National Academies Press: OpenBook
Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×

EVALUATION OF BIOMARKERS AND SURROGATE ENDPOINTS IN CHRONIC DISEASE

Committee on Qualification of Biomarkers and Surrogate Endpoints in Chronic Disease

Board on Health Care Services

Board on Health Sciences Policy

Food and Nutrition Board

Christine M. Micheel and John R. Ball, Editors

INSTITUTE OF MEDICINE
OF THE NATIONAL ACADEMIES

THE NATIONAL ACADEMIES PRESS

Washington, D.C.
www.nap.edu

Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×

THE NATIONAL ACADEMIES PRESS
500 Fifth Street, N.W.
Washington, DC 20001

NOTICE: The project that is the subject of this report was approved by the Governing Board of the National Research Council, whose members are drawn from the councils of the National Academy of Sciences, the National Academy of Engineering, and the Institute of Medicine. The members of the committee responsible for the report were chosen for their special competences and with regard for appropriate balance.

This study was supported by Contract No. HHSF223200810020I between the National Academy of Sciences and the Food and Drug Administration. Any opinions, findings, conclusions, or recommendations expressed in this publication are those of the author(s) and do not necessarily reflect the view of the organizations or agencies that provided support for this project.

Library of Congress Cataloging-in-Publication Data

Evaluation of biomarkers and surrogate endpoints in chronic disease / Committee on Qualification of Biomarkers and Surrogate Endpoints in Chronic Disease, Board on Health Care Services, Board on Health Sciences Policy, Food and Nutrition Board, Institute of Medicine ; Christine M. Micheel and John R. Ball, editors.

p. ; cm.

Includes bibliographical references.

ISBN 978-0-309-15129-0 (pbk.) — ISBN 978-0-309-15130-6 (pdf) 1. Biochemical markers—Evaluation. 2. Chronic diseases. I. Micheel, Christine. II. Ball, John, 1944- III. Institute of Medicine (U.S.). Committee on Qualification of Biomarkers and Surrogate Endpoints in Chronic Disease.

[DNLM: 1. Biological Markers. 2. Chronic Disease. 3. Evidence-Based Practice. QW 541 E917 2010]

R853.B54E93 2010

610.28—dc22

2010020157

Additional copies of this report are available from

The National Academies Press,

500 Fifth Street, N.W., Lockbox 285, Washington, DC 20055; (800) 624-6242 or (202) 334-3313 (in the Washington metropolitan area); Internet, http://www.nap.edu.

For more information about the Institute of Medicine, visit the IOM home page at: www.iom.edu.

Copyright 2010 by the National Academy of Sciences. All rights reserved.

Printed in the United States of America

The serpent has been a symbol of long life, healing, and knowledge among almost all cultures and religions since the beginning of recorded history. The serpent adopted as a logotype by the Institute of Medicine is a relief carving from ancient Greece, now held by the Staatliche Museen in Berlin.

Suggested citation: IOM (Institute of Medicine). 2010. Evaluation of biomarkers and surrogate endpoints in chronic disease. Washington, DC: The National Academies Press.

Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×

“Knowing is not enough; we must apply.

Willing is not enough; we must do.”

—Goethe

INSTITUTE OF MEDICINE
OF THE NATIONAL ACADEMIES


Advising the Nation. Improving Health.

Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×

THE NATIONAL ACADEMIES

Advisers to the Nation on Science, Engineering, and Medicine


The National Academy of Sciences is a private, nonprofit, self-perpetuating society of distinguished scholars engaged in scientific and engineering research, dedicated to the furtherance of science and technology and to their use for the general welfare. Upon the authority of the charter granted to it by the Congress in 1863, the Academy has a mandate that requires it to advise the federal government on scientific and technical matters. Dr. Ralph J. Cicerone is president of the National Academy of Sciences.


The National Academy of Engineering was established in 1964, under the charter of the National Academy of Sciences, as a parallel organization of outstanding engineers. It is autonomous in its administration and in the selection of its members, sharing with the National Academy of Sciences the responsibility for advising the federal government. The National Academy of Engineering also sponsors engineering programs aimed at meeting national needs, encourages education and research, and recognizes the superior achievements of engineers. Dr. Charles M. Vest is president of the National Academy of Engineering.


