Presentation is loading. Please wait.

Presentation is loading. Please wait.

Endocrinologic and Metabolic Drugs Advisory Committee “Cardiovascular Assessment in the Pre- Approval and Post-Approval Settings for Drugs and Biologics.

Published byHarry Ferguson Modified over 8 years ago

Similar presentations

Presentation on theme: "Endocrinologic and Metabolic Drugs Advisory Committee “Cardiovascular Assessment in the Pre- Approval and Post-Approval Settings for Drugs and Biologics."— Presentation transcript:

1 Endocrinologic and Metabolic Drugs Advisory Committee “Cardiovascular Assessment in the Pre- Approval and Post-Approval Settings for Drugs and Biologics Developed for the Treatment of Type 2 Diabetes Mellitus” Endocrinologic and Metabolic Drugs Advisory Committee Hylton V. Joffe, M.D., M.M.Sc.

2 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 2 Overview Introduction Type 2 diabetes mellitus FDA approach to diabetes drug development Cardiovascular assessment: considerations Points for discussion and questions to the panel

3 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 3 Introduction Anti-diabetic drugs are indicated to improve glycemic control and are approved on the basis of HbA1c Safety concerns with some anti-diabetic drugs have led to suggestions for a more extensive cardiovascular assessment during the approval process N Engl J Med. 2007; 357:844 N Engl J Med. 2007; 357:1775-7

4 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 4 Introduction This advisory committee meeting will explore this proposal and associated complex issues: –Should a long-term cardiovascular trial be required? –Show benefit vs. rule out harm? –All new therapies or only those with a safety signal? –Challenges related to trial design? –Timing relative to approval? –What to do with currently marketed therapies?

5 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 5 Presentations Natural history of type 2 diabetes and macrovascular complications (Dr. David Nathan) HbA1c as a surrogate for glycemic control and microvascular complications (Dr. Robert Ratner) Evaluating benefit and risk in type 2 diabetes: statistical considerations (Dr. Thomas Fleming) Clinical macrovascular outcomes with anti-diabetic drugs: What we already know (Professor Rury Holman)

6 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 6 Presentations (continued) Clinical macrovascular outcomes with anti-diabetic drugs: Ongoing studies (Dr. Hertzel Gerstein) Need for cardiovascular assessment during approval process for antidiabetic drugs (Dr. Steven Nissen) Challenges in designing a cardiovascular trial for type 2 diabetes (Dr. Robert Califf)

7 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 7 Agenda Day 1 –Introductory FDA presentation –Presentations from experts in the field –Panel questions to the presenters –Panel discussion (will be continued on Day 2) Day 2 –Open public hearing –FDA Comments (Dr. Mary Parks) –Continued panel discussion –Questions to the panel

8 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 8 Type 2 Diabetes Mellitus >150 million people worldwide >18 million people in the United States 2-4 fold higher risk of cardiovascular death Most deaths due to cardiovascular disease/stroke Other important long-term complications –Peripheral vascular disease –Retinopathy, nephropathy, and neuropathy N Engl J Med. 1998; 339:229-34 JAMA. 2002; 287:2570-81 Lancet. 2005; 365:1333-46

9 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 9 Pharmacological Therapies Alpha-glucosidase inhibitors Amylin analogues (pramlintide acetate) Biguanides (metformin) Bile acid sequestrants (colesevelam) Dipeptidyl peptidase 4 inhibitors (sitagliptin phosphate) Glinides Glucagon-like peptide 1 analogues (exenatide) Insulin Sulfonylureas Thiazolidinediones

10 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 10 Macrovascular Complications Intensive glycemic control appears to reduce macrovascular complications in type 1 diabetes No conclusive evidence of macrovascular risk reduction with any of the FDA- approved treatments for type 2 diabetes

11 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 11 Older Trials with Cardiovascular Findings University Group Diabetes Program (UGDP) –Tolbutamide increased cardiovascular mortality UK Prospective Diabetes Study (UKPDS) –Non-significant reduction (p=0.052) in myocardial infarction/ sudden death with intensive therapy –Reduction in diabetes-related death and all-cause mortality in a substudy of 342 overweight patients given metformin –Increase in diabetes-related death with metformin add-on to sulfonylurea Diabetes. 1970; 19 (Supp 2): 747-830 Lancet. 1998; 352:837-53 and 854-65

