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UP-TAINED: A Study to Assess Disease Activity in Adolescent and Adult Participants With Atopic Dermatitis Who Receive Oral Upadacitinib Tablets in a Real-World Setting

Sponsor
AbbVie (Industry)
Overall Status
Recruiting
CT.gov ID
NCT05139836
Collaborator
(none)
772
Enrollment
80
Locations
41.7
Anticipated Duration (Months)
9.7
Patients Per Site
0.2
Patients Per Site Per Month

Study Details

Study Description

Brief Summary

Atopic dermatitis (AD) is a skin condition that may cause a rash and itching due to inflammation of the skin. Therapies spread over the skin may not be enough to control the AD in trial participants who require systemic anti-inflammatory treatment. This study will assess the real-world effectiveness of upadacitinib on early and sustained response along adolescent and adult participants with AD. This study also aims to understand upadacitinib utilization patterns in real-world clinical practice.

Upadacitinib (RINVOQ) is approved in the EU for the treatment of moderate to severe AD in adults and adolescents 12 years and older who are candidates for systemic therapy. Approximately 772 adolescent and adult participants with AD will be enrolled at up to 200 sites in Germany.

Participants will receive oral upadacitinib tablets as prescribed by the physician prior to enrolling in this study in accordance with the terms of the local marketing authorization and professional and reimbursement guidelines with regards to dose, population, and indication. The overall duration of the study is approximately 2 years.

Participants will attend regular visits per routine clinical practice. The effect of the treatment will be checked by medical assessments, checking for side effects, and questionnaires.

Condition or Disease Intervention/Treatment Phase

    Study Design

    Study Type:
    Observational
    Anticipated Enrollment :
    772 participants
    Observational Model:
    Cohort
    Time Perspective:
    Prospective
    Official Title:
    Non-Interventional, Prospective Observational Cohort Study to Investigate the Effectiveness and Sustained Disease Control of an Upadacitinib Therapy in Moderate to Severe Atopic Dermatitis Patients Over Two Years
    Actual Study Start Date :
    Dec 13, 2021
    Anticipated Primary Completion Date :
    Jun 3, 2025
    Anticipated Study Completion Date :
    Jun 3, 2025

    Arms and Interventions

    Arm Intervention/Treatment
    Participants Receiving Upadacitinib

    Participants receiving upadacitinib for moderate to severe atopic dermatitis.

    Outcome Measures

    Primary Outcome Measures

    1. Percentage of Participants Achieving Disease Control Defined by Atopic Dermatitis Control Tool (ADCT) Total Score <7 Points [Month 3]

      The ADCT is a validated patient self-administered instrument designed to assess atopic dermatitis (AD) control status in adult and adolescent patients (12 years and older). A higher score indicates lower AD control. A score of >=7 indicates that the patient is not in control.

    2. Percentage of Participants Achieving Disease Control Defined by ADCT Total Score <7 Points Among Participants Who Achieved Disease Control at Month 3 [Month 24]

      The ADCT is a validated patient self-administered instrument designed to assess atopic dermatitis (AD) control status in adult and adolescent patients (12 years and older). A higher score indicates lower AD control. A score of >=7 indicates that the patient is not in control.

    Secondary Outcome Measures

    1. Percentage of Participants Achieving Disease Control Defined by ADCT Total Score <7 Points [Up to 24 Months]

      The ADCT is a validated patient self-administered instrument designed to assess atopic dermatitis (AD) control status in adult and adolescent patients (12 years and older). A higher score indicates lower AD control. A score of >=7 indicates that the patient is not in control.

    2. Percentage of Participants with An ADCT Total Score Reduction >=5 from Baseline [Up to 24 Months]

      The ADCT is a validated patient self-administered instrument designed to assess atopic dermatitis (AD) control status in adult and adolescent patients (12 years and older). A higher score indicates lower AD control. A score of >=7 indicates that the patient is not in control.

    3. Percentage of Participants Achieving Disease Control as Defined by ADCT Item 4 (Sleep Problems) <1 Point and All Other Items <2 Points [Up to 24 Months]

      The ADCT is a validated patient self-administered instrument designed to assess atopic dermatitis (AD) control status in adult and adolescent patients (12 years and older). A higher score indicates lower AD control. A score of >=7 indicates that the patient is not in control.

    4. Percentage of Participants Achieving Disease Control as Defined by ADCT Total Score <7 Points at Month 3 and Maintaining Disease Control [Up to 21 Months (Excluding Month 3 - Primary Endpoint)]

      The ADCT is a validated patient self-administered instrument designed to assess atopic dermatitis (AD) control status in adult and adolescent patients (12 years and older). A higher score indicates lower AD control. A score of >=7 indicates that the patient is not in control.

    5. Absolute Score for ADCT Total Score [Up to 24 Months]

      The ADCT is a validated patient self-administered instrument designed to assess atopic dermatitis (AD) control status in adult and adolescent patients (12 years and older). A higher score indicates lower AD control. A score of >=7 indicates that the patient is not in control.

    6. Absolute Change from Baseline for ADCT Total Score [Up to 24 Months]

      The ADCT is a validated patient self-administered instrument designed to assess atopic dermatitis (AD) control status in adult and adolescent patients (12 years and older). A higher score indicates lower AD control. A score of >=7 indicates that the patient is not in control.

    7. Time to Achieve ADCT Total Score Reduction >=5 Points from Baseline [Up to 24 Months]

      The ADCT is a validated patient self-administered instrument designed to assess atopic dermatitis (AD) control status in adult and adolescent patients (12 years and older). A higher score indicates lower AD control. A score of >=7 indicates that the patient is not in control.

    8. Time to Achieve Disease Control as Defined by ADCT Total Score <7 Points [Up to 24 Months]

      The ADCT is a validated patient self-administered instrument designed to assess atopic dermatitis (AD) control status in adult and adolescent patients (12 years and older). A higher score indicates lower AD control. A score of >=7 indicates that the patient is not in control.

