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Recombinant Proteins in Plants
    Problems and Prospects

                  Dr.P.H.Ramanjini Gowda
                    Professor and Co ordinator
               Department of Biotechnology
                       UAS.GKVK
                   Bangalore 560065



Guest lecture delivered at Tamil Nadu Agricultural University, Coimbatore on 6.2.2013
Why Do We Need Vaccines?
   Currently, we have vaccines for TWENTY-SIX different
   infectious diseases.


   The average American child receives about ten different
   vaccinations before the age of 2!


   Many different diseases are rarely seen anymore; in some cases
   the diseases have disappeared completely!


   Vaccinations save countless people all over the world from
   severe and even fatal diseases.
Before
the 1700’s      1796       1970’s       1994        Today



The Chinese    Edward      Smallpox   Polio was     Research
developed      Jenner      was era-   eradicated.   is being
the first      developed   dicated.                 done all
form of        the                                  over the
vaccines -     smallpox                             world in
variolation.   vaccine                              order to
               from                                 improve
               cowpox.                              vaccines.
Costs

                                                       Vaccine production is not at all
                                                       efficient for mass production.
http://whyfiles.org/166plant_vaccines/2.html




                                                       Their use in many parts of the world
                                                       is limited because of the high costs.
“Combining a cost-effective production
system with a safe and efficacious
delivery system, edible vaccines
provide a compelling solution.”
– Plants and Human Health: Delivery of Vaccines Via
Transgenic Plants (2003)
What exactly are
“edible vaccines?”

 • Biopharmaceuticals
 • Plants or crops that produce human
  vaccines
 • The next generation of vaccines
Biopharming
• Biopharming is the crop based production of
  industrial or therapeutic biomolecules.
• Vaccines are the therapeutic biomolecules.
• Plants are amenable for large scale biomass
  production.
• Plants have good system of post
  translational modification of proteins.
Contd….
• Complex multemeric proteins can be
  produced in plants.
• The engineered edible vaccine can be
  consunmed orally without alteration.
• The cost of vaccine is cheap since it needs
  no purification.
• Needs no refrigeration.
Growing plants is much cheaper
The plants that produce the
                                     than producing vaccines.
edible vaccines could be
grown in third world
countries.                          Targeted expression in plant storage
                                    tissues provides stability and




Advantages
                                    accumulation



                                         Plants are already regularly
          Agricultural                   used in pharmaceuticals, so
          products                       there are established
          can be                         purification protocols.
          transported
          around the          Plants can’t host most
          world               human pathogens, so the
          relatively          vaccines won’t pose
          cheaply.            dangers to humans.
Limitations
• Low expression levels.
• Glycosilation and post transcriptional
  modifications.
• Animal and human studies are difficult.
• Formulations of the vaccines.
For the last decade, scientists have known how to genetically engineer a plant
     to produce a desired protein. The two most common tools used to do this are:


Cut out the selected      Infect the plant with
region of the plasmid.    the agrobacteria and
                                                                   DNA is coated on
                          grow it in a medium.                     microscopically tiny gold
             Agrobacteria have a circular                          beads that are placed in a
             form of DNA called plasmids.                          vacuum chamber. The
              The plasmids are easily                              gene gun then allows
             manipulated because they                              compressed gas to expand,
                                                                   pushing the beads down
             naturally have two “cut” Grow the plant like
              Add the desired gene.                                until they hit a filter. The
             points where a gene can beregular crop.
                                        a
                                                                   DNA then flies off of the
             taken out and replaced with                           beads down into the tissue,
             one of the scientist’s choice.                        where some will enter a
                                                                   nucleus and become
                                                                   incorporated.
Plant-derived Vaccine Strategies
Gene encoding an antigenic protein from a pathogen.




         Incorporate into a plant transformation vector for optimized
         expression in plant cells.



          Stable expression:                  Stable expression:
          Nuclear genome                      Chloroplast genome
          integration.                        integration.


         Integrate into a viral coding sequence for expression as a
         “by product” of viral replication.



