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Characterization of a novel peripheral pro-lipolytic mechanism in mice: role of VGF-derived peptide TLQP-21

Authors :
Monia Manieri
Federico Quaini
Antonio Giordano
Paolo Govoni
Corrado Ghè
Anna Moles
Maureen S. Riedl
Gallia Graiani
Lucy Vulchanova
Pamela Petrocchi
Saverio Cinti
Elena Bresciani
I. Bulgarelli
Alessandro Bartolomucci
Giampiero Muccioli
Aderville Cabassi
Roberta Possenti
Andrea Levi
Stefano Parmigiani
Antonio Torsello
Valentina Sanghez
Vittorio Locatelli
Andrea Frontini
Jørgen Petersen
Paola Palanza
Bjarne Due Larsen
Cheryl Cero
Possenti, R
Muccioli, G
Petrocchi, P
Cero, C
Cabassi, A
Vulchanova, L
Riedl, M
Manieri, M
Frontini, A
Giordano, A
Cinti, S
Govoni, P
Graiani, G
Quaini, F
Ghè, C
Bresciani, E
Bulgarelli, I
Torsello, A
Locatelli, V
Sanghez, V
Larsen, B
Petersen, J
Palanza, P
Parmigiani, S
Moles, A
Levi, A
Bartolomucci, A
Source :
Biochemical journal (Lond., 1984) 441 (2012): 511–522., info:cnr-pdr/source/autori:Possenti Roberta1,2; Muccioli Giampiero3; Petrocchi Pamela1,2; Cero Cheryl4,5; Cabassi Aderville6; Vulchanova Lucy7; Riedl Maureen S. 8; Manieri Monia9; Frontini Andrea9; Giordano Antonio9; Cinti Saverio9; Govoni Paolo10; Graiani Gallia11; Quaini Federico11; Ghè Corrado3; Bresciani Elena12; Bulgarelli Ilaria12; Torsello Antonio12; Locatelli Vittorio12; Sanghez Valentina5; Larsen Bjarne D.13; Petersen Jorgen S.13;Palanza Paola 5; Parmigiani Stefano5; Moles Anna1,14; Levi Andrea1; Bartolomucci Alessandro 4,5/titolo:Characterization of a novel peripheral pro-lipolytic mechanism in mice: role of VGF-derived peptide TLQP-21/doi:/rivista:Biochemical journal (Lond., 1984)/anno:2012/pagina_da:511/pagina_a:522/intervallo_pagine:511–522/volume:441
Publication Year :
2012

Abstract

The peptides encoded by the VGF gene are gaining biomedical interest and are increasingly being scrutinized as biomarkers for human disease. An endocrine/neuromodulatory role for VGF peptides has been suggested but never demonstrated. Furthermore, no study has demonstrated so far the existence of a receptormediated mechanism for any VGF peptide. In the present study, we provide a comprehensive in vitro, ex vivo and in vivo identification of a novel pro-lipolytic pathway mediated by the TLQP-21 peptide. We show for the first time that VGF-immunoreactivity is present within sympathetic fibres in the WAT (white adipose tissue) but not in the adipocytes. Furthermore, we identified a saturable receptor-binding activity for the TLQP-21 peptide. The maximum binding capacity for TLQP-21 was higher in the WAT as compared with other tissues, and selectively up-regulated in the adipose tissue of obese mice. TLQP-21 increases lipolysis in murine adipocytes via a mechanism encompassing the activation of noradrenaline/β-adrenergic receptors pathways and dose-dependently decreases adipocytes diameters in two models of obesity. In conclusion, we demonstrated a novel and previously uncharacterized peripheral lipolytic pathway encompassing the VGF peptide TLQP-21. Targeting the sympathetic nerve-adipocytes interaction might prove to be a novel approach for the treatment of obesityassociated metabolic complications. © The Authors Journal compilation © 2012 Biochemical Society.

Details

Language :
English
Database :
OpenAIRE
Journal :
Biochemical journal (Lond., 1984) 441 (2012): 511–522., info:cnr-pdr/source/autori:Possenti Roberta1,2; Muccioli Giampiero3; Petrocchi Pamela1,2; Cero Cheryl4,5; Cabassi Aderville6; Vulchanova Lucy7; Riedl Maureen S. 8; Manieri Monia9; Frontini Andrea9; Giordano Antonio9; Cinti Saverio9; Govoni Paolo10; Graiani Gallia11; Quaini Federico11; Ghè Corrado3; Bresciani Elena12; Bulgarelli Ilaria12; Torsello Antonio12; Locatelli Vittorio12; Sanghez Valentina5; Larsen Bjarne D.13; Petersen Jorgen S.13;Palanza Paola 5; Parmigiani Stefano5; Moles Anna1,14; Levi Andrea1; Bartolomucci Alessandro 4,5/titolo:Characterization of a novel peripheral pro-lipolytic mechanism in mice: role of VGF-derived peptide TLQP-21/doi:/rivista:Biochemical journal (Lond., 1984)/anno:2012/pagina_da:511/pagina_a:522/intervallo_pagine:511–522/volume:441
Accession number :
edsair.doi.dedup.....4d1a6602c5c28fdfacc70923d3aa5884