2. Mission and Vision
Organizational Structure
Research Programs
Education
Consultation
Facilities
Human Capital Development
Contracting Opportunities
Patents Available for Licensing
3. Vision
The leader in innovative, comprehensive solutions to advance medical chemical defense.
Mission
Provide a strong medical defense against chemical warfare agents and toxins.
5. USAMRICD Organizational Structure
6. Primary mission – �war fighter: healthy, physically fit; 18-45 yr
First Responders
Civilian Communities
Geriatric
Pediatric
Sensitive population groups
7. RESEARCH PROGRAMS�
8. Molecular & Cellular Therapeutics Objective: Deliverables:
1) Stoichiometric Bioscavenger + Oxime (Pseudo-catalytic)
2) Catalytic Bioscavenger
3) Encapsulation Methods
4) Stem cell Therapies and Model Systems
5) Small molecule therapies
9. Cutaneous & Ocular Therapeutics and Permeation Objective:
Eliminate or mitigate the toxic manifestations of mustard (HD) and other CWA exposures to the skin and eyes of military and civilian populations at risk. Deliverables:
1) Wound Healing of the HD-induced Wound
2) Therapy for the HD Ocular Injury
3) Improved Concepts for Therapy of HD Skin Injury
4) Understand transport through skin
10. Medical Diagnostics & Forensics Objective: �Develop, validate and implement definitive analytical methods to verify human exposure to nerve agents and sulfur mustard using relevant biomarkers.
Deliverables:
1) Nerve agent urinary metabolites – solid phase micro-extraction (SPME)
2) Beta lyase HD urinary metabolites – LC-MS-MS method
3) HD plasma protein adduct – population background study
4) Fluoride regeneration (nerve agents) – sub ng/ml method
5) Nerve and mustard agent metabolites – Proof of concept
6) Single amino acid-adduct screen for nerve and mustard
11. Neuroprotection Objective: �To eliminate or mitigate the acute and long-term toxic manifestations of nerve agent (NA) exposures of military and civilian populations at risk.
Deliverables:
1) PB-less NA treatment
2) Latent neuroprotection from NA-induced injury
12. Neurologic Therapeutics Objective: �Identify, evaluate, and transition to Drug Development new products for treating nerve agent intoxication.
Deliverables:
1) Cholinergic adjunct to NA treatment
2) Broad spectrum AChE reactivator
13. Respiratory Toxicity &Therapeutics Objective:
To develop and test in vivo and in vitro animal inhalation, percutaneous and cardio-exposure models and evaluate protective and therapeutic compounds by assessing the scope of immediate and/or temporal mechanistic events associated with exposure/treatment. Deliverables:
Establish inhalation, percutaneous, and cardio exposure models to assess chemical agent-induced injury
Identify therapeutic windows for proper medical intervention
Assess FDA-approved medical countermeasures against chemical agent injury
Next generation cyanide medical countermeasure
Cyanide detection in biological tissue
14. Agents of Biologic Origin Objective: �To develop medical countermeasures which eliminate or mitigate the toxic manifestations BoNT in military and civilian populations at risk.
Deliverables:
Establish new integrated drug screening platform
Develop post-exposure therapeutic agents: small molecule inhibitors, peptides and physiological antagonists
Accelerate recovery from BoNT intoxication: role of ubiquitin-proteosome system (UPS) and growth factors
16. 1. AAS (Midazolam):
Midazolam is ~2X more potent than diazepam. Being water-soluble it has improved pharmacokinetics and pharmacodynamics IM - it acts ~2X faster than equipotent doses of diazepam. It works against all!! agents, like diazepam, but again at a lower dose and faster. Operationally, instead of three diazepam CANAs (one w/ soldier, 2 extra w/ medic), there will now be only two (1 w/ soldier, other w/ medic). Human use trial (RAMPARTS), supported by CBMS but not sponsored by them, shows IM autoinjector delivered midazolam equieffective to IV lorazepam (Ativan) which is current standard of care in most of country for EMT Rx of seizing patients before delivery to ER. Data from our lab in conjunction w/ tony and Ben Capacio, shows effectiveness Vs diazepam against all agents in guinea pigs, pharmacokinetics against GD in GP, effectiveness against GD in rhesus along w/ pharmacokinetics and pharmacodynamics in same animals. Battelle now (May 2010) finishing up GLP study w/ ~1800 instrumented GP (vs 8 agents) and 220+ instrumented rhesus against 6 agents. Estimate that Meridian will file NDA by end of this year and first doses available to troops shortly after approval.