          Transient expression:            Modify viral genome to
          Infect plant to initiate         adapt it into a plant
          viral replication.               transformation vector for
                                           subsequent regulated
                                           release as a replicon in
                                           transgenic plants.



        Identify protective          Create viral replicon coding
        epitope within               sequence with epitope
        antigenic protein.           fusions to coat protein.
Choice of the Plant System
• Plant product should be eaten raw.
• The plant is amenable for regeneration.
• Should be rich source of protein.
• Fast growing
• Should grow under tough weather
  conditions.
• Banana,cantaloupes,Peanut,Papaya.
Antigen Expression in Plants




The cumulative number of antigens from pathogens of humans and/or
animals which have been expressed in plants, based upon published reports
(original compilation of the reports was detailed in Khalsa G, Mason H, Arntzen C. Plant-
derived vaccines: progress and constraints. In: R Fischer and S Schillberg (eds.) Molecular
Farming: Plant-made Pharmaceuticals and Technical Proteins. John Wiley and Sons, In
press in 2005).
Pharmaceutical Production in Plants
    Genetically modified plants have been used as “bioreactors” to
    produce therapeutic proteins for more than a decade. A recent
    contribution by transgenic plants is the generation of edible
    vaccines.
      Edible vaccines are vaccines produced in plants that can be
administered directly through the ingestion of plant materials
containing the vaccine. Eating the plant would then confer immunity
against diseases.
Edible vaccines produced by transgenic plants are
attractive for many reasons. The cost associated
with the production of the vaccine is low,
especially since the vaccine can be ingested
directly, and vaccine production can be rapidly up
scaled should the need arises. Edible vaccine is
likely to reach more individuals in developing
countries.

The first human clinical trial took place in 1997.
Vaccine against the toxin from the bacteria E.coli
was produced in potato. Ingestion of this
transgenic potato resulted in satisfactory
vaccinations and no adverse effects.
Edible Vaccines
One focus of current vaccine effort is on hepatitis B, a virus responsible for
causing chromic liver disease. Transgenic tobacco and potatoes were engineered
to express hepatitis B virus vaccine. During the past two years, vaccines against
a E.coli toxin, the respiratory syncytial virus, measles virus, and the Norwalk
virus have been successfully expressed in plants and delivered orally. These
studies have supported the potential of edible vaccines as preventive agents of
many diseases.

There is hope to produce edible vaccines in bananas, which are grown extensively
throughout the developing world.

                                                                      Vol. 19, No. 3 Feb.
                                                                                  1, 1999
Transgenic Plants; Nuclear
     Transformation
Why use this technology?

Familiar Production Systems
   • Genes introduced into field crops
   • New productions systems not needed
   • Producer can use traditional growing strategies

Reduced End-Product Cost
   • Animal system: $1000 - $5000 per gram protein
   • Plant System: $1 - $10 per gram protein
Edible Vaccines – A Biopharming Dream
     Biotech Plants Serving Human Health Needs

• A pathogen protein gene is cloned
• Gene is inserted into the DNA of plant (potato, banana, tomato)
• Humans eat the plant
• The body produces antibodies against pathogen protein
• Human are “immunized” against the pathogen
• Examples:
    Diarrhea
    Hepatitis B
    Measles
Future Health-related Biotech Products

      Vaccines
        Herpes
        hepatitis C
        AIDS
        malaria


           Tooth decay
             Streptococcus mutans, the mouth bacteria
             releases lactic acid that destroys enamel
             engineered Streptococcus mutans
                does not release lactic acid
                destroys the tooth decay strain
Rabies Neutralizing antibody titers(IU/ml)inmice immunized with plant extracts



Plant Extract and route     Neutralizing antibody titer on   Key words
                            Day 30              Day60
Plant 1 IM                  0.4                   0.8        IM=Intramuscular
      IM+FA                 0.7                   1.2        IP=Intraperitoneal
      IP                    0.6                   1.0        FA=Compleate
Plant 2 IM                  0.5                   1.0        Freaunds adjuvant
     IM+FA                  1.0                   1.5        ND=Not detected
     IP                     0.8                   1.2        IU=International units
Plant 3 IM                  0.7                   1.2
    IM+FA                   1.2                   1.6
   IP                       0.8                   1.5
Control Plant IM            ND                     ND
IM+FA                       ND                     ND
IP                          ND                     ND
Protein expression in crop
    plants
   Earlier we have expressed ERA strain of rabies glycoprotein
    gene in Tobacco and Muskmelon and also obtained an Indian
    patent. The ERA strain obtained from Thomas Jefferson
    University has a patent on this gene. Hence, we have designed
    our own gene construct.




