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A Study of Intravenous MK-8226 in Participants With Moderate-to-Severe Atopic Dermatitis (MK-8226-003)

Primary Purpose

Atopic Dermatitis

Status
Terminated
Phase
Phase 1
Locations
Study Type
Interventional
Intervention
MK-8226
Placebo
Sponsored by
Merck Sharp & Dohme LLC
About
Eligibility
Locations
Arms
Outcomes
Full info

About this trial

This is an interventional treatment trial for Atopic Dermatitis

Eligibility Criteria

18 Years - undefined (Adult, Older Adult)All SexesDoes not accept healthy volunteers

Inclusion Criteria:

  • Body weight >=40 kg
  • Clinical diagnosis of atopic dermatitis for at least 6 months prior
  • Candidate for systemic or phototherapy (i.e., failed topical treatment)
  • Moderate-to-severe disease as defined by Body Surface Area (BSA) ≥10%, EASI ≥12, and IGA ≥3
  • No clinically significant abnormality on electrocardiogram
  • No history of active or latent tuberculosis (TB) and no signs or symptoms suggestive of TB
  • No history of active or latent TB and no signs or symptoms suggestive of TB
  • History of inadequate response to a stable (≥ 1 month) regimen of topical corticosteroids or calcineurin inhibitors within 3 months before the screening visit

Exclusion Criteria:

  • Concurrent significant skin disease
  • Any significant organ dysfunction within 6 months prior
  • History of clinically significant heart disease
  • History of neoplastic disease
  • Positive for hepatitis B, hepatitis C, or human immunodeficiency virus (HIV)
  • Infection requiring oral antibiotics within 2 weeks prior
  • Receipt of a live virus vaccine within 4 weeks prior
  • Inability to refrain from topical or systemic therapy during course of the study
  • Had major surgery or donated or lost >=1 unit of blood within 4 weeks prior
  • Participation in another study within 4 weeks prior
  • Current or regular user of illicit drugs or a history of drug or alcohol abuse within 1 year prior
  • Pregnant, breast-feeding, or anticipated to conceive during the course of the study

Sites / Locations

    Arms of the Study

    Arm 1

    Arm 2

    Arm 3

    Arm 4

    Arm 5

    Arm 6

    Arm 7

    Arm Type

    Experimental

    Experimental

    Experimental

    Experimental

    Placebo Comparator

    Experimental

    Placebo Comparator

    Arm Label

    Part 1: MK-8226 0.3 mg/kg

    Part 1: MK-8226 1 mg/kg

    Part 1: MK-8226 3 mg/kg

    Part 1: MK-8226 10 mg/kg

    Part 1: Placebo (pooled)

    Part 2: MK-8226 3 mg/kg

    Part 2: Placebo

    Arm Description

    MK-8226 administered intravenously (IV) at a weight-based dose every 2 weeks for a period of 12 weeks.

    MK-8226 administered IV at a weight-based dose every 2 weeks for a period of 12 weeks.

    MK-8226 administered IV at a weight-based dose every 2 weeks for a period of 12 weeks.

    MK-8226 administered IV at a weight-based dose every 2 weeks for a period of 12 weeks.

    Dose-matched placebo administered IV every 2 weeks for a period of 12 weeks.

    MK-8226 administered IV at a weight-based dose every 2 weeks for a period of 12 weeks.

    Placebo administered IV every 2 weeks for a period of 12 weeks.