The Institute of Medicine was established in 1970 by the National Academy of Sciences to secure the services of eminent members of appropriate professions in the examination of policy matters pertaining to the health of the public. The Institute acts under the responsibility given to the National Academy of Sciences by its congressional charter to be an adviser to the federal government and, upon its own initiative, to identify issues of medical care, research, and education. Dr. Harvey V. Fineberg is president of the Institute of Medicine.


The National Research Council was organized by the National Academy of Sciences in 1916 to associate the broad community of science and technology with the Academy’s purposes of furthering knowledge and advising the federal government. Functioning in accordance with general policies determined by the Academy, the Council has become the principal operating agency of both the National Academy of Sciences and the National Academy of Engineering in providing services to the government, the public, and the scientific and engineering communities. The Council is administered jointly by both Academies and the Institute of Medicine. Dr. Ralph J. Cicerone and Dr. Charles M. Vest are chair and vice chair, respectively, of the National Research Council.


www.national-academies.org

Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×

COMMITTEE ON QUALIFICATION OF BIOMARKERS AND SURROGATE ENDPOINTS IN CHRONIC DISEASE

JOHN R. BALL (Chair), Executive Vice President,

American Society for Clinical Pathology

MICHELLE A. ALBERT, Assistant Professor of Medicine, Associate Physician, and Director of Behavioral and Neurocardiovascular Cardiology,

Brigham and Women’s Hospital, Harvard Medical School

FRED APPLE, Medical Director,

Clinical Laboratories, Hennepin County Medical Center, and

Professor,

Laboratory Medicine and Pathology, University of Minnesota School of Medicine

ROBERT M. CALIFF, Vice Chancellor for Clinical Research and Professor of Medicine, Cardiology,

Duke University School of Medicine

VICTOR G. DE GRUTTOLA, Professor and Chair,

Biostatistics, Harvard School of Public Health

DAVID L. DEMETS, Professor and Chair,

Biostatistics & Medical Informatics, University of Wisconsin–Madison

ROBERT GERSZTEN, Research Director and Faculty Member,

Massachusetts General Hospital, and

Associate Professor of Medicine,

Harvard Medical School

WILLIAM R. HARLAN, JR., Consultant

ALLAN S. JAFFE, Professor of Medicine,

Mayo Clinic

RONALD M. KRAUSS, Director, Atherosclerosis Research and Senior Scientist,

Children’s Hospital Oakland Research Institute

HARLAN M. KRUMHOLZ, Harold H. Hines, Jr., Professor of Medicine and Epidemiology and Public Health,

Yale University School of Medicine

MARIA LOPES-VIRELLA, Professor,

Bioengineering, Medical University of South Carolina

ROBERTA B. NESS, Dean,

University of Texas Health Science Center, School of Public Health

JENNIFER VAN EYK, Associate Professor,

Physiology and Biochemistry, Johns Hopkins University

JOHN A. WAGNER, Vice President,

Clinical Pharmacology, Merck and Company, Inc.

Consultant

ELIZABETH A. YETLEY, Consultant,

National Institutes of Health, Office of Dietary Supplements

Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×

Study Staff

CHRISTINE M. MICHEEL, Study Director

SHARYL NASS, Senior Program Officer

ERIN BALOGH, Research Associate

BERNADETTE MCFADDEN, Research Associate (from July 2009 to January 2010)

LISA BOYETTE, Christine Mirzayan Science and Technology Policy Graduate Fellow (September to November 2009)

ANNA WOLOSZYNSKA-READ, Christine Mirzayan Science and Technology Policy Graduate Fellow (January to April 2009)

CAIRA M. WOODS, Christine Mirzayan Science and Technology Policy Graduate Fellow (January to April 2010)

DESH MOHAN, Intern (June to August 2009)

