What Is the Sweetest UPR Flavor for the β-cell? That Is the Question

Unfolded protein response (UPR) is a process conserved from yeasts to mammals and, based on the generally accepted dogma, helps the secretory performance of a cell, by improving its capacity to cope with a burden in the endoplasmic reticulum (ER). The ER of β-cells, “professional secretory cells”, has to manage tremendous amounts of insulin, which elicits a strong pressure on the ER intrinsic folding capacity. Thus, the constant demand for insulin production results in misfolded proinsulin, triggering a physiological upregulation of UPR to restore homeostasis. Most diabetic disorders are characterized by the loss of functional β-cells, and the pathological side of UPR plays an instrumental role. The transition from a homeostatic to a pathological UPR that ultimately leads to insulin-producing β-cell decay entails complex cellular processes and molecular mechanisms which remain poorly described so far. Here, we summarize important processes that are coupled with or driven by UPR in β-cells, such as proliferation, inflammation and dedifferentiation. We conclude that the UPR comes in different “flavors” and each of them is correlated with a specific outcome for the cell, for survival, differentiation, proliferation as well as cell death. All these greatly depend on the way UPR is triggered, however what exactly is the switch that favors the activation of one UPR as opposed to others is largely unknown. Substantial work needs to be done to progress the knowledge in this important emerging field as this will help in the development of novel and more efficient therapies for diabetes.

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The Pancreatic ß-cell Response to Secretory Demands and Adaption to Stress

Endocrinology ◽

10.1210/endocr/bqab173 ◽

2021 ◽

Vol 162 (11) ◽

Author(s):

Michael A Kalwat ◽

Donalyn Scheuner ◽

Karina Rodrigues-dos-Santos ◽

Decio L Eizirik ◽

Melanie H Cobb

Keyword(s):

Unfolded Protein Response ◽

Cell Function ◽

Protein Translation ◽

Insulin Production ◽

Β Cells ◽

Β Cell ◽

Compensatory Mechanisms ◽

Unfolded Protein ◽

The Unfolded Protein Response ◽

Protein Response

Abstract Pancreatic β cells dedicate much of their protein translation capacity to producing insulin to maintain glucose homeostasis. In response to increased secretory demand, β cells can compensate by increasing insulin production capability even in the face of protracted peripheral insulin resistance. The ability to amplify insulin secretion in response to hyperglycemia is a critical facet of β-cell function, and the exact mechanisms by which this occurs have been studied for decades. To adapt to the constant and fast-changing demands for insulin production, β cells use the unfolded protein response of the endoplasmic reticulum. Failure of these compensatory mechanisms contributes to both type 1 and 2 diabetes. Additionally, studies in which β cells are “rested” by reducing endogenous insulin demand have shown promise as a therapeutic strategy that could be applied more broadly. Here, we review recent findings in β cells pertaining to the metabolic amplifying pathway, the unfolded protein response, and potential advances in therapeutics based on β-cell rest.

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The Role of the ER-Induced UPR Pathway and the Efficacy of Its Inhibitors and Inducers in the Inhibition of Tumor Progression

Oxidative Medicine and Cellular Longevity ◽

10.1155/2019/5729710 ◽

2019 ◽

Vol 2019 ◽

pp. 1-15 ◽

Cited By ~ 13

Author(s):

Anna Walczak ◽

Kinga Gradzik ◽

Jacek Kabzinski ◽

Karolina Przybylowska-Sygut ◽

Ireneusz Majsterek

Keyword(s):

