Evaluating A Systemic Therapy Psoriasis 1.Efficacy 2.Safety 3.Labeling.

Slides:

Advertisements

Similar presentations

Medication Therapy Management The Patient and Provider Variables.

Advertisements

Safety and Extrapolation Steven Hirschfeld, MD PhD Office of Cellular, Tissue and Gene Therapy Center for Biologics Evaluation and Research FDA.

Raptiva™ (efalizumab) Plaque Psoriasis: The Unmet Need

Clinical Trials Medical Interventions

Hyperbilirubinemia: Discussion Alexis Thompson, MD Catherine Wicklund, MS, CGC.

Manufacturer: Celgene Corporation FDA Approval Date: 9/23/14

The ICH E5 Question and Answer Document Status and Content Robert T. O’Neill, Ph.D. Director, Office of Biostatistics, CDER, FDA Presented at the 4th Kitasato-Harvard.

Rituximab (RITUXAN) & Multiple Sclerosis

Office of Drug Evaluation IV, CDER FDA/IDSA/ISAP Workshop 4/16/04 Overview of PK-PD in Drug Development Programs: FDA Perspective FDA/IDSA/ISAP Workshop.

T-PA in Treatment of Acute Stroke: What We Know From NINDS 2004 vs 2000 Sidney Starkman, MD Departments of Emergency Medicine and Neurology, UCLA UCLA.

Drug and Therapeutics Committee Session 7A. Identifying Problems with Medicine Use: Indicator Studies.

1 OTC Omeprazole Magnesium (Prilosec 1 TM ) October 20, 2000 Larry Goldkind MD Division of Gastrointestinal and Coagulation Drug Products CDER, FDA.

As noted by Gary H. Lyman (JCO, 2012) “CER is an important framework for systematically identifying and summarizing the totality of evidence on the effectiveness,

Trastuzumab [Genentech Inc.] Labeling Supplement to Include FISH Testing as a Method to Select Patients for Treatment FDA Clinical Review December 5, 2001.

1 The Chemoprevention of Sporadic Colorectal Cancer Issues Surrounding a Benefit/Risk Analysis in Clinical Trials Mark Avigan MD CM Medical Officer Division.

Gail M. Zimmerman President and CEO National Psoriasis Foundation Portland, Ore. Testimony to the FDA Dermatologic and Ophthalmic Drugs.

Stages of drug development

Design of Clinical Trials of Antibiotic Therapy for Acute Otitis Media

Low Adherence of Hypertension Patients to Treatment – What Is To Be Done? Clinical Problem for Public Health Alexander V. Sergeev, MD, PhD, MPH Irina B.

1 Lotronex ® (alosetron HCl) Tablets Risk-Benefit Issues Victor F. C. Raczkowski, M.D. Director, Division of Gastrointestinal and Coagulation Drug Products.

Alefacept (Amevive ® ) Dosing Efficacy Compliance Links Patient Profile Introduction Clinical Experience Cost of Treatment PsoriasisGuide Side-Effects,

Presented by Lee S. Simon, MD Division Director Analgesic, Anti-inflammatory and Ophthalmology Drug Products ODEV, CDER, FDA at the Arthritis Advisory.

Hormone Refractory Prostate Cancer A Regulatory Perspective of End Points to Measure Safety and Efficacy of Drugs Hormone Refractory Prostate Cancer Bhupinder.

Placebo-Controls in Short-Term Clinical Trials of Hypertension Sana Al-Khatib, MD, MHS Assistant Professor of Medicine Division of Cardiology Duke University.

TAP PHARMACEUTICAL PRODUCTS INC. June 2, Arthritis Drugs Advisory Committee TAP Pharmaceutical Products Inc. June 2, 2004.

Pulmonary-Allergy Drugs Advisory Committee May 1, 2007 FDA Presentation Advair Diskus 500/50 Carol Bosken, MD, ScM, MPH Medical Officer Division of Pulmonary.

PATIENT-CENTERED OUTCOMES RESEARCH INSTITUTE PCORI Board of Governors Meeting Washington, DC September 24, 2012 Anne Beal, MD, MPH, Chief Operating Officer.

DIVISION OF REPRODUCTIVE AND UROLOGIC PRODUCTS Physician Labeling Rule Lisa Soule, M.D.

C-BR- 1 Raptiva ™ (efalizumab) Benefit:Risk Assessment Charles Johnson, MB, ChB Senior Director Head of Specialty Biotherapeutics Genentech, Inc.

History and Overview of OTC Topical Antifungal Drug Products Houda Mahayni, R. Ph., Ph.D. Division of Over-the-Counter Drug Products.

1 Assessing Cancer Risk & Assuring Safe Use of Topical Immunosuppressants: Recent History Susan K. Cummins, MD, MPH Medical Team Leader OCTAP and OPT.