    Outcomes

    Primary Outcome Measures

    Number of Participants Who Experienced at Least One Adverse Event
    An adverse event (AE) is defined as any untoward medical occurrence in a patient or clinical investigation subject administered a pharmaceutical product and which does not necessarily have to have a causal relationship with this treatment. An AE can therefore be any unfavourable and unintended sign (including an abnormal laboratory finding, for example), symptom, or disease temporally associated with the use of a medicinal product or protocol-specified procedure, whether or not considered related to the medicinal product or protocol-specified procedure. Any worsening (i.e., any clinically significant adverse change in frequency and/or intensity) of a preexisting condition that is temporally associated with the use of the Sponsor's product, is also an AE.
    Number of Participants Who Discontinued Study Drug Due to an Adverse Event
    An AE is defined as any untoward medical occurrence in a patient or clinical investigation subject administered a pharmaceutical product and which does not necessarily have to have a causal relationship with this treatment. An AE can therefore be any unfavourable and unintended sign (including an abnormal laboratory finding, for example), symptom, or disease temporally associated with the use of a medicinal product or protocol-specified procedure, whether or not considered related to the medicinal product or protocol-specified procedure. Any worsening (i.e., any clinically significant adverse change in frequency and/or intensity) of a preexisting condition that is temporally associated with the use of the Sponsor's product, is also an AE.
    Change From Baseline in the Eczema Area and Severity Index (EASI) for Study Part 1
    Reduction from baseline in EASI at Week 12 (interim analysis data). The EASI assesses intensity of four lesion characteristics (erythema, infiltration/population, excoriation, lichenification) each rated on a scale of 0 (absent) to 3 (severe) across four regions (head, trunk, upper and lower extremities). Affected areas in each region are assessed as percentage of body surface (head [10%], trunk [30%], upper extremities [20%], and lower extremities [40%]). The total score is a sum of each region score and can range from 0 (absent disease) to 72 (severe disease).