ASHLEY MCWILLIAMS, Senior Program Assistant

PATRICK BURKE, Financial Associate

ROGER HERDMAN, Director,

Board on Health Care Services

LINDA D. MEYERS, Director,

Food and Nutrition Board

ANDREW POPE, Director,

Board on Health Sciences Policy

Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×

Reviewers

This report has been reviewed in draft form by individuals chosen for their diverse perspectives and technical expertise, in accordance with procedures approved by the National Research Council’s Report Review Committee. The purpose of this independent review is to provide candid and critical comments that will assist the institution in making its published report as sound as possible and to ensure that the report meets institutional standards for objectivity, evidence, and responsiveness to the study charge. The review comments and draft manuscript remain confidential to protect the integrity of the deliberative process. We wish to thank the following individuals for their review of this report:

RUSS B. ALTMAN, Stanford University

DIANNE BIRT, Iowa State University

JAMES DE LEMOS, University of Texas Southwestern Medical Center at Dallas

THOMAS R. FLEMING, University of Washington

PHILIP GREENLAND, Northwestern University

CHARLES HENNEKENS, Florida Atlantic University

JANE HENNEY, University of Cincinatti

WOLFGANG KOENIG, University of Ulm Medical Center

VICTOR MONTORI, Mayo Clinic

DAVID RANSOHOFF, University of North Carolina at Chapel Hill

CHRISTINE SEIDMAN, Harvard Medical School and Howard Hughes Medical Institute

Page viii Cite
Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×

ALAN TALL, Columbia University

STEPHEN WILLIAMS, Somalogic, Inc.

ALAN WU, University of California, San Francisco

Although the reviewers listed above have provided many constructive comments and suggestions, they were not asked to endorse the conclusions or recommendations nor did they see the final draft of the report before its release. The review of this report was overseen by CHARLES C. J. CARPENTER, the Miriam Hospital, and KRISTINE M. GEBBIE, Hunter College, City University of New York. Appointed by the National Research Council and the Institute of Medicine, they were responsible for making certain that an independent examination of this report was carried out in accordance with institutional procedures and that all review comments were carefully considered. Responsibility for the final content of this report rests entirely with the authoring committee and the institution.

Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×

Preface

Over breakfast during the second meeting of this committee, the members informally discussed a message on the package of one of the cereal offerings, a box of Cheerios. Against the backdrop of an image of a heart, the message was, “You Can Lower Your Cholesterol 4% in 6 weeks.” A month later (purely coincidentally), the Food and Drug Administration (FDA) sent a letter to the chair of General Mills, the producer of Cheerios. That letter stated, “based on claims made on your product’s label, we have determined that your Cheerios­® Toasted Whole Grain Oat Cereal is promoted for conditions that cause it to be a drug because the product is intended for use in the prevention, mitigation, and treatment of disease.” Five months later, the new FDA Commissioner Margaret Hamburg indicated, in an Industry Letter, that the agency was examining “Front of Package” (FOP) labels for false or misleading claims, citing consumer studies that found that, with FOP labeling, people are less likely to check the Nutrition Facts Panel, generally found on the side or back of food packages. Notably, H.R. 1105, the Omnibus Appropriations Act of 2009, included funds for an Institute of Medicine (IOM) study to examine and make recommendations regarding Front of Package nutrition symbols.

In the context of the committee’s task, this instance illustrates two issues with which the committee wrestled. The first is how science may inform policy decisions when diverse, and sometimes disparate, interests are involved. In this case, consumers wish to choose healthier diets, the food industry has an interest to market its products as healthy, and the FDA needs to minimize risks to the food supply and to inform consumers appropriately. The second is how to make policy decisions before the full process of reaching scientific consensus has been completed.

Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×

This report was initiated by the Center for Food Safety and Applied Nutrition of the FDA, which has received dozens of applications for approval of health claims for foods, most of which reflected claims of effects on a biomarker—a patient characteristic that can be measured and is believed to have a significant biological effect. The principal task requested of the Institute of Medicine was to recommend a framework for the evaluation of biomarkers; additionally, the IOM was to make ancillary recommendations for their application. As shown in Chapter 1, however, the task goes beyond claims on foods alone. A framework has been proposed that can be applied across many of the product areas regulated by the FDA.

