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STEREOISOMERS
Dr.ARAVINDA KUMAR.B
Dept. of Pharmacology,
PIMS.
OUTLINE
 INTRODUCTION
 HISTORY OF CHIRALTY
 TYPES & NOMENCLATURE OF ISOMERS
 CHIRAL DRUGS – INTRODUCTION
 FDA REGULATIONS IN DEVELOPING CHIRAL DRUGS
 ROLE OF STEREOISOMERS IN PHARMACOLOGY –
KINETICS, DYNAMICS, ADVERSE EFFECTS
 PHARMACEUTICAL INDUSTRY & CHIRAL DRUGS
 SUMMARY
…….. “DRUGS” do something in our body as a result of
their molecular structure, which determines:
 Physicochemical properties
 Chemical / biochemical reactivity
 Shape
 STEREOCHEMISTRY
STEREOISOMERS
• Stereoisomers are molecules with one or more
“chiral” centres that allow the possibility of forms
with the same chemical formula but differing
spatial arrangements.
STEREOISOMERS
GEOMETRIC
ISOMERS
OPTICAL
ISOMERS
ENANTIOMERS DIASTEREOISOMERS
HISTORY
CHEIR means “hand” in Greek
Terminologies
 A compound containing an equal proportion of
each enantiomer is called a racemic mixture.
 Chiral switching - development of single
enantiomers from old racemate drugs
 Chiral inversion is the conversion of one
stereoisomeric form into another (ie, R-ibuprofen
to S-ibuprofen)
NOMENCLATURE – 3ways
 According to rotation of polarized light
(+) and (-); dextro or levo rotatory
 D/L – w.r.t glyceraldehyde
 R/S enantiomers - Cahn-Ingold-Prelog priority
rules
CHIRAL DRUGS -Easson-Stedman
Model (1993)
Greatest differences between a pair of enantiomers occur at
the level of receptor interactions.
 Eutomer: enantiomer with higher affinity/activity.
 Distomer: enantiomer with lower affinity/activity.
 Eudismic Ratio: Ratio of the Eutomer/Distomer affinities
or activities.
Racemic drugs with one major
bioactive enantiomers
 Cardiovascular drugs – BBs, CCBs, ACE
inhibitors
 Neurology/Psychiatric drugs – barbiturates,
opiates, anticonvulsants, psychostimulants
 Others – anti-arrhythmics, antibiotics,
hypolipidemics, PPIs, anticoagulants,
antihistamines
Racemic drugs with equally
bioactive enantiomers
 cyclophosphamide (antineoplastic)
 flecainide (antiarrhythmic)
 fluoxetine (antidepressant)
Racemic drugs with chiral
inversion
 Unidirectional - NSAIDS (S-isomer 100 times
more potent )
 Bidirectional - 3-hydroxy-benzodiazepines
(oxazepam, lorazepam, temazepam) and
thalidomide
Advantages of Chiral
switching
 Separating unwanted PD side effects from toxic
effects if these reside exclusively in one
enantiomer
 Expose the patient to less body load and thus
reduce metabolic/hepatic/renal dug load
 Easier assesment of physiology, disease and drug
co-administration effects
Advantages of Chiral
switching…
 Reduce DI / avoid enantiomer-enantiomer
interaction/ avoid bioinversion
 Easier assessment of efficacy & toxicity through
PD/PK monitoring of pure enantiomers
PHARMACOKINETIC &
PHARMACODYNAMIC IMPLICATIONS
OF CHIRALTY
 Bioavailability (esomeprazole)
 Volume of distribution (Levocetrizine)
 Drug metabolizing enzyme systems – differ in
rates of metabolism
 Cytochrome enzyme induction or inhibition
CHIRAL - formulations &
excipients
 Improve solubility, dissolution and stability
 Celluloses / Starch, sugars & derivatives /
Cyclodextrins / Acids / Amino acids, peptides &
derivatives / Fats, oils and essential oils
CHIRALTY – Role in Kinetics &
Dynamics
 Selective beta-1 activity is enhanced (even in
higher doses)
 CYP2D6 polymorphism
S-atenolol S-metoprolol
CHIRALTY – Role in Kinetics &
Dynamics
 Independent of CYP2C19
 Metabolized by CYP3A4/sulfotransferases
CHIRALTY – Role in Kinetics &
Dynamics
 Small Vd
 Low hemato-encephalic barrier passage; low cerebral receptor binding
 Enhanced specific periphery H1 receptor binding
 2-3 times more potent than racemic
 Rapidly eliminated (R-isomer inhibits S-isomer’s elimination)
 Smoother emergence period, profound post-op analgesia, more rapid recovery of cerebral
function
 Psychotomimetic phenomenon – negligibly less.