Er Stress ◽

Molecular Mechanisms ◽

Unfolded Proteins ◽

Cell Protection ◽

Protection Mechanism ◽

Unfolded Protein ◽

Er Stress Response ◽

A Cell ◽

The Unfolded Protein Response ◽

Protein Response

Cancer is the second most frequent cause of death worldwide. It is considered to be one of the most dangerous diseases, and there is still no effective treatment for many types of cancer. Since cancerous cells have a high proliferation rate, it is pivotal for their proper functioning to have the well-functioning protein machinery. Correct protein processing and folding are crucial to maintain tumor homeostasis. Endoplasmic reticulum (ER) stress is one of the leading factors that cause disturbances in these processes. It is induced by impaired function of the ER and accumulation of unfolded proteins. Induction of ER stress affects many molecular pathways that cause the unfolded protein response (UPR). This is the way in which cells can adapt to the new conditions, but when ER stress cannot be resolved, the UPR induces cell death. The molecular mechanisms of this double-edged sword process are involved in the transition of the UPR either in a cell protection mechanism or in apoptosis. However, this process remains poorly understood but seems to be crucial in the treatment of many diseases that are related to ER stress. Hence, understanding the ER stress response, especially in the aspect of pathological consequences of UPR, has the potential to allow us to develop novel therapies and new diagnostic and prognostic markers for cancer.

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Endoplasmic reticulum stress and the unfolded protein response in pancreatic islet inflammation

Journal of Molecular Endocrinology ◽

10.1530/jme-15-0306 ◽

2016 ◽

Vol 57 (1) ◽

pp. R1-R17 ◽

Cited By ~ 31

Author(s):

Kira Meyerovich ◽

Fernanda Ortis ◽

Florent Allagnat ◽

Alessandra K Cardozo

Keyword(s):

Endoplasmic Reticulum ◽

Er Stress ◽

Unfolded Protein Response ◽

Diabetic Patients ◽

Β Cells ◽

Β Cell ◽

Unfolded Protein ◽

Islet Inflammation ◽

The Unfolded Protein Response ◽

Protein Response

Insulin-secreting pancreatic β-cells are extremely dependent on their endoplasmic reticulum (ER) to cope with the oscillatory requirement of secreted insulin to maintain normoglycemia. Insulin translation and folding rely greatly on the unfolded protein response (UPR), an array of three main signaling pathways designed to maintain ER homeostasis and limit ER stress. However, prolonged or excessive UPR activation triggers alternative molecular pathways that can lead to β-cell dysfunction and apoptosis. An increasing number of studies suggest a role of these pro-apoptotic UPR pathways in the downfall of β-cells observed in diabetic patients. Particularly, the past few years highlighted a cross talk between the UPR and inflammation in the context of both type 1 (T1D) and type 2 diabetes (T2D). In this article, we describe the recent advances in research regarding the interplay between ER stress, the UPR, and inflammation in the context of β-cell apoptosis leading to diabetes.

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Endoplasmic Reticulum Stress Signaling in Disease

Physiological Reviews ◽

10.1152/physrev.00015.2006 ◽

2006 ◽

Vol 86 (4) ◽

pp. 1133-1149 ◽

Cited By ~ 621

Author(s):

Stefan J. Marciniak ◽

David Ron

Keyword(s):

Diabetes Mellitus ◽

Endoplasmic Reticulum ◽

Β Cells ◽

Β Cell ◽

Insulin Synthesis ◽

Unfolded Protein ◽

Peripheral Insulin Resistance ◽

Eukaryotic Proteins ◽

The Unfolded Protein Response ◽

Protein Response

The extracellular space is an environment hostile to unmodified polypeptides. For this reason, many eukaryotic proteins destined for exposure to this environment through secretion or display at the cell surface require maturation steps within a specialized organelle, the endoplasmic reticulum (ER). A complex homeostatic mechanism, known as the unfolded protein response (UPR), has evolved to link the load of newly synthesized proteins with the capacity of the ER to mature them. It has become apparent that dysfunction of the UPR plays an important role in some human diseases, especially those involving tissues dedicated to extracellular protein synthesis. Diabetes mellitus is an example of such a disease, since the demands for constantly varying levels of insulin synthesis make pancreatic β-cells dependent on efficient UPR signaling. Furthermore, recent discoveries in this field indicate that the importance of the UPR in diabetes is not restricted to the β-cell but is also involved in peripheral insulin resistance. This review addresses aspects of the UPR currently understood to be involved in human disease, including their role in diabetes mellitus, atherosclerosis, and neoplasia.

