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Presented
By
Sumit Sharma
Raunak Prakash Asopa
Soarab Sharma
Mriganka Mandal
Contents
 Introduction
 DNA based

vaccines

 History
 Why

DNA vaccines
 How DNA vaccines made
 Methods of delivery
 Mechanism
 Advantages and Disadvantages
 Current clinical trials
 Future prospects
Introduction





A vaccine is a biological preparation that
improves immunity to a particular disease.
It contains an agent that resembles a
disease-causing microorganism, and is
often made from weakened or killed forms
of the microbe, its toxins or one of its
surface proteins.
The agent stimulates the body's immune
system to recognize the agent as foreign,
destroy it, and "remember" it, so that the
immune system can more easily recognize
and destroy any of these microorganisms
that it later encounters.
DNA based vaccines






DNA vaccination is a technique for
protecting an organism against disease by
injecting it with genetically engineered
DNA to produce an immunological
response.
Circular double stranded DNA molecule,
referred to as a plasmid fabricated with
DNA sequence containing genes encoding
one or more proteins of a pathogen.
As this DNA inserted into cells it is
translated to form antigenic protein. As this
protein is foreign to cells , so immune
response raised against this protein.
History
 DNA vaccines

are third generation vaccines and are made
up of a small, circular piece of bacterial DNA
 In 1990, University of Wisconsin, Jon Wolff found that
injection of DNA plasmids produce a protein response in
mice.
 In 1993, Merck Research Laboratories, Dr. Margaret Liu
found that intramuscular injection of DNA from influenza
virus into mice produced complete immune response.
 In 1996, trials involving T-cell lymphoma, influenza &
herpes simplex virus were started.
Why DNA vaccines?
 Normal

vaccines having a
possible risk of the vaccine
being fatal. But in DNA
vaccines there is no need of
using
actual
infectious
organism.
 Normal
vaccines provide
primarily Humoral immunity.
On the other hand DNA
vaccines
provide
both
Humoral & Cell mediated
immunity.
DNA vaccine is made
Viral gene
Recombinant DNA
Technology

Expression plasmid

Plasmid with foreign gene
Transform in to bacteria

Plasmid DNA get Amplified
Plasmid DNA isolated

Stored in vials

Ready for Apply
Methods of delivery
 Injection:

Large amount of DNA
vaccines applied directly to the
skeletal tissues.
 Gene Gun: Small amount of vaccine
applied through DNA coated gold
beads to the abdominal skin.
 Pneumatic Jet Injection: Very high
amount of vaccine applied to the
abdominal skin.
Mechanism
BY TWO PATHWAYS
 ENDOGENOUS :Antigenic Protein is
presented by cell in which
it is produced.
 EXOGENOUS

:Antigenic Protein is formed
in one cell but presented by
different cell.
How DNA vaccines work

+
Muscle Cells

Plasmid DNA
Endogenous Pathway
Nucleus
Plasmid
DNA
MHC-I

mRNA

Antigenic
Protein

Antigenic
Peptides
T- Helper Cell

Memory T cells
Exogenous Pathway

Antigenic Protein come outside
Antigen Presenting Cell
Antigenic Peptides
T- Helper Cell

Memory
Antibodies

Cytokines

Plasma B-Cell

MHC-II

Activated B-Cell

Memory B-Cell
When Virus Enter in the Body

Memory T-Cell

Viral Protein

Antibodies
Advantages
 Vaccination

with no risk for infection.
 Antigen presentation by both MHC class I and class II
Molecules.
 Immune response focused only on antigen of interest.
 Stability of vaccine for storage and shipping
 Cost-effectiveness.
 Long-term persistence of immunogen.
Disadvantages
 Limited

to protein immunogens.

 Risk

of affecting genes controlling
cell growth.

 Possibility

of inducing antibody
production against DNA.