Phase 2 Clinical Studies
1st study completed on Dec 20, 2008; No serious or unexpected adverse events
24 subject safety / PK study
2nd study completed Apr 20, 2009; One SAE reported (idiopathic thrombocytopenia)
250 subject safety and tolerability study
3rd study completed May 4, 2009; No serious or unexpected adverse events
24 subject safety / PK study evaluating midazolam when administered with atropine
4th study scheduled completed August 14, 2009
24 subject safety / PK study evaluating midazolam when administered with atropine and 2-PAM
5th study scheduled for September 30 2009
24 subject safety / PK study evaluating midazolam when administered with PB, Atropine, and 2-PAM
2. Bioscavenger:
Incremental Solutions
Increment I: Plasma-derived butyrylcholinesterase human (HuBChE; pBioscavenger)
Increment II: Recombinant HuBChE or small molecule
Increment III: Catalytic product is currently in early tech base
3. INATS
The goal of the INATS program is to develop a treatment system that offers optimal protection against a broad spectrum of nerve agents. INATS will be licensed by the U.S. Food and Drug Administration (FDA) and will be issued to Service Members performing military operations where there is risk of nerve agent attack.
The program objective is to develop the oxime, MMB4 DMS, and atropine loaded in a two-chambered autoinjector delivery system and to obtain sufficient data to support new indications for PB, the component of Soman Nerve Agent Pretreatment Pyridostigmine (SNAPP).
FDA Clinical Hold Letter Received April 13, 2009 – lung damage found in rabbits
NOAEL 25 mg/kg in Rabbit
Will Result in Max Starting Dose of 0.27mg/kg
Efficacious dose for 5LD50 estimated at 5mg/kg
4. SNAPP
FDA approved Pyridostigmine Bromide, 30 mg tablet Feb 5, 2003
For pretreatment to soman threat only
First drug approved under FDA “Animal Rule”
As a condition of approval under the “Animal Rule,” FDA mandated four Phase 4 post-marketing studies
Marmoset study (USAMRICD)
Human intercostal muscle study (University of California-Davis)
Guinea pig study (USAMRICD)
Human blood acetylcholinesterase study (WRAIR)
1. AAS (Midazolam):
Midazolam is ~2X more potent than diazepam. Being water-soluble it has improved pharmacokinetics and pharmacodynamics IM - it acts ~2X faster than equipotent doses of diazepam. It works against all!! agents, like diazepam, but again at a lower dose and faster. Operationally, instead of three diazepam CANAs (one w/ soldier, 2 extra w/ medic), there will now be only two (1 w/ soldier, other w/ medic). Human use trial (RAMPARTS), supported by CBMS but not sponsored by them, shows IM autoinjector delivered midazolam equieffective to IV lorazepam (Ativan) which is current standard of care in most of country for EMT Rx of seizing patients before delivery to ER. Data from our lab in conjunction w/ tony and Ben Capacio, shows effectiveness Vs diazepam against all agents in guinea pigs, pharmacokinetics against GD in GP, effectiveness against GD in rhesus along w/ pharmacokinetics and pharmacodynamics in same animals. Battelle now (May 2010) finishing up GLP study w/ ~1800 instrumented GP (vs 8 agents) and 220+ instrumented rhesus against 6 agents. Estimate that Meridian will file NDA by end of this year and first doses available to troops shortly after approval.
