Chemical and Biological Defense Program (CBDP): Capabilities for Countering the Threat

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Chemical and Biological Defense Program (CBDP): Capabilities for Countering the Threat MG Donna Barbisch, USA Director, CBRN Integration April 26, 2005

Report Documentation Page Form Approved OMB No. 0704-0188 Public reporting burden for the collection of information is estimated to average 1 hour per response, including the time for reviewing instructions, searching existing data sources, gathering and maintaining the data needed, and completing and reviewing the collection of information. Send comments regarding this burden estimate or any other aspect of this collection of information, including suggestions for reducing this burden, to Washington Headquarters Services, Directorate for Information Operations and Reports, 1215 Jefferson Davis Highway, Suite 1204, Arlington VA 22202-4302. Respondents should be aware that notwithstanding any other provision of law, no person shall be subject to a penalty for failing to comply with a collection of information if it does not display a currently valid OMB control number. 1. REPORT DATE 26 APR 2005 2. REPORT TYPE 3. DATES COVERED 00-00-2005 to 00-00-2005 4. TITLE AND SUBTITLE Chemical and Biological Defense Program (CBDP): Capabilities for Countering the Threat 5a. CONTRACT NUMBER 5b. GRANT NUMBER 5c. PROGRAM ELEMENT NUMBER 6. AUTHOR(S) 5d. PROJECT NUMBER 5e. TASK NUMBER 5f. WORK UNIT NUMBER 7. PERFORMING ORGANIZATION NAME(S) AND ADDRESS(ES) Army Medical Research and Material Command,Chemical Biological Defense Program (CBDP),Fort Detrick,MD,21702 8. PERFORMING ORGANIZATION REPORT NUMBER 9. SPONSORING/MONITORING AGENCY NAME(S) AND ADDRESS(ES) 10. SPONSOR/MONITOR S ACRONYM(S) 12. DISTRIBUTION/AVAILABILITY STATEMENT Approved for public release; distribution unlimited 13. SUPPLEMENTARY NOTES The original document contains color images. 14. ABSTRACT 15. SUBJECT TERMS 11. SPONSOR/MONITOR S REPORT NUMBER(S) 16. SECURITY CLASSIFICATION OF: 17. LIMITATION OF ABSTRACT a. REPORT unclassified b. ABSTRACT unclassified c. THIS PAGE unclassified 18. NUMBER OF PAGES 26 19a. NAME OF RESPONSIBLE PERSON Standard Form 298 (Rev. 8-98) Prescribed by ANSI Std Z39-18

Outline Recent Highlights Program Organization Program Guidance and Direction Summary 2

CBDP: Great News Story FY06 Budget submission First input under new management structure First alignment of life-cycle cost and testing (from science & technology through acquisition) Major T&E Investment Moving more into experimentation & rigorous analysis Significant Interagency Collaboration One of Few Growth Areas in DoD Budget $2.1 Billion Increase over FYDP in President s Budget Aligns with President's Global War on Terror Increased Emphasis in Future Technologies High Investment in S&T in FY06 Infrastructure Rebuild Non-Traditional Agents Genetically Engineered Threats New Sensor Approaches Systems Biology Approach to Medical Countermeasures 3

Chemical and Biological Defense Program (CBDP) Program Organization DATSD(CBD) 4

CBDP Major Players Dr. Dale Klein ATSD(NCB) Dr. Klaus Schafer DATSD(CBD) Dr. Barry Fridling JRO-CBRND (Acting) BG Steve Reeves JPEO-CBD Dr. Charles Galloway Director, JSTO Mr. Walter Hollis Joint T&E Executive Agent BG Stan Lillie Joint Combat Developer 5

An Integrated Systems Approach to Counter the Threat CB Threats & Hazards Agent Delivery Doses on Target Downwind Dispersal Doses Absorbed Sustained Combat Power Symptoms Medical Treatment Medical Pretreatment Individual & Collective Protection Information Systems Contamination Avoidance and NBC Battle Management (Detection, Identification, Reconnaissance & Warning) Installation Force Protection Decontamination, Restoration 6

Defense of the Homeland Global War on Terror DOD Role in Bioshield CBRN Defense Program Strategic Environment Proliferation of Weapons of Mass Destruction Challenge of Non-Traditional CBRN Agents Biosurety The greatest threat before humanity today is the possibility of secret and sudden attack with chemical, or biological, or nuclear weapons President George W. Bush Remarks at the National Defense University, 11 February 2004 7

Chemical Biological Defense Program Paradigm Shift Prior to the transformation, the major focus to provide improved capabilities for the warfighter to survive, fight, and win on any battlefield contaminated with chemical and biological weapons. The current paradigm shift directs both a broadening and deepening of the CBDP. CBRN consequence management (about 1997) Force protection (in 1999) Homeland Defense (in 2002) Visibility of radiological and nuclear aspects of the program (2003) Inclusion of the US Coast Guard Transition from Threat Based to Capabilities Based Process This broadening requires a carefully developed program strategy to ensure that warfighter capabilities are maintained and advanced concurrently with these added missions. 8

Chemical and Biological Defense: Strategic Framework

DoD Mission Provide integrated chemical and biological defense capabilities to effectively execute the National Military Strategy. 10

Strategic Imperatives Eliminate technological surprise. Make the threat irrelevant. Detect the threat. Protect against the threat. Eliminate the threat. 11

Enabling the Vision Doctrine Organization Training Materiel Leader development Personnel Facilities Oversight Coordination Integration 12