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XBP1s activation can globally remodel N-glycan structure distribution patterns

Proceedings of the National Academy of Sciences ◽

10.1073/pnas.1805425115 ◽

2018 ◽

Vol 115 (43) ◽

pp. E10089-E10098 ◽

Cited By ~ 10

Author(s):

Madeline Y. Wong ◽

Kenny Chen ◽

Aristotelis Antonopoulos ◽

Brian T. Kasper ◽

Mahender B. Dewal ◽

...

Keyword(s):

Secretory Pathway ◽

Distribution Patterns ◽

Surface Proteins ◽

Glycan Structure ◽

Cellular Processes ◽

Unfolded Protein ◽

A Cell ◽

Wide Scale ◽

The Unfolded Protein Response ◽

Protein Response

Classically, the unfolded protein response (UPR) safeguards secretory pathway proteostasis. The most ancient arm of the UPR, the IRE1-activated spliced X-box binding protein 1 (XBP1s)-mediated response, has roles in secretory pathway maturation beyond resolving proteostatic stress. Understanding the consequences of XBP1s activation for cellular processes is critical for elucidating mechanistic connections between XBP1s and development, immunity, and disease. Here, we show that a key functional output of XBP1s activation is a cell type-dependent shift in the distribution of N-glycan structures on endogenous membrane and secreted proteomes. For example, XBP1s activity decreased levels of sialylation and bisecting GlcNAc in the HEK293 membrane proteome and secretome, while substantially increasing the population of oligomannose N-glycans only in the secretome. In HeLa cell membranes, stress-independent XBP1s activation increased the population of high-mannose and tetraantennary N-glycans, and also enhanced core fucosylation. mRNA profiling experiments suggest that XBP1s-mediated remodeling of the N-glycome is, at least in part, a consequence of coordinated transcriptional resculpting of N-glycan maturation pathways by XBP1s. The discovery of XBP1s-induced N-glycan structural remodeling on a glycome-wide scale suggests that XBP1s can act as a master regulator of N-glycan maturation. Moreover, because the sugars on cell-surface proteins or on proteins secreted from an XBP1s-activated cell can be molecularly distinct from those of an unactivated cell, these findings reveal a potential new mechanism for translating intracellular stress signaling into altered interactions with the extracellular environment.

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Coxsackievirus B Tailors the Unfolded Protein Response to Favour Viral Amplification in Pancreatic β Cells

Journal of Innate Immunity ◽

10.1159/000496034 ◽

2019 ◽

Vol 11 (4) ◽

pp. 375-390 ◽

Cited By ~ 5

Author(s):

Maikel L. Colli ◽

Flavia M. Paula ◽

Lorella Marselli ◽

Piero Marchetti ◽

Merja Roivainen ◽

...

Keyword(s):

Cell Death ◽

Er Stress ◽

Unfolded Protein Response ◽

Pancreatic Β Cell ◽

Β Cells ◽

Β Cell ◽

Unfolded Protein ◽

Islet Inflammation ◽

The Unfolded Protein Response ◽

Protein Response

Type 1 diabetes (T1D) is an autoimmune disease characterized by islet inflammation and progressive pancreatic β cell destruction. The disease is triggered by a combination of genetic and environmental factors, but the mechanisms leading to the triggering of early innate and late adaptive immunity and consequent progressive pancreatic β cell death remain unclear. The insulin-producing β cells are active secretory cells and are thus particularly sensitive to endoplasmic reticulum (ER) stress. ER stress plays an important role in the pathologic pathway leading to autoimmunity, islet inflammation, and β cell death. We show here that group B coxsackievirus (CVB) infection, a putative causative factor for T1D, induces a partial ER stress in rat and human β cells. The activation of the PERK/ATF4/CHOP branch is blunted while the IRE1α branch leads to increased spliced XBP1 expression and c-Jun N-terminal kinase (JNK) activation. Interestingly, JNK1 activation is essential for CVB amplification in both human and rat β cells. Furthermore, a chemically induced ER stress preceding viral infection increases viral replication, in a process dependent on IRE1α activation. Our findings show that CVB tailors the unfolded protein response in β cells to support their replication, preferentially triggering the pro-viral IRE1α/XBP1s/JNK1 pathway while blocking the pro-apoptotic PERK/ATF4/CHOP pathway.

