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1. Global deletion of the immune cell transcription factor, T-bet, alters gut microbiota and insulin sensitivity in mice.

Author

Stolarczyk, E., Vong, C. T., Garrido-Mesa, N., Marks, E., Abdel-Aziz, D., Ju, Q., Jackson, I., Powell, N., Lord, G. M., and Howard, J. K.

Abstract

The gut microbiota plays a role in energy homeostasis: its composition differs in lean and obese mice and may impact insulin sensitivity. The immune system has co-evolved with the gut microbiota, but direct regulation of microbial communities by the immune system and its metabolic impact is unclear. Mice lacking the immune cell specific transcription factor T-bet (Tbx21) are insulin sensitive. Compared with wild-type mice, T-bet deficient mice were found to have a higher proportion of colonic regulatory T cells despite significantly fewer colonic T cells, B cells and NK cells. Microbiota deletion by administration of antibiotics, increased colonic immune cell numbers. Furthermore, we report that T-bet −/− mice have an altered gut microbial composition and fecal short-chain fatty acid content, with an increase in butyrate production, compared with wild-type mice. Finally, in a proof-of concept study, we show that the enhanced insulin sensitivity observed in T-bet −/− mice is temporarily transmissible to antibiotic-treated wild-type mice through fecal transfer. Immune regulation of the gut microbiota by T-bet may be a novel pathway modulating insulin sensitivity. [ABSTRACT FROM AUTHOR]

Published
2024
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7. T-bet fate mapping identifies a novel ILC1-ILC2 subset in vivo

Author

Schroeder, J-H, primary, Garrido-Mesa, N, additional, Zabinski, T, additional, Gallagher, AL, additional, Campbell, L, additional, Roberts, LB, additional, Stolarczyk, E, additional, Beattie, G, additional, Lo, JW, additional, Iseppon, A, additional, Heliodoro, C Moreira, additional, Reis, R, additional, Jenner, RG, additional, Lavender, P, additional, Howard, JK, additional, Grencis, RK, additional, Helmby, H, additional, Neves, J F, additional, and Lord, GM, additional

Published
2020
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8. T-bet controls intestinal mucosa immune responses via repression of type 2 innate lymphoid cell function

Author

Garrido-Mesa, N., Schroeder, J-H., Stolarczyk, E., Gallagher, A. L., Lo, J. W., Bailey, C., Campbell, L., Sexl, V., Macdonald, T. T., Howard, J. K., Grencis, R. K., Powell, N., and Lord, G. M.

Subjects
Science & Technology, PROMOTES, Immunology, FATE, PROGENITOR, hemic and immune systems, chemical and pharmacologic phenomena, 11 Medical And Health Sciences, TRICHINELLA-SPIRALIS, 06 Biological Sciences, TRANSCRIPTION FACTOR GATA3, DIFFERENTIATION, INFLAMMATION, PROTECTION, TH17, Life Sciences & Biomedicine, biological, SUPPRESSION
Abstract

Innate lymphoid cells (ILCs) play an important role in regulating immune responses at mucosal surfaces. The transcription factor T-bet is crucial for the function of ILC1s and NCR+ ILC3s and constitutive deletion of T-bet prevents the development of these subsets. Lack of T-bet in the absence of an adaptive immune system causes microbiota-dependent colitis to occur due to aberrant ILC3 responses. Thus, T-bet expression in the innate immune system has been considered to dampen pathogenic immune responses. Here, we show that T-bet plays an unexpected role in negatively regulating innate type 2 responses, in the context of an otherwise intact immune system. Selective loss of T-bet in ILCs leads to the expansion and increased activity of ILC2s, which has a functionally important impact on mucosal immunity, including enhanced protection from Trichinella spiralis infection and inflammatory colitis. Mechanistically, we show that T-bet controls the intestinal ILC pool through regulation of IL-7 receptor signalling. These data demonstrate that T-bet expression in ILCs acts as the key transcriptional checkpoint in regulating pathogenic vs. protective mucosal immune responses, which has significant implications for the understanding of the pathogenesis of inflammatory bowel diseases and intestinal infections.

Published
2018
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10. Fermentable carbohydrate stimulates FFAR2-dependent colonic PYY cell expansion to increase satiety

Author

Brooks, L, Viardot, A, Tsakmaki, A, Stolarczyk, E, Howard, JK, Cani, PD, Everard, A, Sleeth, ML, Psichas, A, Anastasovskaj, J, Bell, JD, Bell-Anderson, K, Mackay, CR, Ghatei, MA, Bloom, SR, Frost, G, and Bewick, GA

Subjects
Colon, Microbiota, digestive, oral, and skin physiology, Peptide YY, Obesity, Diet
Abstract

Objective Dietary supplementation with fermentable carbohydrate protects against body weight gain. Fermentation by the resident gut microbiota produces short-chain fatty acids, which act at free fatty acid receptor 2 (FFAR2). Our aim was to test the hypothesis that FFAR2 is important in regulating the beneficial effects of fermentable carbohydrate on body weight and to understand the role of gut hormones PYY and GLP-1. Methods Wild-type or Ffar2-/-mice were fed an inulin supplemented or control diet. Mice were metabolically characterised and gut hormone concentrations, enteroendocrine cell density measurements were carried out. Intestinal organoids and colonic cultures were utilised to substantiate the in vivo findings. Results We provide new mechanistic insight into how fermentable carbohydrate regulates metabolism. Using mice that lack FFAR2, we demonstrate that the fermentable carbohydrate, inulin, acts via this receptor to drive an 87% increase in the density of cells that produce the appetite-supressing hormone peptide YY (PYY), reduce food intake and prevent diet-induced obesity. Conclusion Our results demonstrate that FFAR2 is predominantly involved in regulating the effects of fermentable carbohydrate on metabolism and does so, in part, by enhancing PYY cell density and release. This highlights the potential for targeting enteroendocrine cell differentiation to treat obesity.

Published
2016

18. Descent, marriage, and residence practices of a 3,800-year-old pastoral community in Central Eurasia.

Author

Blöcher J, Brami M, Feinauer IS, Stolarczyk E, Diekmann Y, Vetterdietz L, Karapetian M, Winkelbach L, Kokot V, Vallini L, Stobbe A, Haak W, Papageorgopoulou C, Krause R, Sharapova S, and Burger J

Subjects
Adult, Male, Child, Humans, Female, Cell Communication, Fertility, Life Expectancy, Marriage, Burial
Abstract

Our understanding of prehistoric societal organization at the family level is still limited. Here, we generated genome data from 32 individuals from an approximately 3,800-y-old burial mound attributed to the Bronze Age Srubnaya-Alakul cultural tradition at the site of Nepluyevsky, located in the Southern Ural region of Central Eurasia. We found that life expectancy was generally very low, with adult males living on average 8 y longer than females. A total of 35 first-degree, 40 second-degree, and 48 third-degree biological relationships connected 23 of the studied individuals, allowing us to propose a family tree spanning three generations with six brothers at its center. The oldest of these brothers had eight children with two women and the most children overall, whereas the other relationships were monogamous. Notably, related female children above the age of five were completely absent from the site, and adult females were more genetically diverse than males. These results suggest that biological relationships between male siblings played a structural role in society and that descent group membership was based on patrilineality. Women originated from a larger mating network and moved to join the men, with whom they were buried. Finally, the oldest brother likely held a higher social position, which was expressed in terms of fertility.