    9. Percent Change from Baseline for ADCT Total Score [Up to 24 Months]

      The ADCT is a validated patient self-administered instrument designed to assess atopic dermatitis (AD) control status in adult and adolescent patients (12 years and older). A higher score indicates lower AD control. A score of >=7 indicates that the patient is not in control.

    10. Percentage of Participants Achieving Eczema Area and Severity Index (EASI) 50 [Up to 24 Months]

      The EASI is a validated measure used in clinical practice and clinical trials to assess the severity and extent of AD. Four AD disease characteristics (erythema, thickness [induration, papulation, edema], scratching [excoriation], and lichenification) are each assessed for severity by the investigator on a scale of "0" (absent) through "3" (severe). In addition, the area of AD involvement is assessed as a percentage by body area of head, trunk (including the genital area), upper extremities, and lower extremities (including the buttocks), and converted to a score of 0 to 6. The EASI score ranges from 0-72 points with an MCID of 6.6 points. Published score bands: clear (0), almost clear (0.1-1.0), mild AD (1.1-7.0), moderate AD (7.1-21.0), severe AD (21.1-50.0), very severe AD (50.1-72.0).

    11. Percentage of Participants Achieving EASI 75 [Up to 24 Months]

      The EASI is a validated measure used in clinical practice and clinical trials to assess the severity and extent of AD. Four AD disease characteristics (erythema, thickness [induration, papulation, edema], scratching [excoriation], and lichenification) are each assessed for severity by the investigator on a scale of "0" (absent) through "3" (severe). In addition, the area of AD involvement is assessed as a percentage by body area of head, trunk (including the genital area), upper extremities, and lower extremities (including the buttocks), and converted to a score of 0 to 6. The EASI score ranges from 0-72 points with an MCID of 6.6 points. Published score bands: clear (0), almost clear (0.1-1.0), mild AD (1.1-7.0), moderate AD (7.1-21.0), severe AD (21.1-50.0), very severe AD (50.1-72.0).

    12. Percentage of Participants Achieving EASI 90 [Up to 24 Months]

      The EASI is a validated measure used in clinical practice and clinical trials to assess the severity and extent of AD. Four AD disease characteristics (erythema, thickness [induration, papulation, edema], scratching [excoriation], and lichenification) are each assessed for severity by the investigator on a scale of "0" (absent) through "3" (severe). In addition, the area of AD involvement is assessed as a percentage by body area of head, trunk (including the genital area), upper extremities, and lower extremities (including the buttocks), and converted to a score of 0 to 6. The EASI score ranges from 0-72 points with an MCID of 6.6 points. Published score bands: clear (0), almost clear (0.1-1.0), mild AD (1.1-7.0), moderate AD (7.1-21.0), severe AD (21.1-50.0), very severe AD (50.1-72.0).

    13. Percentage of Participants Achieving EASI 100 [Up to 24 Months]

      The EASI is a validated measure used in clinical practice and clinical trials to assess the severity and extent of AD. Four AD disease characteristics (erythema, thickness [induration, papulation, edema], scratching [excoriation], and lichenification) are each assessed for severity by the investigator on a scale of "0" (absent) through "3" (severe). In addition, the area of AD involvement is assessed as a percentage by body area of head, trunk (including the genital area), upper extremities, and lower extremities (including the buttocks), and converted to a score of 0 to 6. The EASI score ranges from 0-72 points with an MCID of 6.6 points. Published score bands: clear (0), almost clear (0.1-1.0), mild AD (1.1-7.0), moderate AD (7.1-21.0), severe AD (21.1-50.0), very severe AD (50.1-72.0).

    14. Percentage of Participants Achieving Absolute EASI <=7 [Up to 24 Months]

      The EASI is a validated measure used in clinical practice and clinical trials to assess the severity and extent of AD. Four AD disease characteristics (erythema, thickness [induration, papulation, edema], scratching [excoriation], and lichenification) are each assessed for severity by the investigator on a scale of "0" (absent) through "3" (severe). In addition, the area of AD involvement is assessed as a percentage by body area of head, trunk (including the genital area), upper extremities, and lower extremities (including the buttocks), and converted to a score of 0 to 6. The EASI score ranges from 0-72 points with an MCID of 6.6 points. Published score bands: clear (0), almost clear (0.1-1.0), mild AD (1.1-7.0), moderate AD (7.1-21.0), severe AD (21.1-50.0), very severe AD (50.1-72.0).

    15. Absolute Score for EASI [Up to 24 Months]

      The EASI is a validated measure used in clinical practice and clinical trials to assess the severity and extent of AD. Four AD disease characteristics (erythema, thickness [induration, papulation, edema], scratching [excoriation], and lichenification) are each assessed for severity by the investigator on a scale of "0" (absent) through "3" (severe). In addition, the area of AD involvement is assessed as a percentage by body area of head, trunk (including the genital area), upper extremities, and lower extremities (including the buttocks), and converted to a score of 0 to 6. The EASI score ranges from 0-72 points with an MCID of 6.6 points. Published score bands: clear (0), almost clear (0.1-1.0), mild AD (1.1-7.0), moderate AD (7.1-21.0), severe AD (21.1-50.0), very severe AD (50.1-72.0).

    16. Absolute Change from Baseline for EASI [Up to 24 Months]

      The EASI is a validated measure used in clinical practice and clinical trials to assess the severity and extent of AD. Four AD disease characteristics (erythema, thickness [induration, papulation, edema], scratching [excoriation], and lichenification) are each assessed for severity by the investigator on a scale of "0" (absent) through "3" (severe). In addition, the area of AD involvement is assessed as a percentage by body area of head, trunk (including the genital area), upper extremities, and lower extremities (including the buttocks), and converted to a score of 0 to 6. The EASI score ranges from 0-72 points with an MCID of 6.6 points. Published score bands: clear (0), almost clear (0.1-1.0), mild AD (1.1-7.0), moderate AD (7.1-21.0), severe AD (21.1-50.0), very severe AD (50.1-72.0).

