Transcript Slide 1
Michael A. Swit, Esq.
Vice President
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FDA Regulatory Issues and
Ophthalmic Drug Development
Pharmaceutical Education Associates
4th Annual Ophthalmic Drug Development & Delivery Summit
September 2008
Del Mar, California
Standard Disclaimers
Views expressed here are solely my own and do not
necessarily reflect those of my firm or any of our clients.
These slides support an oral briefing and may not be relied
upon solely on their own to support any conclusion of law
or fact.
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FDA Path – New and Old Hurdles
New Hurdles
Changed realities –
Drug Safety focus – post-Vioxx
Pressure on use of accelerated approvals
Pressure on use of priority reviews
Impact of FDAAA – new FDA weaponry and company duties
REMS
Clinical Trial Registries
PDUFA
Pediatric studies
Old Hurdles
Traditional challenges of regulatory path – will be our focus today, with
an emphasis on taking a look at a couple recent ophthalmic approvals for
guidance
Speaking of guidance – there is not much out of FDA in the ophthalmic
arena
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The FDA Path – Start to Finish
Lab Studies (most) – not FDA regulated – not our concern today
Preclinical aka Tox – beginning of FDA concern
Pre-IND Submission and Package
IND
Phase 1
Phase 2
End of Phase 2 Meeting
Phase 3
Pre-NDA/BLA Filing Meeting
NDA/BLA Filing
Review Clock
Advisory Committee
Approval
Post-Marketing Commitments – commonly:
Pediatric Study
REMS
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Two Drugs – How They Progressed
Lucentis (ranibizumab injection) -- for treatment of patients
with neovascular (wet) age-related macular degeneration
– June 2006
Macugen (pegaptanib sodium injection) – for treatment of
wet age-related macular degeneration –
-- December 2004
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Preclinical/Tox
Goal – to develop
sufficient data to
support an IND to
institute human studies
Lucentis – key issue – appropriate animal
model – because Lucentis was thought to act
on vascular endothelial growth factor
(VEGF) – chose cynomologous monkey
model – 99% homology to human VEGF
Macugen –
Able to secure a waiver of carcinogenicity
studies by showing low systemic absorption
and negative SHE cell assays
Consistent with ICH guidance
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Pre-IND Submission and Package
Key Step in Development
Need to lay out both tox work done and best statement of rest of
development plan
Trying to secure “buy-in” for Phase 1 and 2, if possible
Essential that it be very well-prepared and asks the questions in the best
way as to assure FDA provides the correct reply
Actual meeting
Rehearse, rehearse, rehearse
Be careful who you bring
Coordinate with EU “scientific advice” process – despite
“harmonization,” never assume what FDA wants will satisfy the EMEA
or member states
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Investigational New Drug Exemption -- IND
If you did the pre-IND well, this will follow easily
Remember – is not an “approval” – is a notice system.
30 days
If FDA has a problem, will issue “clinical hold” letter
Exemptions – limited –
marketed products under some circumstances
Even if marketed product, will need IND if seeking to change
new claims
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Phase 1
Goal – establish the
pharmacology, safety,
and, occasionally,
preliminary evidence
of effectiveness
Safety – of different
Lucentis – instead of volunteers, used AMD
patients due to the risk linked to the
intravitreal injection
Macugen – 4 different Phase 1/2 studies –
an aggregate of about 60 individuals
dosages and to see if
there are any doselimiting toxicities
Dose selection –
commonly – those
with fewest reactions
go to Phase 2 and 3
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Phase 2
Goal – determine
minimum dose that is
maximally effective in
target populations
Lucentis – key issue – tested various
doses and dosing regimens
Macugen – did four Phase 1/2 studies for
dose ranging – relatively small number of
patients
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End of Phase (EOP) 2 Meeting
Critical Meeting –
Forms basis for Phase 3 approach – get input on design of
Phase 3 pivotal clinicals
Some will use to obtain a SPA – Special Protocol
Assessment – that (theoretically) binds FDA to not change
the rules
Challenges of an SPA
Can lock you into a format that might restrict your ability to adjust the
clinical as you learn more about the drug
If you miss on study endpoints, you may have less of an ability to use
sound science as to why the studies may still support an approval of an
appropriate indication
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Phase 3
Goal – perform two
“adequate and wellcontrolled” clinical
investigations
Result – will satisfy
“substantial evidence”
requirement of Federal
Food, Drug, and
Cosmetic Act needed to
support NDA approval
(parallel legal
requirements for BLA
licensing)
Lucentis –
Multi-center, randomized, double blind with
sham injection as an inactive control
Bias – minimized by using separate treating
and evaluating physicians
Strict inclusion/exclusion criteria
Two different treatment doses to look for
dose response
Study endpoints – AMD
Visual acuity – FDA -- doubling of visual
angle – 15 letters on the Early Treatment
Diabetic Retinopathy Study (ETDRS) visual
acuity chart measured at 4 m or more =
clinically relevant
Surrogates (e.g., retinal thickness) – must be
validated to clinical effect
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Phase 3 …
Goal – perform two
“adequate and wellcontrolled” clinical
investigations
Result – will satisfy
“substantial evidence”
requirement of Federal
Food, Drug, and
Cosmetic Act needed to
support NDA approval
Note: legal requirements
for BLA licensing are
worded differently, but
essentially enforced same
Macugen
Two virtually identically designed studies
Patients
EOP1003 – 622 patients - EOP1004 – 586 patients –
Design – multi-center, randomized, sham-
injection controlled, double blind, dose
finding (.3, 1 or 3 mg.)
