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La pandemia de la obesidad
Are you Biased Against Overweight Patients?
• Fat people are good and lazy; thin people are bad and motivated
• Fat people are bad and motivated; thin people are good and lazy
• Fat people are bad and lazy; thin people are good and motivated
• Fat people are good and motivated; thin people are bad and lazy
Are you Biased ? • Anywhere from 30% to 40% of health care
providers who specialized in obesity treatment answered:
Fat people are bad and lazy; thin people are good and motivated ● Indicating bias or negative attitudes towards the
overweight and obese patient
● Much of this bias is related to a lack of knowledge
Teachman BA, Brownell KD. Int J Obes Relat Metab Disord. 2001;25(10):1525-1531.
Curso MIR SEEN 2016
• “Nuevas fronteras en el tratamiento de la obesidad”……Qué datos han llevado al diseño de nuevos fàrmacos para tratar la obesidad…..y que funcionen!!!
Potential Anti-obesity Drugs and Their Pathways Complex System with Redundancy-That’s Why It’s Hard to Lose
Valentino MA, Lin JE, Waldman SA. Clin Pharm & Therapeutics (2010) 87 6, 652–662. doi:10.1038/clpt.2010.57 Endogenous Signaling of Appetite-regulating Hormones, Neuropeptides, and Neurotransmitters, and The Drugs That Target These Pathways 5
GENES AND FAT DEPOSITION
WHICH GENES? HOW MANY?
More than 400 genes out of 16000 are involved in fat deposition
NATURE, 2003 GENOME-WIDE RNAi ANALYSIS OF Caenorhabditis elegans FAT REGULATORY GENES. Kaveh Ashrafi et al,.
Factores que influyen en el desarrollo de la obesidad
Hypothalamic Appetite Regulation
Farooqi S. Cell Metab 2006;4:260-262
3% of subjects with severe early onset obesity had a LEPR mutation
6% children with severe obesity had a mutation in the MC4 receptor
Lessons from Monogenic Obesity Syndromes
• single genetic defects can lead to severe obesity in humans • • some may be amenable to specific therapy • • insights into mechanisms involved in the regulation of
body weight • • leptin is a potent regular of energy intake, puberty and T
cell function • • MC4R deficiency is the commonest monogenic human
obesity and protects agianst obesity-induced HTA. • • Heterogeneous nature of obesity and associated
complications
Complex interactions underlying polygenic obesity
Mutch D & Clement K, Plos Genetics 2006
Nutrition Exercise Viruses
Social Status
Food Abundance
Peer pressure
Pollution Technological Progress
Psychology
Nutrition Exercise Viruses
hormones Social Status
Food Abundance
Peer pressure
Pollution Technological Progress
Psychology Psychology
Determinants of body weight
• Obesity is a complex multi-factorial disease • Differing susceptibilities in certain ethnic
groups • Heritability of fat mass = 40 - 70% (twin
and adoption studies) • Major genetic defects in severe obesity
THE HYPOTHALAMUS The most relevant part of the CNS?
THE HYPOTHALAMUS REGULATES:
• BODY TEMPERATURE. • GROWTH • REPRODUCTION • LACTATION • WATER BALANCE • COORDINATION ANS • FOOD INTAKE. • EMOTIONAL BAHAVIOUR
BRAINSTEM
LHA LHA
DMN DMN
PVN PVN
VMN VMN
PITUITARY GLAND
CEREBRAL CORTEX
BAT WAT MUSCLE
PANCREAS
LIVER GUT
Vagal
Visceral
Leptin, Adiponectin
(ADIPOSE TISSUE)
Glucocorticoids Thyroid Hormones Gonadal Steroids
(ENDOCRINE GLANDS) Insulin
(PANCREAS)
Ghrelin, PYY, CCK
(STOMACH/GUT)
BBB
NEUROPEPTIDES AND HOMEOSTASIS.THE NEED FOR ENERGY.
-GROWTH -SEX/REPRODUCTION -LACTATION -TERMOGENESIS -STRESS WHAT DO THEY HAVE IN COMMON? ONLY POSSIBLE IF ENERGY AVAILABILITY IS ADEQUATE. HOW DO THEY KNOW THAT?
THE HYPOTHALAMUS The most relevant part of the CNS?