    Secondary Outcome Measures

    Plasma Chemokine (C-C Motif) Ligand 17 (CCL17) Level in Study Part 2
    CCL17 is a pro-allergic chemokine that is assessed in human plasma. Levels of CCL17 are increased in allergic disease states.
    Plasma Chemokine (C-C Motif) Ligand 22 (CCL22) Level in Study Part 2
    CCL22 is a pro-allergic chemokine that is assessed in human plasma. Levels of CCL22 are increased in allergic disease states.
    Area Under the Concentration-time Curve of MK-8226 From Time 0 to Tau (AUC0-tau) Following Multiple Intravenous Dose Administration
    AUC(0-tau) defined as AUC from time zero to tau where tau is the dosing interval (312 hours) was determined for the first and last periods of MK-8226 dosing. MK-8226 was administered on Days 1, 14, 28, 42, 56, and 70. Blood concentrations of MK-8226 were determined on Days 1 (incl. predose), 3, 5, 9, 14 (incl. predose), 70 (incl. predose), 72, 74, 84. The placebo group is not included; this endpoint evaluated only the MK-8226 groups. No analysis was performed for Part 2 non-safety secondary endpoints after the Part 1 primary endpoint (Change from BL in EASI) did not demonstrate adequate effect in an interim futility analysis.
    AUC From Time 0 to Last Measurement (AUC0-last) of MK-8226 Following Multiple Intravenous Dose Administration
    AUC0-last defined as AUC up to the last measured concentration was determined for the last period of dosing (starting Week 10 [Day 70]) up to the last measurement. MK-8226 was administered on Days 1, 14, 28, 42, 56, and 70. Blood concentrations of MK-8226 were determined on Days 70 (incl. predose), 72, 74, 84, 98, 112, 140, 168, 196, and 224. The placebo group is not included; this endpoint evaluated only the MK-8226 groups. No analysis was performed for Part 2 non-safety secondary endpoints after the Part 1 primary endpoint (Change from BL in EASI) did not demonstrate adequate effect in an interim futility analysis.
    Maximum Serum Concentration (Cmax) of MK-8226 Following Multiple Dose Intravenous Administration
    Cmax was determined for the first and last periods of MK-8226 dosing. MK-8226 was administered on Days 1, 14, 28, 42, 56, and 70. Blood concentrations of MK-8226 were determined on Days 1 (incl. predose), 3, 5, 9, 14 (incl. predose), 70 (incl. predose), 72, 74, and 84. The placebo group is not included; this endpoint evaluated only the MK-8226 groups. No analysis was performed for Part 2 non-safety secondary endpoints after the Part 1 primary endpoint (Change from BL in EASI) did not demonstrate adequate effect in an interim futility analysis.
    Clearance (CL) of MK-8226 Following Multiple Dose Intravenous Administration
    CL, the volume of plasma cleared of drug per unit time, was determined for the last period of dosing (starting Week 10 [Day 70]) in the treatment period. MK-8226 was administered on Days 1, 14, 28, 42, 56, and 70. Blood concentrations of MK-8226 were determined on Days 1 (incl. predose), 3, 5, 9, 14 (incl. predose), 28 (incl. predose), 42 (incl. predose), 56 (incl. predose), 70 (incl. predose), 72, 74, and 84. The placebo group is not included; this endpoint evaluated only the MK-8226 groups. No analysis was performed for Part 2 non-safety secondary endpoints after the Part 1 primary endpoint (Change from BL in EASI) did not demonstrate adequate effect in an interim futility analysis.
    Volume of Distribution (Vd) of MK-8226 Following Multiple Intravenous Administration
    Vd, a theoretical approximation of degree to which the drug distributes in body tissue rather than plasma (higher Vd indicates greater tissue distribution), was determined for the last period of dosing (starting Week 10 [Day 70]) in the treatment period. MK-8226 was administered on Days 1, 14, 28, 42, 56, and 70. Blood concentrations of MK-8226 were determined on Days 70 (incl. predose), 72, 74, 84, 98, 112, 140, 168, 196, and 224. The placebo group is not included; this endpoint evaluated only the MK-8226 groups. No analysis was performed for Part 2 non-safety secondary endpoints after the Part 1 primary endpoint (Change from BL in EASI) did not demonstrate adequate effect in an interim futility analysis.
    Terminal Half Life (t1/2) of MK-8226 Following Multiple Dose Intravenous Administration
    t1/2, the time needed for the concentration of drug to reach half the initial concentration, was determined for the last period of dosing (starting Week 10 [Day 70]) up to the last measurement. MK-8226 was administered on Days 1, 14, 28, 42, 56, and 70. Blood concentrations of MK-8226 were determined on Days 70 (incl. predose), 72, 74, 84, 98, 112, 140, 168, 196, and 224. The placebo group is not included; this endpoint evaluated only the MK-8226 groups. No analysis was performed for Part 2 non-safety secondary endpoints after the Part 1 primary endpoint (Change from BL in EASI) did not demonstrate adequate effect in an interim futility analysis.
    Change From Baseline in the Eczema Area and Severity Index (EASI) for Study Part 2
    The EASI assesses intensity of four lesion characteristics (erythema, infiltration/population, excoriation, lichenification) each rated on a scale of 0 (absent) to 3 (severe) across four regions (head, trunk, upper and lower extremities). Affected areas in each region are assessed as percentage of body surface (head [10%], trunk [30%], upper extremities [20%], and lower extremities [40%]). The total score is a sum of each region score and can range from 0 (absent disease) to 72 (severe disease).
    Percentage of Participants With an Investigator Global Assessment (IGA) Score of Clear or Almost Clear in Study Part 2
    Percentage of participants achieving an IGA of atopic dermatitis of "clear-0" or "almost clear-1". The IGA is a six-point scale measuring the severity of disease at time of physical examination of the participant by the physician. The IGA is scored 0 (Clear) to 5 (Very severe disease).
    Change From Baseline in the Scoring Atopic Dermatitis Scale (SCORAD) in Study Part 2
    The SCORAD index scale combines 1) intensity of six lesion characteristics (erythema, edema/papulation, oozing/crusts, excoriations, lichenification, dryness) as assessed by the physician on a scale of 0 (absent) to 3 (severe) across four regions (head, trunk, upper and lower extremities) along with 2) subjective symptoms of pruritus and sleep disturbance as reported by the patient on a visual analog scale (VAS) from 1 to 10 cm (increasing severity). Physician assessment of affected areas in each region is made as percentage of body surface (head [10%], trunk [30%], upper extremities [20%], and lower extremities [40%]). The final SCORAD index score, ranging from 0 (absent disease) to 103 (severe disease), is calculated according to the weighted formula: (0.2 x area) + (3.5 x [sum of intensity score for each of the 6 items]) + participant's subjective score.
    Change From Baseline in Participant Pruritus in Study Part 2
    Skin pruritus (itching) is a typical characteristic of atopic dermatitis. Participant subjective assessment of pruritus (component of SCORAD) is rated on a VAS ranging from 1 to 10 cm (increasing severity).
    Change From Baseline in Participant Sleep Disturbance in Study Part 2
    Sleep disturbance (sleep loss, disruption, or interference) due to unremitting pruritus and other causes is a quality of life issue in moderate to severe atopic dermatitis. Participant subjective assessment of sleep disturbance (component of SCORAD) over the past 3 days is rated on a VAS ranging from 1 to 10 cm (increasing severity).
    Number of Participants Requiring As-Needed Oral Antihistamines as Rescue Medication in Study Part 2
    Oral antihistamines (i.e., diphenhydramine, acrivastine fenistil) were provided as as-needed rescue medication for severe pruritus.
    Percentage of Participants With >=50% Improvement in EASI Score
    The EASI assesses intensity of four lesion characteristics (erythema, infiltration/population, excoriation, lichenification) each rated on a scale of 0 (absent) to 3 (severe) across four regions (head, trunk, upper and lower extremities). Affected areas in each region are assessed as percentage of body surface (head [10%], trunk [30%], upper extremities [20%], and lower extremities [40%]). The total score is a sum of each region score and can range from 0 (absent disease) to 72 (severe disease).
    Number of Participants Positive for Anti-Drug Antibody (ADA) Formation
    Testing for ADA positivity and neutralizing response and antibody titre quantification are performed with blood (serum) samples collected at baseline (Day 1 predose) and Days 14, 28, 42, 56, 74, 112, and 224. Neutralizing response refers to ADA neutralizing interference with study drug assessed in vitro. Non-Treatment emergent ADA refers to presence of ADAs (as determined by assay) in the absence of treatment with study drug (i.e., at predose).