Phase 2 Clinical Studies
1st study completed on Dec 20, 2008; No serious or unexpected adverse events
24 subject safety / PK study
2nd study completed Apr 20, 2009; One SAE reported (idiopathic thrombocytopenia)
250 subject safety and tolerability study
3rd study completed May 4, 2009; No serious or unexpected adverse events
24 subject safety / PK study evaluating midazolam when administered with atropine
4th study scheduled completed August 14, 2009
24 subject safety / PK study evaluating midazolam when administered with atropine and 2-PAM
5th study scheduled for September 30 2009
24 subject safety / PK study evaluating midazolam when administered with PB, Atropine, and 2-PAM
2. Bioscavenger:
Incremental Solutions
Increment I: Plasma-derived butyrylcholinesterase human (HuBChE; pBioscavenger)
Increment II: Recombinant HuBChE or small molecule
Increment III: Catalytic product is currently in early tech base
3. INATS
The goal of the INATS program is to develop a treatment system that offers optimal protection against a broad spectrum of nerve agents. INATS will be licensed by the U.S. Food and Drug Administration (FDA) and will be issued to Service Members performing military operations where there is risk of nerve agent attack.
The program objective is to develop the oxime, MMB4 DMS, and atropine loaded in a two-chambered autoinjector delivery system and to obtain sufficient data to support new indications for PB, the component of Soman Nerve Agent Pretreatment Pyridostigmine (SNAPP).
FDA Clinical Hold Letter Received April 13, 2009 – lung damage found in rabbits
NOAEL 25 mg/kg in Rabbit
Will Result in Max Starting Dose of 0.27mg/kg
Efficacious dose for 5LD50 estimated at 5mg/kg
4. SNAPP
FDA approved Pyridostigmine Bromide, 30 mg tablet Feb 5, 2003
For pretreatment to soman threat only
First drug approved under FDA “Animal Rule”
As a condition of approval under the “Animal Rule,” FDA mandated four Phase 4 post-marketing studies
Marmoset study (USAMRICD)
Human intercostal muscle study (University of California-Davis)
Guinea pig study (USAMRICD)
Human blood acetylcholinesterase study (WRAIR)
18. Training Facilities/Capabilities:
These are Academy of Health Sciences numbered courses for which both continuing medical education (CME) and CEU credit may be earned.
Training Facilities/Capabilities:
These are Academy of Health Sciences numbered courses for which both continuing medical education (CME) and CEU credit may be earned.
19. Consultation Mission Government agencies come to us as SMEs while writing their own policies regarding CWAs
Government agencies come to us as SMEs while writing their own policies regarding CWAs
20. Unique Facilities
21. Recapitalization - 2014
22. Human Capital Development
23. Human Capital Development MRICD’s work force of over 300 people is a mix of �civilian, military, contractor and post-doctoral level scientists
With research expertise in:
Biochemistry
Toxicology
Pharmacology
Immunology
Neuroscience
With administrative expertise in:
Budget management
Program management
Facilities Maintenance
Safety/surety
Civilians may apply through the civil service system
http://cpol.army.mil
The scientific and technical staff makes up a large percentage of our work force, but other functions – including Budget Administration, Security, Safety/Surety, Personnel, Logistics, Maintenance and Consultation – are performed as well. The scientific and technical staff makes up a large percentage of our work force, but other functions – including Budget Administration, Security, Safety/Surety, Personnel, Logistics, Maintenance and Consultation – are performed as well.
24. CONTRACTING �OPPORTUNITIES
25. Types of Contracts Personal Services
Research Collaborations
Other Research Opportunities
26. Personal Services George Washington University - Science and Engineering Apprentice Program (SEAP)
George Washington University – College Qualified Leaders (CQL)
Oak Ridge Institute for Science and Education (ORISE)
U.S. Army Research Office, Scientific Services Program (SSP)
National Research Council
27. For high school students
Placed in Department of Defense (DoD) laboratories for eight continuous weeks during the summer
Students work with scientists and engineers who act as mentors
28. George Washington University – �Science and Engineering Apprentice Program (SEAP) Program offers students a unique and positive experience encouraging them to pursue careers in science and engineering
Contacts:
Dr. Douglas Cerasoli, (410) 436-1338, douglas.cerasoli@us.army.mil
Dr. John McDonough, (410) 436-1942, john.mcdonough1@us.army.mil
29. George Washington University – �College Qualified Leaders (CQL)
30. Oak Ridge Institute for Science and Education (ORISE) U.S. Department of Energy institute focusing on �scientific initiatives to
research health risks from occupational hazards
assess environmental cleanup
respond to radiation medical emergencies
support national security and emergency preparedness
educate the next generation of scientists
Undergraduate students, graduate students, college graduates (B.S., M.S., Ph.D.)