    17. Percent Change from Baseline for EASI [Up to 24 Months]

      The EASI is a validated measure used in clinical practice and clinical trials to assess the severity and extent of AD. Four AD disease characteristics (erythema, thickness [induration, papulation, edema], scratching [excoriation], and lichenification) are each assessed for severity by the investigator on a scale of "0" (absent) through "3" (severe). In addition, the area of AD involvement is assessed as a percentage by body area of head, trunk (including the genital area), upper extremities, and lower extremities (including the buttocks), and converted to a score of 0 to 6. The EASI score ranges from 0-72 points with an MCID of 6.6 points. Published score bands: clear (0), almost clear (0.1-1.0), mild AD (1.1-7.0), moderate AD (7.1-21.0), severe AD (21.1-50.0), very severe AD (50.1-72.0).

    18. Time to Achieve EASI 50 [Up to 24 Months]

      The EASI is a validated measure used in clinical practice and clinical trials to assess the severity and extent of AD. Four AD disease characteristics (erythema, thickness [induration, papulation, edema], scratching [excoriation], and lichenification) are each assessed for severity by the investigator on a scale of "0" (absent) through "3" (severe). In addition, the area of AD involvement is assessed as a percentage by body area of head, trunk (including the genital area), upper extremities, and lower extremities (including the buttocks), and converted to a score of 0 to 6. The EASI score ranges from 0-72 points with an MCID of 6.6 points. Published score bands: clear (0), almost clear (0.1-1.0), mild AD (1.1-7.0), moderate AD (7.1-21.0), severe AD (21.1-50.0), very severe AD (50.1-72.0).

    19. Time to Achieve EASI 75 [Up to 24 Months]

      The EASI is a validated measure used in clinical practice and clinical trials to assess the severity and extent of AD. Four AD disease characteristics (erythema, thickness [induration, papulation, edema], scratching [excoriation], and lichenification) are each assessed for severity by the investigator on a scale of "0" (absent) through "3" (severe). In addition, the area of AD involvement is assessed as a percentage by body area of head, trunk (including the genital area), upper extremities, and lower extremities (including the buttocks), and converted to a score of 0 to 6. The EASI score ranges from 0-72 points with an MCID of 6.6 points. Published score bands: clear (0), almost clear (0.1-1.0), mild AD (1.1-7.0), moderate AD (7.1-21.0), severe AD (21.1-50.0), very severe AD (50.1-72.0).

    20. Time to Achieve EASI 90 [Up to 24 Months]

      The EASI is a validated measure used in clinical practice and clinical trials to assess the severity and extent of AD. Four AD disease characteristics (erythema, thickness [induration, papulation, edema], scratching [excoriation], and lichenification) are each assessed for severity by the investigator on a scale of "0" (absent) through "3" (severe). In addition, the area of AD involvement is assessed as a percentage by body area of head, trunk (including the genital area), upper extremities, and lower extremities (including the buttocks), and converted to a score of 0 to 6. The EASI score ranges from 0-72 points with an MCID of 6.6 points. Published score bands: clear (0), almost clear (0.1-1.0), mild AD (1.1-7.0), moderate AD (7.1-21.0), severe AD (21.1-50.0), very severe AD (50.1-72.0).

    21. Time to Achieve EASI 100 [Up to 24 Months]

      The EASI is a validated measure used in clinical practice and clinical trials to assess the severity and extent of AD. Four AD disease characteristics (erythema, thickness [induration, papulation, edema], scratching [excoriation], and lichenification) are each assessed for severity by the investigator on a scale of "0" (absent) through "3" (severe). In addition, the area of AD involvement is assessed as a percentage by body area of head, trunk (including the genital area), upper extremities, and lower extremities (including the buttocks), and converted to a score of 0 to 6. The EASI score ranges from 0-72 points with an MCID of 6.6 points. Published score bands: clear (0), almost clear (0.1-1.0), mild AD (1.1-7.0), moderate AD (7.1-21.0), severe AD (21.1-50.0), very severe AD (50.1-72.0).

    22. Time to Achieve Absolute EASI <=7 [Up to 24 Months]

      The EASI is a validated measure used in clinical practice and clinical trials to assess the severity and extent of AD. Four AD disease characteristics (erythema, thickness [induration, papulation, edema], scratching [excoriation], and lichenification) are each assessed for severity by the investigator on a scale of "0" (absent) through "3" (severe). In addition, the area of AD involvement is assessed as a percentage by body area of head, trunk (including the genital area), upper extremities, and lower extremities (including the buttocks), and converted to a score of 0 to 6. The EASI score ranges from 0-72 points with an MCID of 6.6 points. Published score bands: clear (0), almost clear (0.1-1.0), mild AD (1.1-7.0), moderate AD (7.1-21.0), severe AD (21.1-50.0), very severe AD (50.1-72.0).

    23. Percentage of Participants Achieving EASI 50 in the Head and/or Neck Body Region [Up to 24 Months]

      The EASI is a validated measure used in clinical practice and clinical trials to assess the severity and extent of AD. Four AD disease characteristics (erythema, thickness [induration, papulation, edema], scratching [excoriation], and lichenification) are each assessed for severity by the investigator on a scale of "0" (absent) through "3" (severe). In addition, the area of AD involvement is assessed as a percentage by body area of head, trunk (including the genital area), upper extremities, and lower extremities (including the buttocks), and converted to a score of 0 to 6. The EASI score ranges from 0-72 points with an MCID of 6.6 points. Published score bands: clear (0), almost clear (0.1-1.0), mild AD (1.1-7.0), moderate AD (7.1-21.0), severe AD (21.1-50.0), very severe AD (50.1-72.0).

