Proteomics Analysis of Human Skeletal Muscle Reveals Novel Abnormalities in Obesity and Type 2 Diabetes

Hwang, Hyonseok; Bowen, Benjamin P.; Lefort, Natalie; Flynn, Charles R.; Filippis, Elena A. De; Roberts, Christine L.; Smoke, Christopher C.; Meyer, Christian; Højlund, Kurt; Yi, Zhengping; Mandarino, Lawrence J.

doi:10.2337/db09-0214

Cited by 221 publications

(256 citation statements)

References 50 publications

(83 reference statements)

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“…Moreover, significant positive correlations were also observed for summative spot volumes (sum of volumes of all spots with the same identified protein) relating to cytoplasmic malate dehydrogenase (MDH1), an enzyme controlling TCA cycle pool size and providing contractile function [27], and the mitochondrial enzymes ACO2, ATP5A1, ATP5B and GBAS. These results, suggesting reduced TCA cycle and mitochondrial protein content in insulin resistance, are consistent with previous findings of reduced enzyme activities [10,28,29], protein expression [16,17,30], altered phosphorylation [16,31,32], altered transcript levels [10,33,34] or altered flux through mitochondrial ATP synthase [8].…”

Section: Discussionsupporting

confidence: 81%

“…Thus, these two-dimensional-gel proteomic studies delivered largely consistent findings. Another recent study used one-dimensional SDS-PAGE and label-free MS/MS-based identification and quantification [17]. Of 92 proteins increased more than twofold and of these, the 15 significantly different between OB and/or obese type 2 diabetic and LE participants in that study, only six and one, respectively, were also identified by us.…”

Section: Discussionmentioning

confidence: 99%

“…Moreover, these earlier attempts involved study groups that were less well matched or rather small. Another more recent study investigated muscle from healthy lean, obese non-diabetic and obese type 2 diabetic individuals using one-dimensional gel separation with SDS-PAGE followed by HPLC-ESI-MS/MS-based identification and quantification [17], and reported significant changes in the abundance of 15 proteins.…”

Section: Introductionmentioning

confidence: 99%

“…There have been several previous approaches to the study of the human skeletal muscle proteome [13,14] and its alterations in insulin-resistant muscle [15][16][17][18]. Two studies have used the two-dimensional gel approach [15,16].…”

Section: Introductionmentioning

confidence: 99%

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The proteomic signature of insulin-resistant human skeletal muscle reveals increased glycolytic and decreased mitochondrial enzymes

et al. 2012

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Aims/hypothesis The molecular mechanisms underlying insulin resistance in skeletal muscle are incompletely understood. Here, we aimed to obtain a global picture of changes in protein abundance in skeletal muscle in obesity and type 2 diabetes, and those associated with whole-body measures of insulin action. Methods Skeletal muscle biopsies were obtained from ten healthy lean (LE), 11 obese non-diabetic (OB), and ten obese type 2 diabetic participants before and after hyperinsulinaemic-euglycaemic clamps. Quantitative proteome analysis was performed by two-dimensional differential-gel electrophoresis and tandem-mass-spectrometry-based protein identification.Results Forty-four protein spots displayed significant (p< 0.05) changes in abundance by at least a factor of 1.5 between groups. Several proteins were identified in multiple spots, suggesting post-translational modifications. Multiple spots containing glycolytic and fast-muscle proteins showed increased abundance, whereas spots with mitochondrial and slow-muscle proteins were downregulated in the OB and obese type 2 diabetic groups compared with the LE group. No differences in basal levels of myosin heavy chains were observed. The abundance of multiple spots representing glycolytic and fast-muscle proteins correlated negatively with insulin action on glucose disposal, glucose oxidation and lipid oxidation, while several spots with proteins J. Giebelstein, G. Poschmann and K. Højlund contributed equally to this work. involved in oxidative metabolism and mitochondrial function correlated positively with these whole-body measures of insulin action. Conclusions/interpretation Our data suggest that increased glycolytic and decreased mitochondrial protein abundance together with a shift in muscle properties towards a fasttwitch pattern in the absence of marked changes in fibretype distribution contribute to insulin resistance in obesity with and without type 2 diabetes. The roles of several differentially expressed or post-translationally modified proteins remain to be elucidated.

