Your search keyword '"Perino, Alessia"' showing total 82 results

51. SIRT2 deficiency modulates macrophage polarization and susceptibility to experimental colitis

Author

Lo Sasso Giuseppe, Menzies Keir Joe, Mottis Adrienne, Piersigilli Alessandra, Perino Alessia, Yamamoto Hiroyasu, Schoonjans Kristina, and Auwerx Johan

Subjects

Antigens, Differentiation, T-Lymphocyte, CD4-Positive T-Lymphocytes, Male, lcsh:Medicine, Severity of Illness Index, Inflammatory bowel disease, Mice, Sirtuin 2, 0302 clinical medicine, Medicine and Health Sciences, lcsh:Science, Cells, Cultured, Mice, Knockout, 0303 health sciences, Multidisciplinary, 630 Agriculture, biology, Dextran Sulfate, NF-kappa B, Cell Polarity, Colitis, 3. Good health, 030220 oncology & carcinogenesis, Sirtuin, Cytokines, Female, Disease Susceptibility, medicine.symptom, Research Article, Colon, Inflammatory Diseases, Macrophage polarization, Bone Marrow Cells, Inflammation, Gastroenterology and Hepatology, SIRT2, 03 medical and health sciences, Antigens, CD, medicine, Animals, Lectins, C-Type, Molecular Biology, 030304 developmental biology, Macrophages, Inflammatory Bowel Disease, lcsh:R, Wild type, Biology and Life Sciences, medicine.disease, Molecular biology, Mice, Inbred C57BL, Disease Models, Animal, Immunology, biology.protein, lcsh:Q, Lymph Nodes, NAD+ kinase

Abstract

Background: SIRT2 belongs to a highly conserved family of NAD(+)-dependent deacylases, consisting of seven members (SIRT1-SIRT7), which vary in subcellular localizations and have substrates ranging from histones to transcription factors and enzymes. Recently SIRT2 was revealed to play an important role in inflammation, directly binding, deacetylating, and inhibiting the p65 subunit of NF-kB. Methods: A Sirt2 deficient mouse line (Sirt2(-/-)) was generated by deleting exons 5-7, encoding part of the SIRT2 deacetylase domain, by homologous recombination. Age-and sex-matched Sirt2(-/-) and Sirt2(+/+) littermate mice were subjected to dextran sulfate sodium (DSS)-induced colitis and analyzed for colitis susceptibility. Results: Sirt2(-/-) mice displayed more severe clinical and histological manifestations after DSS colitis compared to wild type littermates. Notably, under basal condition, Sirt2 deficiency does not affect the basal phenotype and intestinal morphology Sirt2 deficiency, however, affects macrophage polarization, creating a pro-inflammatory milieu in the immune cells compartment. Conclusion: These data confirm a protective role for SIRT2 against the development of inflammatory processes, pointing out a potential role for this sirtuin as a suppressor of colitis. In fact, SIRT2 deletion promotes inflammatory responses by increasing NF-kappa B acetylation and by reducing the M2-associated anti-inflammatory pathway. Finally, we speculate that the activation of SIRT2 may be a potential approach for the treatment of inflammatory bowel disease.

Published

2014

52. Combined inhibition of PI3K beta and PI3K gamma reduces fat mass by enhancing alpha-MSH-dependent sympathetic drive

Author

Perino, Alessia, Beretta, Martina, Kilic, Ana, Ghigo, Alessandra, Carnevale, Daniela, Repetto, Ivan Enrico, Braccini, Laura, Longo, Dario, Liebig-Gonglach, Michaela, Zaglia, Tania, Iacobucci, Roberta, Mongillo, Marco, Wetzker, Reinhard, Bauer, Michael, Aime, Silvio, Vercelli, Alessandro, Lembo, Giuseppe, Pfeifer, Alexander, and Hirsch, Emilio

Subjects

liver insulin PI3K

Abstract

Obesity is defined as an abnormal increase in white adipose tissue and has become a major medical burden worldwide. Signals from the brain control not only appetite but also energy expenditure, both of which contribute to body weight. We showed that genetic or pharmacological inhibition of two phosphatidylinositol 3-kinases (PI3K beta and PI3K gamma) in mice reduced fat mass by promoting increased energy expenditure. This effect was accompanied by stimulation of lipolysis and the acquisition of the energy-burning characteristics of brown adipocytes by white adipocytes, a process referred to as "browning." The browning of the white adipocytes involved increased norepinephrine release from the sympathetic nervous system. We found that PI3K beta and PI3K gamma together promoted a negative feedback loop downstream of the melanocortin 4 receptor in the central nervous system, which controls appetite and energy expenditure in the periphery. Analysis of mice with drug-induced sympathetic denervation suggested that these kinases controlled the sympathetic drive in the brain. Administration of inhibitors of both PI3K beta and PI3K gamma to mice by intracerebroventricular delivery induced a 10% reduction in fat mass as quickly as 10 days. These results suggest that combined inhibition of PI3K beta and PI3K gamma might represent a promising treatment for obesity.