Regulación de la ingesta y peso corporal
Regulación de la masa corporal … pura termodinámica
Gasto energético
Ingesta
Masa normal
Ejercicio
Gasto energético Ingesta
Sobrepeso y obesidad
Ejercicio
FOOD INTAKE
Balance between orexigenic/anorexigenic signals
Programming (fetal /neonatal) and lifestyle
Food preference
Hedonic component
“the hungry brain”:homeostatic vs hedonic components
Comer para sobrevivir Comer por placer: adicción
Ingesta: comer por necesidad (Adaptación) ♦Energía para sobrevivir- (=Necesidades energéticas)
♦ Necesidades nutricionales (= Variedad) ♦ Selección de alimentos –dulce, salado,…>>ácido, amargo (= Comestible>>Venenoso)
“the hungry brain”:homeostatic vs hedonic components
Comer para sobrevivir Comer por placer: adicción
♦Algunas comidas nos hacen comer más (=Refuerzo)
♦ Y provocan asociación entre comida y recompensa (= Condicionamiento) ♦ Promueven la ingesta en ausencia de necesidad energética (= Ingesta hedónica)
Ingesta: comer por placer (Recompensa)
Y qué pasa con los “adictos” a la comida: “the hungry brain”
Limbic: The nature reward pathway
NEURONATOMIA: CONTROL HEDONICO DE LA INGESTA.
sexo comida juego drogas alcoho
Recompensas naturales o artificiales
Are you a food addict?
1. Do you think about your weight constantly ? 2. Do you eat differently in private than with other people? 3. Do you eat to escape from your feeling? 4. Do you eat when you are not hungry? 5. Have you ever stolen other people’s food? 6. Have you ever hid food to make sure you have “enough?” 7. Do you frequently feel shamed or guilty about what you have eaten? 8. Do you feel hopeless about your relationship with food?
There is an ongoing discussion whether food addiction exist. ("Eating addiction", rather than "food addiction", better captures addictive-like eating behavior. Hebebrand J, Albayrak Ö, Adan R, Antel J, Dieguez C, de Jong J, Leng G, Menzies J, Mercer JG, Murphy M, van der Plasse G, Dickson SL.Neurosci Biobehav Rev. 2014 Nov;47:295-306
“the hungry brain”:homeostatic vs hedonic components
Comer para sobrevivir Comer por placer: adicción
• Orexigenic: NPY AgRP MCH β-END (POMC) GAL DYN OX-A/OX-B Endocannabinoids Ghrelin
• Anorexigenic: Leptin PYY3-36 Amilin Oleoyl-estrone Oleylethanolamide α-MSH (POMC) CART TRH CRH
Regulation of food intake
Hypothalamic regulation of energy balance
Brain
Hypothalamus
Liver Skeletal muscle
BAT WAT Beta - cell (pancreas)
Food intake
Autonomic Nervous System
Glucose and lipid metabolism Energy expenditure
Hormonal and nutritional signals
Hypothalamic neuropeptides
Anorexigenic neuropeptides
LEPTIN
Food intake
PVH PVH
DMH DMH
VMH VMH
LHA LHAPVH PVH
DMH DMH
VMH VMH
LHA LHAMCH
AgRP NPY
OXs
CRH TRH
CART
POMC α-MSH
Orexigenic neuropeptides
GHRELIN
BRAINSTEM
LHA LHA
DMN DMN
PVN PVN
VMN VMN
PITUITARY GLAND
CEREBRAL CORTEX
BAT WAT MUSCLE
PANCREAS
LIVER GUT
Vagal
Visceral
Leptin, Adiponectin
(ADIPOSE TISSUE)
Glucocorticoids Thyroid Hormones Gonadal Steroids
(ENDOCRINE GLANDS) Insulin
(PANCREAS)
Ghrelin, PYY, CCK
(STOMACH/GUT)
BBB
ob/ ob: KO de la leptina • Hiperfagia
• Obesidad mórbida • Respuesta normal a leptina
Zhang Y, et al (1994). Nature 372: 425-432
ob/ ob
• Hiperfagia
• Obesidad
ob/ ob + leptina
• Ingesta normal
• Masa corporal normal
Leptina
Zhang Y, et al (1994). Nature 372: 425-432
32 kg; 7 años
¿Existen mutaciones del gen ob en humanos?
Leptina
42 kg; 3 años
Montague CT, et al (1997). Nature 387: 903-908
Leptin
AgRP NPY
POMC CART
- +
LEPTIN. Acts at hypothalamic level -Inhibits food intake, incresed energy expenditure, decrease body weight. -
LEPTIN. Secreted by adipose tissue. -Serum levels related to adipose mass. -MORE OBESE HIGHER LEPTIN LEVELS.