Employed as laboratory technicians, research assistants, post docs
Contacts:
Christina Weber , MRICD Marketing Manager, (410) 436-3042, Christina.L.Weber@us.army.mil
Laura Cook, ORISE Recruiter, (410) 306-9204,
Laura.Cook@orau.org
31. U.S. Army Research Office, Scientific Services Program (SSP) Accelerated contract mechanism
Enables all federal government organizations to obtain scientific/technical services to accomplish organizational goals and mission objectives
Non-government scientists, engineers, analysts, consultants and subject matter experts can be quickly subcontracted to perform short term, well defined efforts when the expertise required is not available at the requesting government organization
32. U.S. Army Research Office, Scientific Services Program (SSP) Scope
Laboratory basic and applied research
Life Sciences
Medical and Health Sciences
Modeling and Simulation
Contact:
Kathryn C. Terry, ARO, (919) 549-4337, terry@arl.aro.army.mil
33. The National Research Council
34. Research Collaborations Outside entities have the capability to have medical chemical defense research conducted at the MRICD
Cooperative Research and Development Agreements (CRADAs)
MRICD currently supports a $1.2 M collaborative research program
Contact
Dr. John Graham, (410) 436-1197, john.s.graham1@us.army.mil
35. Research Collaborations Academia
Private industry
Other government agencies
National
International
37. Outside entities can apply for research grants through several mechanisms
Small Business Innovation Research (SBIR)
Broad Agency Announcements (BAA)
National Institutes of Health, CounterACT Program
38. Administered by the U.S. Small Business Administration Office of Technology
Ensures that the nation's small, high-tech, innovative businesses are a significant part of the federal government's research and development efforts
39. Each year, several topics are authored by MRICD scientists to supplement their research programs
Contact:
J.R. Myers, (301) 619-7377, james.myers@amedd.army.mil
www.sbir.com
40. Defense Threat Reduction Agency� Conducts basic and applied research aimed at the discovery and/or identification of better therapeutic and diagnostic medical countermeasures against chemical threat agents and toxins
Overarching goal of this research program is to enhance diagnostic and treatment response capabilities on the battlefield
Geared toward protecting the military population
41. CWA exposures and other collaborative efforts can be conducted at the MRICD in support of these grants
Contact:
Dr. Judith Laney, (703) 767-6045, judith.laney@dtra.mil
http://www.dtra.mil/Missions/ChemicalBiologicalDefense/ChemicalBiologicalDefenseHome.aspx Defense Threat Reduction Agency�
42. Countermeasures Against Chemical Threats (CounterACT)
Conducts basic, translational, and clinical research aimed at the discovery and/or identification of better therapeutic and diagnostic medical countermeasures against chemical threat agents
Overarching goal of this research program is to enhance diagnostic and treatment response capabilities during an emergency
Geared toward protecting the civilian population
43. CWA exposures and other collaborative efforts can be conducted at the MRICD in support of these grants
Contact:
Dr. David Jett, (301) 496-6035, jettd@ninds.nih.gov
http://www.ninds.nih.gov/research/counterterrorism/counterACT_home.htm
44. Grant opportunities are available at the following websites:
http://www.grants.gov
http://www.usamraa.army.mil/pages/Baa_Paa/baa_choice.cfm