Published

2014

53. Rac signal adaptation controls neutrophil mobilization from the bone marrow

Author

Campa, Carlo Cosimo, primary, Germena, Giulia, additional, Ciraolo, Elisa, additional, Copperi, Francesca, additional, Sapienza, Anna, additional, Franco, Irene, additional, Ghigo, Alessandra, additional, Camporeale, Annalisa, additional, Di Savino, Augusta, additional, Martini, Miriam, additional, Perino, Alessia, additional, Megens, Remco T. A., additional, Kurz, Angela R. M., additional, Scheiermann, Christoph, additional, Sperandio, Markus, additional, Gamba, Andrea, additional, and Hirsch, Emilio, additional

Published

2016

54. Eliciting the mitochondrial unfolded protein response by nicotinamide adenine dinucleotide repletion reverses fatty liver disease in mice

Author

Gariani, Karim, primary, Menzies, Keir J., additional, Ryu, Dongryeol, additional, Wegner, Casey J., additional, Wang, Xu, additional, Ropelle, Eduardo R., additional, Moullan, Norman, additional, Zhang, Hongbo, additional, Perino, Alessia, additional, Lemos, Vera, additional, Kim, Bohkyung, additional, Park, Young‐Ki, additional, Piersigilli, Alessandra, additional, Pham, Tho X., additional, Yang, Yue, additional, Ku, Chai Siah, additional, Koo, Sung I., additional, Fomitchova, Anna, additional, Cantó, Carlos, additional, Schoonjans, Kristina, additional, Sauve, Anthony A., additional, Lee, Ji‐Young, additional, and Auwerx, Johan, additional

Published

2015

55. Farnesoid X receptor inhibits glucagon-like peptide-1 production by enteroendocrine L cells

Author

Trabelsi, Mohamed-Sami, primary, Daoudi, Mehdi, additional, Prawitt, Janne, additional, Ducastel, Sarah, additional, Touche, Véronique, additional, Sayin, Sama I., additional, Perino, Alessia, additional, Brighton, Cheryl A., additional, Sebti, Yasmine, additional, Kluza, Jérôme, additional, Briand, Olivier, additional, Dehondt, Hélène, additional, Vallez, Emmanuelle, additional, Dorchies, Emilie, additional, Baud, Grégory, additional, Spinelli, Valeria, additional, Hennuyer, Nathalie, additional, Caron, Sandrine, additional, Bantubungi, Kadiombo, additional, Caiazzo, Robert, additional, Reimann, Frank, additional, Marchetti, Philippe, additional, Lefebvre, Philippe, additional, Bäckhed, Fredrik, additional, Gribble, Fiona M., additional, Schoonjans, Kristina, additional, Pattou, François, additional, Tailleux, Anne, additional, Staels, Bart, additional, and Lestavel, Sophie, additional

Published

2015

56. Contractile Function During Angiotensin-II Activation

Author

Zhang, Min, primary, Prosser, Benjamin L., additional, Bamboye, Moradeke A., additional, Gondim, Antonio N.S., additional, Santos, Celio X., additional, Martin, Daniel, additional, Ghigo, Alessandra, additional, Perino, Alessia, additional, Brewer, Alison C., additional, Ward, Christopher W., additional, Hirsch, Emilio, additional, Lederer, W. Jonathan, additional, and Shah, Ajay M., additional

Published

2015

57. PI3K-C2γ is a Rab5 effector selectively controlling endosomal Akt2 activation downstream of insulin signalling

Author

Braccini, Laura, primary, Ciraolo, Elisa, additional, Campa, Carlo C., additional, Perino, Alessia, additional, Longo, Dario L., additional, Tibolla, Gianpaolo, additional, Pregnolato, Marco, additional, Cao, Yanyan, additional, Tassone, Beatrice, additional, Damilano, Federico, additional, Laffargue, Muriel, additional, Calautti, Enzo, additional, Falasca, Marco, additional, Norata, Giuseppe D., additional, Backer, Jonathan M., additional, and Hirsch, Emilio, additional

Published

2015

58. Combined inhibition of PI3Kβ and PI3Kγ reduces fat mass by enhancing α-MSH–dependent sympathetic drive

Author

Perino, Alessia, primary, Beretta, Martina, additional, Kilić, Ana, additional, Ghigo, Alessandra, additional, Carnevale, Daniela, additional, Repetto, Ivan Enrico, additional, Braccini, Laura, additional, Longo, Dario, additional, Liebig-Gonglach, Michaela, additional, Zaglia, Tania, additional, Iacobucci, Roberta, additional, Mongillo, Marco, additional, Wetzker, Reinhard, additional, Bauer, Michael, additional, Aime, Silvio, additional, Vercelli, Alessandro, additional, Lembo, Giuseppe, additional, Pfeifer, Alexander, additional, and Hirsch, Emilio, additional

Published

2014

59. Vitamin D and energy homeostasis—of mice and men

Author

Bouillon, Roger, primary, Carmeliet, Geert, additional, Lieben, Liesbet, additional, Watanabe, Mitsuhiro, additional, Perino, Alessia, additional, Auwerx, Johan, additional, Schoonjans, Kristina, additional, and Verstuyf, Annemieke, additional

Published

2013

60. NADPH Oxidases in Heart Failure: Poachers or Gamekeepers?

Author

Zhang, Min, primary, Perino, Alessia, additional, Ghigo, Alessandra, additional, Hirsch, Emilio, additional, and Shah, Ajay M., additional

Published

2013

61. Blockade of Phosphatidylinositol 3-Kinase (PI3K)δ or PI3Kγ Reduces IL-17 and Ameliorates Imiquimod-Induced Psoriasis-like Dermatitis

Author

Roller, Anne, primary, Perino, Alessia, additional, Dapavo, Paolo, additional, Soro, Elisabetta, additional, Okkenhaug, Klaus, additional, Hirsch, Emilio, additional, and Ji, Hong, additional

Published

2012

62. Phosphoinositide 3-Kinase γ Protects Against Catecholamine-Induced Ventricular Arrhythmia Through Protein Kinase A–Mediated Regulation of Distinct Phosphodiesterases