Study endpoints – AMD – same as Lucentis
Visual acuity – FDA -- doubling of visual
angle – 15 letters on the Early Treatment
Diabetic Retinopathy Study (ETDRS) visual
acuity chart measured at 4 m or more =
clinically relevant
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Pre-NDA/BLA Filing Meeting
Vital meeting
To ensure that key issues related to data for filing are properly
addressed
REMS – get buy-in from FDA on any remaining safety signals
and how they might be addressed by the panoply of options
articulated in FDAAA, such as:
Studies (non-clinical)
Clinical trials (e.g., Phase 4)
Patient registries
Education programs
Dispensing restrictions (e.g., only if certain test results filed), etc.
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NDA/BLA Filing
Goal – ensure that the
submission is
sufficiently complete
that it is “accepted for
filing”
Worst scenario –
RTF or “refuse to file”
Lucentis –
Had separate clinical and CMC pre-filing
meetings
Macugen –
filed as a rolling submission
Did not have a pre-NDA meeting
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Review Clock
Goal – if possible,
Lucentis – did get priority review – as
secure fastest review
cycle
Priority – significant
therapeutic advance
over available therapies
– 6 month
Standard – 10 months
regarded as an improvement on existing
therapies (not clear how)
Macugen – Fast Track status awarded
(similar treatment to priority review) –
unmet medical need
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Advisory Committee
Goal – to provide
Lucentis – no unique safety or
expert guidance to
FDA on key safety or
clinical issues
presented by filed
applications
New Rule – as of
10/07, most new
molecular entities will
need an Adv. Com.
meeting
effectiveness issue – thus, did not require
an Advisory Committee
Macugen – did go through as it was first
in class and route of administration for
atypical
Made the recommendation on educating
on aseptic handling
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Approval
Standard – NDA --
“substantial evidence” of
effectiveness and drug can
be safely used per labeling
BLA – “safe, pure and
potent” – but basic
approach is same as with
NDA
FDA Review Responses
RTF – refuse to file
Complete Response –
that the review period has
completed
Approval
July 10, 2008 – Final Rule
issued on FDA replies to
NDAs/BLAs – 73 Fed.
Reg. 39588
Lucentis – Two efficacy studies:
FVF2598g –
Sham control
Monthly injections
Minimally classic or occult
FVF2587g
Active control – verteporfin PDT
Monthly injections
Predominantly classic AMD
Result – nearly 95% of subjects maintained their vision
at 12 months
Approval – based on 12-month data; but studies were
planned as 24-month
FVF3192g – studied dosing of Lucentis every 3 months
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Approval …
Standard – NDA --
“substantial evidence” of
effectiveness and drug can
be safely used per labeling
BLA – “safe, pure and
potent” – but basic
approach is same as with
NDA
FDA Review Responses
Macugen –
Approval based on 1 year data from a 2-year study
and partial 2nd year data
Four-arm study
3 treatment groups
.3 pegaptanib
1 mg.
3 mg
Sham group
RTF – refuse to file
Complete Response –
that the review period has
completed
Approval
July 10, 2008 – Final Rule
issued on FDA replies to
NDAs/BLAs – 73 Fed.
Reg. 39588
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REMS
Used prior to FDAAA
Lucentis -- none
Memorialized by
Macugen – Educate medical providers
FDAAA
Can take many forms
Labeling
of the aseptic conditions required for the
drug’s administration to reduce risk to
patients
Patient education
Doctor education
Testing requirements
Inclusion criteria for
patients (e.g., negative
pregnancy test for
Accutane)
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Post-Marketing Commitments
Goal – may vary –
commonly to track a
safety signal identified in
earlier studies,
particularly Phase 3
May now be required by
FDA as part of a REMS
Will include timelines for
completion
Lucentis –
Develop and validate assays to characterize
immune response to ranibizumab from banked
serum in Phase 3 trials to try to determine
potential antibody response effects
More characterization of dosing regimen
CMC data to reflect mfg. data and stability
Macugen
2-year study (minimum) – see if any
degenerative effects on neurosensory retina
following intravitreal admin.