12 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 12 Trials with Cardiovascular Assessments ACCORD ADVANCE BARI 2D HEART 2D VADT PROactive RECORD ORIGIN NAVIGATOR ACE STOP-NIDDM DREAM Type 2 diabetes Pre- diabetes Primary CV or mortality endpoint Secondary CV endpoint Treatment regimens Specific drugs

13 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 13 Current FDA Approval Process Anti-diabetic drugs are indicated to improve glycemic control HbA1c is the primary efficacy endpoint –Correlates with mean blood glucose over 3 months –Unlike some other biomarkers relied upon for drug approval, there is symptomatic benefit with daily control of hyperglycemia –Lowering of HbA1c reduces the risk of onset, progression of microvascular complications Lancet. 1998; 352:837-53 N Engl J Med. 2008; 358:2560-72 N Engl J Med. 1993; 329:977-86 Diabetes Care. 2004; 27: 1761-73

14 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 14 Package Inserts “Drug X is indicated as an adjunct to diet and exercise to improve glycemic control in adults with type 2 diabetes mellitus” “There have been no clinical studies establishing conclusive evidence of macrovascular risk reduction with Drug X or any other oral antidiabetic drug” Package inserts do not mention improvement in long-term sequelae of diabetes

15 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 15 Phase 2 Program Dose-finding, randomized, double-blind, controlled, trials in patients treated only with diet/exercise or on a stable dose of metformin Dose A Placebo Dose C Dose B Run-in 12 weeks FDA Guidance to Industry on Diabetes Mellitus (Draft)

16 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 16 Phase 3 Program 6-month, randomized, double-blind, controlled trials with 6-18 month extensions Placebo-controlled or active-controlled (non-inferiority) –Monotherapy –Add-on to other commonly used anti-diabetic drugs Placebo-controlled trials usually ≤6 months in duration to limit long-term exposure to hyperglycemia FDA Guidance to Industry on Diabetes Mellitus (Draft)

17 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 17 Phase 3 Program - Monotherapy Placebo (or active comparator) Dose B Dose A Run-in 24 weeks Enrollment of patients treated with diet and exercise only or after washout of a single anti-diabetic drug –Generally low cardiovascular risk FDA Guidance to Industry on Diabetes Mellitus (Draft)

18 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 18 Phase 3 Program – Add-on Trials Placebo + background anti-diabetic drug Dose B + background anti-diabetic drug Dose A + background anti-diabetic drug Run-in 24 weeks Stable near-maximal/maximal doses of background anti-diabetic drug Enrollment of patients with HbA1c 7-10% despite stable maximal/near-maximal doses of a background anti-diabetic drug FDA Guidance to Industry on Diabetes Mellitus (Draft)

19 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 19 Phase 3 Development Program A typical program has the following core phase 3 trials: Placebo-controlled monotherapy trial Add-on to metformin Add-on to sulfonylurea Add-on to thiazolidinedione Other phase 3 trials: Active-controlled, monotherapy trial Add-on to dipeptidyl-peptidase 4 inhibitor Add-on to insulin Add-on to dual agents (e.g., metformin + sulfonylurea)

20 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 20 Phase 3 Program – Extension Trials In active-controlled trials, the randomized treatments can be continued into the extension trial In placebo-controlled trials, placebo-treated patients are given active therapy during the extension trial to limit prolonged hyperglycemia (e.g., another anti- diabetic drug or the investigational agent) Uncontrolled extensions limit interpretability of efficacy and safety

21 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 21 Phase 3 Program - Efficacy Primary efficacy endpoint: HbA1c –Sensitivity analyses –Subgroup analyses Secondary efficacy endpoints: –Fasting plasma glucose –HbA1c responder analyses e.g., proportion of patients achieving HbA1c <7% –Body weight –Mechanistic (e.g., insulin sensitivity, postprandial glucose)

22 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 22 Phase 3 Program - Safety Deaths Non-fatal serious adverse events Discontinuations Other adverse events Events of special interest (some are drug-specific) Laboratory data Vital signs Electrocardiograms

23 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 23 Phase 3 Program - Safety Unpooled analyses –I ndividual trial data Pooled analyses –Grouping of data from two or more similar trials –Useful for analyzing infrequent events (e.g., deaths) Meta-analyses –Not routinely performed but multiple clinical trials required for the marketing application may allow for this to be incorporated in the safety analysis