Author

Ghigo, Alessandra, primary, Perino, Alessia, additional, Mehel, Hind, additional, Zahradníková, Alexandra, additional, Morello, Fulvio, additional, Leroy, Jérôme, additional, Nikolaev, Viacheslav O., additional, Damilano, Federico, additional, Cimino, James, additional, De Luca, Elisa, additional, Richter, Wito, additional, Westenbroek, Ruth, additional, Catterall, William A., additional, Zhang, Jin, additional, Yan, Chen, additional, Conti, Marco, additional, Gomez, Ana Maria, additional, Vandecasteele, Grégoire, additional, Hirsch, Emilio, additional, and Fischmeister, Rodolphe, additional

Published

2012

63. Liver X Receptor Activation Reduces Angiogenesis by Impairing Lipid Raft Localization and Signaling of Vascular Endothelial Growth Factor Receptor-2

Author

Noghero, Alessio, primary, Perino, Alessia, additional, Seano, Giorgio, additional, Saglio, Elisa, additional, Sasso, Giuseppe Lo, additional, Veglio, Franco, additional, Primo, Luca, additional, Hirsch, Emilio, additional, Bussolino, Federico, additional, and Morello, Fulvio, additional

Published

2012

64. Anchoring Proteins as Regulators of Signaling Pathways

Author

Perino, Alessia, primary, Ghigo, Alessandra, additional, Scott, John D., additional, and Hirsch, Emilio, additional

Published

2012

65. Integrating Cardiac PIP3 and cAMP Signaling through a PKA Anchoring Function of p110γ

Author

Perino, Alessia, primary, Ghigo, Alessandra, additional, Ferrero, Enrico, additional, Morello, Fulvio, additional, Santulli, Gaetano, additional, Baillie, George S., additional, Damilano, Federico, additional, Dunlop, Allan J., additional, Pawson, Catherine, additional, Walser, Romy, additional, Levi, Renzo, additional, Altruda, Fiorella, additional, Silengo, Lorenzo, additional, Langeberg, Lorene K., additional, Neubauer, Gitte, additional, Heymans, Stephane, additional, Lembo, Giuseppe, additional, Wymann, Matthias P., additional, Wetzker, Reinhard, additional, Houslay, Miles D., additional, Iaccarino, Guido, additional, Scott, John D., additional, and Hirsch, Emilio, additional

Published

2011

66. Distinct Effects of Leukocyte and Cardiac Phosphoinositide 3-Kinase γ Activity in Pressure Overload–Induced Cardiac Failure

Author

Damilano, Federico, primary, Franco, Irene, additional, Perrino, Cinzia, additional, Schaefer, Katrin, additional, Azzolino, Ornella, additional, Carnevale, Daniela, additional, Cifelli, Giuseppe, additional, Carullo, Pierluigi, additional, Ragona, Riccardo, additional, Ghigo, Alessandra, additional, Perino, Alessia, additional, Lembo, Giuseppe, additional, and Hirsch, Emilio, additional

Published

2011

67. Post-Wortmannin Era: Novel Phosphoinositide 3-Kinase Inhibitors with Potential Therapeutic Applications

Author

Braccini, Laura, primary, Morello, Fulvio, additional, Perino, Alessia, additional, and Hirsch, Emilio, additional

Published

2009

68. Phosphoinositide 3-Kinase γ Gene Knockout Impairs Postischemic Neovascularization and Endothelial Progenitor Cell Functions

Author

Madeddu, Paolo, primary, Kraenkel, Nicolle, additional, Barcelos, Luciola S., additional, Siragusa, Mauro, additional, Campagnolo, Paola, additional, Oikawa, Atsuhiko, additional, Caporali, Andrea, additional, Herman, Andrew, additional, Azzolino, Ornella, additional, Barberis, Laura, additional, Perino, Alessia, additional, Damilano, Federico, additional, Emanueli, Costanza, additional, and Hirsch, Emilio, additional

Published

2008

69. Measuring PI3K Lipid Kinase Activity.

Author

Ciraolo, Elisa, Perino, Alessia, and Hirsch, Emilio

Published

2012

70. Phosphoinositide 3-Kinase y Protects Against Catecholamine-Induced Ventricular Arrhythmia Through Protein Kinase A-Mediated Regulation of Distinct Phosphodiesterases.

Author

Ghigo, Alessandra, Perino, Alessia, Mehel, Hind, Zahradnikovâ Jr., Alexandra, Morello, Fulvio, Leroy, Jérôme, Nikolaev, Viacheslav O., Damilano, Federico, Cimino, James, De Luca, Elisa, Richter, Wito, Westenbroek, Ruth, Catterall, William A., Jin Zhang, Chen Yan, Conti, Marco, Gomez, Ana Maria, Vandecasteele, Grégoire, Hirsch, Emilio, and Fischmeister, Rodolphe

Subjects

*PHOSPHOINOSITIDES, *CATECHOLAMINES, *VENTRICULAR arrhythmia, *CYCLIC-AMP-dependent protein kinase, *PHOSPHODIESTERASES, *ADRENERGIC receptors, *ARRHYTHMIA