CHIRALTY – Role in Kinetics &
Dynamics
ROLE OF CHIRAL DRUGS IN
PREVENTING ADRs
(CH3)2CHCH2
COOH
H
CH3 CH2CH(CH3)2
HOOC
H
H3C
(-)-(R)-ibuprofen (+)-(S)-ibuprofen
ROLE OF CHIRAL DRUGS IN
PREVENTING ADRs
 Most widely used long acting local anesthetic
 Fatal cardiotoxicity – racemate.
ROLE OF CHIRAL DRUGS IN
PREVENTING ADRs
Chiral
inversion
ROLE OF CHIRAL DRUGS IN
PREVENTING ADRs
- Vasodilation
- Increased t1/2
- Decreased peripheral edema
- Safer & long acting
ROLE OF CHIRAL DRUGS IN
PREVENTING ADRs
ROLE OF CHIRAL DRUGS IN
PREVENTING ADRs
• Levorotatory R-salbutamol & dextrorotatory S-salbutamol
• S-salbutamol -- increases airway hyper-reactivity
ROLE OF CHIRAL DRUGS IN
PREVENTING ADRs
• R-Albuterol (levalbuterol)– bronchodilator activity
• S-Albuterol - antagonizes the effect of R-albuterol, pro-inflammatory effects.
ROLE OF CHIRAL DRUGS IN
PREVENTING ADRs
Wilson’s disease blindness & toxic
FAILURES OF CHIRAL
SWITCHING
 Fenfluramine/dexfenfluramine
 Sotalol
 Dilevalol
 Fluoxetine
DILEVALOL – R,R isomer of labetalol
(hepatotoxic)
Chiral Switch : Problems
 Sotalol (-) VS (+)
 (-)- enantiomer 14 to 50 fold more potent
as a β-blocker; equipotent as
antiarrhythmic.
 SWORD trial
Chiral Switch : Problems
Chiral Switch : Problems
 Dexfenfluramine / Fenfluramine:
anoretic agent; racemic drug had been
available for 25 years.
 Valvular heart disease & Pulmonary
hypertension (FEN-PHEN)
 Both single enantiomer and racemate
voluntarily withdrawn.
PHARMACEUTICAL INDUSTRY &
CHIRAL SWITCHES
 Launching chirally pure drugs from racemates –
time & monetory investments on its chemical
separation and clinical evaluation
 Ensure its return on investments
 Innovation in health care system and merits
incentives in the form of patents.
