Efficacy and Safety Study of Apremilast in Subjects With Moderate to Severe Atopic Dermatitis

Phase 2

Completed

Conditions: Dermatitis, Atopic Dermatitis

Interventions: Drug: Apremilast
Drug: Placebo

Registration Number: NCT02087943

Lead Sponsor: Amgen

Brief Summary: A study to evaluate the efficacy and safety of apremilast (CC-10004) in subjects with moderate to severe atopic dermatitis

Detailed Description: Not available

Recruitment & Eligibility

Status: COMPLETED

Sex: All

Target Recruitment: 191

Inclusion Criteria

Males or females, aged ≥ 18 years (≥ 20 for Japanese subjects) at the time of consent.
Have a diagnosis of atopic dermatitis for ≥ 12 months.
Have moderate to severe atopic dermatitis which is considered inappropriate for topical therapy or which cannot be adequately controlled by topical therapy.
Meet the laboratory criteria as defined per protocol
Females of Childbearing Potential (FCBP) must have a negative pregnancy test at Screening and Baseline. Sexually active FCBP must use one of the approved contraceptive options required per protocol while on and for at least 28 days after the last dose of study medication
Male subjects (including those who have had a vasectomy) who engage in activity in which conception is possible must use barrier contraception while on and for at least 28 days after the last dose of study medication.

Exclusion Criteria

Active tuberculosis (TB) or a history of inadequately treated tuberculosis.
Positive for hepatitis B surface antigen or hepatitis C antibody
Pregnant or breast feeding
History of allergy to any component of the study medication.
Active skin infection requiring systemic antimicrobials at Baseline.

Study & Design

Study Type: INTERVENTIONAL

Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
Placebo + Apremilast 30 mg	Placebo	Placebo administered orally BID for 12 weeks, during the placebo controlled phase followed by 30 mg Apremilast tablets orally BID for an additional 12 weeks in the active treatment phase
Placebo	Placebo	Oral Placebo tablets administered twice daily (BID) for 12 weeks during the placebo-controlled phase.
Placebo + Apremilast 40 mg	Placebo	Placebo administered orally BID for 12 weeks, during the placebo controlled phase followed by 40 mg Apremilast tablets orally BID for an additional 12 weeks in the active treatment phase
Apremilast 30 mg	Apremilast	Apremilast 30 mg administered orally BID for 12 weeks (following dose titration) during the placebo controlled phase followed by 30 mg Apremilast tablets orally administered BID for an additional 12 weeks in the active treatment phase
Placebo + Apremilast 40 mg	Apremilast	Placebo administered orally BID for 12 weeks, during the placebo controlled phase followed by 40 mg Apremilast tablets orally BID for an additional 12 weeks in the active treatment phase
Apremilast 40 mg	Apremilast	Apremilast 40 mg administered orally twice daily (BID) for 12 weeks (following dose titration) during the placebo controlled phase followed by 40 mg Apremilast tablets orally administered BID for an additional 12 weeks in the active treatment phase
Placebo + Apremilast 30 mg	Apremilast	Placebo administered orally BID for 12 weeks, during the placebo controlled phase followed by 30 mg Apremilast tablets orally BID for an additional 12 weeks in the active treatment phase

Primary Outcome Measures

Name	Time	Method
Percentage Change From Baseline in the Eczema Area and Severity Index (EASI) Score at Week 12.	Baseline to Week 12	EASI is a validated composite scoring system integrating the proportion of the body region (area) involved and the intensity of key signs of atopic dermatitis (AD). A representative lesion is selected for each of the four body regions for assessing the intensity of each of the four signs (erythema, induration /papulation, excoriation, and lichenification). Symptoms (eg, pruritus) and secondary signs (eg, xerosis, scaling) are excluded from the assessment. The total EASI score ranges from 0 to 72. A higher score indicated worse disease status, and a negative change from baseline indicated improvement.