Abstract

Background--Phosphoinositide 3-kinase y (PI3Ky) signaling engaged by /3-adrenergic receptors is pivotal in the regulation of myocardial contractility and remodeling. However, the role of PI3Ky in catecholamine-induced arrhythmia is currently unknown. Methods and Results--Mice lacking PI3Ky (PI3Ky-/-) showed runs of premature ventricular contractions on adrenergic stimulation that could be rescued by a selective β²-adrenergic receptor blocker and developed sustained ventricular tachycardia after transverse aortic constriction. Consistently, fluorescence resonance energy transfer probes revealed abnormal cAMP accumulation after β²-adrenergic receptor activation in PI3Kɣ-/- cardiomyocytes that depended on the loss of the scaffold but not of the catalytic activity of PI3Ky. Downstream from β-adrenergic receptors, PI3Kɣ was found to participate in multiprotein complexes linking protein kinase A to the activation of phosphodiesterase (PDE) 3A, PDE4A, and PDE4B but not of PDE4D. These PI3Ky-regulated PDEs lowered cAMP and limited protein kinase A-mediated phosphorylation of L-type calcium channel (Cav1.2) and phospholamban. In PI3K-ɣ-/- cardiomyocytes, Cav1.2 and phospholamban were hyperphosphorylated, leading to increased Ca2+ spark occurrence and amplitude on adrenergic stimulation. Furthermore, PI3K-ɣ-/- cardiomyocytes showed spontaneous Ca2+ release events and developed arrhythmic calcium transients. Conclusions--PI3Ky coordinates the coincident signaling of the major cardiac PDE3 and PDE4 isoforms, thus orchestrating a feedback loop that prevents calcium-dependent ventricular arrhythmia. [ABSTRACT FROM AUTHOR]

Published

2012

71. Integrating Cardiac PIP3 and cAMP Signaling through a PKA Anchoring Function of p110γ

Author

Perino, Alessia, Ghigo, Alessandra, Ferrero, Enrico, Morello, Fulvio, Santulli, Gaetano, Baillie, George S., Damilano, Federico, Dunlop, Allan J., Pawson, Catherine, Walser, Romy, Levi, Renzo, Altruda, Fiorella, Silengo, Lorenzo, Langeberg, Lorene K., Neubauer, Gitte, Heymans, Stephane, Lembo, Giuseppe, Wymann, Matthias P., Wetzker, Reinhard, and Houslay, Miles D.

Subjects

*PHOSPHOINOSITIDES, *ADRENERGIC receptors, *PHOSPHODIESTERASES, *PROTEIN kinases, *PHARMACOLOGY, *HEART failure, *CELLULAR signal transduction

Abstract

Summary: Adrenergic stimulation of the heart engages cAMP and phosphoinositide second messenger signaling cascades. Cardiac phosphoinositide 3-kinase p110γ participates in these processes by sustaining β-adrenergic receptor internalization through its catalytic function and by controlling phosphodiesterase 3B (PDE3B) activity via an unknown kinase-independent mechanism. We have discovered that p110γ anchors protein kinase A (PKA) through a site in its N-terminal region. Anchored PKA activates PDE3B to enhance cAMP degradation and phosphorylates p110γ to inhibit PIP3 production. This provides local feedback control of PIP3 and cAMP signaling events. In congestive heart failure, p110γ is upregulated and escapes PKA-mediated inhibition, contributing to a reduction in β-adrenergic receptor density. Pharmacological inhibition of p110γ normalizes β-adrenergic receptor density and improves contractility in failing hearts. [Copyright &y& Elsevier]

Published

2011

72. Farnesoid X receptor inhibits glucagon-like peptide-1 production by enteroendocrine L cells

Author

Trabelsi, Mohamed-Sami, Daoudi, Mehdi, Prawitt, Janne, Ducastel, Sarah, Touche, Véronique, Sayin, Sama I, Perino, Alessia, Brighton, Cheryl A, Sebti, Yasmine, Kluza, Jérôme, Briand, Olivier, Dehondt, Hélène, Vallez, Emmanuelle, Dorchies, Emilie, Baud, Grégory, Spinelli, Valeria, Hennuyer, Nathalie, Caron, Sandrine, Bantubungi, Kadiombo, Caiazzo, Robert, Reimann, Frank, Marchetti, Philippe, Lefebvre, Philippe, Bäckhed, Fredrik, Gribble, Fiona M, Schoonjans, Kristina, Pattou, François, Tailleux, Anne, Staels, Bart, Lestavel, Sophie, Reimann, Frank [0000-0001-9399-6377], Gribble, Fiona [0000-0002-4232-2898], and Apollo - University of Cambridge Repository

Subjects

Blood Glucose, Colon, Enteroendocrine Cells, Colesevelam Hydrochloride, Mice, Obese, Receptors, Cytoplasmic and Nuclear, Diet, High-Fat, Proglucagon, Receptors, G-Protein-Coupled, Bile Acids and Salts, Mice, Glucagon-Like Peptide 1, Ileum, Insulin-Secreting Cells, Insulin Secretion, Animals, Humans, Insulin, Obesity, RNA, Messenger, Intestinal Mucosa, Sequestering Agents, Mice, Knockout, Basic Helix-Loop-Helix Leucine Zipper Transcription Factors, Anticholesteremic Agents, Nuclear Proteins, Intestines, Jejunum, Glycolysis, Signal Transduction, Transcription Factors

Abstract

Bile acids are signalling molecules, which activate the transmembrane receptor TGR5 and the nuclear receptor FXR. BA sequestrants (BAS) complex bile acids in the intestinal lumen and decrease intestinal FXR activity. The BAS-BA complex also induces glucagon-like peptide-1 (GLP-1) production by L cells which potentiates beta-cell glucose-induced insulin secretion. Whether FXR is expressed in L cells and controls GLP-1 production is unknown. Here, we show that FXR activation in L cells decreases proglucagon expression by interfering with the glucose-responsive factor Carbohydrate-Responsive Element Binding Protein (ChREBP) and GLP-1 secretion by inhibiting glycolysis. In vivo, FXR deficiency increases GLP-1 gene expression and secretion in response to glucose hence improving glucose metabolism. Moreover, treatment of ob/ob mice with the BAS colesevelam increases intestinal proglucagon gene expression and improves glycaemia in a FXR-dependent manner. These findings identify the FXR/GLP-1 pathway as a new mechanism of BA control of glucose metabolism and a pharmacological target for type 2 diabetes.