CWA exposures and other collaborative efforts can be conducted at the MRICD in support of these grants
45. Patents Available for Licensing Topical Skin Protectant Against Chemical Warfare Agents Using Perfluoro Ether/PTFE Technology. McCreery, Michael J. US Patent No. 5,607,979, issued 4 March 1997. �
Site-Directed Mutagenesis of Esterases. Broomfield, Clarence A., Millard, Charles B., Lockridge, Oksana. US Patent Number 6,001,625, issued 14 December 1999. �
Method of Reducing Brain Damage Resulting From Seizures. Filbert, Margaret G., Ballough, Gerald P.H. Patent Number 6,211,230, issued 3 April 2001.�
Active Topical Skin Protectants Using Reactive Nanoparticles. Hobson, Stephen T., Braue, Ernest H., Jr., Lehnert, Erich K., Klabunde, Kenneth J., Koper, Olga P., Decker, Shawn. Patent Number 6,403,653 issued, 11 June 2002. �
Active Topical Skin Protectants Containing OPAA Enzymes and CLECs. Braue, Ernest H, Jr., Hobson, Stephen T., Govardhan, Chandrike, Khalaf , Nazar. Patent Number 6,410,604, issued 25 June 2002. �
Active Topical Skin Protectants Using Combinations of Reactive Nanoparticles and Polyoxometalates or Metal Salts. Hobson, Stephen T., Braue, Ernest H, Jr., Lehnert, Erich K., Klabunde, Kenneth J., Decker, Shawn, Hill, Craig L, Rhule, Jeffrey, Boring, Eric, Koper, Olga. Patent Number 6,410,603, issued 25 June 2002.
46. Patents Available for Licensing Active Topical Skin Protectants Containing Polyoxometalates and/or Coinage Metal Complexes. Braue, Ernest H, Jr., Hobson, Stephen T., Hill, Craig L, Boring, Eric, Rhule, Jeff. Patent Number 6,414,039, issued 2 July 2002. �
Active Topical Skin Protectants Using Hybrid Organic Polysilsesquioxane Materiels. Hobson, Stephen T., Braue, Ernest H, Jr., Shea, Kenneth. Patent Number 6,417,236, issued 9 July 2002. �
Active Topical Skin Protectants Using Hybrid Organic Polyoxometallates. Braue, Ernest H, Jr., Hobson, Stephen T., White, James, Bley, Richard. Patent Number 6,420,434, issued 16 July 2002.�
Active Topical Skin Protectants Using Polymer Coated Metal Alloys. Hobson, Stephen T., Braue, Ernest H, Jr., Back, Dwight. Patent Number 6,437,005, issued 20 August 2002. �
Active Topical Skin Protectants. Braue, Ernest H, Jr., Hobson, Stephen T., Lehnert, Erich K. Patent Number 6,472,437, issued 29 October 2002.�
47. Patents Available for Licensing Active Topical Skin Protectants Containing S-330. Braue, Ernest H., Mershon, Millard M., Braue, Catherine R., Way, Ruth A. Patent Number 6,472,438, issued 29 October 2002.
Floating Cryostat Sections for use in Light and Electron Microscopy. Petrali, John P., Kan, Robert Kwai, Hamilton, Tracey A., Oglesby-McGee. Patent Number 6,555,334, issued 29 April 2003. �
Method for Self-Detection of Pupillary Response. Petrali, John P. Patent Number 6,637,885, issued 28 October 2003. �
Automated Method of Identifying and Archiving Nucleic Acid Sequences. Schlager, John J., Sweeney, Richard E., US Patent Number 6,871,147, issued 22 March 2005. �
Compositions and Methods for Reducing Blood and Fluid Loss from Open Wounds. Mershon, Millard M., US Patent Number 7,303,759, issued 4 December 2007.
48. Patents Available for Licensing
Chemical agent decontamination composition comprising a perfluorinated alkyl bromide. Johnston, D; Platoff, G; Baskin, S; Logan, T. US Patent Number 7,371,714, issued 13 May 2008.
Compositions & Methods for Reducing Blood & Fluid Loss from Open Wounds. Mershon, Millard M., 7,303,759, issued 4 December 2007.
Contact:
Suaquita Perry, (410) 436-1339, MRICD-ORTA@amedd.us.army.mil
50. QUESTIONS?��
