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Drugs & Supplements Therapy in
Obesity Management
Dhani Isti - Ikhsan
Why using drugs?
I : BMI > 30 kg/m2 or BMI >27 kg/m2 w/
additional complicating factor(s)
I : Sudden weight gain 10-15 kg
• Reduced BW Maintained for 1-2 years at
minimum
• Reduce <10% of BW  reducing 25% risk of
comorbidities
Role of drugs
• Reduce appetite
• Reduce fat absorption
• Increase energy expenditure
 Reduction of comorbidities
General Precaution
Contraindication
Pregnancy, breast-feeding
Unstable cardiac disease
Uncontrolled hypertension (SBP > 180
mmHg, DBP > 110 mmHg)
Unstable severe systemic illness
History of anorexia nervosa
Active severe psychiatric disorder
Other drug therapy, if incompatible (e.g.
monoamine oxidase inhibitors,
antimigraine
drugs, adrenergic agents, drugs with
arrhythmia potential)
Caution
Presence of any severe systemic illness
History of severe psychiatric disorder
Other drug therapy
Closed angle glaucoma
Age < 18 years or > 65 years
Atkinson RL. Management of obesity:pharmacotherapy. In: Kopelman PG, Caterson ID,
Dietz WH (ed.). Clinical obesity in adults and children. 2nd ed. Oxford: Blackwell
Publishing Ltd; 2005. p.380-9
Type of drugs
• Lipase inhibitor
– Orlistat
– Cetilistat (under development) : fewer adverse
effect
• Amylase inhibitor
– α-glucosidase inhibitor (Acarbose) : only
significant in type 2 diabetes patient
• Biguanid : Metformin
Type of drugs
• Hormones
– HGH :mostly reduce visceral fat (!)cardiac changes
– Testosterone: reduce visceral fat
• Adrenergic agonist
– methamphetamin
• Serotonin agonist
– Sibutramin
Orlistat
• Approved by U.S. FDA : 60 mg in package,
3x/day, may be used for BMI >25kg/m2 (WHO
std)
• Mechanism of action :
– Blocks the action of pancreatic lipase, reducing
tryglyceride digestion and absorption
• Benefit :
– LDL reduction
Coutinho W. The first decade of sibutramine and orlistat: a reappraisal of their expanding roles
in the treatment of obesity and associated conditions. Arq Bras Endocrinol Metab. 2009;53/2
Side effects
Blockage of triglyceride digestion
• Fecal fat loss & GI symptomps
• Small-significant ↓ fat-soluble vitamins (Only
statistically significant for Vit. E
Contraindication
• Pregnancy
• Breastfeeding
• Cholestasis
Pharmacological interaction
• Safe w/ oral contraceptive in healthy women
• Reduce cyclosporin absorpstion
?Sibutramin?
• Mech. Of action: katekolaminergik &
serotoninergik
– Noradrenaline & 5-hydroxyttryptamine reuptake
inhibitor  increase satiety
• activation of sympathetic nervous system
trough β3-adrenergic receptors  increasing
metabolic rates & energy expenditures
Disadvantage
• Increase heart rate, blood pressure &
cardiovascular events
• Common effects:
– Insomnia, headache, dry mouth, constipation
• Serious effects : Seizure, gallstone, manic
episode in bipolar pts.