73. Bile acids deoxycholic acid and ursodeoxycholic acid differentially regulate human beta-defensin-1 and-2 secretion by colonic epithelial cells

Author

Lajczak, Natalia K., Saint-Criq, Vinciane, O'Dwyer, Aoife M., Perino, Alessia, Adorini, Luciano, Schoonjans, Kristina, and Keely, Stephen J.

Subjects

HbD, epithelium, innate immunity, UDCA

Abstract

Bile acids and epithelial-derived human beta-defensins (H beta Ds) are known to be important factors in the regulation of colonic mucosal barrier function and inflammation. We hypothesized that bile acids regulate colonic H beta D expression and aimed to test this by investigating the effects of deoxycholic acid (DCA) and ursodeoxycholic acid on the expression and release of H beta D1 and H beta D2 from colonic epithelial cells and mucosal tissues. DCA (10-150 mu M) stimulated the release of both H beta D1 and H beta D2 from epithelial cell monolayers and human colonic mucosal tissue in vitro. In contrast, ursodeoxycholic acid (50-200 mu M) inhibited both basal and DCA-induced defensin release. Effects of DCA were mimicked by the Takeda GPCR 5 agonist, INT-777 (50 mu M), but not by the farnesoid X receptor agonist, GW4064 (10 mu M). INT-777 also stimulated colonic H beta D1 and H beta D2 release from wild-type, but not Takeda GPCR 5(-/-), mice. DCA stimulated phosphorylation of the p65 subunit of NF-kappa B, an effect that was attenuated by ursodeoxycholic acid, whereas an NF-kappa B inhibitor, BMS-345541 (25 mu M), inhibited DCA-induced H beta D2, but not H beta D1, release. We conclude that bile acids can differentially regulate colonic epithelial H beta D expression and secretion and discuss the implications of our findings for intestinal health and disease.

74. TGR5 reduces macrophage migration through mTOR-induced C/EBP beta differential translation

Author

Perino, Alessia, Pols, Thijs Willem Hendrik, Nomura, Mitsunori, Stein, Sokrates, Pellicciari, Roberto, and Schoonjans, Kristina

Abstract

The bile acid-responsive G protein-coupled receptor TGR5 is involved in several metabolic processes, and recent studies suggest that TGR5 activation may promote pathways that are protective against diet-induced diabetes. Here, we investigated the role of macrophage-specific TGR5 signaling in protecting adipose tissue from inflammation and associated insulin resistance. Examination of adipose tissue from obese mice lacking macrophage Tgr5 revealed enhanced inflammation, increased chemokine expression, and higher macrophage numbers compared with control obese animals. Moreover, macrophage-specific deletion of Tgr5 exacerbated insulin resistance in obese animals. Conversely, pharmacological activation of TGR5 markedly decreased LPS-induced chemokine expression in primary macrophages. This reduction was mediated by AKT-dependent activation of mTOR complex 1, which in turn induced the differential translation of the dominant-negative C/EBP beta isoform, liver inhibitory protein (LIP). Overall, these studies reveal a signaling pathway downstream of TGR5 that modulates chemokine expression in response to high-fat diet and suggest that targeting this pathway has the potential to be therapeutically exploited for prevention of chronic inflammatory diseases and type 2 diabetes mellitus.

75. Short Article Hypothalamic bile acid-TGR5 signaling protects from obesity

Author

Castellanos-Jankiewicz, Ashley, Guzman-Quevedo, Omar, Fenelon, Valerie S., Zizzari, Philippe, Quarta, Carmelo, Bellocchio, Luigi, Tailleux, Anne, Charton, Julie, Fernandois, Daniela, Henricsson, Marcus, Piveteau, Catherine, Simon, Vincent, Allard, Camille, Quemener, Sandrine, Guinot, Valentine, Hennuyer, Nathalie, Perino, Alessia, Duveau, Alexia, Maitre, Marlene, Leste-Lasserre, Thierry, Clark, Samantha, Dupuy, Nathalie, Cannich, Astrid, Gonzales, Delphine, Deprez, Benoit, Mithieux, Gilles, Dombrowicz, David, Backhed, Fredrik, Prevot, Vincent, Marsicano, Giovanni, Staels, Bart, Schoonjans, Kristina, and Cota, Daniela

Subjects

ENERGY-EXPENDITURE, GASTRIC BYPASS, THERMOGENESIS, energy-expenditure, neurons, thermogenesis, MOUSE, GLUCOSE, SERUM, ACTIVATION, secretion, SECRETION, activation, glucose, gastric bypass, ACID RECEPTOR TGR5, NEURONS, acid receptor tgr5, serum, mouse

Abstract

Bile acids (BAs) improve metabolism and exert anti-obesity effects through the activation of the Takeda G protein-coupled receptor 5 (TGR5) in peripheral tissues. TGR5 is also found in the brain hypothalamus, but whether hypothalamic BA signaling is implicated in body weight control and obesity pathophysiology remains unknown. Here we show that hypothalamic BA content is reduced in diet-induced obese mice. Central administration of BAs or a specific TGR5 agonist in these animals decreases body weight and fat mass by activating the sympathetic nervous system, thereby promoting negative energy balance. Conversely, genetic downregulation of hypothalamic TGR5 expression in the mediobasal hypothalamus favors the development of obesity and worsens established obesity by blunting sympathetic activity. Lastly, hypothalamic TGR5 signaling is required for the anti-obesity action of dietary BA supplementation. Together, these findings identify hypothalamic TGR5 signaling as a key mediator of a top-down neural mechanism that counteracts diet induced obesity.

