Exploring the role of the HNF-1αG319S polymorphism in β cell failure and youth-onset type 2 diabetes: Lessons from MODY and Hnf-1α-deficient animal models

Michael E. Jonasson; Brandy A. Wicklow; Elizabeth A.C. Sellers; Vernon W. Dolinsky; Christine A. Doucette

doi:10.1139/bcb-2015-0021

Exploring the role of the HNF-1αG319S polymorphism in β cell failure and youth-onset type 2 diabetes: Lessons from MODY and Hnf-1α-deficient animal models

Biochemistry and Cell Biology ◽

10.1139/bcb-2015-0021 ◽

2015 ◽

Vol 93 (5) ◽

pp. 487-494 ◽

Cited By ~ 2

Author(s):

Michael E. Jonasson ◽

Brandy A. Wicklow ◽

Elizabeth A.C. Sellers ◽

Vernon W. Dolinsky ◽

Christine A. Doucette

Keyword(s):

Type 2 Diabetes ◽

Cell Function ◽

Glucose Sensing ◽

Future Research ◽

Cell Phenotype ◽

Β Cells ◽

Β Cell ◽

Onset Type ◽

The Impact

The prevalence of youth-onset type 2 diabetes (T2D) is rapidly increasing worldwide, disproportionately affecting Indigenous youth with Oji-Cree heritage from central Canada. Candidate gene screening has uncovered a novel and private polymorphism in the Oji-Cree population in the hepatocyte nuclear factor-1 alpha (HNF-1α) gene, where a highly conserved glycine residue at position 319 is changed to a serine (termed HNF-1αG319S or simply G319S). Oji-Cree youth who carry one or two copies of the “S-allele” present at diagnosis with less obesity, reduced indicators of insulin resistance, and lower plasma insulin levels at diagnosis, suggestive of a primary defect in the insulin-secreting β cells. Few studies on the impact of the HNF-1αG319S variant on β cell function have been performed to date; however, much can be learned from other clinical phenotypes of HNF-1α-deficiency, including HNF-1α mutations that cause maturity-onset diabetes of the young 3 (MODY3). In addition, evaluation of Hnf-1α-deficient murine models reveals that HNF-1α plays a central role in the regulation of insulin secretion by regulating the expression of key genes involved in β cell glucose-sensing, mitochondrial function, and the maintenance of the β cell phenotype in differentiated β cells. The overall goal of this minireview is to explore the impact of HNF-1α-deficiency on the β cell to better inform future research into the mechanisms of β cell dysfunction in Oji-Cree youth with T2D.

Download Full-text

Lipotoxicity and β-Cell Failure in Type 2 Diabetes: Oxidative Stress Linked to NADPH Oxidase and ER Stress

Cells ◽

10.3390/cells10123328 ◽

2021 ◽

Vol 10 (12) ◽

pp. 3328

Author(s):

Eloisa Aparecida Vilas-Boas ◽

Davidson Correa Almeida ◽

Leticia Prates Roma ◽

Fernanda Ortis ◽

Angelo Rafael Carpinelli

Keyword(s):

Oxidative Stress ◽

Type 2 Diabetes ◽

Nadph Oxidase ◽

Er Stress ◽

Cell Function ◽

Caloric Intake ◽

Β Cells ◽

Β Cell ◽

Β Cell Function

A high caloric intake, rich in saturated fats, greatly contributes to the development of obesity, which is the leading risk factor for type 2 diabetes (T2D). A persistent caloric surplus increases plasma levels of fatty acids (FAs), especially saturated ones, which were shown to negatively impact pancreatic β-cell function and survival in a process called lipotoxicity. Lipotoxicity in β-cells activates different stress pathways, culminating in β-cells dysfunction and death. Among all stresses, endoplasmic reticulum (ER) stress and oxidative stress have been shown to be strongly correlated. One main source of oxidative stress in pancreatic β-cells appears to be the reactive oxygen species producer NADPH oxidase (NOX) enzyme, which has a role in the glucose-stimulated insulin secretion and in the β-cell demise during both T1 and T2D. In this review, we focus on the acute and chronic effects of FAs and the lipotoxicity-induced β-cell failure during T2D development, with special emphasis on the oxidative stress induced by NOX, the ER stress, and the crosstalk between NOX and ER stress.