24 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 24 Phase 3 Program - Safety Some Caveats: Multiplicity – if 100 associations are tested, 5 may be significant by chance (alpha=0.05) Studies rarely powered for safety –Assessments of infrequent events (e.g., deaths, myocardial ischemia) are inconclusive Do not usually have adjudication committees

25 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 25 Phase 3 Program – Sample Sizes ICH E1A recommended pre-approval exposures for drugs developed for chronic, non-life-threatening conditions: –≥1,500 subjects total –300-600 subjects for ≥6 months –100 subjects for ≥1 year Minimum pre-approval sample sizes for type 2 diabetes: –2,500 phase 2/3 total –1,300-1,500 exposed ≥1 year –300-500 exposed ≥18 months Specific safety concern(s) may require larger exposures

26 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 26 Rule of Three If we expose 2,500 patients to the study drug and see no cases of event A then we have ruled out incidence rates for event A of 0.12% or higher with 95% certainty Patients Exposed to Study Drug Smallest Event Rate Ruled Out (95% confidence) 1,50020/10,000 or 0.20% 2,50012/10,000 or 0.12% 5,0006/10,000 or 0.06% 10,0003/10,000 or 0.03%

27 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 27 Clinical Trial Challenges Worsening glycemia over time if therapy is not altered Protecting participants from prolonged hyperglycemia –HbA1c entry criteria –Duration of placebo-controlled phase –Glycemic rescue therapy Progressive nature of type 2 diabetes necessitates a multidrug anti-diabetic regimen in long-term trials, limiting the ability to tease apart the effects of a single drug

28 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 28 Points for Consideration and Discussion What changes are recommended to phase 2/3 trials to enhance detection of a cardiovascular safety signal prior to drug approval? –Independent, blinded cardiovascular adjudication? –Meta-analysis of safety data from phase 2/3 trials? –Changes to sample sizes/duration of exposures?

29 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 29 Points for Consideration and Discussion Should a long-term cardiovascular trial be required to show benefit or rule out an unacceptable increase in cardiovascular risk? –Conclusive evidence of cardiovascular benefit has not been established for any drug for type 2 diabetes despite several large, long-term trials –If ruling out harm, what non-inferiority margin do you recommend?

30 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 30 Points for Consideration and Discussion In the absence of a concerning cardiovascular safety signal during Phase 2/3, should there still be a requirement to conduct a long-term cardiovascular trial? When should such a study be conducted? What about already marketed therapies?

31 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 31 Benefit vs. rule out harm (if harm, what magnitude)? Patient population? Comparator(s)? Primary endpoint? What should the HbA1c target be? How to define and manage deteriorating glycemia? How to manage other cardiovascular risk factors? Whether to ensure comparability of glycemia and cardiovascular risk factors across treatment groups? Trial size and duration? Large Cardiovascular Trial: Discussion Points

32 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 32 Patient population? –Pre-diabetes? New-onset diabetes? Longstanding diabetes? –Generalizability? –Statistical power? DREAM (pre-diabetes without cardiovascular disease) –~1% with MACE over median 3 year follow-up ADOPT (new-onset diabetes) –Up to 25% with “inadequate glycemic control” over 4-6 years Large Cardiovascular Trial: Discussion Points

33 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 33 What should the comparator be? –Drug X vs. Placebo –Drug X vs. Placebo as add-on to standard therapy –Drug X vs. Drug Y as add-on to standard therapy How should deteriorating glycemia (which may vary between treatment groups) be defined, managed? How do we interpret the effects of one drug within a multidrug regimen? If ruling out harm in an active-controlled trial, how much do we need to know about the cardiovascular effects of the comparator? Large Cardiovascular Trial: Discussion Points

34 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 34 What should the primary endpoint be? Composite? –Cardiovascular death (or all-cause mortality) –Nonfatal myocardial infarction –Nonfatal stroke Include other events in the primary endpoint? –Coronary revascularization? –Lower-extremity amputations? Predefine, justify, accurately capture and analyze Large Cardiovascular Trial: Discussion Points

35 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 35 2008 ADA Treatment Goals in Diabetes HbA1c<7.0% Blood pressure<130/80 mmHg LDL-cholesterol<100 or <70 mg/dL Serum triglycerides<150 mg/dL HDL cholesterol>40 (men); >50 (women) mg/dL Smoking cessationYes Aspirin therapy If history (or increased risk) of cardiovascular disease