76. Eliciting the mitochondrial unfolded protein response via NAD+ repletion reverses fatty liver disease

Author

Gariani, Karim Laurent, Menzies, Keir Joe, Ryu, Dongryeol, Wenger, Casey J, Wang, Xu, Ropelle, Eduardo R, Moullan, Norman, Zhang, Hongbo, Perino, Alessia, Lemos Da Silva, Vera Monica, Canto Alvarez, Carlos, Schoonjans, Kristina, Sauve, Anthony A, Lee, Ji-Young, and Auwerx, Johan

Abstract

With no approved pharmacological treatment, nonalcoholic fatty liver disease (NAFLD) is now the most common cause of chronic liver disease inWestern countries and its worldwide prevalence continues to increase along with the growing obesity epidemic. Here, we show that a high-fat high-sucrose (HFHS) diet, eliciting chronic hepatosteatosis resembling human fatty liver, lowers hepatic nicotinamide adenine dinucleotide (NAD(+)) levels driving reductions in hepatic mitochondrial content, function, and adenosine triphosphate (ATP) levels, in conjunction with robust increases in hepatic weight, lipid content, and peroxidation in C57BL/6J mice. To assess the effect of NAD(+) repletion on the development of steatosis in mice, nicotinamide riboside, a precursor of NAD(+) biosynthesis, was added to theHFHS diet, either as a preventive strategy or as a therapeutic intervention. We demonstrate that NR prevents and reverts NAFLD by inducing a sirtuin (SIRT)1- and SIRT3-dependent mitochondrial unfolded protein response, triggering an adaptive mitohormetic pathway to increase hepatic beta-oxidation and mitochondrial complex content and activity. The cell-autonomous beneficial component of NR treatment was revealed in liver-specific Sirt1 knockout mice (Sirt1(hep-/-)), whereas apolipoprotein E-deficient mice (Apoe(-/-)) challenged with a high-fat high-cholesterol diet affirmed the use of NR in other independent models of NAFLD. Conclusion: Our data warrant the future evaluation of NAD(+) boosting strategies to manage the development or progression of NAFLD.

77. Eliciting the mitochondrial unfolded protein response via NAD(+) repletion reverses fatty liver disease

Author

Ropelle, Eduardo R, Ryu, Dongryeol, Park, Young-Ki, Siah Ku, Chai, Perino, Alessia, Fomitchova, Anna, Cantó, Carlos, Schoonjans, Kristina, Sauve, Anthony A, Wegner, Casey J, Menzies, Keir J, Lemos, Vera, Lee, Ji-Young, Wang, Xu, Gariani, Karim, Yang, Yue, Kim, Bohkyung, Moullan, Norman, Auwerx, Johan, Koo, Sung I, Piersigilli, Alessandra, Pham, Tho X, and Zhang, Hongbo

Subjects

630 Agriculture, 3. Good health

Abstract

With no approved pharmacological treatment, non-alcoholic fatty liver disease (NAFLD) is now the most common cause of chronic liver disease in western countries and its worldwide prevalence continues to increase along with the growing obesity epidemic. Here we show that a high-fat high-sucrose (HFHS) diet, eliciting chronic hepatosteatosis resembling human fatty liver, lowers hepatic NAD(+) levels driving reductions in hepatic mitochondrial content, function and ATP levels, in conjunction with robust increases in hepatic weight, lipid content and peroxidation in C57BL/6J mice. In an effort to assess the effect of NAD(+) repletion on the development of steatosis in mice, nicotinamide riboside (NR), a precursor for NAD(+) biosynthesis, was given to mice concomitant, as preventive strategy (NR-Prev), and as a therapeutic intervention (NR-Ther), to a HFHS diet. We demonstrate that NR prevents and reverts NAFLD by inducing a SIRT1- and SIRT3-dependent mitochondrial unfolded protein response (UPR(mt) ), triggering an adaptive mitohormetic pathway to increase hepatic β-oxidation and mitochondrial complex content and activity. The cell-autonomous beneficial component of NR treatment was revealed in liver-specific Sirt1 KO mice (Sirt1(hep-/-) ), while Apolipoprotein E-deficient (Apoe(-/-) ) mice challenged with a high-fat high-cholesterol diet (HFC), affirmed the use of NR in other independent models of NAFLD. CONCLUSION Our data warrant the future evaluation of NAD(+) boosting strategies to manage the development or progression of NAFLD. This article is protected by copyright. All rights reserved.

78. Asparagine protects pericentral hepatocytes during acute liver injury.

Author

Yu Sun, Demagny, Hadrien, Faure, Adrien, Pontanari, Francesca, Jalil, Antoine, Bresciani, Nadia, Yildiz, Ece, Korbelius, Melanie, Perino, Alessia, and Schoonjans, Kristina

Abstract

The nonessential amino acid asparagine can only be synthesized de novo by the enzymatic activity of asparagine synthetase (ASNS). While ASNS and asparagine have been implicated in the response to numerous metabolic stressors in cultured cells, the in vivo relevance of this enzyme in stress-related pathways remains unexplored. Here, we found ASNS to be expressed in pericentral hepatocytes, a population of hepatic cells specialized in xenobiotic detoxification. ASNS expression was strongly enhanced in 2 models of acute liver injury: carbon tetrachloride (CCl4) and acetaminophen. We found that mice with hepatocyte-specific Asns deletion were more prone to pericentral liver damage than their control littermates after toxin exposure. This phenotype could be reverted by i.v. administration of asparagine. Unexpectedly, the stress-induced upregulation of ASNS involved an ATF4-independent, noncanonical pathway mediated by the nuclear receptor, liver receptor homolog 1 (LRH-1; NR5A2). Altogether, our data indicate that the induction of the asparagine-producing enzyme ASNS acts as an adaptive mechanism to constrain the necrotic wave that follows toxin administration and provide proof of concept that i.v. delivery of asparagine can dampen hepatotoxin-induced pericentral hepatocellular death. [ABSTRACT FROM AUTHOR]