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Characterization of Signaling Pathways Associated with Pancreatic β-cell Adaptive Flexibility in Compensation of Obesity-linked Diabetes in db/db Mice

Molecular & Cellular Proteomics ◽

10.1074/mcp.ra119.001882 ◽

2020 ◽

Vol 19 (6) ◽

pp. 971-993 ◽

Cited By ~ 1

Author(s):

Taewook Kang ◽

Brandon B. Boland ◽

Pia Jensen ◽

Cristina Alarcon ◽

Arkadiusz Nawrocki ◽

...

Keyword(s):

Molecular Mechanisms ◽

Cell Function ◽

Pancreatic Β Cell ◽

Insulin Production ◽

Metabolic Demand ◽

Β Cells ◽

Β Cell ◽

Proinsulin Biosynthesis ◽

Β Cell Function ◽

Insight Into

The onset of obesity-linked type 2 diabetes (T2D) is marked by an eventual failure in pancreatic β-cell function and mass that is no longer able to compensate for the inherent insulin resistance and increased metabolic load intrinsic to obesity. However, in a commonly used model of T2D, the db/db mouse, β-cells have an inbuilt adaptive flexibility enabling them to effectively adjust insulin production rates relative to the metabolic demand. Pancreatic β-cells from these animals have markedly reduced intracellular insulin stores, yet high rates of (pro)insulin secretion, together with a substantial increase in proinsulin biosynthesis highlighted by expanded rough endoplasmic reticulum and Golgi apparatus. However, when the metabolic overload and/or hyperglycemia is normalized, β-cells from db/db mice quickly restore their insulin stores and normalize secretory function. This demonstrates the β-cell's adaptive flexibility and indicates that therapeutic approaches applied to encourage β-cell rest are capable of restoring endogenous β-cell function. However, mechanisms that regulate β-cell adaptive flexibility are essentially unknown. To gain deeper mechanistic insight into the molecular events underlying β-cell adaptive flexibility in db/db β-cells, we conducted a combined proteomic and post-translational modification specific proteomic (PTMomics) approach on islets from db/db mice and wild-type controls (WT) with or without prior exposure to normal glucose levels. We identified differential modifications of proteins involved in redox homeostasis, protein refolding, K48-linked deubiquitination, mRNA/protein export, focal adhesion, ERK1/2 signaling, and renin-angiotensin-aldosterone signaling, as well as sialyltransferase activity, associated with β-cell adaptive flexibility. These proteins are all related to proinsulin biosynthesis and processing, maturation of insulin secretory granules, and vesicular trafficking—core pathways involved in the adaptation of insulin production to meet metabolic demand. Collectively, this study outlines a novel and comprehensive global PTMome signaling map that highlights important molecular mechanisms related to the adaptive flexibility of β-cell function, providing improved insight into disease pathogenesis of T2D.

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ER Stress in Cardiometabolic Diseases: From Molecular Mechanisms to Therapeutics

Endocrine Reviews ◽

10.1210/endrev/bnab006 ◽

2021 ◽

Cited By ~ 2

Author(s):

Amir Ajoolabady ◽

Shuyi Wang ◽

Guido Kroemer ◽

Daniel J Klionsky ◽

Vladimir N Uversky ◽

...

Keyword(s):

Diabetes Mellitus ◽

Er Stress ◽

Molecular Mechanisms ◽

Unfolded Proteins ◽

Cardiometabolic Diseases ◽

Cellular Processes ◽

Unfolded Protein ◽

Protein Response ◽

Available Information ◽

Er Homeostasis

Abstract The endoplasmic reticulum (ER) hosts linear polypeptides and fosters natural folding of proteins through ER-residing chaperones and enzymes. Failure of the ER to align and compose proper protein architecture leads to accumulation of misfolded/unfolded proteins in the ER lumen, which disturbs ER homeostasis to provoke ER stress. Presence of ER stress initiates the cytoprotective unfolded protein response (UPR) to restore ER homeostasis or instigates a rather maladaptive UPR to promote cell death. Although a wide array of cellular processes such as persistent autophagy, dysregulated mitophagy, and secretion of proinflammatory cytokines may contribute to the onset and progression of cardiometabolic diseases, it is well perceived that ER stress also evokes the onset and development of cardiometabolic diseases, particularly cardiovascular diseases (CVDs), diabetes mellitus, obesity, and chronic kidney disease (CKD). Meanwhile, these pathological conditions further aggravate ER stress, creating a rather vicious cycle. Here in this review, we aimed at summarizing and updating the available information on ER stress in CVDs, diabetes mellitus, obesity, and CKD, hoping to offer novel insights for the management of these cardiometabolic comorbidities through regulation of ER stress.