    24. Percentage of Participants Achieving EASI 75 in the Head and/or Neck Body Region [Up to 24 Months]

      The EASI is a validated measure used in clinical practice and clinical trials to assess the severity and extent of AD. Four AD disease characteristics (erythema, thickness [induration, papulation, edema], scratching [excoriation], and lichenification) are each assessed for severity by the investigator on a scale of "0" (absent) through "3" (severe). In addition, the area of AD involvement is assessed as a percentage by body area of head, trunk (including the genital area), upper extremities, and lower extremities (including the buttocks), and converted to a score of 0 to 6. The EASI score ranges from 0-72 points with an MCID of 6.6 points. Published score bands: clear (0), almost clear (0.1-1.0), mild AD (1.1-7.0), moderate AD (7.1-21.0), severe AD (21.1-50.0), very severe AD (50.1-72.0).

    25. Percentage of Participants Achieving EASI 90 in the Head and/or Neck Body Region [Up to 24 Months]

      The EASI is a validated measure used in clinical practice and clinical trials to assess the severity and extent of AD. Four AD disease characteristics (erythema, thickness [induration, papulation, edema], scratching [excoriation], and lichenification) are each assessed for severity by the investigator on a scale of "0" (absent) through "3" (severe). In addition, the area of AD involvement is assessed as a percentage by body area of head, trunk (including the genital area), upper extremities, and lower extremities (including the buttocks), and converted to a score of 0 to 6. The EASI score ranges from 0-72 points with an MCID of 6.6 points. Published score bands: clear (0), almost clear (0.1-1.0), mild AD (1.1-7.0), moderate AD (7.1-21.0), severe AD (21.1-50.0), very severe AD (50.1-72.0).

    26. Percentage of Participants Achieving EASI 100 in the Head and/or Neck Body Region [Up to 24 Months]

      The EASI is a validated measure used in clinical practice and clinical trials to assess the severity and extent of AD. Four AD disease characteristics (erythema, thickness [induration, papulation, edema], scratching [excoriation], and lichenification) are each assessed for severity by the investigator on a scale of "0" (absent) through "3" (severe). In addition, the area of AD involvement is assessed as a percentage by body area of head, trunk (including the genital area), upper extremities, and lower extremities (including the buttocks), and converted to a score of 0 to 6. The EASI score ranges from 0-72 points with an MCID of 6.6 points. Published score bands: clear (0), almost clear (0.1-1.0), mild AD (1.1-7.0), moderate AD (7.1-21.0), severe AD (21.1-50.0), very severe AD (50.1-72.0).

    27. Percentage of Participants Achieving Validated Investigator Global Assessment for Atopic Dermatitis (vIGA-AD) <=1 [Up to 24 Months]

      vIGA-AD is a validated assessment instrument used in clinical studies to rate the severity of AD globally. A 5-point scale is used to measure the severity of disease at the time of the investigator's evaluation of the participant ranging from 0 - Clear (no inflammatory signs of atopic dermatitis (no erythema, no induration/papulation, no lichenification, no oozing/crusting). Post-inflammatory hyperpigmentation and/or hypopigmentation may be present.) to 4 - Severe (marked erythema (deep or bright red), marked induration/papulation, and/or marked lichenification.

    28. Percentage of Participants Achieving Worst Pruritus Numerical Rating Scale (WP-NRS) <=1 [Up to 24 Months]

      WP-NRS is a validated single self-reported item designed to measure peak pruritus, or 'worst' itch, over the previous 24 hours with a higher score denoting worse itch.

    29. Percentage of Participants Achieving WP-NRS <=3 [Up to 24 Months]

      WP-NRS is a validated single self-reported item designed to measure peak pruritus, or 'worst' itch, over the previous 24 hours with a higher score denoting worse itch.

    30. Percentage of Participants Achieving a WP-NRS Reduction >=4 from Baseline [Up to 24 Months]

      WP-NRS is a validated single self-reported item designed to measure peak pruritus, or 'worst' itch, over the previous 24 hours with a higher score denoting worse itch.

    31. Absolute Score for WP-NRS [Up to 24 Months]

      WP-NRS is a validated single self-reported item designed to measure peak pruritus, or 'worst' itch, over the previous 24 hours with a higher score denoting worse itch.

    32. Absolute Change from Baseline for WP-NRS [Up to 24 Months]

      WP-NRS is a validated single self-reported item designed to measure peak pruritus, or 'worst' itch, over the previous 24 hours with a higher score denoting worse itch.

    33. Percent Change from Baseline for WP-NRS [Up to 24 Months]

      WP-NRS is a validated single self-reported item designed to measure peak pruritus, or 'worst' itch, over the previous 24 hours with a higher score denoting worse itch.

    34. Time to Achieve WP-NRS <=1 [Up to 24 Months]

      WP-NRS is a validated single self-reported item designed to measure peak pruritus, or 'worst' itch, over the previous 24 hours with a higher score denoting worse itch.

    35. Absolute Change from Baseline for SCORAD Sleep VAS [Up to 24 Months]

      The sleep VAS is one component from the SCORAD test that measures the intensity of sleeplessness during a three day or night recall period. The test uses a VAS scale of 0 to 10 with 0 being "no sleeplessness" and 10 being "worst imaginable sleeplessness".

    36. Absolute Score for Score Atopic Dermatitis (SCORAD) Sleep Visual Analog Scale (VAS) [Up to 24 Months]

      The sleep VAS is one component from the SCORAD test that measures the intensity of sleeplessness during a three day or night recall period. The test uses a VAS scale of 0 to 10 with 0 being "no sleeplessness" and 10 being "worst imaginable sleeplessness".