REFERENCES
 Patil PA, Kothekar MA. Development of safer
molecules through chirality. Indian J Med
Sci.2006 Oct;60(10):427-37
 Lien AN, Hua H, Chuong PH. Chiral Drugs: An
Overview. Int J Biomed Sci. 2006 June; 2(2): 85-
100
 Tucker GT. Chiral switches. Lancet
2000;355:1085-7
 Burke D, Henderson DJ. Chiralty: a blue print for
the future. J Anaesth 2002;88:563-76
Stereoisomers

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Stereoisomers

  • 2. OUTLINE  INTRODUCTION  HISTORY OF CHIRALTY  TYPES & NOMENCLATURE OF ISOMERS  CHIRAL DRUGS – INTRODUCTION  FDA REGULATIONS IN DEVELOPING CHIRAL DRUGS  ROLE OF STEREOISOMERS IN PHARMACOLOGY – KINETICS, DYNAMICS, ADVERSE EFFECTS  PHARMACEUTICAL INDUSTRY & CHIRAL DRUGS  SUMMARY
  • 3. …….. “DRUGS” do something in our body as a result of their molecular structure, which determines:  Physicochemical properties  Chemical / biochemical reactivity  Shape  STEREOCHEMISTRY
  • 4. STEREOISOMERS • Stereoisomers are molecules with one or more “chiral” centres that allow the possibility of forms with the same chemical formula but differing spatial arrangements.
  • 8.
  • 9. Terminologies  A compound containing an equal proportion of each enantiomer is called a racemic mixture.  Chiral switching - development of single enantiomers from old racemate drugs  Chiral inversion is the conversion of one stereoisomeric form into another (ie, R-ibuprofen to S-ibuprofen)
  • 10. NOMENCLATURE – 3ways  According to rotation of polarized light (+) and (-); dextro or levo rotatory  D/L – w.r.t glyceraldehyde  R/S enantiomers - Cahn-Ingold-Prelog priority rules
  • 11.
  • 13. Greatest differences between a pair of enantiomers occur at the level of receptor interactions.  Eutomer: enantiomer with higher affinity/activity.  Distomer: enantiomer with lower affinity/activity.  Eudismic Ratio: Ratio of the Eutomer/Distomer affinities or activities.
  • 14.
  • 15.
  • 16. Racemic drugs with one major bioactive enantiomers  Cardiovascular drugs – BBs, CCBs, ACE inhibitors  Neurology/Psychiatric drugs – barbiturates, opiates, anticonvulsants, psychostimulants  Others – anti-arrhythmics, antibiotics, hypolipidemics, PPIs, anticoagulants, antihistamines
  • 17.
  • 18. Racemic drugs with equally bioactive enantiomers  cyclophosphamide (antineoplastic)  flecainide (antiarrhythmic)  fluoxetine (antidepressant)
  • 19. Racemic drugs with chiral inversion  Unidirectional - NSAIDS (S-isomer 100 times more potent )  Bidirectional - 3-hydroxy-benzodiazepines (oxazepam, lorazepam, temazepam) and thalidomide
  • 20. Advantages of Chiral switching  Separating unwanted PD side effects from toxic effects if these reside exclusively in one enantiomer  Expose the patient to less body load and thus reduce metabolic/hepatic/renal dug load  Easier assesment of physiology, disease and drug co-administration effects
  • 21. Advantages of Chiral switching…  Reduce DI / avoid enantiomer-enantiomer interaction/ avoid bioinversion  Easier assessment of efficacy & toxicity through PD/PK monitoring of pure enantiomers
  • 22. PHARMACOKINETIC & PHARMACODYNAMIC IMPLICATIONS OF CHIRALTY  Bioavailability (esomeprazole)  Volume of distribution (Levocetrizine)  Drug metabolizing enzyme systems – differ in rates of metabolism  Cytochrome enzyme induction or inhibition
  • 23. CHIRAL - formulations & excipients  Improve solubility, dissolution and stability  Celluloses / Starch, sugars & derivatives / Cyclodextrins / Acids / Amino acids, peptides & derivatives / Fats, oils and essential oils
  • 24.
