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Biotransformation
(Metabolism) of Drugs
A.    General properties

1. Biotransformation is a major mechanism for drug
   elimination;

•    Results of biotransformation:
    – Production of metabolites that are more polar than
       the parent drug
    – usually terminates the pharmacologic action of the
       parent drug
    – After phase I reactions, similar or different
       pharmacologic activity, or toxicologic activity.
Results of biotransformation
2.    Many drugs undergo
     – several sequential biotransformation reactions.
     – Biotransformation is catalyzed by specific enzyme systems


2.    Sites of biotransformation:
     – The liver: the major site
     – other tissues.
4. Biotransformation of drugs can be affected by many
   parameters, including:

  A.   prior administration of the drug in question or of other drugs
  B.   diet
  C.   hormonal status
  D.   genetics
  E.   disease (e.g., decreased in cardiac and pulmonary disease)
  F.   age and developmental status
  G.   liver function
5. Possible consequences of biotransformation
   include the production of:
  –   inactive metabolites (most common)
  –   metabolites with increased or decreased potencies
  –   metabolites with qualitatively different
      pharmacologic actions
  –   toxic metabolites
  –   active metabolites from inactive prodrugs.
• Metabolites are often more polar than the parent
  compounds.

• This increased polarity may lead to:

   – a more rapid rate of clearance because of possible
     secretion by acid or base carriers in the kidney

   – it may lead to decreased tubular reabsorption.
B.    Classification of biotransformation reactions

1. Reactions that involve enzyme-catalyzed
   biotransformation of the drug without any conjugations.

• Phase I reactions include:
  – oxidations
  – reductions
  – hydrolysis reactions


• they introduce a functional group (e.g., -OH) that serves
  as the active center for sequential conjugation in a
  phase II reaction.
2. Reactions that include conjugation reactions, which
   involve the enzyme-catalyzed combination of a drug (or
   drug metabolite) with an endogenous substance.

•   Phase II reactions require:
    – a functional group—an active center—as the site of
      conjugation with the endogenous substance.

    – energy indirectly for the synthesis of “activated
      carriers,” the form of the endogenous substance used
      in the conjugation reaction (e.g., UDP-glucuronate).
Drug metabolism reactions :
C.       Enzymes catalyzing phase I biotransformation
                          reactions
 Enzymes catalyzing phase I biotransformation
  reactions include:

     –   cytochrome P-450
     –   aldehyde and alcohol dehydrogenase
     –   deaminases
     –   esterases
     –   amidases
     –   epoxide hydratases
 Enzymes catalyzing phase II biotransformation
  reactions include:
   – glucuronyl transferase (glucuronide conjugation)
   – sulfotransferase (sulfate conjugation)
   – transacylases (amino acid conjugation)
   – acetylases
   – ethylases
   – methylases
   – glutathione transferase.
• Location of these enzymes:
   – numerous tissues
   – some are present in plasma.


• Subcellular locations include:
   – cytosol
   – mitochondria
   – endoplasmic reticulum


• Only those enzymes located in the endoplasmic
  reticulum are inducible by drugs
1.    Cytochrome P-450 monooxygenase
                  (mixed function oxidase)

a.   General features

•    A large number of families (at least 18 in mammals) of
     cytochrome P-450 (abbreviated “CYP”) enzymes
     exists
•    each member of which catalyzes the biotransformation
     of a unique spectrum of drugs
•    some overlap in the substrate specificities.

•    This enzyme system is the one most frequently
     involved in phase I reactions.
•   The cytochrome P-450 families are referred to using
    an arabic numeral, e.g., CYP1, CYP2, etc.

•   Each family has a number of subfamilies denoted by
    an upper case letter, e.g., CYP2A, CYP2B, etc.

•   The individual enzymes within each subfamily are
    denoted by another arabic numeral, e.g., CYP3A1,
    CYP3A2, etc.
•   Cytochrome P-450 catalyzes numerous reactions,
    including:

    –   aromatic and aliphatic hydroxylations
    –   dealkylations at nitrogen, sulfur, and oxygen atoms
    –   heteroatom oxidations at nitrogen and sulfur atoms
    –   reductions at nitrogen atoms
    –   ester and amide hydrolysis
•    The CYP3A subfamily is:

    – responsible for up to half of the total cytochrome P-
      450 in the liver

    – accounts for approximately 50% of the metabolism of
      clinically important drugs.

    – CYP3A4 is a particularly abundant enzyme.
representative P450 isozymes.
b. Localization

• The primary location of cytochrome P-450 is the liver,

• Other tissues, including:
   – the adrenals
   – ovaries and testis
   – tissues involved in steroidogenesis and steroid metabolism.