Pompe Disease Evidence Evaluation Michael Watson, PhD, on behalf of Piero Rinaldo, MD, PhD, and the Decision-Making Workgroup October 1, 2008.

Peripheral and Central Nervous System Drugs Advisory Committee Meeting - March 14, Issues Related to the Development of Drugs for the Treatment.

06/02/04DRAFT1. 06/02/04DRAFT2 QUESTIONS FOR PANEL Trial Design 1.The sponsor makes outcome comparisons between the selected subgroups of LVAS and control.

1 Agenda  Overview –Burt Adelman MD  Efficacy and Pharmacodynamics –Akshay Vaishnaw MD, PhD  Safety –Gloria Vigliani MD  Alefacept Risk Benefit Profile.

Recommendation Methods Advisory Committee on Heritable Disorders and Genetic Diseases of Newborns and Children Ned Calonge, M.D., M.P.H.

1 Study Design Issues and Considerations in HUS Trials Yan Wang, Ph.D. Statistical Reviewer Division of Biometrics IV OB/OTS/CDER/FDA April 12, 2007.

1 PHOTOFRIN® PDT for High-grade Dysplasia in Barrett’s Esophagus Edvardas Kaminskas, M.D. Medical Officer, CDER, ODE III, DGCDP Milton Fan, Ph.D. Statistical.

1 Observations from Past Approvals for Acute Bacterial Sinusitis Janice Pohlman, M.D. AIDAC Meeting, October 29, 2003.

Long-Term Efficacy Data for Psychiatric Drugs Thomas Laughren, M.D. Director, Division of Psychiatry Products (HFD-130) PDAC Meeting (Oct 25, 2005)

1 Presented by Kenneth M. Verburg, Ph.D. at the Arthritis Advisory Committee meeting 07/29/02.

1 International Society for CNS Clinical Trials and Methodology FDA Advisory Committee Meeting Proposed Requirement for Long-Term Data to Support Initial.

General Regulatory Issues in the Development of Drugs Intended for Treatment of Chronic Illness Sharon Hertz, M.D. Medical Officer Division of Anesthetic,

1 Cardiovascular and Renal Drugs Advisory Committee Questions June 24, 2008 Ira Krefting, MD.

Module IV - Identification of Patients for Buprenorphine Treatment BUPRENORPHINE TREATMENT: A TRAINING FOR MULTIDISCIPLINARY ADDICTION PROFESSIONALS.

Acute Otitis Media: Lessons Learned Thomas Smith, M.D. Division of Anti-Infective Drug Products.

Advisory Committee for Peripheral and Central Nervous System Drugs March 7, 2006 Question 1: 1.Has Biogen demonstrated natalizumab’s efficacy on reduced.

Charge to the Committee Mark Goldberger, M.D., M.P.H. Director, Office of Drug Evaluation IV CDER / FDA.

Pharmacogenetics (PGx) of Irinotecan: Scientific and Clinical Impact of UGT Polymorphism: Background Clinical Pharmacology Subcommittee of ACPS November.

Comments on FDA Concept Paper Sidney N. Kahn, MD, PhD President Pharmacovigilance & Risk Management, Inc. Risk Assessment of Observational.

Circulatory System Devices Panel Questions for Discussion EMBOL·X Aortic Filter October 23, 2002.

1 Agenda  Overview –Burt Adelman MD  Efficacy and Pharmacodynamics –Akshay Vaishnaw MD, PhD  Safety –Gloria Vigliani MD  Alefacept Risk Benefit Profile.

Zometa for Prostate Cancer Bone Metastases Protocol 039 Amna Ibrahim, M.D. Oncology Drug Products FDA.

Blood : R2 임규성.  Immune thrombocytopenic purpura (ITP) is an autoimmune disease characterized by low platelet counts and may be responsible.

Off-Label Use in Managed Care Pharmacy Presentation Developed for the Academy of Managed Care Pharmacy Updated: February 2016.

Drug Development Process Stages involved in Regulating Drugs

Clinical Trials Medical Interventions

The Role of Statistics in Clinical Trials

Critical Reading of Clinical Study Results

Does the Beer’s Criteria Influence Prescribing for Geriatric Patients?

The Nursing Process and Pharmacology Jeanelle F. Jimenez RN, BSN, CCRN

Clinical Trials.

Health care resource use, productivity, and costs among patients with moderate to severe plaque psoriasis in the United States Caroline P. Schaefer,

WORCESTERSHIRE PATHWAY for use of CYTOKINE MODULATORS in

The efficacy of multiple courses of alefacept in patients with moderate to severe chronic plaque psoriasis Alan Menter, MD, Jennifer C. Cather, MD, Diane.