Published

2023

79. Phosphoinositide 3-Kinase Gamma Inhibition Protects from Anthracycline Cardiotoxicity and Reduces Tumor Growth

Author

Susanne Rohrbach, Mauro M. Teixeira, Flora Pirozzi, Miriam Martini, Irene Franco, Alessia Perino, Jean Piero Margaria, Roberto C. P. Lima-Júnior, Jacqueline Heger, Annalisa Angelini, Valentina Sala, Francesco Novelli, Alessandra Ghigo, Maria Chiara De Santis, Marco Mongillo, Anna Di Bona, Mingchuan Li, Julia Bornbaum, Carlo G. Tocchetti, Sebastiano Sciarretta, Emilio Hirsch, Tania Zaglia, Luca Rossi, Paolo E. Porporato, Pietro Ameri, Paola Cappello, Rainer Schulz, Fulvio Morello, Edoardo Lazzarini, Braulio H.F. Lima, Marco Sandri, James Cimino, Nicola Pianca, Li, Mingchuan, Sala, Valentina, De Santis, Maria Chiara, Cimino, Jame, Cappello, Paola, Pianca, Nicola, Di Bona, Anna, Margaria, Jean Piero, Martini, Miriam, Lazzarini, Edoardo, Pirozzi, Flora, Rossi, Luca, Franco, Irene, Bornbaum, Julia, Heger, Jacqueline, Rohrbach, Susanne, Perino, Alessia, Tocchetti, Carlo G, Lima, Braulio H F, Teixeira, Mauro M, Porporato, Paolo E, Schulz, Rainer, Angelini, Annalisa, Sandri, Marco, Ameri, Pietro, Sciarretta, Sebastiano, Lima-Júnior, Roberto César P, Mongillo, Marco, Zaglia, Tania, Morello, Fulvio, Novelli, Francesco, Hirsch, Emilio, and Ghigo, Alessandra

Subjects

0301 basic medicine, medicine.medical_treatment, inbred balb c, Autophagy-Related Proteins, Anthracycline, 030204 cardiovascular system & hematology, antibiotics, PI3Kγ, 0302 clinical medicine, Class Ib Phosphatidylinositol 3-Kinase, animal, Myocytes, Cardiac, Anthracyclines, genes, Phosphoinositide-3 Kinase Inhibitors, Mice, Inbred BALB C, Antibiotics, Antineoplastic, immunosuppression, biology, Immunosuppression, Tumor Burden, Female, Cardiology and Cardiovascular Medicine, medicine.drug, autophagy, mice, Heart Diseases, antineoplastic, cardiac, cardiotoxicity, Anthracyclines, PI3Kγ, autophagy, cardiotoxicity, immunosuppression, Breast Neoplasms, Mice, Transgenic, 03 medical and health sciences, cardiotoxicityb, Physiology (medical), Quinoxalines, medicine, Animals, Doxorubicin, Tumor growth, Protein Kinase Inhibitors, transgenic, Cardiotoxicity, disease models, Phosphoinositide 3-kinase, business.industry, Autophagy, myocytes, Genes, erbB-2, Disease Models, Animal, 030104 developmental biology, Cytoprotection, Toll-Like Receptor 9, Mutation, biology.protein, Cancer research, Thiazolidinediones, anthracyclines, pi3kγ, animals, antibiotics, antineoplastic, autophagy-related proteins, breast neoplasms, class ib phosphatidylinositol 3-kinase, cytoprotection, disease models, animal, doxorubicin, female, genes, erbb-2, heart diseases, mice, inbred balb c, mice, transgenic, mutation, myocytes, cardiac, protein kinase inhibitors, quinoxalines, thiazolidinediones, toll-like receptor 9, tumor burden, phosphoinositide-3 kinase inhibitors, business, erbb-2

Abstract

Background: Anthracyclines, such as doxorubicin (DOX), are potent anticancer agents for the treatment of solid tumors and hematologic malignancies. However, their clinical use is hampered by cardiotoxicity. This study sought to investigate the role of phosphoinositide 3-kinase γ (PI3Kγ) in DOX-induced cardiotoxicity and the potential cardioprotective and anticancer effects of PI3Kγ inhibition. Methods: Mice expressing a kinase-inactive PI3Kγ or receiving PI3Kγ-selective inhibitors were subjected to chronic DOX treatment. Cardiac function was analyzed by echocardiography, and DOX-mediated signaling was assessed in whole hearts or isolated cardiomyocytes. The dual cardioprotective and antitumor action of PI3Kγ inhibition was assessed in mouse mammary tumor models. Results: PI3Kγ kinase-dead mice showed preserved cardiac function after chronic low-dose DOX treatment and were protected against DOX-induced cardiotoxicity. The beneficial effects of PI3Kγ inhibition were causally linked to enhanced autophagic disposal of DOX-damaged mitochondria. Consistently, either pharmacological or genetic blockade of autophagy in vivo abrogated the resistance of PI3Kγ kinase-dead mice to DOX cardiotoxicity. Mechanistically, PI3Kγ was triggered in DOX-treated hearts, downstream of Toll-like receptor 9, by the mitochondrial DNA released by injured organelles and contained in autolysosomes. This autolysosomal PI3Kγ/Akt/mTOR/Ulk1 signaling provided maladaptive feedback inhibition of autophagy. PI3Kγ blockade in models of mammary gland tumors prevented DOX-induced cardiac dysfunction and concomitantly synergized with the antitumor action of DOX by unleashing anticancer immunity. Conclusions: Blockade of PI3Kγ may provide a dual therapeutic advantage in cancer therapy by simultaneously preventing anthracyclines cardiotoxicity and reducing tumor growth.