36 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 36 Should investigators be encouraged to manage blood pressures, lipid profiles, aspirin use, and other cardiovascular factors to current guidelines (which will not necessarily ensure comparability across treatment groups)? OR Should algorithms be used post-randomization with the intent of equalizing these risk factors across treatment groups? Large Cardiovascular Trial: Discussion Points

37 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 37 Total Sample Sizes Annual Event Rate Total Sample Size to Rule Out Increased Risk of DrugComparator 1.21.31.4 2% 16,6008,0005,000 2%1.75%>100,00038,00015,000 4% 8,7004,3002,600 4%3.6%>100,00020,0007,800 6% 5,9002,9001,800 6%5.2%>100,00023,0007,300 α=0.05; 90% power; 5-year trial; 2-year recruitment

38 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 38 Questions to the Committee It should be assumed that an anti-diabetic therapy with a concerning CV safety signal during Phase 2/3 development will be required to conduct a long-term cardiovascular trial. For those drugs or biologics without such a signal, should there be a requirement to conduct a long-term cardiovascular trial ? (vote yes/no requested) If yes, please discuss when such a study should be conducted? –Pre-approval? –Post-approval? If a long-term cardiovascular trial is required post-approval, please discuss whether this study should be ongoing at the time of approval (i.e., trial already initiated at time of approval)

39 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 39 Questions to the Committee No currently marketed therapy for type 2 diabetes has established conclusive evidence of macrovascular benefit Most marketed therapies for type 2 diabetes have not been tested for lack of cardiovascular harm Therefore, please discuss how any suggestion for a requirement for a long-term cardiovascular trial should be applied to existing anti-diabetic therapies

40 Endocrinologic and Metabolic Drugs Advisory Committee (July 1-2, 2008) 40 Acknowledgements Ilan Irony, M.D Karen Mahoney, M.D. Robert Misbin, M.D. Valerie Pratt, M.D. Joanna Zawadzki, M.D. Joy Mele, M.S. Todd Sahlroot, Ph.D. Mary Parks, M.D. Director, Division of Metabolism and Endocrinology Products Curtis Rosebraugh, M.D., M.P.H. Director, Office of Drug Evaluation II Robert Temple, M.D. Associate Director, Office of Medical Policy John Jenkins, M.D. Director, Office of New Drugs Gerald Dal Pan, M.D., M.H.S. Director, Office of Surveillance & Epidemiology FDA clinical diabetes team Statistics

Download ppt "Endocrinologic and Metabolic Drugs Advisory Committee “Cardiovascular Assessment in the Pre- Approval and Post-Approval Settings for Drugs and Biologics."

Similar presentations

Analysis of the ADVANCE Trial Sapna N. Patel UCSF Pharm. D. Candidate 2008 Preceptor Dr. Craig S. Stern March 28, 2008.

Analysis of the ADVANCE Trial Sapna N. Patel UCSF Pharm. D. Candidate 2008 Preceptor Dr. Craig S. Stern March 28, 2008.
THE ACTION TO CONTROL CARDIOVASCULAR RISK IN DIABETES STUDY (ACCORD)

THE ACTION TO CONTROL CARDIOVASCULAR RISK IN DIABETES STUDY (ACCORD)
Aggressive Hyperglycemia Management. Significant hospital hyperglycemia requires close follow-up Previously diagnosed diabetes and elevated A1C Without.

Aggressive Hyperglycemia Management. Significant hospital hyperglycemia requires close follow-up Previously diagnosed diabetes and elevated A1C Without.
1. 2 The primary Objective of IDEAL LDL-C Simvastatin 20-40 mg/d Atorvastatin 80 mg/d risk CHD In stable CHD patients IDEAL: The Incremental Decrease.

1. 2 The primary Objective of IDEAL LDL-C Simvastatin mg/d Atorvastatin 80 mg/d risk CHD In stable CHD patients IDEAL: The Incremental Decrease.
ODAC May 3, 2004 1 Subgroup Analyses in Clinical Trials Stephen L George, PhD Department of Biostatistics and Bioinformatics Duke University Medical Center.

ODAC May 3, Subgroup Analyses in Clinical Trials Stephen L George, PhD Department of Biostatistics and Bioinformatics Duke University Medical Center.
Henry C. Ginsberg, MD College of Physicians & Surgeons, Columbia University, New York For The ACCORD Study Group.