 Possibility

of tolerance to the
antigen (protein) produced.
Current clinical
trials
Review
Recent advance in immunotherapies for Alzheimer
disease (1999)








DNA vaccination has been developed as a
new therapy for Alzheimer Disease
treatment.
Alzheimer disease (AD) is the most
common cause of dementia characterized
by progressive neurodegeneration.
An Adeno-assosiated Viral vector
developed by Zhang and his colleagues
could express Aβ in in-vivo condition.
They prepare DNA vaccine using this
AAV genome and tested on AD model
mice.
of Aβ burden in APP23 mice after DNA
vaccination is shown in the diagram. Prophylactic
administration of Fc-Aβ vaccine prevented the Aβ
deposition to 10–30% of that in untreated animals before
12 months of age and to 40–50% after 15 months (closed
triangles). The effects of therapeutic administration were
almost same as those of prophylactic administration.

 Reduction
Other clinical trials:
 June

2006,DNA vaccine examined on horse. Horse
acquired immunity against west nile viruses.

 August

2007,DNA vaccination against
Sclerosis was reported as being effective.

 In

multiple

Oct. 2011 DNA Vaccines Show Promise in
Preventing Dental Caries. DNA vaccine prepared using
recombinant flagellin protein derived from Salmonella
as mucosal adjuvant for anti-caries DNA vaccine.
Future prospects
 Plasmid

with multiple genes
provide immunity against many
diseases in one booster.
 DNA
vaccines
against
infectious diseases such as
AIDS, Rabies, Malaria can be
available.
 In future DNA vaccines can be
applied to boost up the immune
system.
References








Grammatikos, Alexandros P.; (June 2009). "Meta-analyses on
Pediatric Infections and Vaccines". Infectious Disease Clinics of
North America 23 (2): 431–57.
Alarcon JB, Waine GW, McManus DP (1999). "DNA vaccines:
technology and application as anti-parasite and anti-microbial
agents". Adv. Parasitol. 42: 343–410.
Tang DC, DeVit M, Johnston SA. (1992)“Genetic immunization is a
simple method for eliciting an immune response”. Nature; 356:1524.
Barry MA, Lai WC, Johnston SA.(1995) “Protection against
mycoplasma infection using expression- library immunization”.
Nature; 377:632-5.
DNA Vaccines: A Brief Review of History, Mechanism, Advantages, Clinical Trials & Future

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DNA Vaccines: A Brief Review of History, Mechanism, Advantages, Clinical Trials & Future