Download Full-text

Effects of palmitate on ER and cytosolic Ca2+ homeostasis in β-cells

AJP Endocrinology and Metabolism ◽

10.1152/ajpendo.90525.2008 ◽

2009 ◽

Vol 296 (4) ◽

pp. E690-E701 ◽

Cited By ~ 122

Author(s):

Kamila S. Gwiazda ◽

Ting-Lin B. Yang ◽

Yalin Lin ◽

James D. Johnson

Keyword(s):

Type 2 Diabetes ◽

Fatty Acids ◽

Fatty Acid ◽

Free Fatty Acids ◽

Cell Function ◽

Fluorescent Protein ◽

Β Cells ◽

Β Cell ◽

Β Cell Function

There are strong links between obesity, elevated free fatty acids, and type 2 diabetes. Specifically, the saturated fatty acid palmitate has pleiotropic effects on β-cell function and survival. In the present study, we sought to determine the mechanism by which palmitate affects intracellular Ca2+, and in particular the role of the endoplasmic reticulum (ER). In human β-cells and MIN6 cells, palmitate rapidly increased cytosolic Ca2+ through a combination of Ca2+ store release and extracellular Ca2+ influx. Palmitate caused a reversible lowering of ER Ca2+, measured directly with the fluorescent protein-based ER Ca2+ sensor D1ER. Using another genetically encoded indicator, we observed long-lasting oscillations of cytosolic Ca2+ in palmitate-treated cells. In keeping with this observed ER Ca2+ depletion, palmitate induced rapid phosphorylation of the ER Ca2+ sensor protein kinase R-like ER kinase (PERK) and subsequently ER stress and β-cell death. We detected little palmitate-induced insulin secretion, suggesting that these Ca2+ signals are poorly coupled to exocytosis. In summary, we have characterized Ca2+-dependent mechanisms involved in altered β-cell function and survival induced by the free fatty acid palmitate. We present the first direct evidence that free fatty acids reduce ER Ca2+ and shed light on pathways involved in lipotoxicity and the pathogenesis of type 2 diabetes.

Download Full-text

A Sustained Activation of Pancreatic NMDARs Is a Novel Factor of β-Cell Apoptosis and Dysfunction

Endocrinology ◽

10.1210/en.2017-00366 ◽

2017 ◽

Vol 158 (11) ◽

pp. 3900-3913 ◽

Cited By ~ 13

Author(s):

Xiao-Ting Huang ◽

Shao-Jie Yue ◽

Chen Li ◽

Yan-Hong Huang ◽

Qing-Mei Cheng ◽

...

Keyword(s):

Type 2 Diabetes ◽

Cell Apoptosis ◽

Cell Function ◽

Cell Mass ◽

Nuclear Factor Κb ◽

Β Cells ◽

Β Cell ◽

Stimulation Of ◽

Sustained Activation

Abstract Type 2 diabetes, which features β-cell failure, is caused by the decrease of β-cell mass and insulin secretory function. Current treatments fail to halt the decrease of functional β-cell mass. Strategies to prevent β-cell apoptosis and dysfunction are highly desirable. Recently, our group and others have reported that blockade of N-methyl-d-aspartate receptors (NMDARs) in the islets has been proposed to prevent the progress of type 2 diabetes through improving β-cell function. It suggests that a sustained activation of the NMDARs may exhibit deleterious effect on β-cells. However, the exact functional impact and mechanism of the sustained NMDAR stimulation on islet β-cells remains unclear. Here, we identify a sustained activation of pancreatic NMDARs as a novel factor of apoptotic β-cell death and function. The sustained treatment with NMDA results in an increase of intracellular [Ca2+] and reactive oxygen species, subsequently induces mitochondrial membrane potential depolarization and a decrease of oxidative phosphorylation expression, and then impairs the mitochondrial function of β-cells. NMDA specifically induces the mitochondrial-dependent pathway of apoptosis in β-cells through upregulation of the proapoptotic Bim and Bax, and downregulation of antiapoptotic Bcl-2. Furthermore, a sustained stimulation of NMDARs impairs β-cell insulin secretion through decrease of pancreatic duodenal homeobox-1 (Pdx-1) and adenosine triphosphate synthesis. The activation of nuclear factor–κB partly contributes to the reduction of Pdx-1 expression induced by overstimulation of NMDARs. In conclusion, we show that the sustained stimulation of NMDARs is a novel mediator of apoptotic signaling and β-cell dysfunction, providing a mechanistic insight into the pathological role of NMDARs activation in diabetes.