Henry C. Ginsberg, MD College of Physicians & Surgeons, Columbia University, New York For The ACCORD Study Group.
Critical Appraisal for MRCGP Jim McMorran Coventry GP GP trainer Editor GPnotebook (www.gpnotebook.co.uk)

Critical Appraisal for MRCGP Jim McMorran Coventry GP GP trainer Editor GPnotebook (
Diabetes Mellitus Type 2

Diabetes Mellitus Type 2
Pramlintide Advisory Committee July 26, 2001 Symlin ® Amylin Pharmaceuticals New Drug Application (21-332) Advisory Committee Meeting Bethesda, Maryland.

Pramlintide Advisory Committee July 26, 2001 Symlin ® Amylin Pharmaceuticals New Drug Application (21-332) Advisory Committee Meeting Bethesda, Maryland.
Facts and Fiction about Type 2 Diabetes Michael L. Parchman, MD Department of Family & Community Medicine September 2004.

Facts and Fiction about Type 2 Diabetes Michael L. Parchman, MD Department of Family & Community Medicine September 2004.
Canadian Diabetes Association 2013 Clinical Practice Guidelines Targets for Glycemic Control Chapter 8 S. Ali Imran, Rémi Rabasa-Lhoret, Stuart Ross.

Canadian Diabetes Association 2013 Clinical Practice Guidelines Targets for Glycemic Control Chapter 8 S. Ali Imran, Rémi Rabasa-Lhoret, Stuart Ross.
P H Y S I C I A N S ’ A C A D E M Y F O R C A R D I O V A S C U L A R E D U C A T I O N Oral drugs for type 2 diabetes and all cause mortality in General.

P H Y S I C I A N S ’ A C A D E M Y F O R C A R D I O V A S C U L A R E D U C A T I O N Oral drugs for type 2 diabetes and all cause mortality in General.
Henry N. Ginsberg, MD College of Physicians & Surgeons, Columbia University, New York For The ACCORD Study Group.

Henry N. Ginsberg, MD College of Physicians & Surgeons, Columbia University, New York For The ACCORD Study Group.
Hemoglobin A 1c in Hemodialysis Patients Source: Ix JH. Hemoglobin A1c in hemodialysis patients: Should one size fit all? Clin J Am Soc Nephrol. 2010;5:1539–1541.

Hemoglobin A 1c in Hemodialysis Patients Source: Ix JH. Hemoglobin A1c in hemodialysis patients: Should one size fit all? Clin J Am Soc Nephrol. 2010;5:1539–1541.
ACCORD - Action to Control Cardiovascular Risk in Diabetes ADVANCE - Action in Diabetes to Prevent Vascular Disease VADT - Veterans Administration Diabetes.

ACCORD - Action to Control Cardiovascular Risk in Diabetes ADVANCE - Action in Diabetes to Prevent Vascular Disease VADT - Veterans Administration Diabetes.
Diabetes Mellitus Ibrahim Sales, Pharm.D. Assistant Professor of Clinical Pharmacy King Saud University

Diabetes Mellitus Ibrahim Sales, Pharm.D. Assistant Professor of Clinical Pharmacy King Saud University
Blood glucose: is lower better for diabetic patients?

Blood glucose: is lower better for diabetic patients?
Individualizing Targets and Tactics for High- Risk Patients With Type 2 Diabetes Practical lessons from ACCORD and other cardiovascular trials Featured.

Individualizing Targets and Tactics for High- Risk Patients With Type 2 Diabetes Practical lessons from ACCORD and other cardiovascular trials Featured.
Joint Effects of Routine Blood Pressure Lowering and Intensive Glucose Control ADVANCE Adapted from EASD 2008.

Joint Effects of Routine Blood Pressure Lowering and Intensive Glucose Control ADVANCE Adapted from EASD 2008.
Journal Club 亀田メディカルセンター 糖尿病内分泌内科 Diabetes and Endocrine Department, Kameda Medical Center 松田 昌文 Matsuda, Masafumi 2008 年9月 25 日 8:20-8:50 B 棟8階 カンファレンス室.

Journal Club 亀田メディカルセンター 糖尿病内分泌内科 Diabetes and Endocrine Department, Kameda Medical Center 松田 昌文 Matsuda, Masafumi 2008 年9月 25 日 8:20-8:50 B 棟8階 カンファレンス室.

Similar presentations

Ads by Google