Secondary Outcome Measures

Name	Time	Method
Percentage of Participants Who Achieved a Score of 0 (Cleared) or 1 (Almost Cleared) and at Least a 2-point Reduction From Baseline in a Static Physician's Global Assessment of Acute Signs (sPGA-A) at Week 12.	Baseline to Week 12	The sPGA-A is intended to assess the global severities (ie, a "visual average" integrating all areas of AD) of key acute clinical signs of AD, including erythema, induration/papulation, oozing/crusting (lichenification excluded) based on a 5-point scale of cleared (0), almost cleared (1), mild (2), moderate (3) and severe (4).
Percentage of Participants Who Achieved at Least a 50% Reduction From Baseline in the EASI Score (EASI 50) at Week 12	Baseline to Week 12	The EASI 50 reduction (defined as ≥ 50% reduction from baseline in EASI score) was selected to serve as the key responder endpoint. A ≥ 50% improvement is clinically meaningful for this population.
The Percentage Change From Baseline in the Average Weekly Pruritus Numerical Rating Scale (NRS) Score at Week 4	Baseline to Week 4	The participant completed a daily diary recording the average intensity of pruritus they experienced during the preceding 24 hrs. The intensity of pruritus was assessed using a validated 11-point NRS, ranging from 0 ("no pruritus") to 10 ("the worst pruritus imaginable"). It should be noted that this NRS is distinct from the pruritus, Visual Analogue Scale (VAS) in the Modified SCORAD Index with respect to recall period (three days for the VAS). The weekly NRS score was calculated as the average of the NRS scores over 7 days within the specified week. A higher score indicated worse disease status, and a negative change from baseline indicated improvement.
Number of Participants With Treatment Emergent Adverse Events (TEAEs) During the Placebo Controlled Period	Baseline to Week 12	A TEAE is an adverse event with a start date on or after the date of the first dose of IP and no later than 28 days after the last dose of IP for participants who discontinued early. An adverse event (AE) is any noxious, unintended, or untoward medical occurrence that may appear or worsen during the course of a study. It may be a new intercurrent illness, a worsening concomitant illness, an injury, or any concomitant impairment of the participant's health, including laboratory test values, regardless of etiology. Any worsening (ie, any clinically significant adverse change in the frequency or intensity of a pre existing condition) should be considered an AE. A serious AE is any which results in death, is life-threatening, requires inpatient hospitalization or prolongation of existing hospitalization, results in persistent or significant disability/incapacity, is a congenital anomaly/birth defect; constitutes an important medical event.
Number of Participants With TEAEs During the Apremilast Exposure Period	Baseline to Week 24; median duration of apremilast 30 mg was 23.3 weeks and 22.4 weeks for apremilast 40 mg	A TEAE is an adverse event with a start date on or after the date of the first dose of investigational product (IP) and no later than 28 days after the last dose of IP. An adverse event (AE) is any noxious, unintended, or untoward medical occurrence that may appear or worsen during the course of a study. It may be a new intercurrent illness, a worsening concomitant illness, an injury, or any concomitant impairment of the participant's health, including laboratory test values, regardless of etiology. Any worsening (ie, any clinically significant adverse change in the frequency or intensity of a pre existing condition) should be considered an AE. A serious AE is any which results in death, is life-threatening, requires inpatient hospitalization or prolongation of existing hospitalization, results in persistent or significant disability/incapacity, is a congenital anomaly/birth defect; constitutes an important medical event.

Trial Locations

Locations (31): Virginia Clinical Research Inc
🇺🇸
Norfolk, Virginia, United States
Mount Sinai Medical Center
🇺🇸
New York, New York, United States
Renstar Medical Research
🇺🇸
Ocala, Florida, United States
Hatamoto Dermatology Clinic
🇯🇵
Fukuoka-shi, Fukuoka, Japan
Ultranova Skincare
🇨🇦
Barrie, Ontario, Canada
Northwestern Medicine Lake Forest Hospital
🇺🇸
Lake Forest, Illinois, United States
NYU Department of Dermatology
🇺🇸
New York, New York, United States
Kokubu Abashiri Dermatology Clinic
🇯🇵
Abashiri-shi, Hokkaido, Japan
Asanuma Dermatology Clinic
🇯🇵
Chitose-shi, Hokkaido, Japan
NTT Medical Center Tokyo
🇯🇵
Shinagawa-ku, Tokyo, Japan
K. Papp Clinical Research
🇨🇦
Waterloo, Ontario, Canada
University Hospital, Kyoto Prefectural University of Medicine
🇯🇵
Kyoto-City, Japan
Sapporo Skin Clinic
🇯🇵
Sapporo-shi, Hokkaido, Japan
Bakersfield Dermatology and Skin Cancer Medical Group
🇺🇸
Bakersfield, California, United States
Northwestern University Northwestern Medical Faculty Foundation
🇺🇸
Chicago, Illinois, United States
Dermatology Research Associates
🇺🇸
Los Angeles, California, United States
Dermatology Specialists, PSC
🇺🇸
Louisville, Kentucky, United States
Emory Clinic
🇺🇸
Atlanta, Georgia, United States
PMG Research of Winston-Salem LLC
🇺🇸
Winston-Salem, North Carolina, United States
Advanced Medical Research
🇺🇸
Atlanta, Georgia, United States
Oregon Health and Science University
🇺🇸
Portland, Oregon, United States
Eastern Canada Cutaneous Research Associates Ltd
🇨🇦
Halifax, Nova Scotia, Canada
Kokubu Dermatology
🇯🇵
Kitami-shi, Hokkaido, Japan
Dartmouth Hitchcock Medical Center
🇺🇸
Lebanon, New Hampshire, United States
Fukuoka University Hospital Dermatology
🇯🇵
Fukuoka-shi, Fukuoka, Japan
Arizona Research Center
🇺🇸
Phoenix, Arizona, United States
Tashiro Clinic
🇯🇵
Iizuka-shi, Fukuoka, Japan
Kyoto University Hospital
🇯🇵
Kyoto, Japan
Innovaderm Research
🇨🇦
Montreal, Quebec, Canada
Centre Dermatologique du Quebec Metropolitain
🇨🇦
Ste-Foy, Quebec, Canada
Chih-Ho Hong Medical, Inc.
🇨🇦
Surrey, British Columbia, Canada