Published
2023
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19. Emergence and intensification of dairying in the Caucasus and Eurasian steppes.

Author

Scott A, Reinhold S, Hermes T, Kalmykov AA, Belinskiy A, Buzhilova A, Berezina N, Kantorovich AR, Maslov VE, Guliyev F, Lyonnet B, Gasimov P, Jalilov B, Eminli J, Iskandarov E, Hammer E, Nugent SE, Hagan R, Majander K, Onkamo P, Nordqvist K, Shishlina N, Kaverzneva E, Korolev AI, Khokhlov AA, Smolyaninov RV, Sharapova SV, Krause R, Karapetian M, Stolarczyk E, Krause J, Hansen S, Haak W, and Warinner C

Subjects
Animals, Archaeology, Cattle, Horses, Humans, Livestock, Sheep, White People, Dairying, Grassland
Abstract

Archaeological and archaeogenetic evidence points to the Pontic-Caspian steppe zone between the Caucasus and the Black Sea as the crucible from which the earliest steppe pastoralist societies arose and spread, ultimately influencing populations from Europe to Inner Asia. However, little is known about their economic foundations and the factors that may have contributed to their extensive mobility. Here, we investigate dietary proteins within the dental calculus proteomes of 45 individuals spanning the Neolithic to Greco-Roman periods in the Pontic-Caspian Steppe and neighbouring South Caucasus, Oka-Volga-Don and East Urals regions. We find that sheep dairying accompanies the earliest forms of Eneolithic pastoralism in the North Caucasus. During the fourth millennium BC, Maykop and early Yamnaya populations also focused dairying exclusively on sheep while reserving cattle for traction and other purposes. We observe a breakdown in livestock specialization and an economic diversification of dairy herds coinciding with aridification during the subsequent late Yamnaya and North Caucasus Culture phases, followed by severe climate deterioration during the Catacomb and Lola periods. The need for additional pastures to support these herds may have driven the heightened mobility of the Middle and Late Bronze Age periods. Following a hiatus of more than 500 years, the North Caucasian steppe was repopulated by Early Iron Age societies with a broad mobile dairy economy, including a new focus on horse milking., (© 2022. The Author(s).)

Published
2022
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20. A population of naive-like CD4 + T cells stably polarized to the T H 1 lineage.

Author

Lo JW, de Mucha MV, Henderson S, Roberts LB, Constable LE, Garrido-Mesa N, Hertweck A, Stolarczyk E, Houlder EL, Jackson I, MacDonald AS, Powell N, Neves JF, Howard JK, Jenner RG, and Lord GM

Subjects
Animals, Cell Differentiation, Gene Expression Regulation, Lymphocyte Activation, Mice, T-Lymphocytes, Regulatory metabolism, Th17 Cells metabolism, Th2 Cells, T-Box Domain Proteins genetics, T-Box Domain Proteins metabolism, Th1 Cells
Abstract

T-bet is the lineage-specifying transcription factor for CD4 + T H 1 cells. T-bet has also been found in other CD4 + T cell subsets, including T H 17 cells and Treg, where it modulates their functional characteristics. However, we lack information on when and where T-bet is expressed during T cell differentiation and how this impacts T cell differentiation and function. To address this, we traced the ontogeny of T-bet-expressing cells using a fluorescent fate-mapping mouse line. We demonstrate that T-bet is expressed in a subset of CD4 + T cells that have naïve cell surface markers and transcriptional profile and that this novel cell population is phenotypically and functionally distinct from previously described populations of naïve and memory CD4 + T cells. Naïve-like T-bet-experienced cells are polarized to the T H 1 lineage, predisposed to produce IFN-γ upon cell activation, and resist repolarization to other lineages in vitro and in vivo. These results demonstrate that lineage-specifying factors can polarize T cells in the absence of canonical markers of T cell activation and that this has an impact on the subsequent T-helper response., (© 2022 The Authors. European Journal of Immunology published by Wiley-VCH GmbH.)

Published
2022
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21. Pluripotent Stem Cell-Derived Hepatocytes Inhibit T Cell Proliferation In Vitro through Tryptophan Starvation.

Author

Romano M, Elgueta R, McCluskey D, Ortega-Prieto AM, Stolarczyk E, Dazzi F, Lucendo-Villarin B, Meseguer-Ripolles J, Williams J, Fanelli G, Hay DC, Watt FM, and Lombardi G

Subjects
Allogeneic Cells cytology, Cell Proliferation, Humans, Immunologic Factors metabolism, Immunophenotyping, Indoleamine-Pyrrole 2,3,-Dioxygenase metabolism, Lymphocyte Activation immunology, Receptors, Antigen, T-Cell metabolism, T-Lymphocytes immunology, Hepatocytes cytology, Induced Pluripotent Stem Cells cytology, T-Lymphocytes cytology, T-Lymphocytes metabolism, Tryptophan deficiency
Abstract

Regenerative medicine aims to replace damaged tissues by stimulating endogenous tissue repair or by transplanting autologous or allogeneic cells. Due to their capacity to produce unlimited numbers of cells of a given cell type, pluripotent stem cells, whether of embryonic origin or induced via the reprogramming of somatic cells, are of considerable therapeutic interest in the regenerative medicine field. However, regardless of the cell type, host immune responses present a barrier to success. The aim of this study was to investigate in vitro the immunological properties of human pluripotent stem cell (PSC)-derived hepatocyte-like cells (HLCs). These cells expressed MHC class I molecules while they lacked MHC class II and co-stimulatory molecules, such as CD80 and CD86. Following stimulation with IFN-γ, HLCs upregulated CD40, PD-L1 and MHC class I molecules. When co-cultured with allogeneic T cells, HLCs did not induce T cell proliferation; furthermore, when T cells were stimulated via αCD3/CD28 beads, HLCs inhibited their proliferation via IDO1 and tryptophan deprivation. These results demonstrate that PSC-derived HLCs possess immunoregulatory functions, at least in vitro .

Published
2021
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22. New Supramolecular Drug Carriers: The Study of Organogel Conjugated Gold Nanoparticles.

Author

Kowalczuk J, Łapiński A, Stolarczyk E, Demchuk OM, Kubiński K, Janeczko M, Martyna A, Masłyk M, and Turczyniak-Surdacka S

Subjects
Alanine chemistry, Alanine pharmacology, Delayed-Action Preparations chemistry, Delayed-Action Preparations pharmacokinetics, Delayed-Action Preparations pharmacology, HeLa Cells, Humans, Alanine analogs & derivatives, Drug Carriers chemistry, Drug Carriers pharmacokinetics, Drug Carriers pharmacology, Gold chemistry, Gold pharmacology, Metal Nanoparticles chemistry, Metal Nanoparticles therapeutic use
Abstract

An aqueous solution of sodium citrate stabilized gold nanoparticles (AuNP) in the presence of N- lauroyl-L-alanine (C 12 ALA) forms a stable gel. The structure of the gel and the distribution profile of AuNP in it were analyzed. Will nanoparticles separated from each other with sodium citrate behave in the same way in solution and trapped in the gel matrix? Will the spatial limitation of solvent molecules aggregate nanoparticles and destroy their homogeneity? These questions are very important from the point of view of the use of gold nanoparticles, trapped in the gel structure as carriers of drugs in the slow-release process. The lack of homogeneity of this distribution will have a major impact on the rate of release of the appropriate amount of therapeutic drug from the matrix. In this work, we attempt to answer these questions. The performed biological assays revealed that both C 12 ALA and C 12 ALA-AuNP show an excellent level of biological neutrality. They might be used as a transporting medium for a drug delivery without affecting the drug's activity.