New Team Focused on: Defining Equities Across DoD Streamlining Processes Synchronizing Effort Improving Efficiency Optimizing Capability Promoting Interoperability Transforming BOTTOM LINE: EFFECTIVE SOLUTIONS IN THE HANDS OF THE USER 13

FY06 President s Budget (DoD CB Defense Program + Defense Health Program for Construction of USAMRIID Improvements) ($ in millions) 1,800 1,700 1,600 1,500 1,400 1,300 1,200 1,100 1,000 900 800 700 600 500 400 300 200 100 0 Budget Request CBDP Procurement CBDP Advanced Development CBDP Science & Technology Base Defense Health Program Military Construction (USAMRIID) FY04 FY05 FY06 FY07 FY08 FY09 FY10 FY11 FY06 Highlights Near-Term Shift in Emphasis to Address Future Challenges (NTAs, Emerging Threats) and Improve the T&E Infrastructure Long term trend to Provide Advanced Capabilities to the Warfighter 14

Enhanced Planning Process (EPP) Results T&E Infrastructure Improvements CB T&E Facilities NTA Test Chamber USAMRIID (DHP) RDT&E Improvements Additional Emphasis: S&T for NTA detection Bio point and standoff detection Medical Prophylaxis Battle Analysis Decontamination Bio Defense Initiatives Chem point detection 15

T&E Infrastructure Investment Explosive test (simulant only) Aerosol exposures test chamber Fort Detrick, MD Bang Box, Dugway CB Simulant Test Grid Dugway Proving Ground UT High Containment BL4 lab, USAMRIID Fort Detrick MD CB Aerosol Test Chamber Fort Detrick, MD Man In Simulant Test (MIST) Chamber 16

17

The Problem Slow drug development process leads to economic and social catastrophe jeopardizing national security 10+ years > $800M Attack with new threat DHS funds to NIAID No national strategy, clear responsibility or federal funding to shorten this cycle Safe & effective countermeasure Bioshield Early Stage Research Lead Discovery Preclinical Development Clinical Development Production Models FDA Approval Production Procurement 10+ years 2+ years 2-5 years 5-8 years 1 year 18

R&D - Test and Evaluation Vaccine/Drug Discovery Vaccine/Drug Development Industry DoD BioShield Academia NIAID/NIH DHS/NBACC Other Government Research DoD/Military tech base Genomics/Proteomics Basic Research Funding has increased For the Attractive Work GLP GMP Phase 1 Safety trials Testing/ Proofing Process Product Transition Industry Process Production Distribution Storage Testing Bottleneck FDA-Licensed Vaccines Drugs Diagnostics Funding is needed For the Unglamorous Work 19

Future Emphasis: Systems Biology Today s Threats Anthrax Smallpox Botulinum Plague Tularemia Ebola/Filo Hemorrhagic Fever Encephalitis SARS Influenza Ricin/SEB, others Modes of Action Receptor Binding Signal Transduction Decoys Immune Avoidance Translation/Transcription Immune Deregulation Replication Virulence Expression Parallel Systems Approach Solutions Target Agent Commonalities Block Key Receptors Inhibition by Small Molecules Modulate Immunity Change Gene Expression Block Protein Actions Modulate Physiologic Impacts Bioengineered One PIECE at a time Process Analysis Broad Spectrum 20

Viral Disease Healthy Cells (Untreated) Cells Infected with SARS (Treated with 20μM of TRS2 PMO) Cells Infected with SARS (Untreated) SARS = Severe Acute Respiratory Syndrome PMO = Phosphorodiamidate Morpholino Oligomers 21

Broad Spectrum Therapies for Novel Biodefense Threats $100M funding in FY06 - Budget Activities BA1-BA5-76% in Science and Technology Base Transformational Approaches will be applied leverage genomics, proteomics and systems biology data explosion Technical and program advisory leadership from team of nationally recognized experts - BW defense, microbiology, drug development - Will draw heavily from commercial and academic performers Basic Research/Science ($28M) - Directed at common pathways (modes of action) in pathogen host response - Find novel intervention points 22

Broad Spectrum Therapies for Novel Biodefense Threats (Cont d) Applied Research/Science ($18M) - Directed at expanding technologies - Speed the cycle from discovery to license application Advanced Science/Tech Development ($30M) - Aimed at quick wins based on new compounds and technology approaches demonstrating current success - Strategy to deliver products with IND approval (Phase 1 trials) for BioShield acceptability and further investment Advanced Component Development and System Demonstration ($24M) Ultimate goal is defeat of genetically engineered biological threat 23

Emerging Threats: Path Forward Anticipate the threat Deliver New capabilities Short Term and Long Term Exploit Existing Med CM as Well as Survey Existing Therapeutics Major Investments Needed in Host-pathogen Infection Process to Identify Common Targets for Broad-spectrum Drugs Push Developments to Diagnostics, Therapeutics and Pretreatment Portfolios Needs to Harness all of the Major Bioinformatics and Molecular Biology Breakthroughs 24

Conclusion Finish What we Started on Classic Threats Legacy Products Need Investment to Take These Threats Away from the Enemy The Good Old Days are over Next Generation Threats Need New Thinking, Bold Approaches and Harnessing Information Revolution in Biology Best Approach for Long-term Threats is Looking for Common Virulence Pathways Defeat Next Generation Threats by Attacking Problem at the Common Host Response Pathways 25

Questions? http://www.acq.osd.mil/cp 26