680 likes | 1.36k Views
The Future of Combination Products. Bradley Merrill Thompson, MBA, JD, RAC Epstein Becker & Green PC RAPS San Francisco, CA April 27, 2007. Topics. Overview Where are Combination Products Going? Where is Combination Product Regulation Going?
E N D
The Future of Combination Products Bradley Merrill Thompson, MBA, JD, RAC Epstein Becker & Green PC RAPS San Francisco, CA April 27, 2007
Topics • Overview • Where are Combination Products Going? • Where is Combination Product Regulation Going? • Where is the Combination Product Regulatory Profession Going? • Where are the Challenges and Opportunities?
Overview • What are combination products? • What is the Combination Product Coalition?
What is a Combination Product? • Statute -- 503(g)(1) • Products that constitute a combination of a drug, device, or biologic • Combination products are diverse: • Drug-device • Device-biologic • Drug-biologic • Drug-device-biologic
Three Types of Combination Products • 21 CFR 3.2(e) • Single-entity: a product comprised of two or more regulated components that are physically, chemically or otherwise combined or mixed as a single entity • Kits: two or more separate products packaged together (e.g., drug and device products) • Cross-labeled: provided separately but intended for use together where both are required to achieve the intended use and where cross labeling is needed
Not Combination Products • Most concomitant use of drugs, devices and biologics • Drug-drug, device-device, or biologic-biologic combinations • Example: Products with two biologics, even if shared CDER and CBER role • General devices intended for use with a class of or otherwise unspecified drug/biologic products • Example: Unfilled syringe or diagnostic test without specifying a particular drug
Different Frameworks NDA, BLA, PMA, 510(k), IND, IDE CDRH CDER CBER Device Drug Biologic Different Types Different Reviews How are they Regulated?
CPC: Purpose • To clarify and streamline the regulatory paradigm for combination products • While protecting the public health
Membership • Up to 20 drug, device and biologics companies have engaged in CPC activities. Some members include: • Abbott • Baxter • Becton Dickinson • Pfizer • Roche Diagnostics • Most active participants are regulatory affairs professionals for member companies. • Diversity of industry representation is encouraged.
Activities • Started in 2003 with developing consensus policy positions • Advocating policy positions and working collaboratively with FDA • Providing comments to FDA on proposed rules and guidances • Partnered with RAPS to host January 2005 policy summit attended by about 150 people. • Topics included cross labeling, kit labeling and the labeling of single entity products. • The summit resulted in a consensus white paper that was submitted to FDA.
Current CPC Key Priorities • Cross labeling • Modification of approved combination products • Adverse incident reporting • Quality systems/GMPs • Clarification of OCP role
Companies interested in CPC should visit: www.combinationproducts.com Membership structure Policy Positions
Where Are Combination Products Going? • Drivers • Examples • Quantitative • Reviews • Projections
Combination Product Drivers • Clinical • Need/want enhanced outcomes in both safety and effectiveness • Systemic effects and toxicities eliminate too many candidates, which in turn drives localized delivery, targeting and individualized therapy • Economic • Slow down in pharma industry productivity • Cost and times for new drug development are high • Patent life limitations • Growing tendency to collaborate
Collaboration Leads to Combinations • Study publicized 166 intractable scientific problems owned by high tech companies • Almost 1/3 quickly solved by mostly off-the-shelf technologies • Majority of solutions came from people versed in other fields • Indeed, the further from the field of the problem, the more likely they were to solve it Harvard Business School, Lakhani, et al Oct. 2006
The “Ice Tray” Model of Convergence Dynamics • Silos: Knowledge, methods and discoveries made in isolated technology sectors. • Connection: One well connects to another. Knowledge can be applied quickly to adjacent areas. • Convergence: Greater innovation in the connected region than in the individual wells.
Converging Technologies Genomics Bioinformatics Proteomics BIOTECH Pharmaceuticals Diagnostics Research/Info Tools Industrial INFOTECH Hardware Software Communications INFOTECH Hardware Software Communications Biosensors Biochips Bioelectronics Microfluidics Nanabiotechnology Drug Delivery Nanodevices Nanosensors Nanoelectgronics NANOTECH Electrical Structural Biomedical Energy & Environment Adapted from: Biology, Bioconvergence, Information And Enterprise: Taking the Broad of View May 20, 2004 Alan Barrell.
