CHAPTER 4 – PHARMACOKINETICS, PHARMACODYNAMICS, AND DRUG
INTERACTIONS
PHARMACOKINETICS
The study of drug movement throughout the body
Four processes of pharmacokinetics: absorption, distribution, metabolism, and
excretion
Absorption is the movement of the drug from its site of administration into the blood
Distribution is the movement of the drug from the blood to the interstitial space of
tissues and into cells
Metabolism (biotransformation) is the enzymatically mediated alteration of drug
structure
Excretion is the movement of drugs and their metabolites out of the body
These processes determine the concentration of a drug at its sites of action
The intensity of the response to a drug is directly related to the concentration of the
drug at it site of action
Maximum beneficial effect is achieved with a concentration high enough to elicit the
desired response while avoiding concentrations that cause harm
PASSAGE OF DRUGS ACROSS MEMBRANES
Drugs must cross membranes to move throughout the body.
o Site of administration – bloodstream – site of action – metabolism – excretion
Cells are very close together so drugs usually pass through cells opposed to between
Therefore the ability of a drug to cross a biologic membrane is determined by its
ability to pass through single cells
Three ways to cross a membrane
Through channels or pores
Via a transport system
Direct penetration of the membrane (most common)
Channels and pores
Least common way for drugs to pass
Channels and pores are very small
Only the smallest compounds, like potassium and sodium, can pass through their
correct channels
Transport systems
Role is to move drugs from one side to the other
They are selective and dependent on drug structure
P-glycoprotein (PGP) aka multidrug transporter protein is a transmembrane protein
that transport several drugs OUT of cells
Direct penetration of the membrane
Occurs primarily
, Most drugs are too large to pass through channels and pores, and most lack transport
systems to help them cross all the membranes separating them from the sites of
action, metabolism, and excretion
“like dissolves like.” Membranes are mostly composed of lipids therefore a drug must
be lipid soluble (lipophilic) to directly penetrate.
POLAR MOLECULES AND IONS
Polar molecules and ions are not lipid soluble therefore cannot penetrate membranes
Polar molecules
Have no net charge
Instead have an uneven distribution of electrical charge, meaning the positive and
negative charges within congregate separately
Ex: water, the electrons (negative charges) spend more time in the vicinity of the
oxygen (-) atom than the two hydrogens (+), making the area around the oxygen
more negatively charged and the hydrogen more positively charged
Along with “like dissolves like,” polar molecules dissolve in polar solvents (such as
water) but not in nonpolar solvents (such as lipids)
Ions
Molecules with a positive or negative net electrical charge
Unable to cross membranes! Unless very small.
Must become nonionized to cross
Many drugs are either charged or uncharged weak organic bases or weak organic
acids. The electrical charge it has is determined by the pH of the surrounding
medium
o Acids tend to ionize in basic (alkaline) media
o Bases tend to ionize in acidic media
o Therefore weak acids absorb best in acid environment (ex: gastric acid)
because they remain nonionized
o Ex: aspirin molecules pass from stomach into small intestine where it is more
alkaline, changing the molecules to ionized form, impeding absorption of
aspirin from the intestine
pH partitioning (ion trapping)
The process of drug accumulation on the side of the membrane where the pH favors
its ionization
When there is a difference in pH between two sides of a membrane, drug molecules
tend to accumulate on the side where pH favors their ionization
o Acidic drugs accumulate on alkaline side
o Basic drugs accumulate on acidic side
ABSORPTION
The movement of a drug from its site of administration into the systemic circulation
Rate of absorption determines how soon effects begin
Amount of absorption determines how intense effects will be
Chemical equivalence: when drug preparations contain the same amount of the drug
, Bioavailability: preparations are considered equal in bioavailability if the drug they
contain is absorbed at the same rate and to the same extent
Factors affecting drug absorption
Rate of dissolution
Surface area
Blood flow
Lipid solubility
pH partitioning
Rate of dissolution
drugs must dissolve before they can be absorbed
rate of dissolution determines rate of absorption
Drugs formulated for rapid dissolution = faster onset compared to drugs formulated
for slow dissolution
Surface area
Larger surface area = faster absorption
Absorption of PO drugs is usually greater from smaller intestine than stomach
because its lined with microvilli
Blood flow
Sites with high blood flow = more rapid absorption because blood containing a newly
absorbed drug will be replaced rapidly by drug-free blood, maintaining a large
gradient between concentration of drug outside versus inside the blood. Greater
concentration gradient = greater rate of absorption
Lipid solubility
Highly lipid-soluble drugs are absorbed quicker than lower ones
Lipid-soluble drugs easily pass membranes that separate them from blood
pH partitioning
Absorption is enhanced when the difference in pH of plasma and pH at site of
administration causes drug molecules to be ionized in the plasma
Characteristics of commonly used routes of administration
Route of administration affects rate and extent of absorption
Major routes (see table 4.1):
o PO (enteral)
Absorbed through epithelial lining GI tract; capillary wall
Slow and variable
Easy, convenient, inexpensive, potentially reversible hence safer
Variable; possible inactivation by gastric acid or digestive enzymes,
possible n/v from irritation, pt must be conscious/cooperative
o IV
INTERACTIONS
PHARMACOKINETICS
The study of drug movement throughout the body
Four processes of pharmacokinetics: absorption, distribution, metabolism, and
excretion
Absorption is the movement of the drug from its site of administration into the blood
Distribution is the movement of the drug from the blood to the interstitial space of
tissues and into cells
Metabolism (biotransformation) is the enzymatically mediated alteration of drug
structure
Excretion is the movement of drugs and their metabolites out of the body
These processes determine the concentration of a drug at its sites of action
The intensity of the response to a drug is directly related to the concentration of the
drug at it site of action
Maximum beneficial effect is achieved with a concentration high enough to elicit the
desired response while avoiding concentrations that cause harm
PASSAGE OF DRUGS ACROSS MEMBRANES
Drugs must cross membranes to move throughout the body.