The Institute of Medicine convened a committee of experts from a variety of related fields, supported by a highly capable technical staff. The committee met face to face four times and had several teleconferences. The committee was further supported by presentations from outside experts in a workshop format, and it benefited from comments from interested parties. As always, the committee’s report underwent a rigorous external review, which helped significantly to focus and clarify the findings and recommendations.

The committee met its principal task by recommending a three-part framework for biomarker evaluation: (1) Analytical validation—in essence, is the biomarker able to be accurately measured? (2) Qualification—is the biomarker associated with the clinical endpoint of concern? and (3) Utilization—what is the specific context of the proposed use? The committee met the additional task by making recommendations for implementing the evaluation framework, for supporting evidence-based decision making, and for promoting the public health.

The committee notes that endpoints can be conceptualized in a spectrum. At the end defined by endpoints with less relationship to patient or consumer experience are those that depend on biomarkers alone; in the middle are clinical events that depend on biomarkers as part of the definition; more closely related endpoints are those events that affect patients’ lives; and at the near end of the spectrum are the clearest clinical endpoints, such as death. Furthermore, the committee emphasizes that biomarkers cannot be qualified for a use without understanding the specific use and its context.

The committee heard significant evidence of the public’s (and professionals’) innumeracy, or numerical illiteracy, and the barrier that innumeracy poses to understanding the balance of risk and benefit. Thus, the committee recognizes that significant efforts may be needed, both by government and by professional societies, to inform and educate the public and professionals on how to interpret scientific information so that good science can inform individual decision making.

Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×

Critical to the committee’s recommendations, and flowing from our consideration of the evidence and vigorous debate, is that there is neither rationale nor scientific basis for predicating regulatory decisions on different levels of scientific evidence for different substances: “science is science.” That is, the same level of scientific evidence of benefit and risk should be required of foods as of drugs (and, indeed, of the other substances the FDA regulates—biologics, devices, and cosmetics). The counterargument that some substances (e.g., drugs) pose greater risks than others (e.g., foods) is not dispositive. Counter to that argument is that foods are encountered by a greater population than the target group who encounter drugs, and though drugs are subject to professional mediation (e.g., prescription and counseling), foods are not. As for risk, no one who is allergic to peanuts, eggs, or shellfish would argue that foods are less risky than drugs.

At the risk of using a personal anecdote, I have suffered three episodes of cardiac arrhythmia atrial fibrillation, all associated with drinking two glasses of red wine. Since making the correlation, I’ve ceased drinking red wine, and have ceased having episodes of atrial fibrillation. When I explained to my elderly mother why I no longer drank red wine, she said, “But I thought red wine was good for you.” The answer, of course, is “It depends.” “It depends” means that the context of health claims matters. Biomarkers can enable faster, more efficient clinical trials. They can help public health professionals identify and track disease outbreaks. In addition, they can help healthcare practitioners and patients make decisions about care. But the context of their use matters, and the scientific base for their use should be rigorous.

As chair of the committee, I thank personally all the committee members for their individual and group contributions, their diligence, and their comity. I am very grateful for the time and effort that such busy people were willing, often with short turnaround times, to devote to the work of the committee. As is the case with the best of these deliberations, their engaged back-and-forth nature led to a richer, more accurate, and—we all hope—helpful report for regulators, professionals, and the public. None of this could have been accomplished without the professional IOM staff, led by Christine Micheel, who, in addition to her technical expertise, was uncommonly responsive to the committee’s direction and to individual comments of the members. I know the committee would join in giving my heartfelt thanks to her.


John Ball, Chair

Committee on Qualification of Biomarkers and

Surrogate Endpoints in Chronic Disease

Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×

This page intentionally left blank.