Platforms to Watch • Tissue Engineering • Micro-electrical mechanical systems • Biomaterials • Gene and protein delivery • Targeted medicine • New routes for delivering drugs Nature Biotechnology (March 2006)
Number and Types of Combination Products FY 2005 COMBINATION PRODUCT KEY: 1 = convenience kit or co-package 2 = prefilled drug delivery device/system 3 = prefilled biologic delivery device/system 4 = device coated, impregnated, or otherwise combined with drug 5 = device coated or otherwise combined with biologic 6 = drug/biologic combination 7 = separate products requiring mutually conforming labeling 8 = possible combination based on mutually conforming labeling of separate products 9 = other type of combination product
Combination Product Applications 2005 CBER CDER CDRH
Combination Product Application Trend Number of Submissions
Quantitative Projections • The combination products market is estimated at $5.98B in 2004, and will continue to grow at a compound annual rate of 10% through 2009. By 2009, the market is expected to reach approximately $9.5B worldwide. • Source: Navigant Consulting, Inc. • The global market for drug-device combinations is expected to increase at an average annual growth rate of 13.6% and reach $11.5B in 2010, compared with $5.4B in 2004. • Source: Business Communications Co., Inc. • The US drug delivery market is expected to reach nearly $91B by 2009. • Source: Fuji-Keizai, 2006
Nanotechnology Projections • The 2005 market size for nanotechnology drug delivery systems alone was estimated at $980 million and expected to gross 54% annually over the next five years. • Source: The Nanotech Report 4th Edition, Lux Research, 2006. • The demand for nanotechnology medical products will grow by more than 17% annually to reach $53 billion in 2011. • Source: The Fredonia Group, Nanotechnology in Health Care to 2011 Report, February, 2007.
Nanotechnology Projections • With at least 12 nanomedicines already approved and progressively more in active development, the next five years should see a steady succession of new nanotech-based drugs, imaging agents, and diagnostic products entering the marketplace. • Source: Advance Tech Monitor, 2006. • As of mid-2006, 130 nanotech-based drugs and delivery systems and 125 devices or diagnostic tests were in preclinical, clinical or commercial development. • Source: The Nanotech Report 4th Edition, Lux Research, 2006. • The combined market for nano-enabled medicine (drug delivery, therapeutics and diagnostics) will jump from just over $1B in 2005 to almost $10B in 2010. The US National Science Foundation predicts that nanotechnology will produce half of the pharmaceutical industry product line for 2015. • Source: The Nanotech Report 4th Edition, Lux Research, 2006.
Congress FDA Internationally Where Is Combination Product Regulation Going?
Congress • Where has Congress been recently? • Where is Congress going?
Historical Development • Safe Medical Devices Act (1990) • Added § 503(g) • Required determination of “primary mode of action” (i.e., drug, device, or biologic) • Gave primary jurisdiction to the center with premarket review authority for that type of product
Historical Development • Food and Drug Administration Modernization Act of 1997 (“FDAMA”) • Added § 563, Request For Designation • Allowed sponsor to request designation as drug, biologic, device, or combination product, and/or reviewing center
Historical Development • Medical Device User Fee and Modernization Act of 2002 (“MDUFMA”) • Established Office of Combination Products in order to assure: • Prompt designations and review assignments • Timely and effective premarket review • Consistent and appropriate postmarket regulation
Where is Congress Going? • New user fee bill • No specific talk about combination products • Future issues • Some talk of unified regulation for combination products, but not serious yet • Other talk of unified adverse reporting system • Congress trails technology, instead of leading • That’s not a bad thing, unless they fall too far behind
Where is FDA Going? • Office of Combination Products • GMPs • Adverse Events • Cross Labeling • Submissions • User Fees
Office of Combination Products • In a state of flux, with new leadership • Dr. Joanne Less replaces Mark Kramer • Formerly Associate Director for Clinical Research at CDRH • Statutory Duties • Assignment of combination products • Ensure timely and effective premarket review • Consistent and appropriate postmarket regulation • Dispute resolution (timeliness vs. substance) • Review/update guidance, agreement, practices • Reports to Congress • Resource to sponsors and review staff • P.L. 107-250 – enacted 10-26-02
GMPs • Proposed Rule due any week/month • Likely themes • Combination product manufacturers must meet the requirements of both sets of applicable GMP regulations. Manufacturers may choose an “umbrella” system under which to operate, but this system must meet the requirements of both sets of applicable GMP regulations. • Manufacturers must implement certain specific provisions in order to achieve compliance with both sets of regulations (e.g., design controls, purchasing controls, and CAPA for devices).
GMPs • More Likely Themes • May be a regulatory obligation to comply with certain GMP requirements even before constituent parts are physically combined, merged, or joined. • For example, design controls may come into play before actual physical combination of a combination product’s constituent parts. • Manufacturers cannot delegate ultimate responsibility for GMP compliance. • While it might be acceptable to accept supplier design controls, a manufacturer is ultimately responsible for ensuring adequate compliance with all GMP requirements, including those where a contractor helps. • Manufacturers should be cognizant of separate design control issues at the overall combination product level – i.e., after the manufacturer doing the final assembly receives the component/constituent part from the supplier. • Design controls apply to all constituent parts and the finished combination product--not just the device constituent part.