    Full Information

    First Posted
    November 19, 2012
    Last Updated
    February 27, 2019
    Sponsor
    Merck Sharp & Dohme LLC
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    1. Study Identification

    Unique Protocol Identification Number
    NCT01732510
    Brief Title
    A Study of Intravenous MK-8226 in Participants With Moderate-to-Severe Atopic Dermatitis (MK-8226-003)
    Official Title
    A Phase Ib Randomized, Double-Blinded, Placebo-Controlled Multiple Rising Dose Clinical Trial to Evaluate the Safety, Efficacy, Pharmacokinetics, Pharmacodynamics, and Immunogenicity of Intravenous MK-8226 in Patients With Moderate to Severe Atopic Dermatitis
    Study Type
    Interventional

    2. Study Status

    Record Verification Date
    February 2019
    Overall Recruitment Status
    Terminated
    Why Stopped
    The study was prematurely stopped due to business reasons.
    Study Start Date
    December 21, 2012 (Actual)
    Primary Completion Date
    October 20, 2014 (Actual)
    Study Completion Date
    October 20, 2014 (Actual)

    3. Sponsor/Collaborators

    Responsible Party, by Official Title
    Sponsor
    Name of the Sponsor
    Merck Sharp & Dohme LLC

    4. Oversight

    Data Monitoring Committee
    No

    5. Study Description

    Brief Summary
    This is a 3-part study to assess the safety, tolerability, efficacy, pharmacokinetics (PK), pharmacodynamics (PD), and immunogenicity of MK-8226 in participants with moderate to severe atopic dermatitis. Part 1 (multiple rising dose study) objectives were to find the maximum tolerated dose (MTD) of MK-8226 and to assess safety and PK. Part 2 objectives were to determine safety, PK, and preliminary efficacy. Part 3 objectives were to further define safety and PK, and explore MK-8226 PK/PD to model the optimal dose range for future studies. The study was terminated early due to business reasons on 08 May 2014; final results from an analysis for Part 1 (efficacy, PK, safety, immunogenicity) and Part 2 (safety, immunogenicity) are summarized.
    Detailed Description
    Part 1 of the study is a multiple rising dose assessment of the safety, tolerability, and pharmacokinetics of MK-8226 for a period of 12 weeks followed by a 20-week off-treatment follow-up period. Part 2 of the study is an assessment of the safety, tolerability, and efficacy of MK-8226 for 12 weeks followed by a 20-week off-treatment follow-up period. In Part 3 of the study, participants will be treated with MK-8226 for a period of 12 weeks followed by a 20-week off-treatment follow-up period to evaluate pharmacokinetic and pharmacokinetic correlations to assist with modeling the dose range planned for further studies.