Page xiii Cite
Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×

Acknowledgments

The committee and IOM staff would like to thank many individuals for their contributions to this study. Elizabeth Yetley, consultant to the committee, provided needed guidance. We thank Thomas H. Lee, Susan Mayne, Gil Omenn, David Ransohoff, and John Wagner for their project initiation assistance. We thank Joseph Bonventre, Kathleen Ellwood, Federico Goodsaid, and Paula Trumbo for presentations at the first committee meeting. We thank Nancy Cook, Charles Hennekens, and Marshall Joffe for their assistance with editing report sections. We thank all of the workshop speakers for their participation (please see Appendix E for the list of speakers). IOM staff Sharyl Nass, Christine L. Taylor, Roger Herdman, Linda Meyers, and Andrew Pope provided needed assistance. Finally, we thank the FDA for study funding.

The committee would like to thank IOM staff for their assistance with report drafting.

We would like to thank the fellows and interns involved with this study for their assistance. Lisa Boyette contributed to writing and editing tasks. Anna Woloszynska-Read contributed to workshop planning and background research, Caira Woods contributed to report review and creation of report dissemination material, and Desh Mohan provided research and meeting assistance.

Finally, the study director would like to thank project staff for their contributions. Research associates Erin Balogh and Bernadette McFadden were involved in writing many sections of the report. Ashley McWilliams arranged meetings and many other administrative tasks and contributed to research and writing tasks.

Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×

This page intentionally left blank.

Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×
Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×
Page xvii Cite
Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×

Boxes, Figures, and Tables

Summary

Boxes

S-1

 

Summary of Recommendations for Effective Biomarker Evaluation,

 

2

S-2

 

Important Definitions,

 

3

S-3

 

Ancillary Recommendations,

 

14

Figures

S-1

 

The steps of the evaluation framework are interdependent,

 

7

S-2

 

Multiple ingredients, multiple biological pathways, and multiple outcomes illustrate some of the complexities of the use of biomarkers and surrogate endpoints in chronic disease,

 

14

Chapter 1

Box

1-1

 

Important Definitions,

 

23

Tables

1-1

 

Use of Biomarkers in Chronic Disease Patient Care,

 

24

1-2

 

Use of Biomarkers in Drug Development,

 

24

1-3

 

Regulatory Definitions of Surrogate Endpoint,

 

25

1-4

 

Literature Definitions of Surrogate Endpoint,

 

26

Page xviii Cite
Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×

Chapter 2

Boxes

2-1

 

Characteristics of Comparative Effectiveness Research (CER),

 

37

2-2

 

Hill’s Criteria,

 

55

2-3

 

Five Unique Features of Decision Analysis for Surrogate Endpoint Evaluation,

 

60

2-4

 

FDA’s Risk Communication Advisory Committee,

 

69

Figures

2-1

 

Reasons for failure of surrogate endpoints,

 

48

2-2

 

The setting that provides the greatest potential for the surrogate endpoint to be valid,

 

49

2-3

 

Receiver operating characteristic (ROC) graph of a varying decision threshold compared with a “useless test,”

 

61

2-4

 

Outline of the Food and Drug Administration’s (FDA’s) biomarker qualification pilot process,

 

70

2-5

 

Food and Drug Administration ranking system to approve health claims,

 

78

Tables

2-1

 

Categories of Biomarker Use,

 

35

2-2

 

Altar et al. (2008) Proposed Evidence Map for Biomarker Qualification,

 

64

2-3

 

List of Regulations and Guidances Pertaining to Surrogate Endpoints,

 

66

2-4

 

Health Claims Based on Surrogate Endpoints,

 

75

2-5

 

Qualified Health Claims Approved by the Food and Drug Administration,

 

76

Chapter 3

Boxes

3-1

 

Recommendations 1–4,

 

98

3-2

 

Tumor Size and Analytical Validation (Recommendation 1a),

 

107

3-3

 

CRP, Inflammatory Markers, and Qualification (Recommendation 1b),

 

110

3-4

 

Troponin and Utilization (Recommendation 1c),

 

115

3-5

 

LDL and HDL Cholesterol and Surrogacy (Recommendation 1c),

 

117

3-6

 

Blood Levels of β-Carotene,

 

122

Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×

Figure

3-1

 

The steps of the evaluation framework are interdependent,

 

99

Tables

3-1

 

Sources of Variability in Biomarker Measurements,

 

104

3-2

 