    37. Percent Change from Baseline for SCORAD Sleep VAS [Up to 24 Months]

      The sleep VAS is one component from the SCORAD test that measures the intensity of sleeplessness during a three day or night recall period. The test uses a VAS scale of 0 to 10 with 0 being "no sleeplessness" and 10 being "worst imaginable sleeplessness".

    38. Percentage of Participants Achieving Dermatology Life Quality Index (DLQI)/Children's Dermatology Life Quality Index (cDLQI) <=1 [Up to 24 Months]

      DLQI is a 10-item, validated questionnaire used in clinical practice and clinical trials to assess the impact of AD disease symptoms and treatment on health-related quality of life (HRQoL). It consists of 10 questions assessing impact of skin diseases on different aspects of subject's QoL over the prior week. Each item is scored on a 4-point scale: 0 = not at all/not relevant; 1 = a little; 2 = a lot; and 3 = very much. Item scores (0 to 3) are added to provide a total score range of 0 to 30. Higher scores indicate greater impairment of HRQoL. For patients from age 12-15 the cDLQI is used.

    39. Percentage of Participants Achieving DLQI/cDLQI <=5 [Up to 24 Months]

      DLQI is a 10-item, validated questionnaire used in clinical practice and clinical trials to assess the impact of AD disease symptoms and treatment on health-related quality of life (HRQoL). It consists of 10 questions assessing impact of skin diseases on different aspects of subject's QoL over the prior week. Each item is scored on a 4-point scale: 0 = not at all/not relevant; 1 = a little; 2 = a lot; and 3 = very much. Item scores (0 to 3) are added to provide a total score range of 0 to 30. Higher scores indicate greater impairment of HRQoL. For patients from age 12-15 the cDLQI is used.

    40. Percentage of Participants Achieving DLQI/cDLQI Reduction >=4 from Baseline [Up to 24 Months]

      DLQI is a 10-item, validated questionnaire used in clinical practice and clinical trials to assess the impact of AD disease symptoms and treatment on health-related quality of life (HRQoL). It consists of 10 questions assessing impact of skin diseases on different aspects of subject's QoL over the prior week. Each item is scored on a 4-point scale: 0 = not at all/not relevant; 1 = a little; 2 = a lot; and 3 = very much. Item scores (0 to 3) are added to provide a total score range of 0 to 30. Higher scores indicate greater impairment of HRQoL. For patients from age 12-15 the cDLQI is used.

    41. Absolute Score for DLQI/cDLQI [Up to 24 Months]

      DLQI is a 10-item, validated questionnaire used in clinical practice and clinical trials to assess the impact of AD disease symptoms and treatment on health-related quality of life (HRQoL). It consists of 10 questions assessing impact of skin diseases on different aspects of subject's QoL over the prior week. Each item is scored on a 4-point scale: 0 = not at all/not relevant; 1 = a little; 2 = a lot; and 3 = very much. Item scores (0 to 3) are added to provide a total score range of 0 to 30. Higher scores indicate greater impairment of HRQoL. For patients from age 12-15 the cDLQI is used.

    42. Absolute Change from Baseline for DLQI/cDLQI [Up to 24 Months]

      DLQI is a 10-item, validated questionnaire used in clinical practice and clinical trials to assess the impact of AD disease symptoms and treatment on health-related quality of life (HRQoL). It consists of 10 questions assessing impact of skin diseases on different aspects of subject's QoL over the prior week. Each item is scored on a 4-point scale: 0 = not at all/not relevant; 1 = a little; 2 = a lot; and 3 = very much. Item scores (0 to 3) are added to provide a total score range of 0 to 30. Higher scores indicate greater impairment of HRQoL. For patients from age 12-15 the cDLQI is used.

    43. Percent Change from Baseline for DLQI/cDLQI [Up to 24 Months]

      DLQI is a 10-item, validated questionnaire used in clinical practice and clinical trials to assess the impact of AD disease symptoms and treatment on health-related quality of life (HRQoL). It consists of 10 questions assessing impact of skin diseases on different aspects of subject's QoL over the prior week. Each item is scored on a 4-point scale: 0 = not at all/not relevant; 1 = a little; 2 = a lot; and 3 = very much. Item scores (0 to 3) are added to provide a total score range of 0 to 30. Higher scores indicate greater impairment of HRQoL. For patients from age 12-15 the cDLQI is used.

    44. Time to Achieve DLQI/cDLQI <=1 [Up to 24 Months]

      DLQI is a 10-item, validated questionnaire used in clinical practice and clinical trials to assess the impact of AD disease symptoms and treatment on health-related quality of life (HRQoL). It consists of 10 questions assessing impact of skin diseases on different aspects of subject's QoL over the prior week. Each item is scored on a 4-point scale: 0 = not at all/not relevant; 1 = a little; 2 = a lot; and 3 = very much. Item scores (0 to 3) are added to provide a total score range of 0 to 30. Higher scores indicate greater impairment of HRQoL. For patients from age 12-15 the cDLQI is used.

    45. Absolute Score for Hospital Anxiety and Depression Scale for Anxiety (HADS-A) [Up to 24 Months]

      The HADS is a 14-item self-report scale, It contains two 7-item scales: one for anxiety (HADS-A) and one for depression (HADS-D). Each HADS item is rated on a 4-point Likert-type scale with total scores on each subscale ranging from 0 to 21, and with higher scores corresponding to greater respective symptom severity.

    46. Absolute Change from Baseline for HADS-A [Up to 24 Months]

      The HADS is a 14-item self-report scale, It contains two 7-item scales: one for anxiety (HADS-A) and one for depression (HADS-D). Each HADS item is rated on a 4-point Likert-type scale with total scores on each subscale ranging from 0 to 21, and with higher scores corresponding to greater respective symptom severity.