Download Full-text

The effect of chronic twice daily exenatide treatment on β-cell function in new onset type 2 diabetes

Clinical Endocrinology ◽

10.1111/cen.12199 ◽

2013 ◽

Vol 80 (4) ◽

pp. 545-553 ◽

Cited By ~ 14

Author(s):

Amalia Gastaldelli ◽

Robert G. Brodows ◽

David D'Alessio

Keyword(s):

Type 2 Diabetes ◽

Cell Function ◽

Β Cell ◽

Onset Type ◽

Β Cell Function ◽

New Onset

Download Full-text

BLX-1002, a novel thiazolidinedione with no PPAR affinity, stimulates AMP-activated protein kinase activity, raises cytosolic Ca2+, and enhances glucose-stimulated insulin secretion in a PI3K-dependent manner

AJP Cell Physiology ◽

10.1152/ajpcell.00444.2008 ◽

2009 ◽

Vol 296 (2) ◽

pp. C346-C354 ◽

Cited By ~ 16

Author(s):

Fan Zhang ◽

Deben Dey ◽

Robert Bränström ◽

Lars Forsberg ◽

Ming Lu ◽

...

Keyword(s):

Type 2 Diabetes ◽

Insulin Secretion ◽

High Glucose ◽

Cell Function ◽

Dependent Manner ◽

Β Cells ◽

Β Cell ◽

Β Cell Function ◽

Amp Activated Protein Kinase

BLX-1002 is a novel small thiazolidinedione with no apparent affinity to peroxisome proliferator-activated receptors (PPAR) that has been shown to reduce glycemia in type 2 diabetes without adipogenic effects. Its precise mechanisms of action, however, remain elusive, and no studies have been done with respect to possible effects of BLX-1002 on pancreatic β-cells. We have investigated the influence of the drug on β-cell function in mouse islets in vitro. BLX-1002 enhanced insulin secretion stimulated by high, but not low or intermediate, glucose concentrations. BLX-1002 also augmented cytoplasmic free Ca2+ concentration ([Ca2+]i) at high glucose, an effect that was abolished by pretreatment with the Ca2+-ATPase inhibitor thapsigargin. In contrast, BLX-1002 did not interfere with voltage-gated Ca2+ channel or ATP-sensitive K+ channel activities. In addition, cellular NAD(P)H stimulated by glucose was not affected by the drug. The stimulatory effect of BLX-1002 on insulin secretion at high glucose was completely abolished by treatment with the phosphatidylinositol 3-kinase (PI3K) inhibitors wortmannin or LY-294002. Stimulation of the β-cells with BLX-1002 also induced activation of AMP-activated protein kinase (AMPK) at high glucose. Our study suggests that BLX-1002 potentiates insulin secretion only at high glucose in β-cells in a PI3K-dependent manner. This effect of BLX-1002 is associated with an increased [Ca2+]i mediated through Ca2+ mobilization, and an enhanced activation of AMPK. The glucose-sensitive stimulatory impact of BLX-1002 on β-cell function may translate into substantial clinical benefits of the drug in the management of type 2 diabetes, by avoidance of hypoglycemia.

Download Full-text

Regulating insulin signaling and β-cell function through IRS proteinsThis paper is one of a selection of papers published in this Special Issue, entitled Second Messengers and Phosphoproteins—12th International Conference.