Information Needed for Package Inserts and Peer-Reviewed Publications Describing Biomarker Assays,

 

106

3-3

 

Utilization: Critical and Important Factors for Consideration (Recommendation 1c),

 

112

Chapter 4

Box

4-1

 

Conditions Associated with High Cardiac Troponins,

 

157

Figure

4-1

 

Inflammatory risk factors,

 

144

Tables

4-1

 

Brief Summary of the Results of the Case Studies,

 

132

4-2

 

Assays of Inflammatory Markers for Potential Clinical Use,

 

146

Chapter 5

Boxes

5-1

 

Expanding FDA Responsibilities,

 

201

5-2

 

Core FDA Regulatory Functions,

 

203

5-3

 

Dietary Supplements,

 

212

5-4

 

Role of NIH in Biomarker Data Collection,

 

224

Figures

5-1

 

Food and Drug Administration—Regulatory Industry (FY2006): The people, science, and information needed to support innovation, grow industries, and protect the public both in our country and around the world,

 

202

5-2

 

Comparison of Food and Drug Administration (FDA) health-related food label statements,

 

216

Table

5-1

 

Types of Claims,

 

210

Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×

Appendix A

Tables

A-1

 

Historical Review of the Biomarker–Surrogate Endpoint Literature with Special Reference to the Nomenclature, Initial Reports, Systems of Classification, and Statistical Methods Developed for Their Evaluation,

 

252

A-2

 

Continuation of Table A-1 for 2007–2009,

 

267

Appendix B

Boxes

B-1

 

Summary of Recommendations to Develop Biomarker-Based Tools for Cancer,

 

278

B-2

 

Summary of Recommendations for The Future of Drug Safety: Promoting and Protecting the Health of the Public,

 

279

Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×
Page R1
Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×
Page R2
Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×
Page R3
Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×
Page R4
Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×
Page R5
Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×
Page R6
Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×
Page R7
Page viii Cite
Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×
Page R8
Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×
Page R9
Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×
Page R10
Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×
Page R11
Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×
Page R12
Page xiii Cite
Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×
Page R13
Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×
Page R14
Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×
Page R15
Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×
Page R16
Page xvii Cite
Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×
Page R17
Page xviii Cite
Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×
Page R18
Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×
Page R19
Suggested Citation:"Front Matter." Institute of Medicine. 2010. Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease. Washington, DC: The National Academies Press. doi: 10.17226/12869.
×
Page R20
Next: Summary »
Evaluation of Biomarkers and Surrogate Endpoints in Chronic Disease Get This Book
×
Buy Paperback | $60.00 Buy Ebook | $47.99
MyNAP members save 10% online.
Login or Register to save!
Download Free PDF

Many people naturally assume that the claims made for foods and nutritional supplements have the same degree of scientific grounding as those for medication, but that is not always the case. The IOM recommends that the FDA adopt a consistent scientific framework for biomarker evaluation in order to achieve a rigorous and transparent process.

  1. ×

    Welcome to OpenBook!

    You're looking at OpenBook, NAP.edu's online reading room since 1999. Based on feedback from you, our users, we've made some improvements that make it easier than ever to read thousands of publications on our website.

    Do you want to take a quick tour of the OpenBook's features?

    No Thanks Take a Tour »
  2. ×

    Show this book's table of contents, where you can jump to any chapter by name.

    « Back Next »
  3. ×

    ...or use these buttons to go back to the previous chapter or skip to the next one.

    « Back Next »
  4. ×

    Jump up to the previous page or down to the next one. Also, you can type in a page number and press Enter to go directly to that page in the book.

    « Back Next »
  5. ×

    Switch between the Original Pages, where you can read the report as it appeared in print, and Text Pages for the web version, where you can highlight and search the text.

    « Back Next »
  6. ×

    To search the entire text of this book, type in your search term here and press Enter.

    « Back Next »
  7. ×

    Share a link to this book page on your preferred social network or via email.

    « Back Next »
  8. ×

    View our suggested citation for this chapter.

    « Back Next »
  9. ×

    Ready to take your reading offline? Click here to buy this book in print or download it as a free PDF, if available.

    « Back Next »
Stay Connected!