Published
2021
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23. Supplementation with a prebiotic (polydextrose) in obese mouse pregnancy improves maternal glucose homeostasis and protects against offspring obesity.

Author

Maragkoudaki X, Naylor M, Papacleovoulou G, Stolarczyk E, Rees D, Pombo JM, Abu-Hayyeh S, Czajka A, Howard JK, Malik AN, Williamson C, Poston L, and Taylor PD

Subjects
Animals, Body Composition, Body Weight, Diet, Energy Intake, Energy Metabolism, Female, Gastrointestinal Microbiome, Glucose metabolism, Glucose Tolerance Test, Homeostasis, Male, Mice, Mice, Inbred C57BL, Mice, Obese, Pregnancy, Glucans administration & dosage, Obesity, Maternal complications, Prebiotics administration & dosage, Prenatal Exposure Delayed Effects
Abstract

Objectives: We hypothesised that maternal diet-induced-obesity has adverse consequences for offspring energy expenditure and susceptibility to obesity in adulthood, and that the prebiotic polydextrose (PDX) would prevent the consequences of programming by maternal obesity., Methods: Female mice were fed a control (Con) or obesogenic diet (Ob) for 6 weeks prior to mating and throughout pregnancy and lactation. Half the obese dams were supplemented with 5% PDX (ObPDX) in drinking water throughout pregnancy and lactation. Offspring were weaned onto standard chow. At 3 and 6 months, offspring energy intake (EI) and energy expenditure (EE by indirect calorimetry) were measured, and a glucose-tolerance test performed. Offspring of control (OffCon), obese (OffOb) and PDX supplemented (OffObP) dams were subsequently challenged for 3 weeks with Ob, and energy balanced reassessed. Potential modifiers of offspring energy balance including gut microbiota and biomarkers of mitochondrial activity were also evaluated., Results: Six-month-old male OffOb demonstrated increased bodyweight (BW, P < 0.001) and white adipose tissue mass (P < 0.05), decreased brown adipose tissue mass (BAT, P < 0.01), lower night-time EE (P < 0.001) versus OffCon, which were prevented in OffObP. Both male and female OffOb showed abnormal glucose-tolerance test (peak [Glucose] P < 0.001; AUC, P < 0.05) which was prevented by PDX. The Ob challenge resulted in greater BW gain in both male and female OffOb versus OffCon (P < 0.05), also associated with increased EI (P < 0.05) and reduced EE in females (P < 0.01). OffObP were protected from accelerated BW gain on the OB diet compared with controls, associated with increased night-time EE in both male (P < 0.05) and female OffObP (P < 0.001). PDX also prevented an increase in skeletal muscle mtDNA copy number in OffOb versus OffCon (P < 0.01) and increased the percentage of Bacteroides cells in faecal samples from male OffObP relative to controls., Conclusions: Maternal obesity adversely influences adult offspring energy balance and propensity for obesity, which is ameliorated by maternal PDX treatment with associated changes in gut microbiota composition and skeletal muscle mitochondrial function.

Published
2020
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24. Interleukin-22 orchestrates a pathological endoplasmic reticulum stress response transcriptional programme in colonic epithelial cells.

Author

Powell N, Pantazi E, Pavlidis P, Tsakmaki A, Li K, Yang F, Parker A, Pin C, Cozzetto D, Minns D, Stolarczyk E, Saveljeva S, Mohamed R, Lavender P, Afzali B, Digby-Bell J, Tjir-Li T, Kaser A, Friedman J, MacDonald TT, Bewick GA, and Lord GM

Subjects
Animals, Anti-Bacterial Agents pharmacology, Apoptosis drug effects, Apoptosis genetics, Cell Survival drug effects, Chronic Disease, Colitis blood, Colitis drug therapy, Colitis pathology, Colon pathology, Crohn Disease pathology, Disease Models, Animal, Endoplasmic Reticulum Stress drug effects, Gastrointestinal Agents pharmacology, Gastrointestinal Agents therapeutic use, Humans, Interleukin-17 pharmacology, Interleukin-23 antagonists & inhibitors, Interleukins blood, Interleukins genetics, Intestinal Mucosa pathology, Mice, Organoids, Patient Acuity, Phenylbutyrates pharmacology, Recombinant Proteins pharmacology, Tunicamycin pharmacology, Unfolded Protein Response, Ustekinumab pharmacology, Ustekinumab therapeutic use, Interleukin-22, Colitis genetics, Crohn Disease physiopathology, Endoplasmic Reticulum Stress genetics, Epithelial Cells physiology, Interleukins pharmacology, Transcription, Genetic drug effects
Abstract

Objective: The functional role of interleukin-22 (IL22) in chronic inflammation is controversial, and mechanistic insights into how it regulates target tissue are lacking. In this study, we evaluated the functional role of IL22 in chronic colitis and probed mechanisms of IL22-mediated regulation of colonic epithelial cells., Design: To investigate the functional role of IL22 in chronic colitis and how it regulates colonic epithelial cells, we employed a three-dimentional mini-gut epithelial organoid system, in vivo disease models and transcriptomic datasets in human IBD., Results: As well as inducing transcriptional modules implicated in antimicrobial responses, IL22 also coordinated an endoplasmic reticulum (ER) stress response transcriptional programme in colonic epithelial cells. In the colon of patients with active colonic Crohn's disease (CD), there was enrichment of IL22-responsive transcriptional modules and ER stress response modules. Strikingly, in an IL22-dependent model of chronic colitis, targeting IL22 alleviated colonic epithelial ER stress and attenuated colitis. Pharmacological modulation of the ER stress response similarly impacted the severity of colitis. In patients with colonic CD, antibody blockade of IL12p40, which simultaneously blocks IL12 and IL23, the key upstream regulator of IL22 production, alleviated the colonic epithelial ER stress response., Conclusions: Our data challenge perceptions of IL22 as a predominantly beneficial cytokine in IBD and provide novel insights into the molecular mechanisms of IL22-mediated pathogenicity in chronic colitis. Targeting IL22-regulated pathways and alleviating colonic epithelial ER stress may represent promising therapeutic strategies in patients with colitis., Trial Registration Number: NCT02749630., Competing Interests: Competing interests: None declared., (© Author(s) (or their employer(s)) 2020. Re-use permitted under CC BY. Published by BMJ.)

Published
2020
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25. Adipose tissue inflammation in obesity: a metabolic or immune response?