LEPTIN. Obese human subjects: leptin resistance. Leptin gene or leptin receptor gene: massive obesity. -
Hypothalamic neuropeptides
Anorexigenic neuropeptides
LEPTIN
Food intake
PVH PVH
DMH DMH
VMH VMH
LHA LHAPVH PVH
DMH DMH
VMH VMH
LHA LHAMCH
AgRP NPY
OXs
CRH TRH
CART
POMC α-MSH
Orexigenic neuropeptides
GHRELIN
In 1999, Kojima et al. isolated the endogenous ligand for the GHS receptor in rat stomach.
Peptide of 28 aminoacids with a esterification in serine-3, which is essential for the biological activity.
It was identified two other forms that is different in a glutamine in position 14, Des-Gln14-Ghrelin.
GHRELIN
GHRELIN (HUMANO) GHRELIN (HUMANO)
BODY COMPOSITION
0
5
10
15
20
25
VehicleGhrelin
**
**
**
fat m
ass (
g)
7 14 21 28 Days after pump implantation
Ghrelin administration
Ghrelin
Ghrelin agonists to reverse cachexia?
• Anamorelin for patients with cancer cachexia: an integrated analysis of two phase 2, randomised, placebo-controlled, double-blind trials (Garcia et al Lancet Oncology 2015)
• Anamorelin, a ghrelin agonist, treatment for 12 weeks had a favourable clinical response profile in patients with cancer anorexia-cachexia syndrome.
NPY
AgRP
ghrelin
Hypothalamic neuron
SIRT1
p53 AMPK pAMPK
pACC
ACC Malonyl-CoA Acetyl-CoA
MCD
Palmitoyl
FAS
CPT-1
mitochondria
β-oxidation ROS
UCP-2
cytoplasm
FOOD INTAKE
BSX pCREB
FOXO 1
Figure 6
Ghrelin’s orexigenic effect is mediated by AMPK
Andersson M et al (2004) JBC 279:12005-12008
Sakkou M et al (2007) Cell Metab 5, 450-463
Kola M et al (2008) PLoS ONE 3:e1797
López M et al (2008) Cell Metab 7:389-399
Andrews ZB et al (2008) Nature 454:846-851
Lage R et al (2010) FASEB J 24:2670-2679
Velásquez DA et al (2011) Diabetes 60:1177-1185
Ramírez S et al (2013) Diabetes 62:2329-2337
Ghrelin Signals Hunger BR LU DI
(24 hour clock)
Ghrelin Level
Adapted from Williams DL, Cummings DE. J Nutr 2005;135:1320-1325
Figure 2. Relationship between plasma ghrelin concentrations and subjective ratings of hunger. Individuals with PWS (♦, overnight fast) and controls (○, 36-h fast) were asked to rate their subjective sensation of hunger in response to the questions “How much food do you think you could eat right now?” (top) and “How hungry do you feel?” (bottom)
Published in: Angelo DelParigi et al The Journal of Clinical Endocrinology & Metabolism 2002, 87, 5461-5464.
Ghrelin antagonist in obesity?
• This clinical data clearly illustrates the therapeutic potential of AZP-531, combining insulin sensitization and weight reduction, therefore supporting further developments in type 2 diabetes and Prader-Willi syndrome” said Thierry Abribat, manager of TAB Consulting, president of Alizé Pharma SAS.
DRUG TARGETS
• Most of the drug targets failed when tested in humans....Leptin only beneficial in a subjects with mutation leptin gene.
• Ghrelin? Yet promising… • We tell patients: eat less and do exercise • Think!!!! • Nicotine? • GLP-1 and combinations… • Thyroid hormones ?
Thyroid hormones and energy balance
Hyperthyroidism induces marked alterations in energy balance
López M et al (2010). Nat Med 16: 1001-1008
Days1 3 5 7 9 11 13 15 17 19 21
Body
wei
ghtc
hang
e(g
)
0
20
40
60
80
100
120
140
160 VehicleT4VehicleT4
c
c
b c
a
bb b
c c
bb
b
b b
bb
b
cc
Food
inta
ke (g
)
Days1 3 5 7 9 11 13 15 17 19 21
20
25
30
35
40c
c
cccc
ccc
ccc
ac
c
VehicleT4VehicleT4
Leanness Hyperphagia
02040
6080
100120
140160
AgRP NPY CART POMC
mR
NA
leve
ls (%
eut
hyro
id) ** **
**
02040
6080
100120
140160
AgRP NPY CART POMC
mR
NA
leve
ls (%
eut
hyro
id) ** **
** Increased hypothalamic orexigenic signalling
EuthyroidHyperthyroidEuthyroidHyperthyroid
Thyroid hormones stimulate BAT in humans
Skarulis MC et al (2009). JCEM 95: 256–262
Without T4 With T4
Increased glucose uptake after T4 treatment
Increased BAT UCP-1 after T4 treatment
Storage (fat)
Food intake
Metabolism
Energy expenditure
Thermogenesis
Physical activity
Metabolism
Energy expenditure
HYPOTHESIS
• In hyperthyroidism there is an alteration in cellular sensors of energy availability leading to increased energy expenditure and increase food intake.