   The CVS glycoprotein gene will be subcloned to plant expression
    vector (pPS1)
   The pPS1 vector containing CaMV 35S promoter with the rabies
    glycoprotein gene will be transferred to Agrobacterium strain
    EHA105 and will be used for developing transgenic crop plants
    expressing Rabies Glycoprotein.
Alternative means of pilot production




Production facility      bioreactor    refined product
Plants as bioreactors for
       pharmaceutical proteins
                  PRESENT STATUS
• Useful human proteins produced in plants
   – Human antibodies & other blood proteins
   – Protein and peptide hormones
   – Enzymes
   – Subunit vaccines
• Proteins from plants are in the clinical pipeline
   – Human antibodies
   – Subunit vaccines
   – Enzymes
• Regulatory Environment is evolving
Plants as bioreactors for
    pharmaceutical proteins
            FUTURE APPLICATIONS
• Clinical unmet needs in cancer, infectious
  disease, cardiovascular disease, CNS
  disease, metabolic disorders, inflammatory
  disease, biowarfare agents
• Options for injectable, oral and topical
  application
• Treatment and prevention modalities
What is the challenge?

• Developing drugs to treat human disease;
  protein based drugs are the fastest growing
  class of new drugs for treatment and
  prevention of human disease. But we face
  these barriers:

• Capacity:
  – Insufficient capacity for drugs in the pipeline
• Cost
  – Cost of goods
  – Capital for manufacturing facilities
• Safety and Efficacy
Advantages of plants as
            bioreactors
• Plants are the most efficient producers of
  proteins on earth
  – Plants are scalable bioreactors
  – Plants provide cost advantages

• Plants cells are similar to human cells
  – Similar protein synthesis machinery
  – Read the same genetic code
  – Assemble, fold and secrete complex proteins
Antibodies:
A Compelling Success Story

• Inherently stable human proteins
• High specificity; low toxicity
• High drug approval rates
• Injectable, topical and oral
  applications
• Appropriate for chronic conditions
• Potential long-lasting benefits
Antibodies: Natural Defense
• Circulating antibodies protect us from
  invading viruses, bacteria and toxins
• Secretory antibodies protect our vulnerable
  surfaces from pathogens and toxins,
  preventing entry and colonization
• Passive antibodies in colostrum and milk
  provide passive immunity to neonates and
  infants
• We make ~3g of antibodies a day
• Like most animals, we surrender most of
  our antibodies to the environment
Antibodies: Natural Defense




ORAL/GASTROINTESTINAL   NASAL     GENITO-URINARY
        TRACT         PULMONARY        TRACT
                        TRACT
Emerging Antibody
         Opportunities
Therapeutic areas requiring high
quantities of antibodies, and low cost
– Inflammatory diseases
– CNS diseases
– Cardiovascular diseases
– Infectious diseases
 _ topical applications
Plant-produced Antibodies work
• Anti-Streptococcus mutans (Guy’s 13)
  – Prevents dental caries in humans
  – Plant sIgA 10X more stable than IgG
     • Nature Medicine 1998



• Anti-Herpes simplex virus (HSV8)
  – Prevents vaginal transmission of herpes
  – Proved in mice with rice and soybean PAb’s
     • Nature Biotechnology 1998
Plants Produce Assembled
        Antibodies



     Site of production: corn
     endosperm (starch and
              protein)




