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Physicochemical
properties of drug
substances.
- Vishnu Datta.M
Physicochemical properties of drug
substances
•
•
•
•
•
•
•
•
•

Drug solubility and dissolution rate
Particle size and effective surface area
Polymorphism and Amorphism
Pseudo polymorphism (hydrates/solvates)
Drug stability
Salt form of the drug
Lipophilicity of the drug
pka of the drug and gastrointestinal pH
Stereochemical nature of the drug
Particle size &
Effective surface area
Particle size &
Effective surface area
• Particle size and surface area of a solid
drug are inversely related.
• Two types of surface area of interest are:
 Absolute surface area
 Effective surface area
Particle size &
Effective surface area
• Absolute surface area which is the total area
of solid surface of any particle.
• Effective surface area which is the area of
solid surface exposed to the dissolution
medium.
Particle size &
Effective surface area
Particle size &
Effective surface area
• Micronisation>>>reduction of particle size
• Surface of such small particles has higher
energy than the bulk of the solid
>>>increased interaction with the solvent
Particle size &
Effective surface area
• In case of non hydrophobic
drugs(griseofulvin, chloramphenicol, salts of
tetracycline) >>>micronisation>>>superior
dissolution rate in comparison to the simple
milled form of these drugs.
>>>decreased dose >>>increased absorption
efficiency
• Ex: Griseofulvin reduced to half and
Spironolactone decreased 20 times
Particle size &
Effective surface area
• In case of hydrophobic drugs (aspirin,
phenacetin, phenobarbital)>>>decrease in
effective surface area of such
powders>>>fall in the dissolution rate.
Reasons suggested for the
outcome
• The hydrophobic surface of the drug
adsorbs air onto their surface which inhibits
wettability.
• The particles re-aggregate to form larger
particles due to their high surface free
energy which either float on the surface or
settle at the bottom of dissolution medium
Overcome the effects to increase
the effective surface area
• Use of surfactant as a wetting agent
Decreases the interfacial tension
Displaces the adsorbed air with the solvent
Ex: polysorbate 80 increases the bioavailability
of phenacetin by promoting wettability
• Adding hydrophilic diluents such as PEG,
PVP, Dextrose etc which coat the surface of
hydrophobic drug particles and render them
hydrophilic. …
Physicochemical properties of drug
substances
•
•
•
•
•
•
•
•
•

Drug solubility and dissolution rate
Particle size and effective surface area
Polymorphism and Amorphism
Pseudo polymorphism (hydrates/solvates)
Drug stability
Salt form of the drug
Lipophilicity of the drug
pka of the drug and gastrointestinal pH
Stereochemical nature of the drug
Polymorphism
• Depending on the internal structure a solid
can exist either in a crystalline or
amorphous.
• When a substance exists in more than one
crystalline form, the different forms are
designated as polymorphs and the
phenomenon as polymorphism .
Polymorphism
• Polymorphs are two types
Enantiotropic polymorph is the one which
can be reversibly changed into another
form by altering the temperature or
pressure.ex:sulphur
Monotropic polymorph is the one which is
unstable at all temperatures and
pressures eg:glyceryl stearates.
Polymorphism
• Polymorphs differs in physical properties
>>> solubility, Melting point, density,
hardness and compression characteristics
• The existence of the polymorphs can be
determined by using techniques
like>>>optical crystallography, x-ray
diffraction, differential scanning
calorimetry etc.
Polymorphism
• Among the polymorphic forms>>>stable
form>>>lowest energy>>>highest melting
point>>>least aqueous solubility
• Remaining polymorphs are called
metastable forms which represent>>>higher
energy state>>>lower melting
point>>>higher aqueous solubility
Polymorphism
• As the metastable forms have greater
solubility they show better availability and
are preferred in formulation
• Ex chloramphenicol palmitate A,B,C,D
B shows best bioavailability
A is virtually inactive biologically
Amorphous form
• Drugs also exist as amorphous form
>>>have greater aqueous solubility than
the crystalline forms>>>energy required to
transfer a molecule from lattice is greater
than that required for amorphous
• Ex: cortisone acetate is 3 times more
soluble than crystalline form
• Order of dissolution is
Amorphous>metastable>stable
Physicochemical properties of drug
substances
•
•
•
•
•
•
•
•
•