Safety, efficacy, and drug survival of biologics and biosimilars for moderate-to-severe plaque psoriasis Alexander Egeberg, MD PhD; Mathias Bo Ottosen,

EXPERT INSIGHTS: IL-17 INHIBITION IN PSORIASIS CARE

Efficacy and safety of brodalumab in patients with psoriasis who had inadequate responses to ustekinumab: subgroup analysis of two randomized phase 3 trials.

Algorithm based on the 2015 European League Against Rheumatism (EULAR)/American College of Rheumatology (ACR) recommendations for the management of polymyalgia.

Efficacy of guselkumab in subpopulations of patients with moderate-to-severe plaque psoriasis: A pooled analysis of the Phase 3 VOYAGE 1 and VOYAGE.

Presentation transcript:

Evaluating A Systemic Therapy Psoriasis 1.Efficacy 2.Safety 3.Labeling

What patients want!!! Effective –Clear or nearly clear is what patients want Keeps on working –Patients do not wish to constantly use therapy when the disease returns treatment should work at least as well. Convenient- limited trips to MD –Not messy –Does not require much time

What patients want cont’d. Safe –Does not make patient uncomfortable (or worse) while being used –Safe long term / repeated use does not preclude or interact with other treatments

Psoriasis –Psoriasis is a chronic disease (average duration about 50 years!!! –Extent and impact vary greatly among patients and in the affected individual over time.

Questions for today –Does it work? –Does it keep working? –Is it safe? –Do its potential benefits outweigh its risks?

Does it work? In what types of patients has efficacy been demonstrated? How well/often does it work? –(statistically significant is not enough) What are factors associated with success/failure? – ( Do available data help select patients for when the drug is most effective?)

Does it keep working? Psoriasis is a chronic disease. If a treatment has risks, its utility depends on –Low incidence of rebound –Length of remission –Efficacy (by patient criteria)

Is it safe? Short time and long term safety with use repeated must be assessed Concerns for this class: 1.Infection 2.Cancer – especially lymphoma and SCC 3.Immunologically mediated diseases (LE, MS, etc). 4.Immunologic reaction to the drug (I.e. antibodies) May decrease efficacy May be a health risk

Is it safe cont’d Do we have sufficient and robust data? Is it likely PMS will provide timely and Robust date? (I.e can we rely on Phase IV commitments?)

Do its benefits outweigh its risks? Short term perspective insufficient. A long term view is needed Do available data allow us to recommend approval? What labeling will put the drug in proper perspective given when we know?

PASI This meeting is not about the PASI ( or what percentage improvement represents significant clinical improvement.) The PASI is a flawed scale. We could (and have) spent many hours extolling its virtues and condemning its shortcomings.

Past Comments about the PASI at Advisory Committee Meetings Dr. Joseph McGuire: “I think no one is satisfied with the clinical fidelity of PASI….” Dr. Robert Stern “ Lets pass on the PASI” –(not a compliment to the PASI) Dr. Mark Lebwohl –“ Now I entirely agree with Dr. Stern, we have to pass on the PASI……..

The Literature Dr. Michael Bigby ( JAAD, 1996) –“ The major problem with indices ( PASI) is that they confound area of involvement with extent of disease.” –“Until better scales are developed trials with the simplest and most objective outcome variables are best.” ( Bigby, JAAD, 1996)

A Proposal Acknowledging the limitations of the evaluation metrics utilized in the studies we will review today, let us agree to utilize the agreed upon two primary end points today. 1.PASI 75% improvement 2.Clear or almost clear And try not to complicate the discussion of this product with debate about how to measure psoriasis.

Current Labeling (Indication) of Systemic Therapies for Psoriasis.

Caution: Methoxsalen is a potent drug. 1.Photochemotherapy (Methoxsalen with long wave UVA radiation) is indicated for the symptomatic control of severe, recalcitrant disabling psoriasis not adequately responsive to other forms of therapy and when the diagnosis has been supported by biopsy.

Soriatane Soriatane is indicated for the treatment of severe psoriasis. – Because of significant adverse effects associated with its use, Soriatane should be prescribed only by physicians knowledgeable in the systemic use of retinoids. –Methotrexate is indicated in the symptomatic control of severe, recalcitrant, disabling psoriasis that is not adequately responsive to other forms of therapy, but only when the diagnosis has been established, as a biopsy and/or after dermatologic consultation.

Neoral –Psoriasis: Neoral is indicated for the treatment of adult, nonimmunocompromised patients with severe (I.e extensive and/or disabling) recalcitrant, plaque psoriasis who have failed to respond to at least one systemic therapy.

Amevive Amevive is indicated for the treatment of adult patients with moderate to severe chronic plaque psoriasis who are candidates for systemic therapy or phototherapy.

Today’s Task Answers FDA’s questions. Judge if benefits outweigh Risk Suggest Additional Data Needs for Judging Long Term Role