                                Nature 342:76-78 (1989)
                                Science 268: 716-9 (1995)
                                Nature Biotechnology: 16:1361-
                                1364 (1998)
Comparison of Plant and
Mammalian Derived Antibodies
• Peptide sequence: identical
• Affinity: identical
• Antibody types: Plant system more
  versatile
  – Can make any isotype including secretory
    IgA
• Post-translational processing: different
  – core glycan identical, terminal sugar
    different
  – antigenicity & clearance: apparently
    identical
A Plant-produced antibody is
scheduled for clinical development
 • Clinical trials planned to begin in 2003
 • Clinical importance: herpes simplex virus
   – Over 50 million chronic sufferers
   – Over 1.5 million new cases/year in U.S.
 • Antibodies provide promising application in
   both prevention and treatment
 • Plant-produced antibodies are ideal
   – High quantities required
   – Scalable and have lower costs than traditional
     production
Capacity Shortage
            60000


            50000

            40000
Kg of MAb




            30000

            20000


            10000

                0
                    2001   2002   2003    2004    2005     2006     2007     2008    2009   2010

                                     Mammalian Cell Culture Protein Capacity in Kg
                                     Optimistic MAb Demand (Dain Rauscher '00)
                                     Realistic MAb Demand (CSFB '01)
Processing Comparison




*After harvest, the seeds can be stored indefinitely; therefore, when the protein is
needed, the purification process can begin immediately.
Source: Cline, M.,”Plant-Made Pharmaceuticals: Overview of Technology and
Stewardship,” Fifth Biotechnology Roundtable, American Bar Association, St. Louis,
May 2003.
Plant-derived pharmaceuticals have a full load of technology.
Can the load be moved to benefit public health?
       • Finalize regulatory regime through commercialization
       • Currently pilot scale; commercial scale-up required
       • Secure public acceptance of technology
First Pant Made Drug on the
              Market
• US FDA approved drug produced in
  carrots
• The drug Taliglucerase alfa produced for
  the rare lysosomal storage disorder
  (Gaucher disease).
• Israeli Biotech Protalix Biotherapeutics
  developed the method.
• This drug can replace the avialble drug
  Cerezyme.
THANK YOU

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Recombinant Proteins in Plants :Problems and Prospects