    47. Percent Change from Baseline for HADS-A [Up to 24 Months]

      The HADS is a 14-item self-report scale, It contains two 7-item scales: one for anxiety (HADS-A) and one for depression (HADS-D). Each HADS item is rated on a 4-point Likert-type scale with total scores on each subscale ranging from 0 to 21, and with higher scores corresponding to greater respective symptom severity.

    48. Absolute Score for Hospital Anxiety and Depression Scale for Depression (HADS-D) [Up to 24 Months]

      The HADS is a 14-item self-report scale, It contains two 7-item scales: one for anxiety (HADS-A) and one for depression (HADS-D). Each HADS item is rated on a 4-point Likert-type scale with total scores on each subscale ranging from 0 to 21, and with higher scores corresponding to greater respective symptom severity.

    49. Absolute Change from Baseline for HADS-D [Up to 24 Months]

      The HADS is a 14-item self-report scale, It contains two 7-item scales: one for anxiety (HADS-A) and one for depression (HADS-D). Each HADS item is rated on a 4-point Likert-type scale with total scores on each subscale ranging from 0 to 21, and with higher scores corresponding to greater respective symptom severity.

    50. Percent Change from Baseline for HADS-D [Up to 24 Months]

      The HADS is a 14-item self-report scale, It contains two 7-item scales: one for anxiety (HADS-A) and one for depression (HADS-D). Each HADS item is rated on a 4-point Likert-type scale with total scores on each subscale ranging from 0 to 21, and with higher scores corresponding to greater respective symptom severity.

    51. Absolute Score for Stigmatization (6-Item Stigmatization Scale) [Up to 24 Months]

      The scale consists of 6 items that address the feeling of stigmatization because of this condition. The participants respond to each item by 0 (not at all), 1 (sometimes), 2 (very often), or 3 (always). The sum of the responses to the 6 items generates a score ranging from 0 to 18 with higher scores corresponding to a higher feeling of stigmatization.

    52. Absolute Change from Baseline for Stigmatization (6-Item Stigmatization Scale) [Up to 24 Months]

      The scale consists of 6 items that address the feeling of stigmatization because of this condition. The participants respond to each item by 0 (not at all), 1 (sometimes), 2 (very often), or 3 (always). The sum of the responses to the 6 items generates a score ranging from 0 to 18 with higher scores corresponding to a higher feeling of stigmatization.

    53. Percent Change from Baseline for Stigmatization (6-Item Stigmatization Scale) [Up to 24 Months]

      The scale consists of 6 items that address the feeling of stigmatization because of this condition. The participants respond to each item by 0 (not at all), 1 (sometimes), 2 (very often), or 3 (always). The sum of the responses to the 6 items generates a score ranging from 0 to 18 with higher scores corresponding to a higher feeling of stigmatization.

    54. Absolute Score for Asthma Control Test (ACT) in Participants Having a Confirmed Diagnosis of Asthma at Baseline [Up to 24 Months]

      The ACT consists of 5 simple questions regarding the patients' asthma symptom burden. For each question there is a range from 1 to 5. A lower score indicates lower asthma control.

    55. Absolute Change from Baseline in ACT in Participants Having a Confirmed Diagnosis of Asthma at Baseline [Up to 24 Months]

      The ACT consists of 5 simple questions regarding the patients' asthma symptom burden. For each question there is a range from 1 to 5. A lower score indicates lower asthma control.

    56. Percent Change from Baseline in ACT in Participants Having a Confirmed Diagnosis of Asthma at Baseline [Up to 24 Months]

      The ACT consists of 5 simple questions regarding the patients' asthma symptom burden. For each question there is a range from 1 to 5. A lower score indicates lower asthma control.

    57. Percentage of Participants Achieving Absolute Score >=20 for ACT in Participants Having a Confirmed Diagnosis of Asthma at Baseline [Up to 24 Months]

      The ACT consists of 5 simple questions regarding the patients' asthma symptom burden. For each question there is a range from 1 to 5. A lower score indicates lower asthma control.

    58. Percentage of Participants Starting on Upadacitinib 15 mg or 30 mg [Baseline]

      Percentage of participants initiating upadacitinib at 15 mg or 30 mg with rationale.

    59. Percentage of Participants with Modification of Upadacitinib Therapy, Timing of Modifications, and Reasons for Modifications [24 Months]

      This includes change in upadacitinib dose with rationale, e.g., dose change, temporary or permanent discontinuation.

    60. Percentage of Participants with Modification of Concomitant AD Therapy, Timing of Modifications, and Reasons for Modifications [24 Months]

      This includes change in concomitant AD therapy with rationale, e.g., adding or removing or changing dose of topical corticosteroids/topical calcineurin inhibitors.

    61. Absolute Score for Skin Pain on the Atopic Dermatitis Symptom Scale (ADerm-SS) [Up to 24 Months]

      Skin pain and skin cracking are assessed by a one item test from the ADERM-SS to measure the intensity of skin pain/skin cracking during the past 24 hours. The test uses a scale of 0 to 10, with 0 being "no skin pain"/"no skin cracking" and 10 bring the "worst imaginable skin pain"/"worst imaginable skin cracking".

    62. Absolute Change from Baseline for Skin Pain on the ADerm-SS [Up to 24 Months]

      Skin pain and skin cracking are assessed by a one item test from the ADERM-SS to measure the intensity of skin pain/skin cracking during the past 24 hours. The test uses a scale of 0 to 10, with 0 being "no skin pain"/"no skin cracking" and 10 bring the "worst imaginable skin pain"/"worst imaginable skin cracking".

    63. Percent Change from Baseline for Skin Pain on the ADerm-SS [Up to 24 Months]

      Skin pain and skin cracking are assessed by a one item test from the ADERM-SS to measure the intensity of skin pain/skin cracking during the past 24 hours. The test uses a scale of 0 to 10, with 0 being "no skin pain"/"no skin cracking" and 10 bring the "worst imaginable skin pain"/"worst imaginable skin cracking".