    6. Conditions and Keywords

    Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
    Atopic Dermatitis

    7. Study Design

    Primary Purpose
    Treatment
    Study Phase
    Phase 1
    Interventional Study Model
    Parallel Assignment
    Masking
    ParticipantCare ProviderInvestigatorOutcomes Assessor
    Allocation
    Randomized
    Enrollment
    65 (Actual)

    8. Arms, Groups, and Interventions

    Arm Title
    Part 1: MK-8226 0.3 mg/kg
    Arm Type
    Experimental
    Arm Description
    MK-8226 administered intravenously (IV) at a weight-based dose every 2 weeks for a period of 12 weeks.
    Arm Title
    Part 1: MK-8226 1 mg/kg
    Arm Type
    Experimental
    Arm Description
    MK-8226 administered IV at a weight-based dose every 2 weeks for a period of 12 weeks.
    Arm Title
    Part 1: MK-8226 3 mg/kg
    Arm Type
    Experimental
    Arm Description
    MK-8226 administered IV at a weight-based dose every 2 weeks for a period of 12 weeks.
    Arm Title
    Part 1: MK-8226 10 mg/kg
    Arm Type
    Experimental
    Arm Description
    MK-8226 administered IV at a weight-based dose every 2 weeks for a period of 12 weeks.
    Arm Title
    Part 1: Placebo (pooled)
    Arm Type
    Placebo Comparator
    Arm Description
    Dose-matched placebo administered IV every 2 weeks for a period of 12 weeks.
    Arm Title
    Part 2: MK-8226 3 mg/kg
    Arm Type
    Experimental
    Arm Description
    MK-8226 administered IV at a weight-based dose every 2 weeks for a period of 12 weeks.
    Arm Title
    Part 2: Placebo
    Arm Type
    Placebo Comparator
    Arm Description
    Placebo administered IV every 2 weeks for a period of 12 weeks.
    Intervention Type
    Drug
    Intervention Name(s)
    MK-8226
    Intervention Description
    MK-8226 administered IV at a weight-based dose every 2 weeks for 12 weeks.
    Intervention Type
    Drug
    Intervention Name(s)
    Placebo
    Intervention Description
    Placebo administered IV every 2 weeks for a period of 12 weeks.
    Primary Outcome Measure Information:
    Title
    Number of Participants Who Experienced at Least One Adverse Event
    Description
    An adverse event (AE) is defined as any untoward medical occurrence in a patient or clinical investigation subject administered a pharmaceutical product and which does not necessarily have to have a causal relationship with this treatment. An AE can therefore be any unfavourable and unintended sign (including an abnormal laboratory finding, for example), symptom, or disease temporally associated with the use of a medicinal product or protocol-specified procedure, whether or not considered related to the medicinal product or protocol-specified procedure. Any worsening (i.e., any clinically significant adverse change in frequency and/or intensity) of a preexisting condition that is temporally associated with the use of the Sponsor's product, is also an AE.
    Time Frame
    Up to 32 Weeks
    Title
    Number of Participants Who Discontinued Study Drug Due to an Adverse Event
    Description
    An AE is defined as any untoward medical occurrence in a patient or clinical investigation subject administered a pharmaceutical product and which does not necessarily have to have a causal relationship with this treatment. An AE can therefore be any unfavourable and unintended sign (including an abnormal laboratory finding, for example), symptom, or disease temporally associated with the use of a medicinal product or protocol-specified procedure, whether or not considered related to the medicinal product or protocol-specified procedure. Any worsening (i.e., any clinically significant adverse change in frequency and/or intensity) of a preexisting condition that is temporally associated with the use of the Sponsor's product, is also an AE.
    Time Frame
    Up to 12 Weeks
    Title
    Change From Baseline in the Eczema Area and Severity Index (EASI) for Study Part 1
    Description
    Reduction from baseline in EASI at Week 12 (interim analysis data). The EASI assesses intensity of four lesion characteristics (erythema, infiltration/population, excoriation, lichenification) each rated on a scale of 0 (absent) to 3 (severe) across four regions (head, trunk, upper and lower extremities). Affected areas in each region are assessed as percentage of body surface (head [10%], trunk [30%], upper extremities [20%], and lower extremities [40%]). The total score is a sum of each region score and can range from 0 (absent disease) to 72 (severe disease).
    Time Frame
    Baseline, Week 12
    Secondary Outcome Measure Information:
    Title
    Plasma Chemokine (C-C Motif) Ligand 17 (CCL17) Level in Study Part 2
    Description
    CCL17 is a pro-allergic chemokine that is assessed in human plasma. Levels of CCL17 are increased in allergic disease states.
    Time Frame
    Baseline, 48 Hours, Week 2, Week 4, Week 12, Week 16
    Title
    Plasma Chemokine (C-C Motif) Ligand 22 (CCL22) Level in Study Part 2
    Description
    CCL22 is a pro-allergic chemokine that is assessed in human plasma. Levels of CCL22 are increased in allergic disease states.