  • 1. Recombinant Proteins in Plants Problems and Prospects Dr.P.H.Ramanjini Gowda Professor and Co ordinator Department of Biotechnology UAS.GKVK Bangalore 560065 Guest lecture delivered at Tamil Nadu Agricultural University, Coimbatore on 6.2.2013
  • 2. Why Do We Need Vaccines? Currently, we have vaccines for TWENTY-SIX different infectious diseases. The average American child receives about ten different vaccinations before the age of 2! Many different diseases are rarely seen anymore; in some cases the diseases have disappeared completely! Vaccinations save countless people all over the world from severe and even fatal diseases.
  • 3. Before the 1700’s 1796 1970’s 1994 Today The Chinese Edward Smallpox Polio was Research developed Jenner was era- eradicated. is being the first developed dicated. done all form of the over the vaccines - smallpox world in variolation. vaccine order to from improve cowpox. vaccines.
  • 4. Costs Vaccine production is not at all efficient for mass production. http://whyfiles.org/166plant_vaccines/2.html Their use in many parts of the world is limited because of the high costs.
  • 5. “Combining a cost-effective production system with a safe and efficacious delivery system, edible vaccines provide a compelling solution.” – Plants and Human Health: Delivery of Vaccines Via Transgenic Plants (2003)
  • 6. What exactly are “edible vaccines?” • Biopharmaceuticals • Plants or crops that produce human vaccines • The next generation of vaccines
  • 7. Biopharming • Biopharming is the crop based production of industrial or therapeutic biomolecules. • Vaccines are the therapeutic biomolecules. • Plants are amenable for large scale biomass production. • Plants have good system of post translational modification of proteins.
  • 8. Contd…. • Complex multemeric proteins can be produced in plants. • The engineered edible vaccine can be consunmed orally without alteration. • The cost of vaccine is cheap since it needs no purification. • Needs no refrigeration.
  • 9. Growing plants is much cheaper The plants that produce the than producing vaccines. edible vaccines could be grown in third world countries. Targeted expression in plant storage tissues provides stability and Advantages accumulation Plants are already regularly Agricultural used in pharmaceuticals, so products there are established can be purification protocols. transported around the Plants can’t host most world human pathogens, so the relatively vaccines won’t pose cheaply. dangers to humans.
  • 10. Limitations • Low expression levels. • Glycosilation and post transcriptional modifications. • Animal and human studies are difficult. • Formulations of the vaccines.
  • 11. For the last decade, scientists have known how to genetically engineer a plant to produce a desired protein. The two most common tools used to do this are: Cut out the selected Infect the plant with region of the plasmid. the agrobacteria and DNA is coated on grow it in a medium. microscopically tiny gold Agrobacteria have a circular beads that are placed in a form of DNA called plasmids. vacuum chamber. The The plasmids are easily gene gun then allows manipulated because they compressed gas to expand, pushing the beads down naturally have two “cut” Grow the plant like Add the desired gene. until they hit a filter. The points where a gene can beregular crop. a DNA then flies off of the taken out and replaced with beads down into the tissue, one of the scientist’s choice. where some will enter a nucleus and become incorporated.
  • 12.
  • 13. Plant-derived Vaccine Strategies Gene encoding an antigenic protein from a pathogen. Incorporate into a plant transformation vector for optimized expression in plant cells. Stable expression: Stable expression: Nuclear genome Chloroplast genome integration. integration. Integrate into a viral coding sequence for expression as a “by product” of viral replication. Transient expression: Modify viral genome to Infect plant to initiate adapt it into a plant viral replication. transformation vector for subsequent regulated release as a replicon in transgenic plants. Identify protective Create viral replicon coding epitope within sequence with epitope antigenic protein. fusions to coat protein.
  • 14. Choice of the Plant System • Plant product should be eaten raw. • The plant is amenable for regeneration. • Should be rich source of protein. • Fast growing • Should grow under tough weather conditions. • Banana,cantaloupes,Peanut,Papaya.
  • 15. Antigen Expression in Plants The cumulative number of antigens from pathogens of humans and/or animals which have been expressed in plants, based upon published reports (original compilation of the reports was detailed in Khalsa G, Mason H, Arntzen C. Plant- derived vaccines: progress and constraints. In: R Fischer and S Schillberg (eds.) Molecular Farming: Plant-made Pharmaceuticals and Technical Proteins. John Wiley and Sons, In press in 2005).
