefore, investigation of the molecular mechanisms of pancreatic β cell differentiation and function is necessary to elucidate the processes involved in the onset of diabetes. Although numerous studies have shown that transcriptional regulation is essential for the differentiation and function of pancreatic β cells, increasing evidence indicates that epigenetic mechanisms participate in controlling the fate and regulation of these cells. Epigenetics involves heritable alterations in gene expression caused by DNA methylation, histone modification and non-coding RNA activity that does not result in DNA nucleotide sequence alterations. Recent research has revealed that a variety of epigenetic modifications play an important role in the development of diabetes. Here, we review the mechanisms by which epigenetic regulation affects β cell differentiation and function.

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Section: Introductionmentioning

confidence: 99%

RETRACTED: Roles of Epigenetic Modifications in the Differentiation and Function of Pancreatic β-Cells

Liu

et al. 2020

Front. Cell Dev. Biol.

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“…This insulin sensitivity impairment after recovery period was probably due, at least in part, to the persistently increased WAT and lipid content in skeletal muscle (Geer et al 2014, Hamrick et al 2016. Moreover, it is worth noting that recent data from studies using the same adult mice model of CS report a marked positive effect on β-cell mass until 4 weeks after remission of hypercortisolism (Courty et al 2019), despite the toxic effects due to GC previously observed in vitro (Lambillotte et al 1997, Rafacho et al 2014. Compared with CORT, HFD treatment induced glucose intolerance and insulin resistance, which fits with the increased adiposity and lipid content in liver and skeletal muscle (Winzell et al 2007, Montgomery et al 2017.…”

Section: Figurementioning

confidence: 96%

Chronic hypercortisolism causes more persistent visceral adiposity than HFD-induced obesity

García-Eguren

Giró

Romero

et al. 2019

Journal of Endocrinology

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Excessive and prolonged glucocorticoid (GC) exposure, resulting from either prescribed or endogenous hypercortisolism, is associated with a high cardiovascular and metabolic burden (Cushing’s syndrome). Although previous studies in humans and mice have reported heterogeneous data about the persistence of metabolic syndrome features after remission of hypercortisolism, there is still controversy as to whether this is due to the deleterious changes induced by GCs during active disease or the result of various other factors interfering in the recovery period. In order to study metabolic effects after remission, we used a reversible mouse model of corticosterone (CORT) (100 µg/mL) administration in drinking water for 5 weeks, followed by a 10-week recovery period. We compared CORT-induced effects at these time points with a high-fat diet-treated group (HFD 45%) and a vehicle group (VEH). Plasma CORT, 11β-HSD activity, food intake, glucose levels, interscapular brown adiposity, hepatic triglycerides and muscle mass were found altered during CORT treatment but normalized after recovery. Although hyperinsulinemia and insulin resistance were increased during CORT and HFD treatment, insulin homeostasis remained altered following the recovery period only in CORT-treated mice. Subcutaneous and visceral adipose tissues (SAT and VAT) were enlarged during HFD and CORT treatment as measured by MRI. However, increased muscle lipid content, adiposity and macrophage infiltration in VAT were only present in the CORT group following recovery. Taken together, CORT-induced insulin alterations were more potent than HFD-induced ones during the same period of treatment, and also more persistent long term. Moreover, we demonstrated that CORT treatment induces more long-lasting VAT enlargement than HFD.

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“…In clinical studies, Van et al [8] found that after prednisolone treatment, there was an impaired glucose tolerance, reduced C peptide secretion stimulated by arginine, and islet cell dysfunction in healthy volunteers. However, some studies reported that islet β cell function and mass increased following glucocorticoid treatment, due to the body's compensatory effect [9,10]. Skeletal muscle is the main organ involved in insulin-mediated glucose uptake (> 80%).…”

Section: Introductionmentioning

confidence: 99%

The difference between steroid diabetes mellitus and type 2 diabetes mellitus: a whole-body 18F-FDG PET/CT study

et al. 2020

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Aims Steroid diabetes mellitus (SDM) is a metabolic syndrome caused by an increase in glucocorticoids, and its pathogenesis is unclear. 18F-FDG PET/CT can reflect the glucose metabolism of tissues and organs under living conditions. Here, PET/CT imaging of SDM and type 2 diabetes mellitus (T2DM) rats was used to visualize changes in glucose metabolism in the main glucose metabolizing organs and investigate the pathogenesis of SDM. Methods SDM and T2DM rat models were established. During this time, PET/CT imaging was used to measure the %ID/g value of skeletal muscle and liver to evaluate glucose uptake. The pancreatic, skeletal muscle and liver were analyzed by immunohistochemistry. Results SDM rats showed increased fasting blood glucose and insulin levels, hyperplasia of islet α and β cells, increased FDG uptake in skeletal muscle accompanied by an up-regulation of PI3Kp85α, IRS-1, and GLUT4, no significant changes in liver uptake, and that glycogen storage in the liver and skeletal muscle increased. T2DM rats showed atrophy of pancreatic islet β cells and decreased insulin levels, significantly reduced FDG uptake and glycogen storage in skeletal muscle and liver. Conclusions The pathogenesis of SDM is different from that of T2DM. The increased glucose metabolism of skeletal muscle may be related to the increased compensatory secretion of insulin. Glucocorticoids promote the proliferation of islet α cells and cause an increase in gluconeogenesis in the liver, which may cause increased blood glucose.

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Adaptive β-Cell Neogenesis in the Adult Mouse in Response to Glucocorticoid-Induced Insulin Resistance

Cited by 27 publications

References 62 publications

RETRACTED: Roles of Epigenetic Modifications in the Differentiation and Function of Pancreatic β-Cells

RETRACTED: Roles of Epigenetic Modifications in the Differentiation and Function of Pancreatic β-Cells

Chronic hypercortisolism causes more persistent visceral adiposity than HFD-induced obesity

The difference between steroid diabetes mellitus and type 2 diabetes mellitus: a whole-body 18F-FDG PET/CT study

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