  • 1. Presented By Sumit Sharma Raunak Prakash Asopa Soarab Sharma Mriganka Mandal
  • 2. Contents  Introduction  DNA based vaccines  History  Why DNA vaccines  How DNA vaccines made  Methods of delivery  Mechanism  Advantages and Disadvantages  Current clinical trials  Future prospects
  • 3. Introduction    A vaccine is a biological preparation that improves immunity to a particular disease. It contains an agent that resembles a disease-causing microorganism, and is often made from weakened or killed forms of the microbe, its toxins or one of its surface proteins. The agent stimulates the body's immune system to recognize the agent as foreign, destroy it, and "remember" it, so that the immune system can more easily recognize and destroy any of these microorganisms that it later encounters.
  • 4. DNA based vaccines    DNA vaccination is a technique for protecting an organism against disease by injecting it with genetically engineered DNA to produce an immunological response. Circular double stranded DNA molecule, referred to as a plasmid fabricated with DNA sequence containing genes encoding one or more proteins of a pathogen. As this DNA inserted into cells it is translated to form antigenic protein. As this protein is foreign to cells , so immune response raised against this protein.
  • 5. History  DNA vaccines are third generation vaccines and are made up of a small, circular piece of bacterial DNA  In 1990, University of Wisconsin, Jon Wolff found that injection of DNA plasmids produce a protein response in mice.  In 1993, Merck Research Laboratories, Dr. Margaret Liu found that intramuscular injection of DNA from influenza virus into mice produced complete immune response.  In 1996, trials involving T-cell lymphoma, influenza & herpes simplex virus were started.
  • 6. Why DNA vaccines?  Normal vaccines having a possible risk of the vaccine being fatal. But in DNA vaccines there is no need of using actual infectious organism.  Normal vaccines provide primarily Humoral immunity. On the other hand DNA vaccines provide both Humoral & Cell mediated immunity.
  • 7. DNA vaccine is made Viral gene Recombinant DNA Technology Expression plasmid Plasmid with foreign gene
  • 8. Transform in to bacteria Plasmid DNA get Amplified
  • 9. Plasmid DNA isolated Stored in vials Ready for Apply
  • 10. Methods of delivery  Injection: Large amount of DNA vaccines applied directly to the skeletal tissues.  Gene Gun: Small amount of vaccine applied through DNA coated gold beads to the abdominal skin.  Pneumatic Jet Injection: Very high amount of vaccine applied to the abdominal skin.
  • 11. Mechanism BY TWO PATHWAYS  ENDOGENOUS :Antigenic Protein is presented by cell in which it is produced.  EXOGENOUS :Antigenic Protein is formed in one cell but presented by different cell.
  • 12. How DNA vaccines work + Muscle Cells Plasmid DNA
  • 16. Antigen Presenting Cell Antigenic Peptides T- Helper Cell Memory Antibodies Cytokines Plasma B-Cell MHC-II Activated B-Cell Memory B-Cell
  • 17. When Virus Enter in the Body Memory T-Cell Viral Protein Antibodies
  • 18. Advantages  Vaccination with no risk for infection.  Antigen presentation by both MHC class I and class II Molecules.  Immune response focused only on antigen of interest.  Stability of vaccine for storage and shipping  Cost-effectiveness.  Long-term persistence of immunogen.
  • 19. Disadvantages  Limited to protein immunogens.  Risk of affecting genes controlling cell growth.  Possibility of inducing antibody production against DNA.  Possibility of tolerance to the antigen (protein) produced.
  • 21. Review Recent advance in immunotherapies for Alzheimer disease (1999)     DNA vaccination has been developed as a new therapy for Alzheimer Disease treatment. Alzheimer disease (AD) is the most common cause of dementia characterized by progressive neurodegeneration. An Adeno-assosiated Viral vector developed by Zhang and his colleagues could express Aβ in in-vivo condition. They prepare DNA vaccine using this AAV genome and tested on AD model mice.
  • 22. of Aβ burden in APP23 mice after DNA vaccination is shown in the diagram. Prophylactic administration of Fc-Aβ vaccine prevented the Aβ deposition to 10–30% of that in untreated animals before 12 months of age and to 40–50% after 15 months (closed triangles). The effects of therapeutic administration were almost same as those of prophylactic administration.  Reduction
  • 23. Other clinical trials:  June 2006,DNA vaccine examined on horse. Horse acquired immunity against west nile viruses.  August 2007,DNA vaccination against Sclerosis was reported as being effective.  In multiple Oct. 2011 DNA Vaccines Show Promise in Preventing Dental Caries. DNA vaccine prepared using recombinant flagellin protein derived from Salmonella as mucosal adjuvant for anti-caries DNA vaccine.
  • 24. Future prospects  Plasmid with multiple genes provide immunity against many diseases in one booster.  DNA vaccines against infectious diseases such as AIDS, Rabies, Malaria can be available.  In future DNA vaccines can be applied to boost up the immune system.
  • 25. References     Grammatikos, Alexandros P.; (June 2009). "Meta-analyses on Pediatric Infections and Vaccines". Infectious Disease Clinics of North America 23 (2): 431–57. Alarcon JB, Waine GW, McManus DP (1999). "DNA vaccines: technology and application as anti-parasite and anti-microbial agents". Adv. Parasitol. 42: 343–410. Tang DC, DeVit M, Johnston SA. (1992)“Genetic immunization is a simple method for eliciting an immune response”. Nature; 356:1524. Barry MA, Lai WC, Johnston SA.(1995) “Protection against mycoplasma infection using expression- library immunization”. Nature; 377:632-5.

Notas del editor

  1. What is vaccine?Why vaccine?
  2. Alzheimer Disease is the most common cause of age-related cognitive decline, affecting more than 12 million people in worldwide. The disease is characterized by progressive memory impairment, cognitive decline, altered behavior and language deficit.