o Site of administration – bloodstream – site of action – metabolism – excretion
Cells are very close together so drugs usually pass through cells opposed to between
Therefore the ability of a drug to cross a biologic membrane is determined by its
ability to pass through single cells
Three ways to cross a membrane
Through channels or pores
Via a transport system
Direct penetration of the membrane (most common)
Channels and pores
Least common way for drugs to pass
Channels and pores are very small
Only the smallest compounds, like potassium and sodium, can pass through their
correct channels
Transport systems
Role is to move drugs from one side to the other
They are selective and dependent on drug structure
P-glycoprotein (PGP) aka multidrug transporter protein is a transmembrane protein
that transport several drugs OUT of cells
Direct penetration of the membrane
Occurs primarily
, Most drugs are too large to pass through channels and pores, and most lack transport
systems to help them cross all the membranes separating them from the sites of
action, metabolism, and excretion
“like dissolves like.” Membranes are mostly composed of lipids therefore a drug must
be lipid soluble (lipophilic) to directly penetrate.
POLAR MOLECULES AND IONS
Polar molecules and ions are not lipid soluble therefore cannot penetrate membranes
Polar molecules
Have no net charge
Instead have an uneven distribution of electrical charge, meaning the positive and
negative charges within congregate separately
Ex: water, the electrons (negative charges) spend more time in the vicinity of the
oxygen (-) atom than the two hydrogens (+), making the area around the oxygen
more negatively charged and the hydrogen more positively charged
Along with “like dissolves like,” polar molecules dissolve in polar solvents (such as
water) but not in nonpolar solvents (such as lipids)
Ions
Molecules with a positive or negative net electrical charge
Unable to cross membranes! Unless very small.
Must become nonionized to cross
Many drugs are either charged or uncharged weak organic bases or weak organic
acids. The electrical charge it has is determined by the pH of the surrounding
medium
o Acids tend to ionize in basic (alkaline) media
o Bases tend to ionize in acidic media
o Therefore weak acids absorb best in acid environment (ex: gastric acid)
because they remain nonionized
o Ex: aspirin molecules pass from stomach into small intestine where it is more
alkaline, changing the molecules to ionized form, impeding absorption of
aspirin from the intestine
pH partitioning (ion trapping)
The process of drug accumulation on the side of the membrane where the pH favors
its ionization
When there is a difference in pH between two sides of a membrane, drug molecules
tend to accumulate on the side where pH favors their ionization
o Acidic drugs accumulate on alkaline side
o Basic drugs accumulate on acidic side
ABSORPTION
The movement of a drug from its site of administration into the systemic circulation
Rate of absorption determines how soon effects begin
Amount of absorption determines how intense effects will be
Chemical equivalence: when drug preparations contain the same amount of the drug
, Bioavailability: preparations are considered equal in bioavailability if the drug they
contain is absorbed at the same rate and to the same extent
Factors affecting drug absorption
Rate of dissolution
Surface area
Blood flow
Lipid solubility
pH partitioning
Rate of dissolution
drugs must dissolve before they can be absorbed
rate of dissolution determines rate of absorption
Drugs formulated for rapid dissolution = faster onset compared to drugs formulated
for slow dissolution
Surface area
Larger surface area = faster absorption
Absorption of PO drugs is usually greater from smaller intestine than stomach
because its lined with microvilli
Blood flow
Sites with high blood flow = more rapid absorption because blood containing a newly
absorbed drug will be replaced rapidly by drug-free blood, maintaining a large
gradient between concentration of drug outside versus inside the blood. Greater
concentration gradient = greater rate of absorption
Lipid solubility
Highly lipid-soluble drugs are absorbed quicker than lower ones
Lipid-soluble drugs easily pass membranes that separate them from blood
pH partitioning
Absorption is enhanced when the difference in pH of plasma and pH at site of
administration causes drug molecules to be ionized in the plasma
Characteristics of commonly used routes of administration
Route of administration affects rate and extent of absorption
Major routes (see table 4.1):
o PO (enteral)
Absorbed through epithelial lining GI tract; capillary wall
Slow and variable
Easy, convenient, inexpensive, potentially reversible hence safer
Variable; possible inactivation by gastric acid or digestive enzymes,
possible n/v from irritation, pt must be conscious/cooperative
o IV