  • 25. CHIRALTY – Role in Kinetics & Dynamics  Selective beta-1 activity is enhanced (even in higher doses)  CYP2D6 polymorphism S-atenolol S-metoprolol
  • 26. CHIRALTY – Role in Kinetics & Dynamics  Independent of CYP2C19  Metabolized by CYP3A4/sulfotransferases
  • 27. CHIRALTY – Role in Kinetics & Dynamics  Small Vd  Low hemato-encephalic barrier passage; low cerebral receptor binding  Enhanced specific periphery H1 receptor binding
  • 28.  2-3 times more potent than racemic  Rapidly eliminated (R-isomer inhibits S-isomer’s elimination)  Smoother emergence period, profound post-op analgesia, more rapid recovery of cerebral function  Psychotomimetic phenomenon – negligibly less. CHIRALTY – Role in Kinetics & Dynamics
  • 29.
  • 30.
  • 31. ROLE OF CHIRAL DRUGS IN PREVENTING ADRs (CH3)2CHCH2 COOH H CH3 CH2CH(CH3)2 HOOC H H3C (-)-(R)-ibuprofen (+)-(S)-ibuprofen
  • 32. ROLE OF CHIRAL DRUGS IN PREVENTING ADRs  Most widely used long acting local anesthetic  Fatal cardiotoxicity – racemate.
  • 33. ROLE OF CHIRAL DRUGS IN PREVENTING ADRs Chiral inversion
  • 34. ROLE OF CHIRAL DRUGS IN PREVENTING ADRs - Vasodilation - Increased t1/2 - Decreased peripheral edema - Safer & long acting
  • 35. ROLE OF CHIRAL DRUGS IN PREVENTING ADRs
  • 36. ROLE OF CHIRAL DRUGS IN PREVENTING ADRs • Levorotatory R-salbutamol & dextrorotatory S-salbutamol • S-salbutamol -- increases airway hyper-reactivity
  • 37. ROLE OF CHIRAL DRUGS IN PREVENTING ADRs • R-Albuterol (levalbuterol)– bronchodilator activity • S-Albuterol - antagonizes the effect of R-albuterol, pro-inflammatory effects.
  • 38. ROLE OF CHIRAL DRUGS IN PREVENTING ADRs Wilson’s disease blindness & toxic
  • 39. FAILURES OF CHIRAL SWITCHING  Fenfluramine/dexfenfluramine  Sotalol  Dilevalol  Fluoxetine
  • 40. DILEVALOL – R,R isomer of labetalol (hepatotoxic)
  • 41. Chiral Switch : Problems  Sotalol (-) VS (+)  (-)- enantiomer 14 to 50 fold more potent as a β-blocker; equipotent as antiarrhythmic.  SWORD trial
  • 42. Chiral Switch : Problems
  • 43. Chiral Switch : Problems  Dexfenfluramine / Fenfluramine: anoretic agent; racemic drug had been available for 25 years.  Valvular heart disease & Pulmonary hypertension (FEN-PHEN)  Both single enantiomer and racemate voluntarily withdrawn.
  • 44. PHARMACEUTICAL INDUSTRY & CHIRAL SWITCHES  Launching chirally pure drugs from racemates – time & monetory investments on its chemical separation and clinical evaluation  Ensure its return on investments  Innovation in health care system and merits incentives in the form of patents.
  • 45.
  • 46. REFERENCES  Patil PA, Kothekar MA. Development of safer molecules through chirality. Indian J Med Sci.2006 Oct;60(10):427-37  Lien AN, Hua H, Chuong PH. Chiral Drugs: An Overview. Int J Biomed Sci. 2006 June; 2(2): 85- 100  Tucker GT. Chiral switches. Lancet 2000;355:1085-7  Burke D, Henderson DJ. Chiralty: a blue print for the future. J Anaesth 2002;88:563-76

Hinweis der Redaktion

  1. Louis Pasteur (1848-1853) - studied tartaric acid Isolated differing crystal types by hand – differing physical appearance of the salt crystals recognized that two of the isomers polarized light differently
  2. Left handed molecule bind with left handed receptor., chiral centre – C,P (cyclophosphamide),S (sulindac) ---- no.of isomers – 2 power n.
  3. ADME – influenced by chirality.
  4. R – depression, S-= migraine; R- cardiac toxicity (prolong QT interval)