    Time Frame
    Baseline, 48 Hours, Week 2, Week 4, Week 12, Week 16
    Title
    Area Under the Concentration-time Curve of MK-8226 From Time 0 to Tau (AUC0-tau) Following Multiple Intravenous Dose Administration
    Description
    AUC(0-tau) defined as AUC from time zero to tau where tau is the dosing interval (312 hours) was determined for the first and last periods of MK-8226 dosing. MK-8226 was administered on Days 1, 14, 28, 42, 56, and 70. Blood concentrations of MK-8226 were determined on Days 1 (incl. predose), 3, 5, 9, 14 (incl. predose), 70 (incl. predose), 72, 74, 84. The placebo group is not included; this endpoint evaluated only the MK-8226 groups. No analysis was performed for Part 2 non-safety secondary endpoints after the Part 1 primary endpoint (Change from BL in EASI) did not demonstrate adequate effect in an interim futility analysis.
    Time Frame
    Days 1, 3, 5, 9, 14, 70, 72, 74, 84
    Title
    AUC From Time 0 to Last Measurement (AUC0-last) of MK-8226 Following Multiple Intravenous Dose Administration
    Description
    AUC0-last defined as AUC up to the last measured concentration was determined for the last period of dosing (starting Week 10 [Day 70]) up to the last measurement. MK-8226 was administered on Days 1, 14, 28, 42, 56, and 70. Blood concentrations of MK-8226 were determined on Days 70 (incl. predose), 72, 74, 84, 98, 112, 140, 168, 196, and 224. The placebo group is not included; this endpoint evaluated only the MK-8226 groups. No analysis was performed for Part 2 non-safety secondary endpoints after the Part 1 primary endpoint (Change from BL in EASI) did not demonstrate adequate effect in an interim futility analysis.
    Time Frame
    Days 70, 72, 74, 84, 98, 112, 140, 168, 196, 224
    Title
    Maximum Serum Concentration (Cmax) of MK-8226 Following Multiple Dose Intravenous Administration
    Description
    Cmax was determined for the first and last periods of MK-8226 dosing. MK-8226 was administered on Days 1, 14, 28, 42, 56, and 70. Blood concentrations of MK-8226 were determined on Days 1 (incl. predose), 3, 5, 9, 14 (incl. predose), 70 (incl. predose), 72, 74, and 84. The placebo group is not included; this endpoint evaluated only the MK-8226 groups. No analysis was performed for Part 2 non-safety secondary endpoints after the Part 1 primary endpoint (Change from BL in EASI) did not demonstrate adequate effect in an interim futility analysis.
    Time Frame
    Days 1, 3, 5, 9, 14, 70, 72, 74, 84
    Title
    Clearance (CL) of MK-8226 Following Multiple Dose Intravenous Administration
    Description
    CL, the volume of plasma cleared of drug per unit time, was determined for the last period of dosing (starting Week 10 [Day 70]) in the treatment period. MK-8226 was administered on Days 1, 14, 28, 42, 56, and 70. Blood concentrations of MK-8226 were determined on Days 1 (incl. predose), 3, 5, 9, 14 (incl. predose), 28 (incl. predose), 42 (incl. predose), 56 (incl. predose), 70 (incl. predose), 72, 74, and 84. The placebo group is not included; this endpoint evaluated only the MK-8226 groups. No analysis was performed for Part 2 non-safety secondary endpoints after the Part 1 primary endpoint (Change from BL in EASI) did not demonstrate adequate effect in an interim futility analysis.
    Time Frame
    Days 1, 3, 5, 9, 14, 28, 42, 56, 70, 72, 74, 84
    Title
    Volume of Distribution (Vd) of MK-8226 Following Multiple Intravenous Administration
    Description
    Vd, a theoretical approximation of degree to which the drug distributes in body tissue rather than plasma (higher Vd indicates greater tissue distribution), was determined for the last period of dosing (starting Week 10 [Day 70]) in the treatment period. MK-8226 was administered on Days 1, 14, 28, 42, 56, and 70. Blood concentrations of MK-8226 were determined on Days 70 (incl. predose), 72, 74, 84, 98, 112, 140, 168, 196, and 224. The placebo group is not included; this endpoint evaluated only the MK-8226 groups. No analysis was performed for Part 2 non-safety secondary endpoints after the Part 1 primary endpoint (Change from BL in EASI) did not demonstrate adequate effect in an interim futility analysis.
    Time Frame
    Days 70, 72, 74, 84, 98, 112, 140, 168, 196, 224
    Title
    Terminal Half Life (t1/2) of MK-8226 Following Multiple Dose Intravenous Administration
    Description
    t1/2, the time needed for the concentration of drug to reach half the initial concentration, was determined for the last period of dosing (starting Week 10 [Day 70]) up to the last measurement. MK-8226 was administered on Days 1, 14, 28, 42, 56, and 70. Blood concentrations of MK-8226 were determined on Days 70 (incl. predose), 72, 74, 84, 98, 112, 140, 168, 196, and 224. The placebo group is not included; this endpoint evaluated only the MK-8226 groups. No analysis was performed for Part 2 non-safety secondary endpoints after the Part 1 primary endpoint (Change from BL in EASI) did not demonstrate adequate effect in an interim futility analysis.