• Banned by FDA since 2010
References
1. Bray GA, Van Gaal LF. Drugs that modify fat absorption and
alter metabolism. In: Bray GA, Bouchard C (ed.). Handbook
of obesity: clinical applications. 3rd ed. New York: Informa
Healthcare; 2008. p.315-29
2. Atkinson RL. Management of obesity:pharmacotherapy. In:
Kopelman PG, Caterson ID, Dietz WH (ed.). Clinical obesity in
adults and children. 2nd ed. Oxford: Blackwell Publishing Ltd;
2005. p.380-9
3. Coutinho W. The first decade of sibutramine and orlistat: a
reappraisal of their expanding roles in the treatment of
obesity and associated conditions. Arq Bras Endocrinol
Metab. 2009;53/2
4. Sibutramine. [online] 10 Jan 2010. Diunduh dari:
http://www.nlm.nih.gov/medlineplus/druginfo/meds/a6011
10.html
• Mediator inflamasi berlebihan  merusak
hormon  resistensi insulin
• HGH  efisiensinya (?)  lipolisis & protein
sintesis  adiposit  TG  FFA & gliserol 
meningkat  cardiovascular disease

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Topic Discussion: Drugs Therapy in Obesity Management

  • 1. Drugs & Supplements Therapy in Obesity Management Dhani Isti - Ikhsan
  • 2. Why using drugs? I : BMI > 30 kg/m2 or BMI >27 kg/m2 w/ additional complicating factor(s) I : Sudden weight gain 10-15 kg • Reduced BW Maintained for 1-2 years at minimum • Reduce <10% of BW  reducing 25% risk of comorbidities
  • 3. Role of drugs • Reduce appetite • Reduce fat absorption • Increase energy expenditure  Reduction of comorbidities
  • 4. General Precaution Contraindication Pregnancy, breast-feeding Unstable cardiac disease Uncontrolled hypertension (SBP > 180 mmHg, DBP > 110 mmHg) Unstable severe systemic illness History of anorexia nervosa Active severe psychiatric disorder Other drug therapy, if incompatible (e.g. monoamine oxidase inhibitors, antimigraine drugs, adrenergic agents, drugs with arrhythmia potential) Caution Presence of any severe systemic illness History of severe psychiatric disorder Other drug therapy Closed angle glaucoma Age < 18 years or > 65 years Atkinson RL. Management of obesity:pharmacotherapy. In: Kopelman PG, Caterson ID, Dietz WH (ed.). Clinical obesity in adults and children. 2nd ed. Oxford: Blackwell Publishing Ltd; 2005. p.380-9
  • 5. Type of drugs • Lipase inhibitor – Orlistat – Cetilistat (under development) : fewer adverse effect • Amylase inhibitor – α-glucosidase inhibitor (Acarbose) : only significant in type 2 diabetes patient • Biguanid : Metformin
  • 6. Type of drugs • Hormones – HGH :mostly reduce visceral fat (!)cardiac changes – Testosterone: reduce visceral fat • Adrenergic agonist – methamphetamin • Serotonin agonist – Sibutramin
  • 7. Orlistat • Approved by U.S. FDA : 60 mg in package, 3x/day, may be used for BMI >25kg/m2 (WHO std) • Mechanism of action : – Blocks the action of pancreatic lipase, reducing tryglyceride digestion and absorption • Benefit : – LDL reduction
  • 8. Coutinho W. The first decade of sibutramine and orlistat: a reappraisal of their expanding roles in the treatment of obesity and associated conditions. Arq Bras Endocrinol Metab. 2009;53/2
  • 9. Side effects Blockage of triglyceride digestion • Fecal fat loss & GI symptomps • Small-significant ↓ fat-soluble vitamins (Only statistically significant for Vit. E Contraindication • Pregnancy • Breastfeeding • Cholestasis
  • 10. Pharmacological interaction • Safe w/ oral contraceptive in healthy women • Reduce cyclosporin absorpstion
  • 11. ?Sibutramin? • Mech. Of action: katekolaminergik & serotoninergik – Noradrenaline & 5-hydroxyttryptamine reuptake inhibitor  increase satiety • activation of sympathetic nervous system trough β3-adrenergic receptors  increasing metabolic rates & energy expenditures
  • 12. Disadvantage • Increase heart rate, blood pressure & cardiovascular events • Common effects: – Insomnia, headache, dry mouth, constipation • Serious effects : Seizure, gallstone, manic episode in bipolar pts. • Banned by FDA since 2010
  • 13. References 1. Bray GA, Van Gaal LF. Drugs that modify fat absorption and alter metabolism. In: Bray GA, Bouchard C (ed.). Handbook of obesity: clinical applications. 3rd ed. New York: Informa Healthcare; 2008. p.315-29 2. Atkinson RL. Management of obesity:pharmacotherapy. In: Kopelman PG, Caterson ID, Dietz WH (ed.). Clinical obesity in adults and children. 2nd ed. Oxford: Blackwell Publishing Ltd; 2005. p.380-9 3. Coutinho W. The first decade of sibutramine and orlistat: a reappraisal of their expanding roles in the treatment of obesity and associated conditions. Arq Bras Endocrinol Metab. 2009;53/2 4. Sibutramine. [online] 10 Jan 2010. Diunduh dari: http://www.nlm.nih.gov/medlineplus/druginfo/meds/a6011 10.html
  • 14. • Mediator inflamasi berlebihan  merusak hormon  resistensi insulin • HGH  efisiensinya (?)  lipolisis & protein sintesis  adiposit  TG  FFA & gliserol  meningkat  cardiovascular disease