Author

Stolarczyk E

Subjects
Animals, Humans, Inflammation immunology, Inflammation metabolism, Adipose Tissue immunology, Adipose Tissue metabolism, Obesity immunology, Obesity metabolism
Abstract

Adipose tissue is not only a reservoir for energy, but also an immune organ. In the context of obesity, the development of insulin resistance is now recognised to be initiated by inflammation of the adipose tissue. However, the primary events triggering this inflammation are still unclear, as a complex combination of endocrine and immune factors act to regulate this adipose tissue microenvironment. Below we discuss the different factors involved and how they affect the biology of the adipose tissue in obesity., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published
2017
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26. Fermentable carbohydrate stimulates FFAR2-dependent colonic PYY cell expansion to increase satiety.

Author

Brooks L, Viardot A, Tsakmaki A, Stolarczyk E, Howard JK, Cani PD, Everard A, Sleeth ML, Psichas A, Anastasovskaj J, Bell JD, Bell-Anderson K, Mackay CR, Ghatei MA, Bloom SR, Frost G, and Bewick GA

Subjects
Animals, Body Weight, Colon cytology, Dietary Supplements, Eating, Fatty Acids, Volatile metabolism, Fermentation, Fermented Foods, Gastrointestinal Hormones metabolism, Gastrointestinal Microbiome physiology, Glucagon-Like Peptide 1 metabolism, Inulin metabolism, Male, Mice, Mice, Knockout, Obesity metabolism, Receptors, Cell Surface physiology, Weight Gain, Dietary Carbohydrates metabolism, Peptide YY metabolism, Receptors, Cell Surface metabolism
Abstract

Objective: Dietary supplementation with fermentable carbohydrate protects against body weight gain. Fermentation by the resident gut microbiota produces short-chain fatty acids, which act at free fatty acid receptor 2 (FFAR2). Our aim was to test the hypothesis that FFAR2 is important in regulating the beneficial effects of fermentable carbohydrate on body weight and to understand the role of gut hormones PYY and GLP-1., Methods: Wild-type or Ffar2 -/- mice were fed an inulin supplemented or control diet. Mice were metabolically characterized and gut hormone concentrations, enteroendocrine cell density measurements were carried out. Intestinal organoids and colonic cultures were utilized to substantiate the in vivo findings., Results: We provide new mechanistic insight into how fermentable carbohydrate regulates metabolism. Using mice that lack FFAR2, we demonstrate that the fermentable carbohydrate inulin acts via this receptor to drive an 87% increase in the density of cells that produce the appetite-suppressing hormone peptide YY (PYY), reduce food intake, and prevent diet-induced obesity., Conclusion: Our results demonstrate that FFAR2 is predominantly involved in regulating the effects of fermentable carbohydrate on metabolism and does so, in part, by enhancing PYY cell density and release. This highlights the potential for targeting enteroendocrine cell differentiation to treat obesity.

Published
2016
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27. Developing in vitro expanded CD45RA+ regulatory T cells as an adoptive cell therapy for Crohn's disease.

Author

Canavan JB, Scottà C, Vossenkämper A, Goldberg R, Elder MJ, Shoval I, Marks E, Stolarczyk E, Lo JW, Powell N, Fazekasova H, Irving PM, Sanderson JD, Howard JK, Yagel S, Afzali B, MacDonald TT, Hernandez-Fuentes MP, Shpigel NY, Lombardi G, and Lord GM

Subjects
Animals, Crohn Disease immunology, DNA Methylation, Enzyme-Linked Immunosorbent Assay, Forkhead Transcription Factors genetics, Humans, In Vitro Techniques, Interleukin-17 metabolism, Leukocyte Common Antigens immunology, Mice, Mice, SCID, Phenotype, Polymerase Chain Reaction, Transplantation, Heterologous, Adoptive Transfer, Cell- and Tissue-Based Therapy methods, Crohn Disease therapy, T-Lymphocytes, Regulatory immunology
Abstract

Background and Aim: Thymus-derived regulatory T cells (Tregs) mediate dominant peripheral tolerance and treat experimental colitis. Tregs can be expanded from patient blood and were safely used in recent phase 1 studies in graft versus host disease and type 1 diabetes. Treg cell therapy is also conceptually attractive for Crohn's disease (CD). However, barriers exist to this approach. The stability of Tregs expanded from Crohn's blood is unknown. The potential for adoptively transferred Tregs to express interleukin-17 and exacerbate Crohn's lesions is of concern. Mucosal T cells are resistant to Treg-mediated suppression in active CD. The capacity for expanded Tregs to home to gut and lymphoid tissue is unknown., Methods: To define the optimum population for Treg cell therapy in CD, CD4(+)CD25(+)CD127(lo)CD45RA(+) and CD4(+)CD25(+)CD127(lo)CD45RA(-) Treg subsets were isolated from patients' blood and expanded in vitro using a workflow that can be readily transferred to a good manufacturing practice background., Results: Tregs can be expanded from the blood of patients with CD to potential target dose within 22-24 days. Expanded CD45RA(+) Tregs have an epigenetically stable FOXP3 locus and do not convert to a Th17 phenotype in vitro, in contrast to CD45RA(-) Tregs. CD45RA(+) Tregs highly express α4β7 integrin, CD62L and CC motif receptor 7 (CCR7). CD45RA(+) Tregs also home to human small bowel in a C.B-17 severe combined immune deficiency (SCID) xenotransplant model. Importantly, in vitro expansion enhances the suppressive ability of CD45RA(+) Tregs. These cells also suppress activation of lamina propria and mesenteric lymph node lymphocytes isolated from inflamed Crohn's mucosa., Conclusions: CD4(+)CD25(+)CD127(lo)CD45RA(+) Tregs may be the most appropriate population from which to expand Tregs for autologous Treg therapy for CD, paving the way for future clinical trials., (Published by the BMJ Publishing Group Limited. For permission to use (where not already granted under a licence) please go to http://www.bmj.com/company/products-services/rights-and-licensing/)

Published
2016
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28. Cutting Edge: Retinoic Acid Signaling in B Cells Is Essential for Oral Immunization and Microflora Composition.

Author

Pantazi E, Marks E, Stolarczyk E, Lycke N, Noelle RJ, and Elgueta R

Subjects
Animals, B-Lymphocytes cytology, Cell Differentiation immunology, Gastrointestinal Tract immunology, Gastrointestinal Tract microbiology, Gene Expression, Immunoglobulin A biosynthesis, Immunoglobulin A immunology, Mice, Mice, Transgenic, Microbiota immunology, Plasma Cells cytology, Plasma Cells immunology, Plasma Cells metabolism, Receptors, Retinoic Acid genetics, Receptors, Retinoic Acid metabolism, B-Lymphocytes immunology, B-Lymphocytes metabolism, Immunization, Signal Transduction, Tretinoin metabolism
Abstract

Retinoic acid (RA) is a critical regulator of the intestinal adaptive immune response. However, the intrinsic impact of RA on B cell differentiation in the regulation of gut humoral immunity in vivo has never been directly shown. To address this issue, we have been able to generate a mouse model where B cells specifically express a dominant-negative receptor α for RA. In this study, we show that the silencing of RA signaling in B cells reduces the numbers of IgA(+) Ab-secreting cells both in vitro and in vivo, suggesting that RA has a direct effect on IgA plasma cell differentiation. Moreover, the lack of RA signaling in B cells abrogates Ag-specific IgA responses after oral immunization and affects the microbiota composition. In conclusion, these results suggest that RA signaling in B cells through the RA receptor α is important to generate an effective gut humoral response and to maintain a normal microbiota composition., (Copyright © 2015 by The American Association of Immunologists, Inc.)

