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5:
Video 1 – Drug
Administration
LAS20061 – Lecture 5
Pharmacokinetics 1 – Drug Absorption and
Distribution
Routes of Administration
Enteral – via the GI tract (mouth
to rectum) to increase blood levels
Parenteral – avoiding the GI tract
to increase blood levels
Topical – at the site where the
drug is needed (avoiding increased
blood levels)
Enteral
Administration
Oral
Buccal,
Lingual
Rectal
 Convenient & cheap
 Absorption along whole GI Tract
 Hurdles to absorption
 First pass metabolism
 Effects on GI
 N&V, emergency situations
• High drug concentration
in portal vein cf
peripheral circulation
• High rate of enzyme
activity (because of
Michaelis Menten
kinetics)
• Large proportion of drug
removed from hepatic
circulation
Enteral
Administration
Oral
Buccal,
Lingual
Rectal
 Convenient & cheap
 Absorption along whole GI Tract
 Hurdles to absorption
 First pass metabolism
 Effects on GI
 N&V, emergency situations
 First pass
avoided
 Rapid absorption
 Low surface area
for absorption
 Mouth-
experience
 Small doses
 First-pass
reduced
 Rapid absorption
 Absorption
erratic
 Compliance
Parenteral
Administration
Injection
Inhalation
Topical
Intravenous Injection
Intramuscular Injection
Inhalation
ADVANTAGES
 LOCAL DELIVERY
 HIGHER
CONCENTRATIONS IN
TARGET ORGAN
 AVOID SYSTEMIC
Adverse Drug Responses
 NO FIRST PASS
METABOLISM
DISADVANTAGES
 DELIVERY CUMBERSOME
AND TIME CONSUMING
 COMPLIANCE
 DELIVERY SYSTEMS
COSTLY
 LOCAL IRRITATION RISK
 HARD TO USE IN
RESPIRATORY EMERGENCY
Video 2 – Drug
Absorption
LAS20061 – Lecture 5
Pharmacokinetics 1 – Drug Absorption and
Distribution
There are four main ways by which a small molecule can
cross a cell membrane:
A. Diffusion through the
lipid bilayer
B. Passive transport via
transporter proteins
C. Active transport via
pumps or co-
transporters
D. Vesicular transport
(pinocytosis, endo- and
exo-cytosis)
A. Diffusion through the
lipid bilayer
Extracellular Compartment Intracellular Compartment
Drugs diffuse from high concentration to low
• High extracellular concentrations drive absorption
• Drug solubility determines drug concentration available for absorption in GI tract
Cell
Membrane
Low Solubility Can Limit Absorption
Faeces
Blood
Stream
Blood
Stream
Low Absorption Can Limit Bioavailability
Faeces
Blood
Stream
Blood
Stream
Extracellular Compartment Intracellular Compartment
Lipophilicity and Absorption
• Lipophilicity determines a drug’s propensity to diffuse from the gut lumen into the cell
membrane…
• …and from the membrane into the cell cytoplasm
Cell
Membrane
Lipophilicity measured by LogP
Concentration
in octanol
Concentration
in water
LogP=log
[Drug]octanol
[Drug]water
LogP>0, [Drug]octanol > [Drug]water - lipophilic
LogP<0, [Drug]water > [Drug]octanol - hydrophilic
Lipophilicity affects rate of absorption
Drugs that are not rapidly
absorbed will be metabolised
and excreted before
intracellular concentrations
reach desired levels
When pKa=pH,
pKa-pH=0
10pKa-pH= 1
[BH+]=[B]
Lipophilicity measured by LogP
pH>pKa
(Low proton
concentration)
pH=pKa
pH<pKa
(High proton
concentration)
pKa-pH<0
10pKa-pH< 1
pKa-pH=0
10pKa-pH= 1
pKa-pH>0
10pKa-pH> 1
Weak Base [BH+]<[B] [BH+]=[B] [BH+]>[B]
Weak Acid [AH]<[A-] [AH]=[A-] [AH]>[A-]
Weak bases
absorbed better
Weak acids
absorbed better
• pH changes throughout the
intestine
• Drugs with different pKa will
be ionised to different
extents at different parts of
the intestine
• Absorption will be greatedt
when ionisation is lowest
• pKa will affect degree to
which drugs are absorbed
Gut pH affects ionisation and rate of absorption
Video 3 – Drug
Distribution
LAS20061 – Lecture 5
Pharmacokinetics 1 – Drug Absorption and
Distribution
Enable active pumping
of drugs out of brain Rich in metabolic enzymes –
destroy drugs entering the brain
logP = 1.52
Octanol:water = 38.0
logP = 0.43
Octanol:water = 7.4
Assuming same brain:plasma ratios, this allows >5-fold lower blood concentrations for the same
brain concentration. This reduces overall dose, and side effect risk – or alternatively, for the
same dose induces greater “recreational” effects.