• The enzyme's subcellular location is the endoplasmic
  reticulum.
c.    Mechanism of reaction
1.    In the overall reaction:
     – the drug is oxidized
     – oxygen is reduced to water.
•     Reducing equivalents are provided by nicotinamide
      adenine dinucleotide phosphate (NADPH), and
      generation of this cofactor is coupled to cytochrome
      P-450 reductase.
Metabolism of phenytoin :

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Biotransformation (metabolism) of drugs

  • 2. A. General properties 1. Biotransformation is a major mechanism for drug elimination; • Results of biotransformation: – Production of metabolites that are more polar than the parent drug – usually terminates the pharmacologic action of the parent drug – After phase I reactions, similar or different pharmacologic activity, or toxicologic activity.
  • 4.
  • 5. 2. Many drugs undergo – several sequential biotransformation reactions. – Biotransformation is catalyzed by specific enzyme systems 2. Sites of biotransformation: – The liver: the major site – other tissues.
  • 6. 4. Biotransformation of drugs can be affected by many parameters, including: A. prior administration of the drug in question or of other drugs B. diet C. hormonal status D. genetics E. disease (e.g., decreased in cardiac and pulmonary disease) F. age and developmental status G. liver function
  • 7. 5. Possible consequences of biotransformation include the production of: – inactive metabolites (most common) – metabolites with increased or decreased potencies – metabolites with qualitatively different pharmacologic actions – toxic metabolites – active metabolites from inactive prodrugs.
  • 8. • Metabolites are often more polar than the parent compounds. • This increased polarity may lead to: – a more rapid rate of clearance because of possible secretion by acid or base carriers in the kidney – it may lead to decreased tubular reabsorption.
  • 9. B. Classification of biotransformation reactions 1. Reactions that involve enzyme-catalyzed biotransformation of the drug without any conjugations. • Phase I reactions include: – oxidations – reductions – hydrolysis reactions • they introduce a functional group (e.g., -OH) that serves as the active center for sequential conjugation in a phase II reaction.
  • 10. 2. Reactions that include conjugation reactions, which involve the enzyme-catalyzed combination of a drug (or drug metabolite) with an endogenous substance. • Phase II reactions require: – a functional group—an active center—as the site of conjugation with the endogenous substance. – energy indirectly for the synthesis of “activated carriers,” the form of the endogenous substance used in the conjugation reaction (e.g., UDP-glucuronate).
  • 12. C. Enzymes catalyzing phase I biotransformation reactions  Enzymes catalyzing phase I biotransformation reactions include: – cytochrome P-450 – aldehyde and alcohol dehydrogenase – deaminases – esterases – amidases – epoxide hydratases
  • 13.  Enzymes catalyzing phase II biotransformation reactions include: – glucuronyl transferase (glucuronide conjugation) – sulfotransferase (sulfate conjugation) – transacylases (amino acid conjugation) – acetylases – ethylases – methylases – glutathione transferase.
  • 14. • Location of these enzymes: – numerous tissues – some are present in plasma. • Subcellular locations include: – cytosol – mitochondria – endoplasmic reticulum • Only those enzymes located in the endoplasmic reticulum are inducible by drugs
  • 15. 1. Cytochrome P-450 monooxygenase (mixed function oxidase) a. General features • A large number of families (at least 18 in mammals) of cytochrome P-450 (abbreviated “CYP”) enzymes exists • each member of which catalyzes the biotransformation of a unique spectrum of drugs • some overlap in the substrate specificities. • This enzyme system is the one most frequently involved in phase I reactions.
  • 16. The cytochrome P-450 families are referred to using an arabic numeral, e.g., CYP1, CYP2, etc. • Each family has a number of subfamilies denoted by an upper case letter, e.g., CYP2A, CYP2B, etc. • The individual enzymes within each subfamily are denoted by another arabic numeral, e.g., CYP3A1, CYP3A2, etc.
  • 17. Cytochrome P-450 catalyzes numerous reactions, including: – aromatic and aliphatic hydroxylations – dealkylations at nitrogen, sulfur, and oxygen atoms – heteroatom oxidations at nitrogen and sulfur atoms – reductions at nitrogen atoms – ester and amide hydrolysis
  • 18. The CYP3A subfamily is: – responsible for up to half of the total cytochrome P- 450 in the liver – accounts for approximately 50% of the metabolism of clinically important drugs. – CYP3A4 is a particularly abundant enzyme.
  • 20. b. Localization • The primary location of cytochrome P-450 is the liver, • Other tissues, including: – the adrenals – ovaries and testis – tissues involved in steroidogenesis and steroid metabolism. • The enzyme's subcellular location is the endoplasmic reticulum.
  • 21. c. Mechanism of reaction 1. In the overall reaction: – the drug is oxidized – oxygen is reduced to water. • Reducing equivalents are provided by nicotinamide adenine dinucleotide phosphate (NADPH), and generation of this cofactor is coupled to cytochrome P-450 reductase.