Drug solubility and dissolution rate
Particle size and effective surface area
Polymorphism and Amorphism
Pseudo polymorphism (hydrates/solvates)
Drug stability
Salt form of the drug
Lipophilicity of the drug
pka of the drug and gastrointestinal pH
Stereochemical nature of the drug
Pseudopolymorphism
 When the solvent molecules are

incorporated in the crystal lattice of the
solid are called as the solvates
 The solvates can exist in different
crystalline form called as
pseudopolymorphs. The phenomenon is
called pseudopolymorphism.
Hydrates and Solvates
• If case Entrapped Solvent is water then it is

referred as Hydrate.
• Anhydrous form of the drug has greater aqueous
solubility then the hydrates. (because already in
interaction with water have less energy for
crystal break up in comparison to the
anhydrates).
• Solvates differ in their physical parameters.
Physicochemical properties of drug
substances
•
•
•
•
•
•
•
•
•

Drug solubility and dissolution rate
Particle size and effective surface area
Polymorphism and Amorphism
Pseudo polymorphism (hydrates/solvates)
Drug stability
Salt form of the drug
Lipophilicity of the drug
pka of the drug and gastrointestinal pH
Stereochemical nature of the drug
Drug stability
• A drug for oral use may destabilize either
during its shelf-life or in the GIT
• Major stability problems resulting in poor
bioavailability of an orally administered drug
Degradation of drug into inactive form
Interaction with one or more different
component(s) to form a complex that is
poorly soluble or is unabsorbable
~~REFERENCES~~
• Physical pharmacy, fourth edition,
Alfred martin.
• Pharmaceutics The science of dosage form
design 2nd edition- M.E Aulton
• Dissolution, Bioavailability & Bioequivalence
Hamed M.Abdou
• Brahmankar D.M., Biopharmaceutics &
pharmacokinetics A Treatise
• Biopharmaceutics and clinical
pharmacokinetics an introducion fourth
edition Robert E.Notari
~~THANK YOU~~
• Knowledge of what is does not open the door directly to what
should be……….
Âť Albert Einstein

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Physicochemical properties Biopharmaceutics and Pharmacokinetics by Vishnu Datta M