    64. Absolute Score for Skin Cracking on the ADerm-SS [Up to 24 Months]

      Skin pain and skin cracking are assessed by a one item test from the ADERM-SS to measure the intensity of skin pain/skin cracking during the past 24 hours. The test uses a scale of 0 to 10, with 0 being "no skin pain"/"no skin cracking" and 10 bring the "worst imaginable skin pain"/"worst imaginable skin cracking".

    65. Absolute Change from Baseline for Skin Cracking on the ADerm-SS [Up to 24 Months]

      Skin pain and skin cracking are assessed by a one item test from the ADERM-SS to measure the intensity of skin pain/skin cracking during the past 24 hours. The test uses a scale of 0 to 10, with 0 being "no skin pain"/"no skin cracking" and 10 bring the "worst imaginable skin pain"/"worst imaginable skin cracking".

    66. Percent Change from Baseline for Skin Cracking on the ADerm-SS [Up to 24 Months]

      Skin pain and skin cracking are assessed by a one item test from the ADERM-SS to measure the intensity of skin pain/skin cracking during the past 24 hours. The test uses a scale of 0 to 10, with 0 being "no skin pain"/"no skin cracking" and 10 bring the "worst imaginable skin pain"/"worst imaginable skin cracking".

    67. Absolute Score for Validated Investigator Global Assessment Scale for Atopic Dermatitis (vIGA-AD) of Hand Eczema [Up to 24 Months]

      The vIGA-AD is a validated assessment instrument used in clinical studies to rate the severity of AD globally. It consists of a 5-point scale used by the investigator to measure the severity of disease ranging from 0 - Clear to 4 - Severe.

    68. Absolute Change from Baseline for vIGA-AD of Hand Eczema [Up to 24 Months]

      The vIGA-AD is a validated assessment instrument used in clinical studies to rate the severity of AD globally. It consists of a 5-point scale used by the investigator to measure the severity of disease ranging from 0 - Clear to 4 - Severe.

    69. Percent Change from Baseline for vIGA-AD of Hand Eczema [Up to 24 Months]

      The vIGA-AD is a validated assessment instrument used in clinical studies to rate the severity of AD globally. It consists of a 5-point scale used by the investigator to measure the severity of disease ranging from 0 - Clear to 4 - Severe.

    70. Absolute Score for vIGA-AD of Facial Eczema [Up to 24 Months]

      The vIGA-AD is a validated assessment instrument used in clinical studies to rate the severity of AD globally. It consists of a 5-point scale used by the investigator to measure the severity of disease ranging from 0 - Clear to 4 - Severe.

    71. Absolute Change from Baseline for vIGA-AD of Facial Eczema [Up to 24 Months]

      The vIGA-AD is a validated assessment instrument used in clinical studies to rate the severity of AD globally. It consists of a 5-point scale used by the investigator to measure the severity of disease ranging from 0 - Clear to 4 - Severe.

    72. Percent Change from Baseline for vIGA-AD of Facial Eczema [Up to 24 Months]

      The vIGA-AD is a validated assessment instrument used in clinical studies to rate the severity of AD globally. It consists of a 5-point scale used by the investigator to measure the severity of disease ranging from 0 - Clear to 4 - Severe.

    73. Absolute Score for Pruritis (5-D Pruritis Scale) [Up to 24 Months]

      The 5-D pruritis scale is a brief but multidimensional questionnaire for the quantification of pruritis that is sensitive to change over time. The five dimensions are degree, duration, direction, disability and distribution. The duration, degree and direction domains each include one item, while the disability domain has four items. All items on the first four domains are measured on a five-point Likert scales. The scores of each of the five domains are achieved separately and then summed together to obtain a total 5-D score. 5-D scores can potentially range between 5 (no pruritis) and 25 (most severe pruritis).

    74. Absolute Change from Baseline for Pruritis (5-D Pruritis Scale) [Up to 24 Months]

      The 5-D pruritis scale is a brief but multidimensional questionnaire for the quantification of pruritis that is sensitive to change over time. The five dimensions are degree, duration, direction, disability and distribution. The duration, degree and direction domains each include one item, while the disability domain has four items. All items on the first four domains are measured on a five-point Likert scales. The scores of each of the five domains are achieved separately and then summed together to obtain a total 5-D score. 5-D scores can potentially range between 5 (no pruritis) and 25 (most severe pruritis).

    75. Percent Change from Baseline for Pruritis (5-D Pruritis Scale) [Up to 24 Months]

      The 5-D pruritis scale is a brief but multidimensional questionnaire for the quantification of pruritis that is sensitive to change over time. The five dimensions are degree, duration, direction, disability and distribution. The duration, degree and direction domains each include one item, while the disability domain has four items. All items on the first four domains are measured on a five-point Likert scales. The scores of each of the five domains are achieved separately and then summed together to obtain a total 5-D score. 5-D scores can potentially range between 5 (no pruritis) and 25 (most severe pruritis).

    76. Absolute Score for Flare Frequency [Up to 24 Months]

      Flare frequency is assessed by acquiring information about the number of flares in the last six months before baseline. During the study the patient is asked about number of flares since the last visit. Additionally, the presence of a current flare is assessed at each visit.

    77. Absolute Change from Baseline for Flare Frequency [Up to 24 Months]

      Flare frequency is assessed by acquiring information about the number of flares in the last six months before baseline. During the study the patient is asked about number of flares since the last visit. Additionally, the presence of a current flare is assessed at each visit.

    78. Percent Change from Baseline for Flare Frequency [Up to 24 Months]

      Flare frequency is assessed by acquiring information about the number of flares in the last six months before baseline. During the study the patient is asked about number of flares since the last visit. Additionally, the presence of a current flare is assessed at each visit.