In fact, Heroin is only ~2x more potent – other factors are also important
Case Study: Morphine and Heroin
Case Study: L-DOPA
LSC-20061 L5 - PK Absorption and distribution 2021.pdf

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LSC-20061 L5 - PK Absorption and distribution 2021.pdf

  • 1. 5:
  • 2. Video 1 – Drug Administration LAS20061 – Lecture 5 Pharmacokinetics 1 – Drug Absorption and Distribution
  • 3.
  • 4. Routes of Administration Enteral – via the GI tract (mouth to rectum) to increase blood levels Parenteral – avoiding the GI tract to increase blood levels Topical – at the site where the drug is needed (avoiding increased blood levels)
  • 5. Enteral Administration Oral Buccal, Lingual Rectal  Convenient & cheap  Absorption along whole GI Tract  Hurdles to absorption  First pass metabolism  Effects on GI  N&V, emergency situations
  • 6. • High drug concentration in portal vein cf peripheral circulation • High rate of enzyme activity (because of Michaelis Menten kinetics) • Large proportion of drug removed from hepatic circulation
  • 7. Enteral Administration Oral Buccal, Lingual Rectal  Convenient & cheap  Absorption along whole GI Tract  Hurdles to absorption  First pass metabolism  Effects on GI  N&V, emergency situations  First pass avoided  Rapid absorption  Low surface area for absorption  Mouth- experience  Small doses  First-pass reduced  Rapid absorption  Absorption erratic  Compliance
  • 11. Inhalation ADVANTAGES  LOCAL DELIVERY  HIGHER CONCENTRATIONS IN TARGET ORGAN  AVOID SYSTEMIC Adverse Drug Responses  NO FIRST PASS METABOLISM DISADVANTAGES  DELIVERY CUMBERSOME AND TIME CONSUMING  COMPLIANCE  DELIVERY SYSTEMS COSTLY  LOCAL IRRITATION RISK  HARD TO USE IN RESPIRATORY EMERGENCY
  • 12.
  • 13. Video 2 – Drug Absorption LAS20061 – Lecture 5 Pharmacokinetics 1 – Drug Absorption and Distribution
  • 14.
  • 15. There are four main ways by which a small molecule can cross a cell membrane: A. Diffusion through the lipid bilayer B. Passive transport via transporter proteins C. Active transport via pumps or co- transporters D. Vesicular transport (pinocytosis, endo- and exo-cytosis) A. Diffusion through the lipid bilayer
  • 16. Extracellular Compartment Intracellular Compartment Drugs diffuse from high concentration to low • High extracellular concentrations drive absorption • Drug solubility determines drug concentration available for absorption in GI tract Cell Membrane
  • 17. Low Solubility Can Limit Absorption Faeces Blood Stream Blood Stream
  • 18. Low Absorption Can Limit Bioavailability Faeces Blood Stream Blood Stream
  • 19. Extracellular Compartment Intracellular Compartment Lipophilicity and Absorption • Lipophilicity determines a drug’s propensity to diffuse from the gut lumen into the cell membrane… • …and from the membrane into the cell cytoplasm Cell Membrane
  • 20. Lipophilicity measured by LogP Concentration in octanol Concentration in water LogP=log [Drug]octanol [Drug]water LogP>0, [Drug]octanol > [Drug]water - lipophilic LogP<0, [Drug]water > [Drug]octanol - hydrophilic
  • 21. Lipophilicity affects rate of absorption Drugs that are not rapidly absorbed will be metabolised and excreted before intracellular concentrations reach desired levels
  • 22.
  • 24. Lipophilicity measured by LogP pH>pKa (Low proton concentration) pH=pKa pH<pKa (High proton concentration) pKa-pH<0 10pKa-pH< 1 pKa-pH=0 10pKa-pH= 1 pKa-pH>0 10pKa-pH> 1 Weak Base [BH+]<[B] [BH+]=[B] [BH+]>[B] Weak Acid [AH]<[A-] [AH]=[A-] [AH]>[A-] Weak bases absorbed better Weak acids absorbed better
  • 25. • pH changes throughout the intestine • Drugs with different pKa will be ionised to different extents at different parts of the intestine • Absorption will be greatedt when ionisation is lowest • pKa will affect degree to which drugs are absorbed Gut pH affects ionisation and rate of absorption
  • 26.
  • 27.
  • 28. Video 3 – Drug Distribution LAS20061 – Lecture 5 Pharmacokinetics 1 – Drug Absorption and Distribution
  • 29.
  • 30.
  • 31.
  • 32. Enable active pumping of drugs out of brain Rich in metabolic enzymes – destroy drugs entering the brain
  • 33.
  • 34.
  • 35.
  • 36. logP = 1.52 Octanol:water = 38.0 logP = 0.43 Octanol:water = 7.4 Assuming same brain:plasma ratios, this allows >5-fold lower blood concentrations for the same brain concentration. This reduces overall dose, and side effect risk – or alternatively, for the same dose induces greater “recreational” effects. In fact, Heroin is only ~2x more potent – other factors are also important Case Study: Morphine and Heroin
  • 37.