  • 2. Physicochemical properties of drug substances • • • • • • • • • Drug solubility and dissolution rate Particle size and effective surface area Polymorphism and Amorphism Pseudo polymorphism (hydrates/solvates) Drug stability Salt form of the drug Lipophilicity of the drug pka of the drug and gastrointestinal pH Stereochemical nature of the drug
  • 4. Particle size & Effective surface area • Particle size and surface area of a solid drug are inversely related. • Two types of surface area of interest are:  Absolute surface area  Effective surface area
  • 5. Particle size & Effective surface area • Absolute surface area which is the total area of solid surface of any particle. • Effective surface area which is the area of solid surface exposed to the dissolution medium.
  • 7. Particle size & Effective surface area • Micronisation>>>reduction of particle size • Surface of such small particles has higher energy than the bulk of the solid >>>increased interaction with the solvent
  • 8. Particle size & Effective surface area • In case of non hydrophobic drugs(griseofulvin, chloramphenicol, salts of tetracycline) >>>micronisation>>>superior dissolution rate in comparison to the simple milled form of these drugs. >>>decreased dose >>>increased absorption efficiency • Ex: Griseofulvin reduced to half and Spironolactone decreased 20 times
  • 9. Particle size & Effective surface area • In case of hydrophobic drugs (aspirin, phenacetin, phenobarbital)>>>decrease in effective surface area of such powders>>>fall in the dissolution rate.
  • 10. Reasons suggested for the outcome • The hydrophobic surface of the drug adsorbs air onto their surface which inhibits wettability. • The particles re-aggregate to form larger particles due to their high surface free energy which either float on the surface or settle at the bottom of dissolution medium
  • 11. Overcome the effects to increase the effective surface area • Use of surfactant as a wetting agent Decreases the interfacial tension Displaces the adsorbed air with the solvent Ex: polysorbate 80 increases the bioavailability of phenacetin by promoting wettability • Adding hydrophilic diluents such as PEG, PVP, Dextrose etc which coat the surface of hydrophobic drug particles and render them hydrophilic. …
  • 12. Physicochemical properties of drug substances • • • • • • • • • Drug solubility and dissolution rate Particle size and effective surface area Polymorphism and Amorphism Pseudo polymorphism (hydrates/solvates) Drug stability Salt form of the drug Lipophilicity of the drug pka of the drug and gastrointestinal pH Stereochemical nature of the drug
  • 13. Polymorphism • Depending on the internal structure a solid can exist either in a crystalline or amorphous. • When a substance exists in more than one crystalline form, the different forms are designated as polymorphs and the phenomenon as polymorphism .
  • 14.
  • 15. Polymorphism • Polymorphs are two types Enantiotropic polymorph is the one which can be reversibly changed into another form by altering the temperature or pressure.ex:sulphur Monotropic polymorph is the one which is unstable at all temperatures and pressures eg:glyceryl stearates.
  • 16. Polymorphism • Polymorphs differs in physical properties >>> solubility, Melting point, density, hardness and compression characteristics • The existence of the polymorphs can be determined by using techniques like>>>optical crystallography, x-ray diffraction, differential scanning calorimetry etc.
  • 17. Polymorphism • Among the polymorphic forms>>>stable form>>>lowest energy>>>highest melting point>>>least aqueous solubility • Remaining polymorphs are called metastable forms which represent>>>higher energy state>>>lower melting point>>>higher aqueous solubility
  • 18. Polymorphism • As the metastable forms have greater solubility they show better availability and are preferred in formulation • Ex chloramphenicol palmitate A,B,C,D B shows best bioavailability A is virtually inactive biologically
  • 19. Amorphous form • Drugs also exist as amorphous form >>>have greater aqueous solubility than the crystalline forms>>>energy required to transfer a molecule from lattice is greater than that required for amorphous • Ex: cortisone acetate is 3 times more soluble than crystalline form • Order of dissolution is Amorphous>metastable>stable
  • 20. Physicochemical properties of drug substances • • • • • • • • • Drug solubility and dissolution rate Particle size and effective surface area Polymorphism and Amorphism Pseudo polymorphism (hydrates/solvates) Drug stability Salt form of the drug Lipophilicity of the drug pka of the drug and gastrointestinal pH Stereochemical nature of the drug
  • 21. Pseudopolymorphism  When the solvent molecules are incorporated in the crystal lattice of the solid are called as the solvates  The solvates can exist in different crystalline form called as pseudopolymorphs. The phenomenon is called pseudopolymorphism.
  • 22. Hydrates and Solvates • If case Entrapped Solvent is water then it is referred as Hydrate. • Anhydrous form of the drug has greater aqueous solubility then the hydrates. (because already in interaction with water have less energy for crystal break up in comparison to the anhydrates). • Solvates differ in their physical parameters.
  • 23. Physicochemical properties of drug substances • • • • • • • • • Drug solubility and dissolution rate Particle size and effective surface area Polymorphism and Amorphism Pseudo polymorphism (hydrates/solvates) Drug stability Salt form of the drug Lipophilicity of the drug pka of the drug and gastrointestinal pH Stereochemical nature of the drug
  • 24. Drug stability • A drug for oral use may destabilize either during its shelf-life or in the GIT • Major stability problems resulting in poor bioavailability of an orally administered drug Degradation of drug into inactive form Interaction with one or more different component(s) to form a complex that is poorly soluble or is unabsorbable
  • 25. ~~REFERENCES~~ • Physical pharmacy, fourth edition, Alfred martin. • Pharmaceutics The science of dosage form design 2nd edition- M.E Aulton • Dissolution, Bioavailability & Bioequivalence Hamed M.Abdou • Brahmankar D.M., Biopharmaceutics & pharmacokinetics A Treatise • Biopharmaceutics and clinical pharmacokinetics an introducion fourth edition Robert E.Notari
  • 26. ~~THANK YOU~~ • Knowledge of what is does not open the door directly to what should be………. Âť Albert Einstein