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Preclinical and Biodistribution Assessments
Supporting Development of Gene Therapy
Products
Janet M. Benson, PhD, DABT
Lovelace Respiratory Research Institute,
Albuquerque, NM
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About LRRI
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Founded in 1947 in the State of New Mexico
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Three subsidiaries
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LRRI – Commercial and non-government contracts
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LBERI – Government Grants and Contracts
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LSR – For Profit Entity conducting clinical trails
throughout USA.
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80 PhDs, MDs, and DVMs
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$67 million revenue (projected for 2008)
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$50 million endowment
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450,000 square feet of facilities
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LRRI Headquarters
and Research Facility
(125,000 sq. ft.)
Inhalation Toxicology
Laboratory
(325,000 sq. ft.)
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Principal Research Activities
Inflammation (triggers, mediators, cell damage and repair)
Lung cancer (responsible genes, early detection)
Asthma and immunology (determinants of allergic asthma,
immunosuppression)
Infectious disease (defenses, impairment of resistance to viruses and
bacteria)
Emphysema (mechanisms, animal models, tobacco and
environmental causes)
Preclinical studies of new drugs (efficacy, safety, FDA compliance)
Development of Countermeasures against
Biological/Chemical/Nuclear Threats
Safety and Biodistribution of Gene Therapeutics
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FY 2008 Forecasted Revenue $67MM
LSR 10%
NIH
Sponsored
Construction
5%
State 1%
Pharmaceutical
7%
NIH
42%
Trade Associations,
Other Commercial
Sources, etc.,
Sponsored
Construction 6%
Trade Associations,
Other Commercial
Sources, etc., 16%
Endowment
Contributions 3%
= NIH Sponsored Construction
EPA
1%
DOE Cooperative
Agreement 2%
DOD DOE
7% Other 0%
= Trade Associations, etc., Sponsored Construction
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Role of the Pharmacology/Toxicology Testing
Core
 Assess the biodistribution and/or safety of gene therapy
products in studies conducted using Good Laboratory
Practice Guidelines.
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The objective of the Pharmacology/Biodistribution Studies
is to assess:
– Vector tropism
– Gene expression efficiency and kinetics
– Vector Clearance
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The objectives of the Toxicology Studies are to
– identify any potential adverse effects
– Identify a no adverse effect level.
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Pharmacology Toxicology Testing Core Key
Personnel
PI: Janet Benson, PhD, DABT
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30 years experience in basic and applied toxicology at LRRI
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25+ years experience directing studies under FDA or EPA
regulatory guidelines
Co PI: Thomas March, DVM, PhD, DACVP
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11 years at LRRI as a toxicologic pathologist
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Experienced in study design and animal model development
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Experienced in histological assessment in a variety of species
and under regulatory guidelines.
Virologist: Adriana Kajon, PhD
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8 years at LRRI
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Molecular epidemiology of adenovirus respiratory infections
–
Animal modeling of adenovirus pathogenesis
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Scope of Research (Benson) – Animal Model
Development, Efficacy and Safety Evaluations
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Safety and Biodistribution of Gene Therapy Products
(NHLBI).
Toxicity/Toxicokinetics/Pathophysiology of ingested and
inhaled ricin (NIAID).
Animal Model Development and Efficacy Assessment of
Botulinum Toxin Therapeutics (NIAID)
Development and Assessment of Countermeasures against
sulfur mustard induced toxicity to the lung, skin and eye
(NINDS).
Immunotoxicity/Developmental Toxicity of Inhaled
Brevetoxin (Florida Red Tide; NIEHS).
Commercial Clients.
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LRRI Scientific Staff Supporting the Core
Board-certified toxicologists
Board-certified laboratory animal
veterinarians
Virologists
Immunologists
Board-certified veterinary
pathologists
Certified quality assurance
specialists
Certified health and safety
specialists
Supporting Consultants
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Indoor Kennels (Canine or Swine)
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Large Animal Necropsy
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Clinical
Chemistry
Hematology
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Histopathology
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Flow Cytometry
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Basic Overview of the RSA Sumbission
and Review Process
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Investigator Registers with the program, receive password
and further instructions.
Investigator selects RSA type(s) and begins RSA
completion process – contact Core if desired.
Submit preliminary RSA.
Core staff and Investigator work to complete and submit
final version of RSA.