  • 16. Pharmaceutical Production in Plants Genetically modified plants have been used as “bioreactors” to produce therapeutic proteins for more than a decade. A recent contribution by transgenic plants is the generation of edible vaccines. Edible vaccines are vaccines produced in plants that can be administered directly through the ingestion of plant materials containing the vaccine. Eating the plant would then confer immunity against diseases. Edible vaccines produced by transgenic plants are attractive for many reasons. The cost associated with the production of the vaccine is low, especially since the vaccine can be ingested directly, and vaccine production can be rapidly up scaled should the need arises. Edible vaccine is likely to reach more individuals in developing countries. The first human clinical trial took place in 1997. Vaccine against the toxin from the bacteria E.coli was produced in potato. Ingestion of this transgenic potato resulted in satisfactory vaccinations and no adverse effects.
  • 17. Edible Vaccines One focus of current vaccine effort is on hepatitis B, a virus responsible for causing chromic liver disease. Transgenic tobacco and potatoes were engineered to express hepatitis B virus vaccine. During the past two years, vaccines against a E.coli toxin, the respiratory syncytial virus, measles virus, and the Norwalk virus have been successfully expressed in plants and delivered orally. These studies have supported the potential of edible vaccines as preventive agents of many diseases. There is hope to produce edible vaccines in bananas, which are grown extensively throughout the developing world. Vol. 19, No. 3 Feb. 1, 1999
  • 18. Transgenic Plants; Nuclear Transformation
  • 19. Why use this technology? Familiar Production Systems • Genes introduced into field crops • New productions systems not needed • Producer can use traditional growing strategies Reduced End-Product Cost • Animal system: $1000 - $5000 per gram protein • Plant System: $1 - $10 per gram protein
  • 20. Edible Vaccines – A Biopharming Dream Biotech Plants Serving Human Health Needs • A pathogen protein gene is cloned • Gene is inserted into the DNA of plant (potato, banana, tomato) • Humans eat the plant • The body produces antibodies against pathogen protein • Human are “immunized” against the pathogen • Examples: Diarrhea Hepatitis B Measles
  • 21. Future Health-related Biotech Products Vaccines  Herpes  hepatitis C  AIDS  malaria Tooth decay  Streptococcus mutans, the mouth bacteria  releases lactic acid that destroys enamel  engineered Streptococcus mutans does not release lactic acid destroys the tooth decay strain
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  • 36. Rabies Neutralizing antibody titers(IU/ml)inmice immunized with plant extracts Plant Extract and route Neutralizing antibody titer on Key words Day 30 Day60 Plant 1 IM 0.4 0.8 IM=Intramuscular IM+FA 0.7 1.2 IP=Intraperitoneal IP 0.6 1.0 FA=Compleate Plant 2 IM 0.5 1.0 Freaunds adjuvant IM+FA 1.0 1.5 ND=Not detected IP 0.8 1.2 IU=International units Plant 3 IM 0.7 1.2 IM+FA 1.2 1.6 IP 0.8 1.5 Control Plant IM ND ND IM+FA ND ND IP ND ND
  • 37. Protein expression in crop plants  Earlier we have expressed ERA strain of rabies glycoprotein gene in Tobacco and Muskmelon and also obtained an Indian patent. The ERA strain obtained from Thomas Jefferson University has a patent on this gene. Hence, we have designed our own gene construct.  The CVS glycoprotein gene will be subcloned to plant expression vector (pPS1)  The pPS1 vector containing CaMV 35S promoter with the rabies glycoprotein gene will be transferred to Agrobacterium strain EHA105 and will be used for developing transgenic crop plants expressing Rabies Glycoprotein.
  • 38.
  • 39.
  • 40. Alternative means of pilot production Production facility    bioreactor    refined product
  • 41. Plants as bioreactors for pharmaceutical proteins PRESENT STATUS • Useful human proteins produced in plants – Human antibodies & other blood proteins – Protein and peptide hormones – Enzymes – Subunit vaccines • Proteins from plants are in the clinical pipeline – Human antibodies – Subunit vaccines – Enzymes • Regulatory Environment is evolving
  • 42. Plants as bioreactors for pharmaceutical proteins FUTURE APPLICATIONS • Clinical unmet needs in cancer, infectious disease, cardiovascular disease, CNS disease, metabolic disorders, inflammatory disease, biowarfare agents • Options for injectable, oral and topical application • Treatment and prevention modalities
  • 43. What is the challenge? • Developing drugs to treat human disease; protein based drugs are the fastest growing class of new drugs for treatment and prevention of human disease. But we face these barriers: • Capacity: – Insufficient capacity for drugs in the pipeline • Cost – Cost of goods – Capital for manufacturing facilities • Safety and Efficacy
  • 44. Advantages of plants as bioreactors • Plants are the most efficient producers of proteins on earth – Plants are scalable bioreactors – Plants provide cost advantages • Plants cells are similar to human cells – Similar protein synthesis machinery – Read the same genetic code – Assemble, fold and secrete complex proteins
