Post on 16-Dec-2015
ANNA MOLES
Institute of Neuroscience CNR- Rome, Italy
A metabolic role for the VGF-derived peptides
Neurotrophins are proteins required for neuronal differentiation and survival. Pioneering work by Rita Levi-Montalcini, Stanley Cohen and Viktor Hamburger in the 1950s and early 1960s identified nerve growth factor (NGF) and demonstrated that this protein was required for sympathetic neuron survival both in vivo and in vitro. The later purification and characterization of brain-derived neurotrophic factor (BDNF), a close relative of NGF, allowed the cloning of additional family members. Six members of the neurotrophin family have been identified in vertebrates, namely NGF, BDNF, NT-3, NT-4/5, NT-6 and NT-7. These polypeptides bind, with different affinities, to the Trk family of receptor tyrosine kinases (TrkA, TrkB and TrkC) and with similar affinities to the p75 neurotrophin receptor (p75NTR), a member of the tumor necrosis factor receptor
Vgf gene discovered in PC12 cells following NGF treatment (Levi et al., Science 1985)
Possenti et al PNAS, 1992
TISSUE SPECIFIC EXPRESSION OF VGF
Salton et al. Front Neuroendocrinol, 2000
Nature Neuroscience 6, 736 - 742 (2003)
Brain-derived neurotrophic factor regulates energy balance downstream of melanocortin-4 receptorBaoji Xu1, 5, Evan H Goulding2, Keling Zang1, David Cepoi3, Roger D Cone3, Kevin R Jones4, Laurence H Tecott2 & Louis F Reichardt1
VGF a possible link between neurotrophines and energy homeostasis?
Resistant to several types of obesity
VGF-gene acts downstream of MC4R in PVN, LH or brain stem nuclei, that project via the autonomic nervous
system to peripheral metabolic tissues and regulate energy homeostasis
Vgf encodes a 617 amino acid protein in rodents that, upon processing by the neuroendocrine-specific prohormone convertases (PC)1/3 and PC2, yields several peptides that are stored in dense core granules and secreted through the regulated pathway
Ferri & Possenti, Trends Endocrinol Metab, 1996
VGF CONSTRUCTS
Trombin cleaves at :…...LVPR GSPRTLQ…..
GST VGF
TROMBIN
pep20
pep20-10
pep10
pep10-3
pep3
NAPPEPVPPPRAAPAPTHVRSPQPPPPAPARDELPDWNEVLPPWDREEDEVFPPGPYHPFPNYIRPR
TLQPPASSRRRHFHHALPPARHHPDLEAQARRAQEEADAEERRLQEQEELENYIEHVLLHRP
IDENTIFICATION OF VGF DERIVED PEPTIDE
TLQPPASSRRRHFHHALPPARHHPDLEAQARRAQEEADAEERRLQEQEELENYIEHVLLHRP
TLQPPASSRRRHFHHALPPARHHPDLEAQARRAQEEADAEERRLQEQEELENYIEHVLLHRP
Mouse TLQP-21 sequence
Human TLQP-21 sequence
basal Chronic TLQP-21 icv treatment
0 1 3 5 7 9 11 13 Body weight
Food intake
days
Surgery, start treatment
Can TLQP-21 modulate energy homeostasis?
Experimental procedure:
Male CD1 mice injected icv with TLQP-21 (6nmol/day) for 14 days with Alzet microsmotic pumps.
BATb1AR
b2AR
b3AR
UCP1
UCP2
UCP3
Norepi
WATUCP1
UCP2
b1AR
b2AR
b3AR
ADRENALSEpinephrine
Norepinephrine
Corticosterone
HYPOTHALAMUSAGRP POMC
NPY CRH
MCH
GHS-R
UCP3
PPAR-d
PGC-1a
Adipon
HemeOx1
Norepi
THYROIDfT3
fT4
Body weight
Food intake
Locomotor activity
Temperature
Energy expenditure
Triglycerides
FFA/TG
Leptine
Ghreline
BAT
WAT
Increased T, epinephrine and resting EE & adrenal weight
Normal food intake and locomotor activity,and thyroid hormones
Decreased TG and increased FFA/TG ratio; slight reduction in WAT and leptin
No changes in the hypothalamus; 2-AR increase in BAT; UCP1, PPAR-delta and 3-AR in WAT
BAT WAT
WATWAT
CONCLUSION 1
Central TLQP-21 determines:
Increased EE, hyperthermia, conversion of TG in FFA
Proposed mechanism:
Increased sympathetic stimulation to WAT and adrenomedullary release of E
Increased UCP1 and catabolic mediator in the WAT
Can central TLQP-21 affects development of diet induced obesity?