Adverse Events • Proposed Rule expected any week/month. • Likely content • Might propose mechanisms by which the postmarket safety reporting requirements ordinarily associated with the marketing application used to approve or clear a combination product may be supplemented, as appropriate, to take into account the combination nature of the product, or • Might propose a reporting scheme in which the same types of postmarket safety reports would be submitted for a combination product, regardless of the type of marketing application used for its approval or clearance • Look at September 2005 Concept Paper
Cross Labeling • May 10, 2005 Public Meeting • Transcript and presentations accessible on OCP website • New straw man proposal due out any week/month • New public meeting planned to discuss proposal
What is Cross Labeling? • A drug, device, or biological product packaged separately that according to its investigational plan or proposed labeling is intended for use only with an approved individually specified drug, device, or biological product where both are required to achieve the intended use, indication or effect and where upon approval of the proposed product the labeling of the approved product would need to be changed, e.g. to reflect a change in intended use, dosage form, strength, route of administration, or significant change in dose…. 21 CFR 3.2(e)(3)
What’s So Hard About That? Hypothetical Company A is the sponsor of approved Drug A. Company B wants to obtain premarket approval for Device B that will administer Drug A in a new dosage form, strength, route of administration, or intended use. Company A does not want to cooperate with Company B in this venture. Can FDA approve Device B?
Some of the Questions… What does individually specified mean? What if Device B has other approved intended uses? When does label of Drug A “need to be changed”? If labeling of Drug A does need to be changed, but Company A does not want to submit a supplement to its marketing application, does that mean that Device B cannot be approved?
Protect and Promote the Public Health • FDA prefers cooperation. • In the absence of cooperation, FDA’s goal is to identify a regulatory pathway for Device B while ensuring adequate regulatory oversight. • Consider whether labeling of Drug A “needs to be changed”: • Is Drug A intended to be used for a new intended use, dosage form, strength, or route of administration? • Is end user confusion likely? • What would happen if Drug A is reformulated or redesigned without notice to Company B? • Would Company B rely on proprietary information in application covering Drug A?
Submissions • Questions: • Initial submissions—number of them • Supplements for product modifications • Guidance • September 2005 Concept Paper for initial submissions • Close to guidance on product modifications, unless goes to rulemaking
Initial Submissions • Agency goal seems to be to prescribe the number and type to be filed • CPC has argued for greater freedom to determine the approval pathway, within the confines of the law. • We explain that a lot of factors, many of which the agency won’t know, affect the optimal approval route • Not clear where the agency is going
Submissions for Product Modifications • Agency has a draft guidance in hand • However, still grappling with fundamental questions such as guidance or rulemaking • Addresses pathway/type of submission issue, rather than type of evidence or data required • CPC has a draft guidance in hand • Will shift to developing questions and case studies
Draft User Fee Guidance • Single marketing application: fee associated with that type of application • Multiple marketing applications: fee for each application • Sponsor may choose to submit two marketing applications (limited waivers/reductions possible) • FDA may require multiple applications -- fees still required for each application (waivers/reductions possible)
Draft User Fee Guidance • Draft User Fee Guidance (cont.) • Waivers: • Innovative combination products (only if FDA requires multiple applications) • MDUFMA and PDUFA waivers available
Draft User Fee Guidance • CPC Comments • FDA needs to address issue of what assignment means • Specific enhancements recommended: • Clarify when multiple filings required • Provide automatic waiver of partial fee when FDA requires multiple applications • Expand eligibility for Innovative Combination Product waiver to: • Sponsors choosing to file multiple applications • Products approved and labeled for another use • Products that offer significant benefits other than “clinical”
International Trends • Other jurisdictions are lagging behind FDA in the development of new guidance and approaches • In Europe, specific regs not yet in place • Europe's approach is similarly based on primary mode of action, although it is determined differently • Medical Device Directive lays out pathway for combination products that operate as devices • If the drug and device are a single integral product that is intended exclusively for use in a given combination, gets regulated as a drug. • On the other hand, if a device incorporates a drug as an integral part and the drug acts on the body in an ancillary manner, the product is regulated as a device. • In the case of a tie, it’s a drug • There is a consultation procedure (MEDDEV 2.1/3 rev. 2 (2001)) • Little energy is being directed at harmonization
Growth • RAPS research shows steady growth in the number of regulatory professionals involved in combination products – from an estimated 12% in 1999 to nearly 30% today. • Source: Sherry Keramidas, PhD, RAPS Executive Director, September 2006.