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Eradication of Solid Tumor via
   Gancyclovir-based Activation of
VP22-tk Toxicity and Liposomal Toxin
               Delivery



  Cellular Engineering - K. Parker, Professor
  Lawler, M. • Cartwright, W. • Thaker, M.
Relevance
• Prevalence and Challenges native to Breast Cancer
  ▫ Second most prevalent form of cancer amongst females
  ▫ Resistance to treatment
  ▫ Increased Metastatic Potential/Tumor Growth due to
    Autocrine Signaling
  ▫ Autocrine Signaling    Increased Angiogenesis
Overview
• Autocrine Signal Manipulation (Prolactin)
• CE Pluripotency Manipulation
• Engineered to contain Suicide Gene under
  control of Chimeric Prolactin Receptor
• Cells will also contain Toxin-Loaded
  Microcapsules
Expected Benefits
• Combination of Suicide Gene/Prolactin
  Trigger will allow for Selective
  Cytotoxicity
• Spares non-cancerous Angiogenic Regions
• Localized Microcapsular Toxin Delivery
  leads to site-specific Chemotherapeutic
  Agent delivery
Specific Pathways of Exploitation - 1

• Prolactin
  ▫ Strong Association b/w High Serum Prolactin
    Levels and Rapid Mammary Tumor Growth
  ▫ Role of Dopamine Agonists
  ▫ Shortcomings of Rodent Model vs. Human Model
Specific Pathways of Exploitation - 2

• Angiogenesis Exploitation
  ▫ Use of Modified Capillary Endothelial
    Progenitor Cells
  ▫ Cultured to encourage differentiation into
    CE cells
  ▫ Modifications In Vitro
    Suicide Gene
    Conversion of Prodrug    Toxic Compound
Prodrug                    Toxic Compound Pathway
           • Neither Enzyme in SG nor Prodrug Toxic
             Individually
                ▫ Cytotoxicity only present when cells
                  expressing gene + prodrug




                    Gancyclovir                                    HSV-1 TK Analog

Image 1: http://www.bmb.leeds.ac.uk/mbiology/ug/ugteach/icu8/antibiotics/antivirals.html
Image 2: http://www.strubi.ox.ac.uk/strubi/research/DKSgroup/vzk2.html
Mechanisms of Destruction
• 2 Effects of Toxic Product at Tumor Sites:
 ▫ Death of Modified CE Cells
 ▫ “Bystander Effect”
• Tumor Mass Decreased via:
 ▫ Direct Toxic Killing of Tumor Cells
 ▫ Nutrient Starvation Resulting from Breakdown
   of Tumor Vasculature
Limitations of Current
            Therapies
• Percentage of modified cells which
  differentiate into CE not high enough.
• Modified Cells = only small % of total CE
  cells
• Does not differentiate between
  Cancerous/non-Cancerous Regions
 ▫ Cannot be used post-op/chronic sores/ulcers
• Modified Cells could lodge anywhere
 ▫ Toxicity-induced Inflammation/Vascular
   Failure
Mechanism of Destruction - Targeted
       Microcapsular Delivery
• Architecture of Microcapsule
 ▫ Lipid Based Outer Coating
 ▫ Core of Toxic Chemicals
 ▫ Small Enough to be Endocytosed by Cells
• Disruption Mechanisms
 ▫ Heat
 ▫ Light
 ▫ Ultrasound
Microcapsular Size
         • Counterclockwise from
           upper-left:
           ▫ Engulfing of beads
             under 1 micron in
             diameter (fig 1 & 2)
           ▫ Chen, Geometric
            Control of Cell Life
            and Death - 10 micron
            beads engulfed
            w/normal function, no
            elevated apopototic
            activity
Therapy Outline - I

                                 Therapy Outline


                         Scope and Screening
       Breast Cancer - must express autocrine signaling of Prolactin

    Ensure Presence of Prolactin via ELISA/RT-PCR for Prolactin mRNA

Harvest Capillary Endothelial Progenitors from Bone Marrow/Peripheral Blood

             Administration of Dopamine Agonist (Cabergoline)

       Prolactin Release Inhibited/Circulating Prolactin Eliminated
  Remaining Prolactin comes from Autocrine Prolactin Producing Regions
Therapy Outline - 2
             Outline - 2 (fig. 4)


   Harvested CE Progenitor Cells

Incorporate Synthetic Gene Construct

     Suicide/VP22 Fusion Gene
        - Controlled by Gal4

    Chimeric Prolactin Receptor

    Neomycin Resistance Marker
   Integrate cassette into Genome
Therapy Outline - 3


Cell Culture in Neomycin - Selects cells which have been effecively modified


              Culture in Tissue Flasks Coated with Fibronectin


                              FACS Sorting
                   Fluorescence Activated Cell Signaling
Therapy Outline - 4
              Microcapsule Delivery


    Delivery of Toxin-Loaded Microcapsules


    Cells will be Homing to Tumor Regions
Provdes Ideal Vector for Microcapsular Carriage


   CE Cells Actively Endocytose Liposomes


    Microcapsular Activation via Ultrasound
Therapy Outline - 5


         Administration of Modified Cells


3-4 Day Incorporation Period into Angiogenic sites


              Express Suicide Gene


      Begin VP-22 Mediated Export of Gene
Therapy Outline - 6


                     Administration of Prodrug


                         Inject Ganciclovir


Converts to Toxic Drug only in Presence of Suicide Gene Expression
Therapy Outline - 7


       Activate Microcapsules via Ultrasound


      Microcapsule Disruption/Drug Release


Death of Tumor Related Vasculature/Bystander Effect
Emergency Extraction Plan
• Toxicity Mediated Sepsis
 ▫ Stop administration of ganciclovir and the
   ultrasound microcapsule activation
• Loss of Control over Modified Cells
 ▫ Teratoma?
    Cease Administration of Dopamine Agonist
    Continue Ganciclovir Administration
Potential Drawbacks of Approach
• Contingent upon Tumor Engaging in Active
  Angiogenesis
• Tumor Cells Halt Autocrine/Paracrine
  Prolactin Signaling
• Side Effects of CE-Injection
 ▫ Proliferative Diabetic Retinopathy
 ▫ Pre-existing Capillary Proliferation-Related
   Conditions not eligible for treatment
Benefits of Proposed Approach
• Specific Targeting of Tumor Regions
 ▫ Spares other tissues
 ▫ Allows for very strong agents with limited
   side effects
• Microcapsules
 ▫ Allows use of chemotherapeutic agents that
   are highly effective, but difficult to
   administer via other means
Benefits - 2
• Destruction of Tumor Vasculature/Nutrient
  Supply as well as Neoplastic Cells
• Can destroy small, intravasated metastases
  previously undetected
• Maintenance of Remission
• Does not rely on delivery of transgenes to
  tumors in vivo
Benefits - 3
• Ex Vivo - Transgenes delivered only to
  desired cells
• Transgenic Cassette maintained in dipolid
  cells with intact DNA - decreases
  likelihood of transgenes being
  lost/altered.
• No reliance on viral vector
• Relies heavily on materials derived from
  patient (lipids, cells, etc.)

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Cellular Engineering - Milap Thaker, Matt Lawler, W. Cartwright et. al Eradication of Solid Tumor via Gancyclovir-based Activation of VP22-tk Toxicity and Liposomal Toxin Delivery

  • 1. Eradication of Solid Tumor via Gancyclovir-based Activation of VP22-tk Toxicity and Liposomal Toxin Delivery Cellular Engineering - K. Parker, Professor Lawler, M. • Cartwright, W. • Thaker, M.
  • 2. Relevance • Prevalence and Challenges native to Breast Cancer ▫ Second most prevalent form of cancer amongst females ▫ Resistance to treatment ▫ Increased Metastatic Potential/Tumor Growth due to Autocrine Signaling ▫ Autocrine Signaling Increased Angiogenesis
  • 3. Overview • Autocrine Signal Manipulation (Prolactin) • CE Pluripotency Manipulation • Engineered to contain Suicide Gene under control of Chimeric Prolactin Receptor • Cells will also contain Toxin-Loaded Microcapsules
  • 4. Expected Benefits • Combination of Suicide Gene/Prolactin Trigger will allow for Selective Cytotoxicity • Spares non-cancerous Angiogenic Regions • Localized Microcapsular Toxin Delivery leads to site-specific Chemotherapeutic Agent delivery
  • 5. Specific Pathways of Exploitation - 1 • Prolactin ▫ Strong Association b/w High Serum Prolactin Levels and Rapid Mammary Tumor Growth ▫ Role of Dopamine Agonists ▫ Shortcomings of Rodent Model vs. Human Model
  • 6. Specific Pathways of Exploitation - 2 • Angiogenesis Exploitation ▫ Use of Modified Capillary Endothelial Progenitor Cells ▫ Cultured to encourage differentiation into CE cells ▫ Modifications In Vitro  Suicide Gene  Conversion of Prodrug Toxic Compound
  • 7. Prodrug Toxic Compound Pathway • Neither Enzyme in SG nor Prodrug Toxic Individually ▫ Cytotoxicity only present when cells expressing gene + prodrug Gancyclovir HSV-1 TK Analog Image 1: http://www.bmb.leeds.ac.uk/mbiology/ug/ugteach/icu8/antibiotics/antivirals.html Image 2: http://www.strubi.ox.ac.uk/strubi/research/DKSgroup/vzk2.html
  • 8. Mechanisms of Destruction • 2 Effects of Toxic Product at Tumor Sites: ▫ Death of Modified CE Cells ▫ “Bystander Effect” • Tumor Mass Decreased via: ▫ Direct Toxic Killing of Tumor Cells ▫ Nutrient Starvation Resulting from Breakdown of Tumor Vasculature
  • 9. Limitations of Current Therapies • Percentage of modified cells which differentiate into CE not high enough. • Modified Cells = only small % of total CE cells • Does not differentiate between Cancerous/non-Cancerous Regions ▫ Cannot be used post-op/chronic sores/ulcers • Modified Cells could lodge anywhere ▫ Toxicity-induced Inflammation/Vascular Failure
  • 10. Mechanism of Destruction - Targeted Microcapsular Delivery • Architecture of Microcapsule ▫ Lipid Based Outer Coating ▫ Core of Toxic Chemicals ▫ Small Enough to be Endocytosed by Cells • Disruption Mechanisms ▫ Heat ▫ Light ▫ Ultrasound
  • 11. Microcapsular Size • Counterclockwise from upper-left: ▫ Engulfing of beads under 1 micron in diameter (fig 1 & 2) ▫ Chen, Geometric Control of Cell Life and Death - 10 micron beads engulfed w/normal function, no elevated apopototic activity
  • 12. Therapy Outline - I Therapy Outline Scope and Screening Breast Cancer - must express autocrine signaling of Prolactin Ensure Presence of Prolactin via ELISA/RT-PCR for Prolactin mRNA Harvest Capillary Endothelial Progenitors from Bone Marrow/Peripheral Blood Administration of Dopamine Agonist (Cabergoline) Prolactin Release Inhibited/Circulating Prolactin Eliminated Remaining Prolactin comes from Autocrine Prolactin Producing Regions
  • 13. Therapy Outline - 2 Outline - 2 (fig. 4) Harvested CE Progenitor Cells Incorporate Synthetic Gene Construct Suicide/VP22 Fusion Gene - Controlled by Gal4 Chimeric Prolactin Receptor Neomycin Resistance Marker Integrate cassette into Genome
  • 14. Therapy Outline - 3 Cell Culture in Neomycin - Selects cells which have been effecively modified Culture in Tissue Flasks Coated with Fibronectin FACS Sorting Fluorescence Activated Cell Signaling
  • 15. Therapy Outline - 4 Microcapsule Delivery Delivery of Toxin-Loaded Microcapsules Cells will be Homing to Tumor Regions Provdes Ideal Vector for Microcapsular Carriage CE Cells Actively Endocytose Liposomes Microcapsular Activation via Ultrasound
  • 16. Therapy Outline - 5 Administration of Modified Cells 3-4 Day Incorporation Period into Angiogenic sites Express Suicide Gene Begin VP-22 Mediated Export of Gene
  • 17. Therapy Outline - 6 Administration of Prodrug Inject Ganciclovir Converts to Toxic Drug only in Presence of Suicide Gene Expression
  • 18. Therapy Outline - 7 Activate Microcapsules via Ultrasound Microcapsule Disruption/Drug Release Death of Tumor Related Vasculature/Bystander Effect
  • 19. Emergency Extraction Plan • Toxicity Mediated Sepsis ▫ Stop administration of ganciclovir and the ultrasound microcapsule activation • Loss of Control over Modified Cells ▫ Teratoma?  Cease Administration of Dopamine Agonist  Continue Ganciclovir Administration
  • 20. Potential Drawbacks of Approach • Contingent upon Tumor Engaging in Active Angiogenesis • Tumor Cells Halt Autocrine/Paracrine Prolactin Signaling • Side Effects of CE-Injection ▫ Proliferative Diabetic Retinopathy ▫ Pre-existing Capillary Proliferation-Related Conditions not eligible for treatment
  • 21. Benefits of Proposed Approach • Specific Targeting of Tumor Regions ▫ Spares other tissues ▫ Allows for very strong agents with limited side effects • Microcapsules ▫ Allows use of chemotherapeutic agents that are highly effective, but difficult to administer via other means
  • 22. Benefits - 2 • Destruction of Tumor Vasculature/Nutrient Supply as well as Neoplastic Cells • Can destroy small, intravasated metastases previously undetected • Maintenance of Remission • Does not rely on delivery of transgenes to tumors in vivo
  • 23. Benefits - 3 • Ex Vivo - Transgenes delivered only to desired cells • Transgenic Cassette maintained in dipolid cells with intact DNA - decreases likelihood of transgenes being lost/altered. • No reliance on viral vector • Relies heavily on materials derived from patient (lipids, cells, etc.)