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Section: Discussionsupporting

confidence: 81%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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The proteomic signature of insulin-resistant human skeletal muscle reveals increased glycolytic and decreased mitochondrial enzymes

et al. 2012

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“…1,2 Proteomic methods have been used to investigate human and mouse obesity, but most reports have focused on changes in adipose tissue. [3][4][5][6] Recent results suggest that the blood-brain barrier (BBB) is activated in obesity; for example, mice with adult-onset obesity show resistance to leptin transport across the BBB, region-specific astrogliosis, and upregulation of astrocytic leptin receptors. 7,8 The BBB is a regulatory interface between the central nervous system (CNS) and the peripheral circulation.…”

Section: Introductionmentioning

confidence: 99%

Diet-Induced Obesity Suppresses Expression of Many Proteins at the Blood–Brain Barrier

Ouyang

Hsuchou

Kastin

et al. 2013

J Cereb Blood Flow Metab

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The blood-brain barrier (BBB) is a regulatory interface between the central nervous system and the rest of the body. However, BBB changes in obesity and metabolic syndrome have not been fully elucidated. We hypothesized that obesity reduces energy metabolism in the cerebral microvessels composing the BBB, reflected by downregulation of protein expression and function. We performed comparative proteomic analyses in enriched microvessels from the cerebral cortex of mice 2 months after ingestion of a high-fat diet or regular rodent chow. In mice with diet-induced obesity (DIO), there was downregulation of 47 proteins in the cerebral microvessels, including cytoskeletal proteins, chaperons, enzymes, transport-related proteins, and regulators for transcriptional and translational activities. Only two proteins, involved in messenger RNA (mRNA) transport and processing, were upregulated. The changes of these proteins were further validated by quantitative polymerase chain reaction (qPCR), western blotting, and immunofluorescent staining of freshly isolated microvessels, in samples obtained from different batches of mice. The predominant downregulation suggests that DIO suppresses metabolic activity of BBB microvessels. The finding of a hypometabolic state of the BBB in mice at the chronic stage of DIO is unexpected and unprecedented; it may provide novel mechanistic insight into how obesity influences CNS function via regulatory changes of the BBB. Keywords: blood-brain barrier; cerebral microvessels; high-fat diet; mass spectrometry; obesity; proteomics INTRODUCTION Obesity has become one of the most critical problems in human health and is associated with many complications of metabolic diseases. 1,2 Proteomic methods have been used to investigate human and mouse obesity, but most reports have focused on changes in adipose tissue. [3][4][5][6] Recent results suggest that the blood-brain barrier (BBB) is activated in obesity; for example, mice with adult-onset obesity show resistance to leptin transport across the BBB, region-specific astrogliosis, and upregulation of astrocytic leptin receptors. 7,8 The BBB is a regulatory interface between the central nervous system (CNS) and the peripheral circulation. It is a complex threedimensional structure composed of specialized endothelial cells that are reinforced by pericytes, astrocytic endfeet, and extracellular matrix. The tight junctions between the endothelia and the continuous basement membrane prevent diffusion of large non-lipophilic molecules between the CNS parenchyma (brain and spinal cord) and the circulation. The function of the BBB is further reinforced by a high mitochondrial content that ensures sufficient energy, an abundance of enzymes, and metabolically active astrocytes. The functions of the BBB in obesity, however, remain unclear. We predicted that BBB homeostasis is disturbed by metabolic changes in obesity.Although normal transport and secretory functions of the BBB are essential for CNS function, proteomic analyses have shown that BBB activity is ch...

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MICOS and the mitochondrial inner membrane morphology – when things get out of shape

2021

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Mitochondria play a key role in cellular signalling, metabolism and energetics. Proper architecture and remodelling of the inner mitochondrial membrane are essential for efficient respiration, apoptosis and quality control in the cell. Several protein complexes including mitochondrial contact site and cristae organising system (MICOS), F 1 F O -ATP synthase, and Optic Atrophy 1 (OPA1), facilitate formation, maintenance and stability of cristae membranes. MICOS, the F 1 F O -ATP synthase, OPA1 and inner membrane phospholipids such as cardiolipin and phosphatidylethanolamine interact with each other to organise the inner membrane ultrastructure and remodel cristae in response to the cell's demands. Functional alterations in these proteins or in the biosynthesis pathway of cardiolipin and phosphatidylethanolamine result in an aberrant inner membrane architecture and impair mitochondrial function. Mitochondrial dysfunction and abnormalities hallmark several human conditions and diseases including neurodegeneration, cardiomyopathies and diabetes mellitus. Yet, they have long been regarded as secondary pathological effects. This review discusses emerging evidence of a direct relationship between protein-and lipid-dependent regulation of the inner mitochondrial membrane morphology and diseases such as fatal encephalopathy, Leigh syndrome, Parkinson's disease, and cancer.

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Proteomics Analysis of Human Skeletal Muscle Reveals Novel Abnormalities in Obesity and Type 2 Diabetes

Cited by 221 publications

References 50 publications

The proteomic signature of insulin-resistant human skeletal muscle reveals increased glycolytic and decreased mitochondrial enzymes

The proteomic signature of insulin-resistant human skeletal muscle reveals increased glycolytic and decreased mitochondrial enzymes

Diet-Induced Obesity Suppresses Expression of Many Proteins at the Blood–Brain Barrier

MICOS and the mitochondrial inner membrane morphology – when things get out of shape

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