Pharm/Tox Core completes Feasibility Assessment
(ongoing process from start)
Application submitted for Scientific Review Board review
Application submitted for Steering Committee Review
Recommendations on funding submitted to the Gene
Therapy Group..
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RSA Process - Beginnings
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Investigator should ideally begin the process by having
discussions with the FDA regarding appropriate
experimental design.
– LRRI staff can be part of these discussions
– Guidance provided by FDA should be shared with
LRRI and GTRP/NHLBI staff early on, so required
resources can be identified.
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Source of GLP or GMP-grade vector product should be
identified.
Investigator will register with Program
Draft RSA form will be submitted and Core will assist in
developing to final stage.
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Pharm/Tox RSA
Section I
Investigator Information
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Investigator Name, and Contact Information (Alternate
contact)
Biographical Sketch
Are you a NHLBI investigator?
Funding Sources
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Pharm/Tox RSA
Section II
Study Information
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Study Title
Study Abstract
Rationale for Conducting Study
Identify Disease Category (Heart, Lung, or Blood)
Targeted Disease
Target organ, tissues or cells
Gene /Vector Name
Route of Administration
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Pharm/Tox RSA
Section II
Continued
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Study Design
– Tox, Biodistribution study, or both?
– Animal Species, numbers, sex
– Normal animals or disease model? If disease model,
how established?
– Vector Doses (rational for establishing, sites delivery
method).
– Has delivery device been approved for clinical use?
– Euthanasia Schedule
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Pharm/Tox RSA
Section II
Continued
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Study Endpoints
– Assays indicating toxicity/efficacy (tissue, timing?)
– Assays for gene product or vector.
– Antibodies developed to protein product/vector?
– Physiological endpoints – (pulmonary function,
electrocardiograms, echocardiograms?)
– Clinical pathology (hematology, serum chemistry,
coagualtion profiles).
– Histopathology (need for microdissection,
immunohistochemistry?)
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Pharm/Tox RSA
Section II
Concluded
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Description of the Clinical Study
Any other RSA’s submitted relating to this RSA or clinical
study.
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RSA Section III
Regulatory Information
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Have you discussed the study design with FDA in a pre-IND
setting?
– If “Yes”, list date(s) and provide discussion summary.
 Information ideally shared with Core and NHLBI
early to enable assessment of resources
required and feasibility assessments.
– If “No”, then this needs to be done.
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Reason(s) for Pharmacology/Toxicology testing
– Initial testing required by FDA?
– Is this study to provide follow-up testing required by
FDA? List reasons.
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RSA Section IV
Study-Specific Support
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Current and Pending funding for this study
– NIH
– NHLBI
– Other (institution or company)
– None
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RSA Section V
Vector Information
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Has the material been made?
Vector/Gene Name
Vector Source ( a GTRP core – specified, or other source)
Lot numbers
Amounts to be provided,
Grade (GMP, Partial GMP, or non GMP)
Product details (titer, vehicle, storage conditions, stability,
special handling procedures, known toxicities.
Method used to make vector.
Vector Construct
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RSA Section V
Vector Information Continued
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Vector Construct
– Transgene, promoter, serotypes, transgene species
specificity, packaging cell line.
– Sequence data
– Vector map
– Strategy in constructing the vector.
– Expected level of transgene expression
– Criteria for therapeutic gene expression
– Tissue specificity of transgene expression?
– Will primers for specific transcript or probe to detect
gene expression be provided to the Core – if so,
upload requested detail.
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Pharmacology/Toxicology Testing Requested
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Testing Assays
– Hematology
– Serum Chemistry
– Biodistribution
– Histopathology
– Testing organs for viral genomes
– Transgene expression and antibodies
– Biomarkers of Gene Function
– Other.
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Timelines (constraints)
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Feasibility Assessment
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Feasibility assessed based on:
– Core capacity and capabilities
– Timeline
– Vector Availability
– Vector stability or other characteristics
– Special animal requirements
– Other resource requirements
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Cost analysis
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Summary
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Preclinical Assessment of Gene Therapy products is
complex – more complex than for traditional compounds
Early interaction with the FDA and communication of these
discussions with the Core and NHLBI will facilitate RSA
development, assembly of required resources, and
feasibility assessment.
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PI Contact Information
Janet Benson
LRRI
505-348-9457
[email protected]
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