Published
2015
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29. Interleukin 6 Increases Production of Cytokines by Colonic Innate Lymphoid Cells in Mice and Patients With Chronic Intestinal Inflammation.

Author

Powell N, Lo JW, Biancheri P, Vossenkämper A, Pantazi E, Walker AW, Stolarczyk E, Ammoscato F, Goldberg R, Scott P, Canavan JB, Perucha E, Garrido-Mesa N, Irving PM, Sanderson JD, Hayee B, Howard JK, Parkhill J, MacDonald TT, and Lord GM

Subjects
Animals, CD3 Complex metabolism, Cell Culture Techniques, Colon cytology, Colon immunology, Disease Models, Animal, Enzyme-Linked Immunosorbent Assay, Flow Cytometry, Humans, Inflammatory Bowel Diseases drug therapy, Interferon-gamma metabolism, Interleukin-17 metabolism, Interleukin-1alpha metabolism, Interleukin-23 metabolism, Interleukin-6 administration & dosage, Interleukins metabolism, Lymphocytes immunology, Mice, Mice, Knockout, Receptors, Natural Cytotoxicity Triggering metabolism, Interleukin-22, CD4 Antigens metabolism, Cytokines metabolism, Immunity, Innate drug effects, Inflammatory Bowel Diseases immunology, Interleukin-6 pharmacology, Lymphocytes drug effects
Abstract

Background & Aims: Innate lymphoid cells (ILCs) are a heterogeneous group of mucosal inflammatory cells that participate in chronic intestinal inflammation. We investigated the role of interleukin 6 (IL6) in inducing activation of ILCs in mice and in human beings with chronic intestinal inflammation., Methods: ILCs were isolated from colons of Tbx21(-/-) × Rag2(-/-) mice (TRUC), which develop colitis; patients with inflammatory bowel disease (IBD); and patients without colon inflammation (controls). ILCs were characterized by flow cytometry; cytokine production was measured by enzyme-linked immunosorbent assay and cytokine bead arrays. Mice were given intraperitoneal injections of depleting (CD4, CD90), neutralizing (IL6), or control antibodies. Isolated colon tissues were analyzed by histology, explant organ culture, and cell culture. Bacterial DNA was extracted from mouse fecal samples to assess the intestinal microbiota., Results: IL17A- and IL22-producing, natural cytotoxicity receptor-negative, ILC3 were the major subset of ILCs detected in colons of TRUC mice. Combinations of IL23 and IL1α induced production of cytokines by these cells, which increased further after administration of IL6. Antibodies against IL6 reduced colitis in TRUC mice without significantly affecting the structure of their intestinal microbiota. Addition of IL6 increased production of IL17A, IL22, and interferon-γ by human intestinal CD3-negative, IL7-receptor-positive cells, in a dose-dependent manner., Conclusions: IL6 contributes to activation of colonic natural cytotoxicity receptor-negative, CD4-negative, ILC3s in mice with chronic intestinal inflammation (TRUC mice) by increasing IL23- and IL1α-induced production of IL17A and IL22. This pathway might be targeted to treat patients with IBD because IL6, which is highly produced in colonic tissue by some IBD patients, also increased the production of IL17A, IL22, and interferon-γ by cultured human colon CD3-negative, IL7-receptor-positive cells., (Copyright © 2015 AGA Institute. Published by Elsevier Inc. All rights reserved.)

Published
2015
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30. Transitional-2 B cells acquire regulatory function during tolerance induction and contribute to allograft survival.

Author

Moreau A, Blair PA, Chai JG, Ratnasothy K, Stolarczyk E, Alhabbab R, Rackham CL, Jones PM, Smyth L, Elgueta R, Howard JK, Lechler RI, and Lombardi G

Subjects
Allografts, Animals, Graft Survival genetics, Interleukin-10 genetics, Interleukin-10 immunology, Mice, Mice, Knockout, Graft Survival immunology, Lymphocyte Activation, Precursor Cells, B-Lymphoid immunology, Skin Transplantation, T-Lymphocytes, Regulatory immunology, Transplantation Tolerance
Abstract

In humans, tolerance to renal transplants has been associated with alterations in B-cell gene transcription and maintenance of the numbers of circulating transitional B cells. Here, we use a mouse model of transplantation tolerance to investigate the contribution of B cells to allograft survival. We demonstrate that transfer of B cells from mice rendered tolerant to MHC class I mismatched skin grafts can prolong graft survival in a dose-dependent and antigen-specific manner to a degree similar to that afforded by graft-specific regulatory T (Treg) cells. Tolerance in this model was associated with an increase in transitional-2 (T2) B cells. Only T2 B cells from tolerized mice, not naïve T2 nor alloantigen experienced T2, were capable of prolonging skin allograft survival, and suppressing T-cell activation. Tolerized T2 B cells expressed lower levels of CD86, increased TIM-1, and demonstrated a preferential survival in vivo. Furthermore, we demonstrate a synergistic effect between tolerized B cells and graft-specific Treg cells. IL-10 production by T2 B cells did not contribute to tolerance, as shown by transfer of B cells from IL-10(-/-) mice. These results suggest that T2 B cells in tolerant patients may include a population of regulatory B cells that directly inhibit graft rejection., (© 2014 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published
2015
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31. The immune cell transcription factor T-bet: A novel metabolic regulator.

Author

Stolarczyk E, Lord GM, and Howard JK

Abstract

Obesity-associated insulin resistance is accompanied by an alteration in the Th1/Th2 balance in adipose tissue. T-bet (Tbx21) is an immune cell transcription factor originally described as the master regulator of Th1 cell development, although is now recognized to have a role in both the adaptive and innate immune systems. T-bet also directs T-cell homing to pro-inflammatory sites by the regulation of CXCR3 expression. T-bet(-/-) mice have increased visceral adiposity but are more insulin-sensitive, exhibiting reduced immune cell content and cytokine secretion specifically in the visceral fat depot, perhaps due to altered T-cell trafficking. Studies of T-bet deficiency on Rag2-- and IFN-γ-deficient backgrounds indicate the importance of CD4(+) T cells and IFN-γ in this model. This favorable metabolic phenotype, uncoupling adiposity from insulin resistance, is present in young lean mice yet persists with age and increasing obesity. We suggest a novel role for T-bet in metabolic regulation.

Published
2014
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32. LXR activation by GW3965 alters fat tissue distribution and adipose tissue inflammation in ob/ob female mice.