Canadian Journal of Physiology and Pharmacology ◽

10.1139/y06-008 ◽

2006 ◽

Vol 84 (7) ◽

pp. 725-737 ◽

Cited By ~ 104

Author(s):

Morris F. White

Keyword(s):

Insulin Resistance ◽

Type 2 Diabetes ◽

Insulin Signaling ◽

Cell Function ◽

Second Messengers ◽

Glucose Sensing ◽

Β Cell ◽

Peripheral Insulin Resistance ◽

Chronic Hyperglycemia

Diabetes mellitus is a complex disorder that arises from various causes, including dysregulated glucose sensing and impaired insulin secretion (maturity onset diabetes of youth, MODY), autoimmune-mediated β-cell destruction (type 1), or insufficient compensation for peripheral insulin resistance (type 2). Type 2 diabetes is the most prevalent form that usually occurs at middle age; it afflicts more than 30 million people over the age of 65, but is appearing with greater frequency in children and adolescents. Dysregulated insulin signaling exacerbated by chronic hyperglycemia promotes a cohort of systemic disorders—including dyslipidemia, hypertension, cardiovascular disease, and female infertility. Understanding the molecular basis of insulin resistance can prevent these disorders and their inevitable progression to type 2 diabetes.

Download Full-text

Obesity and Type 2 Diabetes: What Can Be Unified and What Needs to Be Individualized?

The Journal of Clinical Endocrinology & Metabolism ◽

10.1210/jc.2011-0585 ◽

2011 ◽

Vol 96 (6) ◽

pp. 1654-1663 ◽

Cited By ~ 205

Author(s):

Robert H. Eckel ◽

Steven E. Kahn ◽

Ele Ferrannini ◽

Allison B. Goldfine ◽

David M. Nathan ◽

...

Keyword(s):

Type 2 Diabetes ◽

Cell Function ◽

Clinical Care ◽

Surgical Approaches ◽

Future Research ◽

Diabetes Incidence ◽

Β Cell ◽

Endocrine Society ◽

Writing Group

Objective: This report examines what is known about the relationship between obesity and type 2 diabetes and how future research in these areas might be directed to benefit prevention, interventions, and overall patient care. Research Design and Methods: An international working group of 32 experts in the pathophysiology, genetics, clinical trials, and clinical care of obesity and/or type 2 diabetes participated in a conference held on 6–7 January 2011 and cosponsored by The Endocrine Society, the American Diabetes Association, and the European Association for the Study of Diabetes. A writing group comprising eight participants subsequently prepared this summary and recommendations. Participants reviewed and discussed published literature and their own unpublished data. Results: The writing group unanimously supported the summary and recommendations as representing the working group's majority or unanimous opinions. Conclusions: The major questions linking obesity to type 2 diabetes that need to be addressed by combined basic, clinical, and population-based scientific approaches include the following: 1) Why do not all patients with obesity develop type 2 diabetes? 2) Through what mechanisms do obesity and insulin resistance contribute to β-cell decompensation, and if/when obesity prevention ensues, how much reduction in type 2 diabetes incidence will follow? 3) How does the duration of type 2 diabetes relate to the benefits of weight reduction by lifestyle, weight-loss drugs, and/or bariatric surgery on β-cell function and glycemia? 4) What is necessary for regulatory approval of medications and possibly surgical approaches for preventing type 2 diabetes in patients with obesity? Improved understanding of how obesity relates to type 2 diabetes may help advance effective and cost-effective interventions for both conditions, including more tailored therapy. To expedite this process, we recommend further investigation into the pathogenesis of these coexistent conditions and innovative approaches to their pharmacological and surgical management.

Download Full-text

The impact of family history of type 2 diabetes on pancreatic β-cell function

Diabetes Research and Clinical Practice ◽

10.1016/j.diabres.2009.04.004 ◽

2009 ◽

Vol 86 (1) ◽

pp. 61-66 ◽

Cited By ~ 5

Author(s):

Zhi-hong Wang ◽

Su-Hua Zhang ◽

Li-lin Gong ◽

Wei Ren ◽

Rong Li ◽

...