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Molecular Mechanisms Underlying TDP-43 Pathology in Cellular and Animal Models of ALS and FTLD

International Journal of Molecular Sciences ◽

10.3390/ijms22094705 ◽

2021 ◽

Vol 22 (9) ◽

pp. 4705

Author(s):

Alistair Wood ◽

Yuval Gurfinkel ◽

Nicole Polain ◽

Wesley Lamont ◽

Sarah Lyn Rea

Keyword(s):

Animal Models ◽

Rna Splicing ◽

Molecular Mechanisms ◽

Neuromuscular Junctions ◽

Cellular Processes ◽

Unfolded Protein ◽

Disease Spectrum ◽

Genetic Overlap ◽

The Unfolded Protein Response ◽

Protein Response

Amyotrophic lateral sclerosis (ALS) and frontotemporal lobar degeneration (FTLD) are neurodegenerative disorders that exist on a disease spectrum due to pathological, clinical and genetic overlap. In up to 97% of ALS cases and ~50% of FTLD cases, the primary pathological protein observed in affected tissues is TDP-43, which is hyperphosphorylated, ubiquitinated and cleaved. The TDP-43 is observed in aggregates that are abnormally located in the cytoplasm. The pathogenicity of TDP-43 cytoplasmic aggregates may be linked with both a loss of nuclear function and a gain of toxic functions. The cellular processes involved in ALS and FTLD disease pathogenesis include changes to RNA splicing, abnormal stress granules, mitochondrial dysfunction, impairments to axonal transport and autophagy, abnormal neuromuscular junctions, endoplasmic reticulum stress and the subsequent induction of the unfolded protein response. Here, we review and discuss the evidence for alterations to these processes that have been reported in cellular and animal models of TDP-43 proteinopathy.

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Bax and Bak jointly control survival and dampen the early unfolded protein response in pancreatic β-cells under glucolipotoxic stress

10.1101/855239 ◽

2019 ◽

Author(s):

Sarah A. White ◽

Lisa Zhang ◽

Yu Hsuan Carol Yang ◽

Dan S. Luciani

Keyword(s):

Cell Death ◽

Er Stress ◽

Unfolded Protein Response ◽

Β Cells ◽

Β Cell ◽

Pancreatic Β Cells ◽

Unfolded Protein ◽

Protein Response

ABSTRACTER stress and apoptosis contribute to the loss of pancreatic β-cells under the pro-diabetic conditions of glucolipotoxicity. Although activation of the canonical pathway of intrinsic apoptosis is known to require Bax and Bak, their individual and combined involvement in glucolipotoxic β-cell death have not been demonstrated. It has also remained an open question if Bax and Bak in β-cells have non-apoptotic roles in mitochondrial function and ER stress signaling, as suggested in other cell types. Using mice with individual or combined β-cell deletion of Bax and Bak, we demonstrated that glucolipotoxic β-cell death in vitro happens in sequential stages; first via non-apoptotic mechanisms and later by apoptosis, which Bax and Bak were redundant in triggering. In contrast, they had non-redundant roles in mediating staurosporine-induced β-cell apoptosis. We further established that Bax and Bak do not affect normal glucose-stimulated β-cell Ca2+ responses, insulin secretion, or in vivo glucose tolerance. Finally, our experiments revealed that Bax and Bak together dampen the unfolded protein response in β-cells during the early stages of chemical- or glucolipotoxicity-induced ER stress. These findings identify novel roles of the canonical apoptosis machinery in modulating stress signals that are important for the pathobiology of β-cells in diabetes.

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