Published

2018

80. Hepatic lipid overload triggers biliary epithelial cell activation via E2Fs.

Author

Yildiz E, El Alam G, Perino A, Jalil A, Denechaud PD, Huber K, Fajas L, Auwerx J, Sorrentino G, and Schoonjans K

Subjects

Animals, Mice, Liver metabolism, Epithelial Cells metabolism, Cell Division, Lipids, Non-alcoholic Fatty Liver Disease metabolism

Abstract

During severe or chronic hepatic injury, biliary epithelial cells (BECs) undergo rapid activation into proliferating progenitors, a crucial step required to establish a regenerative process known as ductular reaction (DR). While DR is a hallmark of chronic liver diseases, including advanced stages of non-alcoholic fatty liver disease (NAFLD), the early events underlying BEC activation are largely unknown. Here, we demonstrate that BECs readily accumulate lipids during high-fat diet feeding in mice and upon fatty acid treatment in BEC-derived organoids. Lipid overload induces metabolic rewiring to support the conversion of adult cholangiocytes into reactive BECs. Mechanistically, we found that lipid overload activates the E2F transcription factors in BECs, which drive cell cycle progression while promoting glycolytic metabolism. These findings demonstrate that fat overload is sufficient to reprogram BECs into progenitor cells in the early stages of NAFLD and provide new insights into the mechanistic basis of this process, revealing unexpected connections between lipid metabolism, stemness, and regeneration., Competing Interests: EY, GE, AP, AJ, PD, KH, LF, JA, GS, KS No competing interests declared, (© 2023, Yildiz et al.)

Published

2023

81. Measuring PI3K lipid kinase activity.

Author

Ciraolo E, Perino A, and Hirsch E

Subjects

Animals, Antibodies, Monoclonal metabolism, Chromatography, Thin Layer, Enzyme Activation drug effects, Enzyme Inhibitors pharmacology, Immunoprecipitation, Mice, NIH 3T3 Cells, Recombinant Proteins metabolism, Enzyme Assays methods, Phosphatidylinositol 3-Kinases metabolism

Abstract

Class IA phosphoinositide-3 kinases (PI3Ks) signaling has recently emerged as a key element in cancer development because of its ability to trigger a complex panoply of cellular responses controlling survival and proliferation. Many cancers show inappropriately activated PI3K pathway, and tumors with high PI3K activity are frequently resistant to traditional chemotherapy. Indeed, preclinical studies demonstrated a prominent role for the PI3K pathway in cancer cell survival and growth, thus validating PI3K as a potential drug target in cancer. The emerging interest in inhibiting PI3Ks in cancer have prompted the aggressive development of new selective PI3K pathway inhibitors as cancer therapy, and many of these molecules are currently in early-phase clinical trials. In this chapter, we describe methods to measure the PI3K lipid kinase activity in vitro, which is the standard procedure to test the efficacy of inhibitors.

Published

2012

82. Phosphoinositide 3-kinase gamma gene knockout impairs postischemic neovascularization and endothelial progenitor cell functions.

Author

Madeddu P, Kraenkel N, Barcelos LS, Siragusa M, Campagnolo P, Oikawa A, Caporali A, Herman A, Azzolino O, Barberis L, Perino A, Damilano F, Emanueli C, and Hirsch E

Subjects

Animals, Class Ib Phosphatidylinositol 3-Kinase, Disease Models, Animal, Extremities blood supply, Isoenzymes genetics, Isoenzymes physiology, Male, Mice, Mice, Knockout, Muscle, Smooth physiology, Phosphatidylinositol 3-Kinases genetics, Transplants, Endothelial Cells physiology, Ischemia physiopathology, Neovascularization, Physiologic physiology, Phosphatidylinositol 3-Kinases physiology, Stem Cells physiology

Abstract

Objective: We evaluated whether phosphatidylinositol 3-kinase gamma (PI3Kgamma) plays a role in reparative neovascularization and endothelial progenitor cell (EPC) function., Methods and Results: Unilateral limb ischemia was induced in mice lacking the PI3Kgamma gene (PI3Kgamma-/-) or expressing a catalytically inactive mutant (PI3Kgamma(KD/KD)) and wild-type controls (WT). Capillarization and arteriogenesis were reduced in PI3Kgamma-/- ischemic muscles resulting in delayed reperfusion compared with WT, whereas reparative neovascularization was preserved in PI3Kgamma(KD/KD). In PI3Kgamma-/- muscles, endothelial cell proliferation was reduced, apoptosis was increased, and interstitial space was infiltrated with leukocytes but lacked cKit+ progenitor cells that in WT muscles typically surrounded arterioles. PI3Kgamma is constitutively expressed by WT EPCs, with expression levels being upregulated by hypoxia. PI3Kgamma-/- EPCs showed a defect in proliferation, survival, integration into endothelial networks, and migration toward SDF-1. The dysfunctional phenotype was associated with nuclear constraining of FOXO1, reduced Akt and eNOS phosphorylation, and decreased nitric oxide (NO) production. Pretreatment with an NO donor corrected the migratory defect of PI3Kgamma-/- EPCs. PI3Kgamma(KD/KD) EPCs showed reduced Akt phosphorylation, but constitutive activation of eNOS and preserved proliferation, survival, and migration., Conclusions: We newly demonstrated that PI3Kgamma modulates angiogenesis, arteriogenesis, and vasculogenesis by mechanisms independent from its kinase activity.

Published

2008