  • 45. Antibodies: A Compelling Success Story • Inherently stable human proteins • High specificity; low toxicity • High drug approval rates • Injectable, topical and oral applications • Appropriate for chronic conditions • Potential long-lasting benefits
  • 46. Antibodies: Natural Defense • Circulating antibodies protect us from invading viruses, bacteria and toxins • Secretory antibodies protect our vulnerable surfaces from pathogens and toxins, preventing entry and colonization • Passive antibodies in colostrum and milk provide passive immunity to neonates and infants • We make ~3g of antibodies a day • Like most animals, we surrender most of our antibodies to the environment
  • 47. Antibodies: Natural Defense ORAL/GASTROINTESTINAL NASAL GENITO-URINARY TRACT PULMONARY TRACT TRACT
  • 48. Emerging Antibody Opportunities Therapeutic areas requiring high quantities of antibodies, and low cost – Inflammatory diseases – CNS diseases – Cardiovascular diseases – Infectious diseases _ topical applications
  • 49. Plant-produced Antibodies work • Anti-Streptococcus mutans (Guy’s 13) – Prevents dental caries in humans – Plant sIgA 10X more stable than IgG • Nature Medicine 1998 • Anti-Herpes simplex virus (HSV8) – Prevents vaginal transmission of herpes – Proved in mice with rice and soybean PAb’s • Nature Biotechnology 1998
  • 50. Plants Produce Assembled Antibodies Site of production: corn endosperm (starch and protein) Nature 342:76-78 (1989) Science 268: 716-9 (1995) Nature Biotechnology: 16:1361- 1364 (1998)
  • 51. Comparison of Plant and Mammalian Derived Antibodies • Peptide sequence: identical • Affinity: identical • Antibody types: Plant system more versatile – Can make any isotype including secretory IgA • Post-translational processing: different – core glycan identical, terminal sugar different – antigenicity & clearance: apparently identical
  • 52. A Plant-produced antibody is scheduled for clinical development • Clinical trials planned to begin in 2003 • Clinical importance: herpes simplex virus – Over 50 million chronic sufferers – Over 1.5 million new cases/year in U.S. • Antibodies provide promising application in both prevention and treatment • Plant-produced antibodies are ideal – High quantities required – Scalable and have lower costs than traditional production
  • 53. Capacity Shortage 60000 50000 40000 Kg of MAb 30000 20000 10000 0 2001 2002 2003 2004 2005 2006 2007 2008 2009 2010 Mammalian Cell Culture Protein Capacity in Kg Optimistic MAb Demand (Dain Rauscher '00) Realistic MAb Demand (CSFB '01)
  • 54. Processing Comparison *After harvest, the seeds can be stored indefinitely; therefore, when the protein is needed, the purification process can begin immediately. Source: Cline, M.,”Plant-Made Pharmaceuticals: Overview of Technology and Stewardship,” Fifth Biotechnology Roundtable, American Bar Association, St. Louis, May 2003.
  • 55. Plant-derived pharmaceuticals have a full load of technology. Can the load be moved to benefit public health? • Finalize regulatory regime through commercialization • Currently pilot scale; commercial scale-up required • Secure public acceptance of technology
  • 56. First Pant Made Drug on the Market • US FDA approved drug produced in carrots • The drug Taliglucerase alfa produced for the rare lysosomal storage disorder (Gaucher disease). • Israeli Biotech Protalix Biotherapeutics developed the method. • This drug can replace the avialble drug Cerezyme.

Notas del editor

  1. Here I would like to briefly explain how to make transgenic plant expressing vaccine antigens. First, a plant expression vector for antigen of choice is designed. Among various gene delivery methods, we mainly use agrobacterium-mediated transformation method, where the gene encoding the antigen will be inserted in a vectorderived from plant pathogen agrobacterium shown here, and then the vector is transferred to the bacteia. Now this bacteria can transfer the genes into chromosome of plant cells. Finally, transformed plant cells are selected and then regenerated to whole plants.
  2. This technology is being used for several reasons. First, by introducing the transgene into a crop like corn, the farmer can use traditional production techniques to grow the crop. From the pharmaceutical side, the cost of producing the end product is greatly reduced compared to techniques currently in place.
  3. Edible vaccines may be the most important and accepted biotech product.
  4. The health and pharmaceutical industry uses biotech approaches for vaccine production. The normal bacteria in the mouth produces an acid that destroys enamel. The engineered version of the bacteria does not produce the acid. Children will be treated with the engineered version, which also has a gene that will destroy the other bacteria in the mouth, allowing it to become established.