• AMPK? • mTOR?
WAT Liver
Skeletal muscle Pancreatic β cell
Heart Hypothalamus
Fatty acid oxidation
Glucose uptake
Mitochondrial biogenesis
Food intake Fatty acid oxidation
Glucose uptake
Glycolysis
AMPK
Insulin secretion
Fatty acid synthesis
Cholesterol synthesis
Gluconeogenesis
Fatty acid synthesis
Lipolysis
AMPK-Cellular Sensor
• Expressed in key hypothalamic nuclei. • Regulated by feeding and fasting. • Activation of AMPK increased feeding. • Play a key role in in hypothalamic
hypoglycaemia sensing. • Regulated by different hormones and
neurotransmitters, including ghrelin.
Hypothalamic mTOR a novel whole body energy sensor
mTOR: mammalian target of rapamycin S6K1: S6 kinase 1
Woods et al (2008). Annu.Rev.Nutr. 28: 295-311 Cota D et al (2006). Science 312: 927-930
HYPOTHESIS
• In hyperthyroidism there is an alteration in cellular sensors of energy availability leading to increased energy expenditure and increase food intake.
• AMPK? ENERGY EXPENDITURE (VMH)
• mTOR? FOOD INTAKE (ARC)
New model of central T3 actions on energy balance
López M et al (2010). Nat Med 16: 1001-1008
Thyroid gland
Energy expenditure
SNS
Hypothalamus
3V
ARC
RPa IO
Body weight Body weight
SNS
3V
ARC
T3
Complex lipids
Malonyl-CoA
Acetyl-CoA
AMPK
ACC
FAS
Ucp1 Ppargc1a
Ppargc1b Ucp3
VMH
X
X TR
β3-AR
BAT
DRUG TARGETS
• Most of the drug targets failed when tested in humans....Leptin only beneficial in a few subjects (mutation leptin gene).
• Thyroid hormones ?
• Nicotine?
• GLP-1 + Glucagon/TH/ E2….
Time (days)
60
40
20
0
80
Bod
y w
eigh
tcha
nge
(g)
1 3 5 7 9 11 13 15 17-10
##
#
***
Withdrawal
Time (days)
60
40
20
0
80
Bod
y w
eigh
tcha
nge
(g)
1 3 5 7 9 11 13 15 17-10
##
#
***
Withdrawal
10
25
1 3 5 7 9 11 13 15 17
20
30
15
Time (days)
***#
##
Food
inta
ke(g
)
Withdrawal
10
25
1 3 5 7 9 11 13 15 17
20
30
15
Time (days)
***#
##
Food
inta
ke(g
)
10
25
1 3 5 7 9 11 13 15 17
2020
3030
1515
Time (days)
***#
##
Food
inta
ke(g
)
Withdrawal
Vehicle
WithdrawalNicotineVehicleVehicle
WithdrawalNicotineWithdrawalNicotine
39 ºC
26 ºC
Vehicle Nicotine
BAT
BAT
39 ºC
26 ºC
39 ºC
26 ºC
Vehicle Nicotine
BAT
BAT
What’s about pharmacology? Nicotine
Martínez de Morentin PB et al (2012). Diabetes 61:807-817
What’s about pharmacology? Nicotine
Seoane-Collazo P et al (2014). Endocrinology 155:1679-1689
Time (days)
Foo d
i nta
ke(K
cal/ d
a y)
1 3 5 7 9 11 13 15 1740
50
60
70
80
90 Withdrawal
***##
Time (days)
Foo d
i nta
ke(K
cal/ d
a y)
1 3 5 7 9 11 13 15 1740
50
60
70
80
90
Time (days)
Foo d
i nta
ke(K
cal/ d
a y)
1 3 5 7 9 11 13 15 1740
50
60
70
80
90 WithdrawalWithdrawal
***##
Withdrawal
***###
Time (days)Body
we i
ghtc
hang
e(g
)
1 3 5 7 9 11 13 15 17
-40
-20
0
20
40
HFD vehicleHFD nicotineHFD withdrawal
WithdrawalWithdrawal
***###
Time (days)Body
we i
ghtc
hang
e(g
)
1 3 5 7 9 11 13 15 17
-40
-20
0
20
40
Time (days)Body
we i
ghtc
hang
e(g
)
1 3 5 7 9 11 13 15 17
-40
-20
0
20
40
Time (days)Body
we i
ghtc
hang
e(g
)
1 3 5 7 9 11 13 15 17
-40
-20
0
20
40
HFD vehicleHFD nicotineHFD withdrawal
HFD vehicleHFD nicotineHFD nicotineHFD withdrawalHFD withdrawal
10
0
2
4
6
8
Sta
ined
area
(%)
*
0
2
4
6
8
Sta
ined
area
(%)
*
Vehicle Nicotine
Nicotine acts at hyothalamic level
• Decrease food intake at the ARC via orexigenic/anorexigenic peptides (NPY/AgRP and POMC).