Keyword(s):

Type 2 Diabetes ◽

Family History ◽

Cell Function ◽

Pancreatic Β Cell ◽

Β Cell ◽

Β Cell Function ◽

History Of ◽

The Impact

Download Full-text

β-Cell compensation concomitant with adaptive endoplasmic reticulum stress and β-cell neogenesis in a diet-induced type 2 diabetes model

Applied Physiology Nutrition and Metabolism ◽

10.1139/apnm-2019-0144 ◽

2019 ◽

Vol 44 (12) ◽

pp. 1355-1366 ◽

Cited By ~ 2

Author(s):

Hui Huang ◽

Kaiyuan Yang ◽

Rennian Wang ◽

Woo Hyun Han ◽

Sharee Kuny ◽

...

Keyword(s):

Type 2 Diabetes ◽

Endoplasmic Reticulum ◽

Insulin Secretion ◽

Cell Function ◽

Cell Mass ◽

Temporal Association ◽

Adaptive Responses ◽

Β Cells ◽

Β Cell

Insulin-secreting pancreatic β-cells adapt to obesity-related insulin resistance via increases in insulin secretion and β-cell mass. Failed β-cell compensation predicts the onset of type 2 diabetes (T2D). However, the mechanisms of β-cell compensation are not fully understood. Our previous study reported changes in β-cell mass during the progression of T2D in the Nile rat (NR; Arvicanthis niloticus) fed standard chow. In the present study, we measured other β-cell adaptive responses, including glucose metabolism and β-cell insulin secretion in NRs at different ages, thus characterizing NR at 2 months as a model of β-cell compensation followed by decompensation at 6 months. We observed increased proinsulin secretion in the transition from compensation to decompensation, which is indicative of impaired insulin processing. Subsequently, we compared adaptive unfolded protein response in β-cells and demonstrated a positive role of endoplasmic reticulum (ER) chaperones in insulin secretion. In addition, the incidence of insulin-positive neogenic but not proliferative cells increased during the compensation phase, suggesting nonproliferative β-cell growth as a mechanism of β-cell mass adaptation. In contrast, decreased neogenesis and β-cell dedifferentiation were observed in β-cell dysfunction. Furthermore, the progression of T2D and pathophysiological changes of β-cells were prevented by increasing fibre content of the diet. Novelty Our study characterized a novel model for β-cell compensation with adaptive responses in cell function and mass. The temporal association of adaptive ER chaperones with blood insulin and glucose suggests upregulated chaperone capacity as an adaptive mechanism. β-Cell neogenesis but not proliferation contributes to β-cell mass adaptation.

Download Full-text

The Anna Karenina model of β cell maturation in development and their dedifferentiation in type 1 and type 2 diabetes

10.1101/2021.02.16.431507 ◽

2021 ◽

Author(s):

Sutichot D. Nimkulrat ◽

Zijian Ni ◽

Jared Brown ◽

Christina Kendziorski ◽

Barak Blum

Keyword(s):

Type 2 Diabetes ◽

Cell Function ◽

Lineage Tracing ◽

Β Cells ◽

Β Cell ◽

Cell Dedifferentiation ◽

Anna Karenina ◽

Β Cell Function

AbstractLoss of mature β cell function and identity, or β cell dedifferentiation, is seen in all types of diabetes mellitus. Two competing models explain β cell dedifferentiation in diabetes. In the first model, β cells dedifferentiate in the reverse order of their developmental ontogeny. This model predicts that dedifferentiated β cells resemble β cell progenitors. In the second model, β cell dedifferentiation depends on the type of diabetogenic stress. This model, which we call the “Anna Karenina” model, predicts that in each type of diabetes, β cells dedifferentiate in their own way, depending on how their mature identity is disrupted by any particular diabetogenic stress. We directly tested the two models using a β cell-specific lineage-tracing system coupled with RNA-sequencing in mice. We constructed a multidimensional map of β cell transcriptional trajectories during the normal course of β cell postnatal development and during their dedifferentiation in models of both type 1 diabetes (NOD) and type 2 diabetes (BTBR-Lepob/ob). Using this unbiased approach, we show here that despite some similarities between immature and dedifferentiated β cells, β cells dedifferentiation in the two mouse models is not a reversal of developmental ontogeny and is different between different types of diabetes.

Download Full-text