Author

Archer A, Stolarczyk E, Doria ML, Helguero L, Domingues R, Howard JK, Mode A, Korach-André M, and Gustafsson JÅ

Subjects
Adipogenesis, Animals, Body Fat Distribution, Female, Inflammation metabolism, Inflammation pathology, Lipolysis, Liver X Receptors, Macrophages drug effects, Macrophages metabolism, Mice, Obesity genetics, Obesity pathology, Orphan Nuclear Receptors agonists, Orphan Nuclear Receptors genetics, Adipose Tissue metabolism, Benzoates administration & dosage, Benzylamines administration & dosage, Obesity metabolism, Orphan Nuclear Receptors metabolism
Abstract

To investigate the role of liver X receptor (LXR) in adipose tissue metabolism during obesity, ob/ob mice were treated for 5 weeks with the synthetic LXR agonist GW3965. MRI analysis revealed that pharmacological activation of LXR modified fat distribution by decreasing visceral (VS) fat and inversely increasing subcutaneous (SC) fat storage without affecting whole body fat content. This was concordant with opposite regulation by GW3965 of the lipolytic markers hormone-sensitive lipase (HSL) and adipose triglyceride lipase (ATGL) in the two fat depots; moreover, the expression of genes involved in lipogenesis was significantly induced in SC fat. Lipidomic analysis suggested that changes in lipid composition in response to GW3965 also varied between VS and SC fat. In both depots, the observed alteration in lipid composition indicated an overall change toward less lipotoxic lipids. Flow cytometry analysis showed decreased immune cell infiltration in adipose tissue of ob/ob mice in response to GW3965 treatment, which in VS fat mainly affected the macrophage population and in SC fat the lymphocyte population. In line with this, the expression and secretion of proinflammatory markers was decreased in both fat deposits with GW3965 treatment.

Published
2013
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33. Improved insulin sensitivity despite increased visceral adiposity in mice deficient for the immune cell transcription factor T-bet.

Author

Stolarczyk E, Vong CT, Perucha E, Jackson I, Cawthorne MA, Wargent ET, Powell N, Canavan JB, Lord GM, and Howard JK

Subjects
Adipose Tissue immunology, Adipose Tissue metabolism, Animals, CD4-Positive T-Lymphocytes immunology, CD4-Positive T-Lymphocytes metabolism, Cytokines metabolism, DNA-Binding Proteins deficiency, DNA-Binding Proteins genetics, DNA-Binding Proteins metabolism, Diet, High-Fat, Energy Metabolism, Immune System metabolism, In Vitro Techniques, Interferon-gamma deficiency, Interferon-gamma genetics, Interferon-gamma metabolism, Male, Mice, Mice, Inbred BALB C, Mice, Knockout, Obesity metabolism, Obesity pathology, Phenotype, T-Box Domain Proteins deficiency, T-Box Domain Proteins genetics, Insulin Resistance, Intra-Abdominal Fat metabolism, T-Box Domain Proteins metabolism
Abstract

Low-grade inflammation in fat is associated with insulin resistance, although the mechanisms are unclear. We report that mice deficient in the immune cell transcription factor T-bet have lower energy expenditure and increased visceral fat compared with wild-type mice, yet paradoxically are more insulin sensitive. This striking phenotype, present in young T-bet(-/-) mice, persisted with high-fat diet and increasing host age and was associated with altered immune cell numbers and cytokine secretion specifically in visceral adipose tissue. However, the favorable metabolic phenotype observed in T-bet-deficient hosts was lost in T-bet(-/-) mice also lacking adaptive immunity (T-bet(-/-)xRag2(-/-)), demonstrating that T-bet expression in the adaptive rather than the innate immune system impacts host glucose homeostasis. Indeed, adoptive transfer of T-bet-deficient, but not wild-type, CD4(+) T cells to Rag2(-/-) mice improved insulin sensitivity. Our results reveal a role for T-bet in metabolic physiology and obesity-associated insulin resistance., (Copyright © 2013 Elsevier Inc. All rights reserved.)

Published
2013
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34. The transcription factor T-bet regulates intestinal inflammation mediated by interleukin-7 receptor+ innate lymphoid cells.

Author

Powell N, Walker AW, Stolarczyk E, Canavan JB, Gökmen MR, Marks E, Jackson I, Hashim A, Curtis MA, Jenner RG, Howard JK, Parkhill J, MacDonald TT, and Lord GM

Subjects
Animals, Cells, Cultured, Chronic Disease, Colitis, Ulcerative microbiology, Colitis, Ulcerative pathology, DNA-Binding Proteins deficiency, Helicobacter immunology, Mice, Mice, Inbred BALB C, Mice, Knockout, Signal Transduction, T-Box Domain Proteins deficiency, Colitis, Ulcerative immunology, DNA-Binding Proteins immunology, Immunity, Innate, Lymphocytes immunology, Receptors, Interleukin-7 immunology, T-Box Domain Proteins immunology
Abstract

Mice lacking the transcription factor T-bet in the innate immune system develop microbiota-dependent colitis. Here, we show that interleukin-17A (IL-17A)-producing IL-7Rα(+) innate lymphoid cells (ILCs) were potent promoters of disease in Tbx21(-/-)Rag2(-/-) ulcerative colitis (TRUC) mice. TNF-α produced by CD103(-)CD11b(+) dendritic cells synergized with IL-23 to drive IL-17A production by ILCs, demonstrating a previously unrecognized layer of cellular crosstalk between dendritic cells and ILCs. We have identified Helicobacter typhlonius as a key disease trigger driving excess TNF-α production and promoting colitis in TRUC mice. Crucially, T-bet also suppressed the expression of IL-7R, a key molecule involved in controlling intestinal ILC homeostasis. The importance of IL-7R signaling in TRUC disease was highlighted by the dramatic reduction in intestinal ILCs and attenuated colitis following IL-7R blockade. Taken together, these data demonstrate the mechanism by which T-bet regulates the complex interplay between mucosal dendritic cells, ILCs, and the intestinal microbiota., (Copyright © 2012 Elsevier Inc. All rights reserved.)

Published
2012
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35. Detection of extracellular glucose by GLUT2 contributes to hypothalamic control of food intake.

Author

Stolarczyk E, Guissard C, Michau A, Even PC, Grosfeld A, Serradas P, Lorsignol A, Pénicaud L, Brot-Laroche E, Leturque A, and Le Gall M

Subjects
Analysis of Variance, Animals, Biological Transport physiology, Body Weight physiology, Cell Count, Energy Metabolism, Feeding Behavior physiology, Ghrelin blood, Glucose Transporter Type 2 genetics, Homeostasis physiology, Immunohistochemistry, Insulin blood, Intracellular Signaling Peptides and Proteins genetics, Intracellular Signaling Peptides and Proteins metabolism, Leptin blood, Mice, Mice, Transgenic, Neuropeptides genetics, Neuropeptides metabolism, Orexins, Proto-Oncogene Proteins c-fos metabolism, RNA, Messenger genetics, RNA, Messenger metabolism, Reverse Transcriptase Polymerase Chain Reaction, Signal Transduction physiology, Statistics, Nonparametric, Thyrotropin-Releasing Hormone genetics, Thyrotropin-Releasing Hormone metabolism, Eating physiology, Glucose metabolism, Glucose Transporter Type 2 metabolism, Hypothalamus metabolism
Abstract

The sugar transporter GLUT2, present in several tissues of the gut-brain axis, has been reported to be involved in the control of food intake. GLUT2 is a sugar transporter sustaining energy production in the cell, but it can also function as a receptor for extracellular glucose. A glucose-signaling pathway is indeed triggered, independently of glucose metabolism, through its large cytoplasmic loop domain. However, the contribution of the receptor function over the transporter function of GLUT2 in the control of food intake remains to be determined. Thus, we generated transgenic mice that express a GLUT2-loop domain, blocking the detection of glucose but leaving GLUT2-dependent glucose transport unaffected. Inhibiting GLUT2-mediated glucose detection augmented daily food intake by a mechanism that increased the meal size but not the number of meals. Peripheral hormones (ghrelin, insulin, leptin) were unaffected, leading to a focus on central aspects of feeding behavior. We found defects in c-Fos activation by glucose in the arcuate nucleus and changes in the amounts of TRH and orexin neuropeptide mRNA, which are relevant to poorly controlled meal size. Our data provide evidence that glucose detection by GLUT2 contributes to the control of food intake by the hypothalamus. The sugar transporter receptor, i.e., "transceptor" GLUT2, may constitute a drug target to treat eating disorders and associated metabolic diseases, particularly by modulating its receptor function without affecting vital sugar provision by its transporter function.