• Increase energy expenditure at the VMH through a AMPK-dependent mechanism.
• Nicotine may prevent or impaired obesity development …
• YET SMOKING IS BAD FOR YOUR HELP
DRUG TARGETS
• Most of the drug targets failed when tested in humans....Leptin only beneficial in a few subjects (mutation leptin gene).
• Thyroid hormones ?
• Nicotine?
• GLP-1 + Glucagon/TH/ E2….
Effects of Liraglutide and Orlistat on Body Weight in Nondiabetic Obese Adults
Data are mean (95% CI) for the ITT population 73 Astrup A, et al. Lancet. 2009 Nov 7;374(9701):1606-16.
GLP1-R is widely expressed in hypothalamic nuclei
GLP1-R
GLP1-R
GLP1-R
GLP1-R
GLP1-R
What’s about pharmacology? Liraglutide
Beiroa D et al (2014). Diabetes
The VMH AMPK-SNS-BAT axis: a canonical pathway
Contreras C et al (2014). Ann Med (in press)
• A novel GLUCAGON/GLP-1 AGONIST ELIMINATES OBESITY IN RODENTS.
• M.Tschop.....R.Nogueiras.....R.DiMarchi (Nat Chem Biol
Oct 2009)hem Biol. 2009 Oct;5(10):749-57.
Complementary Actions of Dual Incretin PharmacologyGLP-1R agonists act directly on pancreatic islets to enhance insulin production and secretion, and in neuronal circuitries to reduce food intake. ...
Brian Finan, Timo D. Müller, Christoffer Clemmensen, Diego Perez-Tilve, Richard D. DiMarchi, Matthias H. Tschöp
Trends Mol Med 2016
Effect of long‐term liraglutide and RM‐493, a MC4-R agonist, co‐treatment on obesity and glucose metabolism in DIO mice A–F22 days of treatment of DIO male mice .
Christoffer Clemmensen et al. EMBO Mol Med. 2015;7:288-298
©2015 by European Molecular Biology Organization
Unimolecular triagonism maximizes metabolic
benefits compared with dual incretin coagonism. • A chimera with high affinitty binding to
receptors for: GLP-1 , GIP and glucagon. • More powerful than co-agonist. • (Finan B et al Nat Medcine 2015)
Potential Anti-obesity Drugs and Their Pathways Complex System with Redundancy-That’s Why It’s Hard to Lose
Valentino MA, Lin JE, Waldman SA. Clin Pharm & Therapeutics (2010) 87 6, 652–662. doi:10.1038/clpt.2010.57 Endogenous Signaling of Appetite-regulating Hormones, Neuropeptides, and Neurotransmitters, and The Drugs That Target These Pathways 86
Funded by:
Diego Pérez-Tilve Paul Pfluger
Matthias Tschöp
Rosangela Deoliveira Asish Saha
Clara Álvarez Pablo Blanco
Luz Casas Rosalía Gallego Marta Garrido Ruth González Ricardo Lage Luís Martins
Susana Sangiao Sulay Tovar Luis Varela
María J. Vázquez Douglas Velásquez
Amparo Romero Sulay Tovar
Miguel López Ruben Nogueiras
Margaret Blount Mark Campbell Janice Carter Chris Lelliott Gema Medina
Sergio Rodríguez Sam Virtue
Andy Whittle
Antonio Vidal-Puig
David Carling
Consortiums:
University of Geneva Chrystelle Veyrax-Duberaux Françoise Rohner-Jeanrenaud
UT Southwestern, Dallas Joel K. Elmquist
Beth Israel Medical Center, Boston Bradford B. Lowell
University of Iowa Kamal Rhamouni Donald A. Morgan
German Institute of Human Nutrition Potsdam-Rehbruecke Hans-Georg Joost Annette Schurmmann
Consortiums:
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