basal Chronic TLQP-21 icv treatment
0 1 3 5 7 9 11 13 Body weight
Food intake
days
Surgery, start treatment
Experimental procedure:
Male CD1 mice injected icv with TLQP-21 (6nmol/day) for 14 days with Alzet microsmotic pumps.
Starting the day of surgery mice received a HF diet (+20% lard).
Body weight
Leptin Ghrelin
Food intake
White adipose tissue
Can TLQP-21 modulate energy homeostasis and
somatic growth by modulating the GH/IGF-1
axis?
NO
EFFECTS OF TLQP-21
-Increases energy expenditure -Increase epinephrine and inhibit norepinephrine in the long term-Activate catabolic markers in the adipose tissue-Prevents diet-induced in obesity prone individuals-Increase heart rate-…..
Modulation of the ANS and the sympathoadrenomodellurary pathways.
GENERAL CONCLUSION 1
TLQP-21 is the first VGF-derived peptide which is involved in energy metabolism
Other VGF-derived peptides should have an anabolic role
VGF -/- TLQP-21
TLQP-21 centrally increases energy expenditure
GENERAL CONCLUSION 2
GENERAL CONCLUSION 3
TLQP-21 blocks development of diet induced obesity by increasing energy expenditure
BASELINE (3 days)
SOCIAL INTERACTION(twice a day x 5 days)
COHABITATION(16 days)
PSYCHOSOCIAL STRESS PROCEDURE
PSYCHOSOCIAL
STRESS
0
10
20
30
40
50
60
70
80
90
100
110
foo
d i
ng
es
ted
fro
m d
ay
5-d
ay
21
(g
r)
****
FOOD INTAKE IN DOM, SUB AND CONTROLMICE DURING PS (COHABITATION)
ANOVA F 2,25
= 4.75 p< 0.05
** p< 0.01 vs CONTROL
Mean daily Metabolic rate
0,5
0,55
0,6
0,65
0,7
0,75
0,8
0,85
dom sub con dom sub con
Basale Basale Basale Post Post Post
MEAN DAILY METABOLIC RATE (kcal/h),AND LOCOMOTION IN DOM SUB AND CONTROL MICE BEFORE
AND AFTER THE PS PROCEDURE
Mean activity
0
100
200
300
400
500
600
DomBasal
SubBasal
ConBasal
DomStress D22
SubStress D22
ConStress D22
coun
ts
**
ANOVA F2,13
= 6,77 p< 0.01
**p< 0.01 vs CONTROLANOVA F
2,13 = 0.00 NS
Institute of Neurobiology and Molecular Medicine CNR Rome and Department of Neurobiology Univ. of Rome Tor Vergata
ANDREA LEVI
ROBERTA POSSENTIROBERTO RIZZICINZIA SEVERINIGIORGIO LA CORTE
Institute of Neuroscience CNR Rome FRANCESCA D’AMATOALESSANDRO BARTOLOMUCCIFLAMINIA PAVONELUCIANA GARBUGINOROBERTO COCCURELLO
Univ. of Cagliari
GIAN LUCA FERRI
CARLA BRANCIA
Univ. of Rome La SapienzaDONATELLA BARRAEUGENIA SCHININA’ PINA MIGNOGNAALESSANDRA GIORGI
Univ. Of MilanA.E. RIGAMONTI, E.E. MULLER
Univ. Milan-BicoccaTORSELLO, V. LOCATELLI
Sigma Tau,SPA, PomeziaR. CONTI
A.CAPRIOLIF.BORSINI
O.GHIRARDI
S.Lucia Foundation, RomeT. PASCUCCI