1-year study (minimum) – adverse effects on the
corneal endothelium
2-year study (minimum) – safety & effectiveness
of 2 additional doses below 0.3 mg.
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A Few Tips of the Trade
Non-standard Manufacturing Process
Specialized pharmaceutical dosage forms (certain modified release
preparations)
Incorporation of new technology into a conventional process
Specialized processes involving new technologies
Nonstandard methods of sterilization
If non-standard process, may require validation data
on 3 production scale batches at time of NDA
If using a drug delivery system (device), provide Risk Analysis on
the device (ISO 14971) – required in some countries in the EU before
the CTA can be approved
Some EU countries require a Risk Minimization Plan for the CTA
and also for the MAA
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A Few Tips of the Trade …
Emerging trends in FDA demands:
endothelial cell counts
comfort studies
endotoxin testing for all ophthalmic drugs, not just ones used during
surgery. Can change
how excipients and actives are handled
may require upgrades to manufacturing water systems.
DMFs – make sure updates, especially for new USP residual solvents
requirements
Degradation products - if concentration of your ophthalmic
preparations is low -- and thus the exposure itself is low– may be more
degradation products needing quantitation as above the ICH limit.
Be prepared to justify your specifications
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Resources
FDA website –
Drug Approval Process --
http://www.fda.gov/cder/regulatory/applications/
Drugs @ -- for info on individual drug approvals such as links to reviews,
approval letters, etc.
http://www.accessdata.fda.gov/scripts/cder/drugsatfda/
FDA listservs – updates on key CDER regulatory issues -- visit
“Regulatory Pitfalls in Product Development” – Presentation by
Michael Swit at PEA Pipeline to Product Conference, November 2007 –
available from Michael Swit by request
“Regulatory Considerations in the Development of Ophthalmic
Sustained Drug Delivery Systems.” Susan Caballa, Vice President, Alimera
Biosciences. PEA Ophthalmic Drug and Delivery Summit, Sept. 2007 –
available from Michael Swit by request
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Questions?
Call, e-mail, fax or write:
Michael A. Swit, Esq.
Vice President
The Weinberg Group Inc.
336 North Coast Hwy. 101
Suite C
Encinitas, CA 92024
Phone 760.633.3343
Fax 760.454.2979
Cell 760.815.4762
[email protected]
www.weinberggroup.com
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About your speaker…
Michael A. Swit, Esq., is a Vice President at THE WEINBERG GROUP, where he develops and ensures the
execution of a broad array of regulatory and other services to drug, biologics and medical device/diagnostic clients
seeking to market products in the United States. His expertise includes product development strategies, compliance
and enforcement initiatives, recalls and crisis management, submissions and related traditional FDA regulatory
activities, labeling and advertising, and clinical research efforts.
Mr. Swit has been addressing critical FDA legal and regulatory issues since 1984. His multi-faceted experience
includes serving for three and a half years as corporate vice president, general counsel and secretary of Par
Pharmaceutical, a prominent, publicly-traded, generic drug company and, thus, he brings an industry and commercial
perspective to his work with FDA-regulated companies. Mr. Swit then served for over four years as CEO of
FDANews.com, a premier publisher of FDA regulatory newsletters and other specialty information products for the
FDA-regulated community. His private FDA regulatory law practice has included service as Special Counsel in the
FDA Law Practice Group in the San Diego office of Heller Ehrman White & McAuliffe and with the Food & Drug
Law practice at McKenna & Cuneo, both in the firm’s Washington office and later in San Diego. He first practiced
FDA regulatory law with the D.C. office of Burditt & Radzius.
Mr. Swit has taught and written on a wide variety of subjects relating to FDA law, regulation and related commercial
activities, including, since 1989, co-directing a three-day intensive course on the generic drug approval process and
editing a guide to the generic drug approval process, Getting Your Generic Drug Approved. A former member of the
Food & Drug Law Journal Editorial Board, he also has been a prominent speaker at numerous conferences sponsored
by such organizations as RAPS, FDLI, and DIA. A magna cum laude graduate of Bowdoin College, he received his
law degree from Emory University Law School and is a member of the California, D.C. and Virginia bars.
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