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Adjuvants

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Adjuvant Mechanisms. Influence antigen processing and ... 'The best adjuvant will never correct the choice of the wrong epitope.' Edelman & Tacket, 1990 ... – PowerPoint PPT presentation

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Title: Adjuvants


1
Lecture No. 12. March 25th, 2004 Formulation
and Delivery K.I. Dayalu
2
The Ideal Vaccine
  • Single dose
  • Neonatal Administration
  • Needle-less administration
  • 100 Effective
  • 100 Safe
  • Life-long protection
  • Affordable

3
Vaccine Reality
  • Multiple doses
  • Poor Neonatal Immune Responsiveness
  • Injectable administration
  • Variable Effectiveness
  • Variable Safety
  • Generally short lived protection
  • Affordable

4
Historical Formulation
Not Fancy(Perhaps even rude and crude --- But
it worked!!!!
  • Inactivated Diluted Culture Fluids
  • Modified Live Lyophilized Plugs

5
Historical Adjuvants
  • Freunds Complete, Incomplete
  • Aluminum salts Hydroxide, Phosphate

6
How Do We Achieve the Ideal?
Defined Vaccines

Modified-Live Sub-unit Genetic
Vaccine Components Antigen(s) Adjuvant(s)
Vehicle(s)/Delivery
7
ITS NOT ALL MAGIC
8
Adjuvant Mechanisms
  • Influence antigen processing and trafficking
  • Activate immune cells
  • Influence magnitude quality of immune response

9
Adjuvant Types
Enhance immune response to antigens
  • Immunostimulants
  • Vehicles
  • Surfactants
  • Particulates
  • Conjugates
  • Molecular

10
Adjuvants - Immunostimulants
Bacterial Extracts
  • TDM
  • MPL, MDP
  • CT/LT-oral, mucosal

Plant Extracts and Synthetic
  • Lipoidal Amines
  • Saponins

11
Adjuvants - Vehicles
  • Oil - Emulsions
  • Liposomes
  • Microparticles

12
Adjuvants - Surfactants
  • Saponins
  • Non-ionic Co-block Polymers

13
Saponins
  • Quil A, QS-21
  • S. American tree bark
  • Quillja saponaria molina
  • induces humoral cellular immunity

14
Non-ionic Co-Block Polymers
  • BASF Pluronic Series
  • (i.e. L-121)

15
Adjuvants- Particulate
  • VLP
  • ISCOM
  • Microparticles
  • Liposomes, etc
  • Alum salts.

16
Adjuvants - Conjugates
  • Link antigens to carriers
  • Enhance immunogenicity of poorly immunogenic
    antigens( i.e.peptides)
  • Change TI antigen to TD antigen
  • (eg., Hib conjugate vaccines)

17
Adjuvant Selection
  • Immune response desired
  • Nature of antigen
  • Formulation
  • Complexity
  • Stability
  • Scalability
  • Safety concerns
  • Regulatory issues

18
ITS A FINE BALANCE
EFFICACY
SAFETY
19
We Need to Break our Paradigms
There are no Magic Bullets
Novel SystemsTechnology gtgt Differentiation
20
Adjuvants - Molecular
  • HSP
  • Immunoregulatory Oligomers CpG
  • PADRE
  • C5a

21
The best adjuvant will never correct the choice
of the wrong epitope.
Edelman Tacket, 1990
22
Antigen
Vehicle
Vaccine System
Adjuvant
DELIVERY
23
New Methods in Delivery
  • Vesicles
  • microparticulates of proteins, lipids,
    carbohydrates, polymers
  • passive or active targeting
  • eg. Liposomes

24
New Methods in Delivery
  • Controlled Release
  • nearly independent of environmental conditions
    (pH)
  • pumps
  • synthetic polymeric materials
  • diffusion
  • chemical reaction (degradation/cleavage)
  • solvent activation(swelling/osmotic effects)

25
New Methods in Delivery
  • Polymers
  • Degradable
  • poly-lactide co-glycolide (PLG)
  • Lupron Depot
  • protein released over 30 d
  • Non-degradable
  • Ocusert
  • continuous pilocarpine release for 1 week
  • Norplant
  • 5 yr release

26
Degradable Polymers (PLG)
  • Problems
  • variable release rates
  • protein particle size
  • loading
  • protein solubility
  • molecular weight
  • polymer composition
  • size/shape of matrix
  • protein stability

27
Vaccine Delivery RoutesHow do we get it in
there?
  • Intramuscular
  • Subcutaneous
  • Intradermal
  • Intranasal/Aerosol
  • Oral/Enteric
  • Transdermal
  • Other

28
Vaccine Delivery RoutesIntramuscular
29
Vaccine Delivery RoutesSubcutaneous
30
Vaccine Delivery RoutesIntradermal
31
Vaccine Delivery RoutesIntranasal/Aerosol
32
Vaccine Delivery RoutesOral
33
Vaccine Delivery RoutesTransdermal
34
New Delivery Devices
  • Jet Injection
  • needle free
  • liquid stream lt 0.005 in.
  • 25 ga needle 0.040 in.
  • high pressure (gt4000 psi)
  • SC, ID (?), or IM (?)
  • conventional vaccines
  • individual or multiple dose
  • suitable for mass vaccination

35
New Delivery Devices
  • Ballistic impaction
  • needle-free
  • supersonic spray
  • skin or mucous membrane
  • gt1 square cm area
  • intradermal or intraepidermal
  • access to Langerhans APCs
  • dry powder or coated particles
  • proteins, peptides, DNA

36
New Delivery Devices
  • Transdermal Delivery
  • Occluded Patch
  • Microneedle array
  • needle free
  • skin or mucous membranes
  • access to Langerhans APCs
  • limited volume capacity
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