    Time Frame
    Days 70, 72, 74, 84, 98, 112, 140, 168, 196, 224
    Title
    Change From Baseline in the Eczema Area and Severity Index (EASI) for Study Part 2
    Description
    The EASI assesses intensity of four lesion characteristics (erythema, infiltration/population, excoriation, lichenification) each rated on a scale of 0 (absent) to 3 (severe) across four regions (head, trunk, upper and lower extremities). Affected areas in each region are assessed as percentage of body surface (head [10%], trunk [30%], upper extremities [20%], and lower extremities [40%]). The total score is a sum of each region score and can range from 0 (absent disease) to 72 (severe disease).
    Time Frame
    Baseline, Week 4, Week 8, Week 24
    Title
    Percentage of Participants With an Investigator Global Assessment (IGA) Score of Clear or Almost Clear in Study Part 2
    Description
    Percentage of participants achieving an IGA of atopic dermatitis of "clear-0" or "almost clear-1". The IGA is a six-point scale measuring the severity of disease at time of physical examination of the participant by the physician. The IGA is scored 0 (Clear) to 5 (Very severe disease).
    Time Frame
    Baseline, Week 4, Week 8, Week 12, Week 24
    Title
    Change From Baseline in the Scoring Atopic Dermatitis Scale (SCORAD) in Study Part 2
    Description
    The SCORAD index scale combines 1) intensity of six lesion characteristics (erythema, edema/papulation, oozing/crusts, excoriations, lichenification, dryness) as assessed by the physician on a scale of 0 (absent) to 3 (severe) across four regions (head, trunk, upper and lower extremities) along with 2) subjective symptoms of pruritus and sleep disturbance as reported by the patient on a visual analog scale (VAS) from 1 to 10 cm (increasing severity). Physician assessment of affected areas in each region is made as percentage of body surface (head [10%], trunk [30%], upper extremities [20%], and lower extremities [40%]). The final SCORAD index score, ranging from 0 (absent disease) to 103 (severe disease), is calculated according to the weighted formula: (0.2 x area) + (3.5 x [sum of intensity score for each of the 6 items]) + participant's subjective score.
    Time Frame
    Baseline, Week 4, Week 12, Week 24
    Title
    Change From Baseline in Participant Pruritus in Study Part 2
    Description
    Skin pruritus (itching) is a typical characteristic of atopic dermatitis. Participant subjective assessment of pruritus (component of SCORAD) is rated on a VAS ranging from 1 to 10 cm (increasing severity).
    Time Frame
    Baseline, Week 4, Week 12, Week 24
    Title
    Change From Baseline in Participant Sleep Disturbance in Study Part 2
    Description
    Sleep disturbance (sleep loss, disruption, or interference) due to unremitting pruritus and other causes is a quality of life issue in moderate to severe atopic dermatitis. Participant subjective assessment of sleep disturbance (component of SCORAD) over the past 3 days is rated on a VAS ranging from 1 to 10 cm (increasing severity).
    Time Frame
    Baseline, Week 4, Week 12, Week 24
    Title
    Number of Participants Requiring As-Needed Oral Antihistamines as Rescue Medication in Study Part 2
    Description
    Oral antihistamines (i.e., diphenhydramine, acrivastine fenistil) were provided as as-needed rescue medication for severe pruritus.
    Time Frame
    Up to Week 12
    Title
    Percentage of Participants With >=50% Improvement in EASI Score
    Description
    The EASI assesses intensity of four lesion characteristics (erythema, infiltration/population, excoriation, lichenification) each rated on a scale of 0 (absent) to 3 (severe) across four regions (head, trunk, upper and lower extremities). Affected areas in each region are assessed as percentage of body surface (head [10%], trunk [30%], upper extremities [20%], and lower extremities [40%]). The total score is a sum of each region score and can range from 0 (absent disease) to 72 (severe disease).
    Time Frame
    Baseline, Week 12, Week 24
    Title
    Number of Participants Positive for Anti-Drug Antibody (ADA) Formation
    Description
    Testing for ADA positivity and neutralizing response and antibody titre quantification are performed with blood (serum) samples collected at baseline (Day 1 predose) and Days 14, 28, 42, 56, 74, 112, and 224. Neutralizing response refers to ADA neutralizing interference with study drug assessed in vitro. Non-Treatment emergent ADA refers to presence of ADAs (as determined by assay) in the absence of treatment with study drug (i.e., at predose).
    Time Frame
    Days 1 (predose) and Days 14, 28, 42, 56, 74, 112, and 224
    Other Pre-specified Outcome Measures:
    Title
    Change From Baseline in the Participant's Global Impression of Disease Status in Study Part 2
    Description
    Participant subjective impression of improvement of his/her disease condition is scored on a six-point scale: 0 (Clear) to 5 (Very severe disease).
    Time Frame
    Baseline, Week 4, Week 12, Week 24