Published
2010
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36. Insulin internalizes GLUT2 in the enterocytes of healthy but not insulin-resistant mice.

Author

Tobin V, Le Gall M, Fioramonti X, Stolarczyk E, Blazquez AG, Klein C, Prigent M, Serradas P, Cuif MH, Magnan C, Leturque A, and Brot-Laroche E

Subjects
Animals, Caco-2 Cells, Carbohydrate Metabolism, Cell Membrane drug effects, Cell Membrane metabolism, Enterocytes ultrastructure, Gene Expression Regulation, Glucose Clamp Technique, Humans, Mice, Microvilli metabolism, Protein Transport drug effects, Protein Transport physiology, Enterocytes drug effects, Enterocytes metabolism, Glucose Transporter Type 2 metabolism, Insulin pharmacology, Insulin Resistance physiology
Abstract

Objectives: A physiological adaptation to a sugar-rich meal is achieved by increased sugar uptake to match dietary load, resulting from a rapid transient translocation of the fructose/glucose GLUT2 transporter to the brush border membrane (BBM) of enterocytes. The aim of this study was to define the contributors and physiological mechanisms controlling intestinal sugar absorption, focusing on the action of insulin and the contribution of GLUT2-mediated transport., Research Design and Methods: The studies were performed in the human enterocytic colon carcinoma TC7 subclone (Caco-2/TC7) cells and in vivo during hyperinsulinemic-euglycemic clamp experiments in conscious mice. Chronic high-fructose or high-fat diets were used to induce glucose intolerance and insulin resistance in mice., Results and Conclusions: In Caco-2/TC7 cells, insulin action diminished the transepithelial transfer of sugar and reduced BBM and basolateral membrane (BLM) GLUT2 levels, demonstrating that insulin can target sugar absorption by controlling the membrane localization of GLUT2 in enterocytes. Similarly, in hyperinsulinemic-euglycemic clamp experiments in sensitive mice, insulin abolished GLUT2 (i.e., the cytochalasin B-sensitive component of fructose absorption), decreased BBM GLUT2, and concomitantly increased intracellular GLUT2. Acute insulin treatment before sugar intake prevented the insertion of GLUT2 into the BBM. Insulin resistance in mice provoked a loss of GLUT2 trafficking, and GLUT2 levels remained permanently high in the BBM and low in the BLM. We propose that, in addition to its peripheral effects, insulin inhibits intestinal sugar absorption to prevent excessive blood glucose excursion after a sugar meal. This protective mechanism is lost in the insulin-resistant state induced by high-fat or high-fructose feeding.

Published
2008
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37. Characterisation of glutamine fructose-6-phosphate amidotransferase (EC 2.6.1.16) and N-acetylglucosamine metabolism in Bifidobacterium.

Author

Foley S, Stolarczyk E, Mouni F, Brassart C, Vidal O, Aïssi E, Bouquelet S, and Krzewinski F

Subjects
Amino Acid Sequence, Bacterial Proteins chemistry, Bacterial Proteins genetics, Bacterial Proteins isolation & purification, Bifidobacterium genetics, Catalytic Domain, Cloning, Molecular, Conserved Sequence, Enzyme Stability, Escherichia coli genetics, Fructosephosphates metabolism, Gene Expression, Glucosamine analogs & derivatives, Glucosamine metabolism, Glucose-6-Phosphate analogs & derivatives, Glucose-6-Phosphate metabolism, Glutamic Acid metabolism, Glutaminase metabolism, Glutamine metabolism, Hydrogen-Ion Concentration, Metabolic Networks and Pathways, Models, Biological, Molecular Sequence Data, Sequence Analysis, DNA, Sequence Homology, Amino Acid, Temperature, Acetylglucosamine metabolism, Bacterial Proteins metabolism, Bifidobacterium enzymology, Bifidobacterium metabolism
Abstract

Bifidobacterium bifidum, in contrast to other bifidobacterial species, is auxotrophic for N-acetylglucosamine. Growth experiments revealed assimilation of radiolabelled N-acetylglucosamine in bacterial cell walls and in acetate, an end-product of central metabolism via the bifidobacterial D: -fructose-6-phosphate shunt. While supplementation with fructose led to reduced N-acetylglucosamine assimilation via the D: -fructose-6-phosphate shunt, no significant difference was observed in levels of radiolabelled N-acetylglucosamine incorporated into cell walls. Considering the central role played by glutamine fructose-6-phosphate transaminase (GlmS) in linking the biosynthetic pathway for N-acetylglucosamine to hexose metabolism, the GlmS of Bifidobacterium was characterized. The genes encoding the putative GlmS of B. longum DSM20219 and B. bifidum DSM20082 were cloned and sequenced. Bioinformatic analyses of the predicted proteins revealed 43% amino acid identity with the Escherichia coli GlmS, with conservation of key amino acids in the catalytic domain. The B. longum GlmS was over-produced as a histidine-tagged fusion protein. The purified C-terminal His-tagged GlmS possessed glutamine fructose-6-phosphate amidotransferase activity as demonstrated by synthesis of glucosamine-6-phosphate from fructose-6-phosphate and glutamine. It also possesses an independent glutaminase activity, converting glutamine to glutamate in the absence of fructose-6-phosphate. This is of interest considering the apparently reduced coding potential in bifidobacteria for enzymes associated with glutamine metabolism.

Published
2008
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38. Loss of sugar detection by GLUT2 affects glucose homeostasis in mice.

