Acne Vulgaris:
Establishing Effectiveness
  of Drugs Intended for
        Treatment
   Guidance for Industry




      U.S. Department of Health and Human Services
              Food and Drug Administration
     Center for Drug Evaluation and Research (CDER)

                       May 2018
                    Clinical/Medical
      Acne Vulgaris:
Establishing Effectiveness
  of Drugs Intended for
        Treatment
      Guidance for Industry
                            Additional copies are available from:

                    Office of Communications, Division of Drug Information
                            Center for Drug Evaluation and Research
                                 Food and Drug Administration
                     10001 New Hampshire Ave., Hillandale Bldg., 4th Floor
                                 Silver Spring, MD 20993-0002
    Phone: 855-543-3784 or 301-796-3400; Fax: 301-431-6353; Email: druginfo@fda.hhs.gov
  https://www.fda.gov/Drugs/GuidanceComplianceRegulatoryInformation/Guidances/default.htm




                 U.S. Department of Health and Human Services
                         Food and Drug Administration
                Center for Drug Evaluation and Research (CDER)

                                       May 2018
                                    Clinical/Medical
                                                        TABLE OF CONTENTS

I.           INTRODUCTION............................................................................................................. 1 
II.          BACKGROUND ............................................................................................................... 1 
III.         CLINICAL TRIAL DESIGN FEATURES — KEY CONSIDERATIONS ................ 2 
      A.  Enrollment Criteria ....................................................................................................................... 2 
      B.     Study Design and Efficacy Endpoints .......................................................................................... 2 
      C.  General Analysis Considerations.................................................................................................. 3 
                                 Contains Nonbinding Recommendations


                    Acne Vulgaris: Establishing Effectiveness of
                          Drugs Intended for Treatment
                             Guidance for Industry1



This guidance represents the current thinking of the Food and Drug Administration (FDA or Agency) on
this topic. It does not establish any rights for any person and is not binding on FDA or the public. You
can use an alternative approach if it satisfies the requirements of the applicable statutes and regulations.
To discuss an alternative approach, contact the FDA office responsible for this guidance as listed on the
title page.




I.      INTRODUCTION

The purpose of this guidance is to provide recommendations to industry for establishing clinical
effectiveness of drugs for the treatment of acne vulgaris (acne).2 The recommendations in this
guidance are based on the FDA’s assessment of issues raised in the review of clinical trials for
acne.

This guidance does not address systemic retinoid therapies because they may not have
appropriate risk-benefit profiles for non-nodular acne therapy. Sponsors should discuss
development programs for systemic retinoids with the review division before trial initiation.
This guidance also does not address clinical safety, clinical pharmacokinetics, nonclinical issues,
or chemistry, manufacturing, and controls issues.

In general, FDA’s guidance documents do not establish legally enforceable responsibilities.
Instead, guidances describe the Agency’s current thinking on a topic and should be viewed only
as recommendations, unless specific regulatory or statutory requirements are cited. The use of
the word should in Agency guidances means that something is suggested or recommended, but
not required.


II.     BACKGROUND

Acne is a chronic disease of sebaceous follicles that is multifactorial in etiology. It can wax and
wane in severity according to lesion types, numbers, and extent of involvement and can result in

1
  This guidance has been prepared by the Division of Dermatology and Dental Products in the Center for Drug
Evaluation and Research at the Food and Drug Administration.
2
 For the purposes of this guidance, all references to drugs include human drugs and not therapeutic biological
products unless otherwise specified.


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                                Contains Nonbinding Recommendations


scarring. Acne occurs more frequently on the face, but can also occur on nonfacial skin (e.g.,
trunk).

There are two major types of acne lesions:

       1. Noninflammatory: Noninflammatory lesions are the open (blackheads) or closed
          (whiteheads) comedones.

       2. Inflammatory: Inflammatory lesions include papules, pustules, and nodules.

Although most drug products for acne are intended for the broad indication of acne vulgaris,
some drug products have been developed that only target one of these two lesion subsets.

Acne is primarily a disease of adolescence and young adulthood, but can persist past the third
decade of life.


III.       CLINICAL TRIAL DESIGN FEATURES — KEY CONSIDERATIONS

           A.      Enrollment Criteria

The study population should be defined by the following criteria:

          A minimum number of each type of lesion: inflammatory and noninflammatory.

          A baseline score on an Investigator’s Global Assessment (IGA) severity scale that is
           consistent with the baseline lesion counts.

          An age of enrollment reflective of the onset of acne relative to adrenarche.

           B.      Study Design and Efficacy Endpoints

In the assessment of efficacy, sponsors should consider the following:

          To demonstrate efficacy, we recommend conducting randomized, double-blind, well-
           controlled trials that include a placebo arm.

          Although acne occurs on the face and trunk, efficacy assessment should be limited to the
           face because it is the most frequent site of involvement. However, topical drug products
           can be applied to all affected areas during clinical trials.

          We recommend that the IGA be a static evaluation of overall acne severity.

           ‒    The IGA should be an ordinal scale with approximately five severity grades (reported
                only in whole numbers (e.g., 0 to 4)). Each grade should be defined by a distinct and
                clinically relevant morphologic description to minimize interobserver variability. The


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                          Contains Nonbinding Recommendations


         definitions of the severity grades should not include numerical ranges of lesions
         because the IGA scale is intended to be a qualitative assessment of the subject’s
         condition.

    ‒    The IGA scale should be dichotomized to success or failure, with success defined as
         clear or almost clear (grade 0 or 1) and at least a two-grade improvement from
         baseline; this represents a clinically meaningful outcome.

    ‒    There is no single, standardized grading system for severity of acne. We encourage
         sponsors to discuss their IGA scales and study designs with the FDA before trial
         implementation.

   Inflammatory and noninflammatory lesions should be counted and reported separately.
    All lesions on the face should be counted, including those on the nose.

   The assessment of treatment effect should be based on both changes in lesion counts and
    success on the IGA. Endpoints based on changes in lesion counts and IGA success
    provide both quantitative and qualitative assessments of acne, and thus provide useful
    complementary information.

    ‒    A reduction in lesion counts may indicate improvement of acne severity; however, it
         does not account for the variable expression of acne (e.g., size of lesions, intensity of
         inflammation, and location of lesions). The IGA considers the quality and quantity of
         the acne lesions.

    ‒    Although subjects are considered as success or failure based on the IGA with
         improvement of two grades, this endpoint is not a precise measure of the magnitude
         of improvement. The changes from baseline in lesion counts provide a quantitative
         assessment of the improvement.

    C.      General Analysis Considerations

The statistical analysis should address the following:

   The analysis of lesion counts can be influenced by a few extreme outliers, which may
    cause difficulty in interpretation of the clinical trial findings. The statistical analysis plan
    should consider alternative approaches for analysis of lesion counts if extreme outliers
    are anticipated (such as analyses based on ranks).

   For assessment of the treatment effect on inflammatory and noninflammatory lesion
    counts, analysis of absolute change and percentage change from baseline are both
    relevant and complementary. Absolute change in lesion counts can be affected by
    subjects with large numbers of lesions at baseline, while percent change in lesion counts
    can be affected by subjects with relatively small numbers of lesions at baseline. The
    absolute change in lesion counts is expected to have better analysis properties, such as a
    less skewed distribution. Therefore, we recommend absolute change in lesion counts for



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                    Contains Nonbinding Recommendations


the primary endpoint analysis, and percentage change in lesion counts for the secondary
endpoint analysis.




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