    10. Eligibility

    Sex
    All
    Minimum Age & Unit of Time
    18 Years
    Accepts Healthy Volunteers
    No
    Eligibility Criteria
    Inclusion Criteria: Body weight >=40 kg Clinical diagnosis of atopic dermatitis for at least 6 months prior Candidate for systemic or phototherapy (i.e., failed topical treatment) Moderate-to-severe disease as defined by Body Surface Area (BSA) ≥10%, EASI ≥12, and IGA ≥3 No clinically significant abnormality on electrocardiogram No history of active or latent tuberculosis (TB) and no signs or symptoms suggestive of TB No history of active or latent TB and no signs or symptoms suggestive of TB History of inadequate response to a stable (≥ 1 month) regimen of topical corticosteroids or calcineurin inhibitors within 3 months before the screening visit Exclusion Criteria: Concurrent significant skin disease Any significant organ dysfunction within 6 months prior History of clinically significant heart disease History of neoplastic disease Positive for hepatitis B, hepatitis C, or human immunodeficiency virus (HIV) Infection requiring oral antibiotics within 2 weeks prior Receipt of a live virus vaccine within 4 weeks prior Inability to refrain from topical or systemic therapy during course of the study Had major surgery or donated or lost >=1 unit of blood within 4 weeks prior Participation in another study within 4 weeks prior Current or regular user of illicit drugs or a history of drug or alcohol abuse within 1 year prior Pregnant, breast-feeding, or anticipated to conceive during the course of the study
    Overall Study Officials:
    First Name & Middle Initial & Last Name & Degree
    Medical Director
    Organizational Affiliation
    Merck Sharp & Dohme LLC
    Official's Role
    Study Director

    12. IPD Sharing Statement

    Plan to Share IPD
    Yes
    IPD Sharing Plan Description
    http://engagezone.msd.com/doc/ProcedureAccessClinicalTrialData.pdf
    IPD Sharing URL
    http://engagezone.msd.com/ds_documentation.php

    Learn more about this trial

    A Study of Intravenous MK-8226 in Participants With Moderate-to-Severe Atopic Dermatitis (MK-8226-003)

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