Author

Stolarczyk E, Le Gall M, Even P, Houllier A, Serradas P, Brot-Laroche E, and Leturque A

Subjects
Animals, Glucose Tolerance Test, Glucose Transporter Type 2 genetics, Lipid Metabolism, Mice, Mice, Transgenic, Oxidation-Reduction, Pancreas physiology, Glucose metabolism, Glucose Transporter Type 2 metabolism, Homeostasis
Abstract

Background: Mammals must sense the amount of sugar available to them and respond appropriately. For many years attention has focused on intracellular glucose sensing derived from glucose metabolism. Here, we studied the detection of extracellular glucose concentrations in vivo by invalidating the transduction pathway downstream from the transporter-detector GLUT2 and measured the physiological impact of this pathway., Methodology/principal Findings: We produced mice that ubiquitously express the largest cytoplasmic loop of GLUT2, blocking glucose-mediated gene expression in vitro without affecting glucose metabolism. Impairment of GLUT2-mediated sugar detection transiently protected transgenic mice against starvation and streptozotocin-induced diabetes, suggesting that both low- and high-glucose concentrations were not detected. Transgenic mice favored lipid oxidation, and oral glucose was slowly cleared from blood due to low insulin production, despite massive urinary glucose excretion. Kidney adaptation was characterized by a lower rate of glucose reabsorption, whereas pancreatic adaptation was associated with a larger number of small islets., Conclusions/significance: Molecular invalidation of sugar sensing in GLUT2-loop transgenic mice changed multiple aspects of glucose homeostasis, highlighting by a top-down approach, the role of membrane glucose receptors as potential therapeutic targets.

Published
2007
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39. Sugar sensing by enterocytes combines polarity, membrane bound detectors and sugar metabolism.

Author

Le Gall M, Tobin V, Stolarczyk E, Dalet V, Leturque A, and Brot-Laroche E

Subjects
Animals, Caco-2 Cells, Cloning, Molecular, Fructose metabolism, Glucose metabolism, Glucose Transporter Type 2 chemistry, Glucose Transporter Type 2 genetics, Glucose Transporter Type 2 metabolism, Glucose Transporter Type 5 genetics, Glucose Transporter Type 5 metabolism, Green Fluorescent Proteins metabolism, Humans, Jejunum cytology, Mice, Mice, Inbred C57BL, Mice, Knockout, Monosaccharide Transport Proteins genetics, Oligo-1,6-Glucosidase genetics, Promoter Regions, Genetic, Protein Structure, Tertiary, RNA, Messenger metabolism, Sodium-Glucose Transporter 1 genetics, Sodium-Glucose Transporter 1 metabolism, Sucrase genetics, Transfection, Cell Polarity, Enterocytes metabolism, Hexoses metabolism, Monosaccharide Transport Proteins metabolism, Sucrose metabolism, Sweetening Agents metabolism
Abstract

Sugar consumption and subsequent sugar metabolism are known to regulate the expression of genes involved in intestinal sugar absorption and delivery. Here we investigate the hypothesis that sugar-sensing detectors in membranes facing the intestinal lumen or the bloodstream can also modulate intestinal sugar absorption. We used wild-type and GLUT2-null mice, to show that dietary sugars stimulate the expression of sucrase-isomaltase (SI) and L-pyruvate kinase (L-PK) by GLUT2-dependent mechanisms, whereas the expression of GLUT5 and SGLT1, did not rely on the presence of GLUT2. By providing sugar metabolites, sugar transporters, including GLUT2, fuelled a sensing pathway. In Caco2/TC7 enterocytes, we could disconnect the sensing triggered by detector from that produced by metabolism, and found that GLUT2 generated a metabolism-independent pathway to stimulate the expression of SI and L-PK. In cultured enterocytes, both apical and basolateral fructose could increase the expression of GLUT5, conversely, basolateral sugar administration could stimulate the expression of GLUT2. Finally, we located the sweet-taste receptors T1R3 and T1R2 in plasma membranes, and we measured their cognate G alpha Gustducin mRNA levels. Furthermore, we showed that a T1R3 inhibitor altered the fructose-induced expression of SGLT1, GLUT5, and L-PK. Intestinal gene expression is thus controlled by a combination of at least three sugar-signaling pathways triggered by sugar metabolites and membrane sugar receptors that, according to membrane location, determine sugar-sensing polarity. This provides a rationale for how intestine adapts sugar delivery to blood and dietary sugar provision., (2007 Wiley-Liss, Inc.)

Published
2007
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40. Retention of anions on silica-based metalloporphyrin stationary phases.

Author

Biesaga M, Stolarczyk E, Pyrzyńska K, and Trojanowicz M

Abstract

The silica-based Fe(III)-protoporphyrin and Zn-tetraphenylporphyrin stationary phases were examined for the HPLC separation of anions. The retention of nine common inorganic anions as well as benzoate anion (BA) and its hydroxy analogues (HBA) was examined using tartrate, acetate, and succinate eluents. The retention factors of inorganic anions on the FeProP stationary phase were in the order Cl- < NO3- < ClO4- < I- < SCN- and for organic anions benzoate < p-hydroxybenzoate < m-hydoxybenzoate < o-hydroxybenzoate. The retention factors of organic anions examined for a ZnTPP column were in the order p-HBA < m-HBA < BA < o-HBA.

Published
2002
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41. Direct electrochemical measurement of nitric oxide in vascular endothelium.

Author

Brovkovych V, Stolarczyk E, Oman J, Tomboulian P, and Malinski T

Subjects
Animals, Aorta, Thoracic physiology, Biosensing Techniques, Electrochemistry, Endothelium, Vascular drug effects, Endothelium, Vascular enzymology, Enzyme Inhibitors pharmacology, Femoral Artery physiology, Kinetics, Lung chemistry, Male, Microelectrodes, Myocardium chemistry, Myocardium cytology, Nitric Oxide biosynthesis, Nitric Oxide blood, Nitric Oxide Synthase antagonists & inhibitors, Nitric Oxide Synthase metabolism, Nitric Oxide Synthase Type II, Nitric Oxide Synthase Type III, Rabbits, Rats, Rats, Inbred WKY, Superoxides chemistry, omega-N-Methylarginine pharmacology, Endothelium, Vascular chemistry, Nitric Oxide analysis
Abstract

The endothelium plays a critical role in maintaining vascular tone by releasing vasoconstrictor and vasodilator substances. Endothelium-derived nitric oxide (NO) is a vasodilator rapidly inactivated by superoxide and by Fe(II) and Fe(III), all found in significant quantities in biological systems. Thus due to the short life of NO in tissue (t1/2 = 3-6 s), in situ quantification of NO is a challenging problem. We designed the present study to perform direct measurements of nitric oxide using the electrochemical porphyrinic sensor. The most significant advantages of this sensor is small size (0.5-8 microm), rapid response time (0.1-1 ms), and low detection limit (10(-9) mol l(-1)). The porphyrinic sensor was used for in vitro and in vivo measurements of NO in an isolated single cell or tissue. Effects of hypertension, endotoxemia, and ischemia/reperfusion on the release of NO and/or its interaction with superoxide (O2-) were delineated. In the single endothelial cell (rabbit endocardium), NO concentration was highest at the cell membrane (950 +/- 50 nmol l(-1)), decreasing exponentially with distance from cell, and becoming undetectable at distances beyond 50 microm. The endothelium of spontaneously hypertensive rats (SHR) released 35% less NO (580 +/- 30 nmol l(-1)) than that of normotensive rats (920 +/- 50 nmol l(-1)), due to the higher production of O2- in SHR rats. Endothelial NO synthase (eNOS) generated NO (140 +/- 20 nmol l(-1)) in lung during the acute phase (first 10-15 min) of endotoxemia, followed by production of NO by inducible NOS. High production of O2- was observed during the entire period of endotoxemia. Ischemia (lower limb of rabbit) caused a significant increase of NO peaking at 15 min and decreasing thereafter, also due to O2- production.

Published
1999
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