    79. Absolute Score for Flare Duration [Up to 24 Months]

      Flare frequency is assessed by acquiring information about the number of flares in the last six months before baseline. During the study the patient is asked about number of flares since the last visit. The mean duration of the flares is also documented. Additionally, the presence of a current flare is assessed at each visit.

    80. Absolute Change from Baseline for Flare Duration [Up to 24 Months]

      Flare frequency is assessed by acquiring information about the number of flares in the last six months before baseline. During the study the patient is asked about number of flares since the last visit. The mean duration of the flares is also documented. Additionally, the presence of a current flare is assessed at each visit.

    81. Percent Change from Baseline for Flare Duration [Up to 24 Months]

      Flare frequency is assessed by acquiring information about the number of flares in the last six months before baseline. During the study the patient is asked about number of flares since the last visit. The mean duration of the flares is also documented. Additionally, the presence of a current flare is assessed at each visit.

    82. Absolute Score for Patient Self-Reported Global Assessment of Disease Severity (PtGA) [Up to 24 Months]

      Patients assess the overall severity of their disease by a five-point assessment scale (clear, mild, moderate, severe, or very severe, [0-4]), with higher scores corresponding to greater severity.

    83. Absolute Change from Baseline for PtGA [Up to 24 Months]

      Patients assess the overall severity of their disease by a five-point assessment scale (clear, mild, moderate, severe, or very severe, [0-4]), with higher scores corresponding to greater severity.

    84. Percent Change from Baseline for PtGA [Up to 24 Months]

      Patients assess the overall severity of their disease by a five-point assessment scale (clear, mild, moderate, severe, or very severe, [0-4]), with higher scores corresponding to greater severity.

    85. Percentage of Participants Achieving PtGA <=2 [Up to 24 Months]

      Patients assess the overall severity of their disease by a five-point assessment scale (clear, mild, moderate, severe, or very severe, [0-4]), with higher scores corresponding to greater severity.

    86. Percentage of Participants Achieving PtGA Reduction >=1 from Baseline [Up to 24 Months]

      Patients assess the overall severity of their disease by a five-point assessment scale (clear, mild, moderate, severe, or very severe, [0-4]), with higher scores corresponding to greater severity.

    87. Incidence and Type of Adverse Events [Up to 24 Months]

      An adverse event (AE) is defined as any untoward medical occurrence in a patient or clinical investigation participant administered a pharmaceutical product which does not necessarily have a causal relationship with this treatment. The investigator assesses the relationship of each event to the use of study. A serious adverse event (SAE) is an event that results in death, is life-threatening, requires or prolongs hospitalization, results in a congenital anomaly, persistent or significant disability/incapacity or is an important medical event that, based on medical judgment, may jeopardize the participant and may require medical or surgical intervention to prevent any of the outcomes listed above. Treatment-emergent adverse events/treatment-emergent serious adverse events (TEAEs/TESAEs) are defined as any event that began or worsened in severity on or after the first dose of study drug but within 30 days after the last dose of study drug.

    Eligibility Criteria

    Criteria

    Ages Eligible for Study:
    12 Years and Older
    Sexes Eligible for Study:
    All
    Accepts Healthy Volunteers:
    No
    Inclusion Criteria:

    • Body weight >=30 kg at baseline for participants between >=12 and <18 years of age.

    • Physician confirmed diagnosis of moderate to severe atopic dermatitis at the time of enrollment.

    • Upadacitinib initiated as per the local label. The decision to prescribe upadacitinib must have been made prior to and independently of study participation.

    • Medical and medication history available at least for the last 6 months.

    Exclusion Criteria:
    • Current participation in interventional research (note: this does not include non-interventional, post-marketing observational studies, or registry participation).

    Contacts and Locations

    Locations

    Site City State Country Postal Code
    1 Universitaetsklinik Heidelberg /ID# 245834 Heidelberg Baden-Wuerttemberg Germany 69120
    2 CMS3 Company for Medical Study /ID# 241659 Selters Rheinland-Pfalz Germany 56242
    3 Universitaetsklinikum Schleswig-Holstein Campus Kiel /ID# 240096 Kiel Schleswig-Holstein Germany 24105
    4 Hoeller-Obrigkeit, Aachen, DE /ID# 245430 Aachen Germany 52064
    5 Petri, Ahaus, DE /ID# 243452 Ahaus Germany 48683
    6 Praxis Dr. Mihaescu /ID# 241825 Augsburg Germany 86150
    7 Praxis S. Bresgulewski /ID# 244331 Bad Bertrich Germany 56864
    8 Mauer, Bad Kreuznach, DE /ID# 241990 Bad Kreuznach Germany 55543
    9 Timmel/Timm/Vorwerk, Bergen /ID# 241661 Bergen Germany 18528
    10 Praxis Dermatologie am Savigny /ID# 248846 Berlin Germany 10623
    11 Schirmer, Berlin, DE /ID# 241684 Berlin Germany 12489
    12 Kors, Berlin, DE /ID# 241847 Berlin Germany 13086
    13 Dues/Manasterski, Berlin, DE /ID# 243885 Berlin Germany 13507
    14 Hautarztzentrum Tegel /ID# 241826 Berlin Germany 13507
    15 Haut Pur - Dermatologische Gemeinschaftspraxis /ID# 243943 Berlin Germany 13597
    16 Klinikum Rosenhoehe /ID# 241601 Bielefeld Germany 33647
    17 Praxis fuer Innere Medizin/Rheumatologie /ID# 241846 Blaubeuren Germany 89143
    18 Praxis T. Schadeck /ID# 241768 Bogen Germany 94327
    19 Barth, Borna, DE /ID# 248871 Borna Germany 04552
    20 Studiengesellschaft an der Hase GbR Praxis Weyergraf/Frick/Heiber /ID# 241658 Bramsche Germany 49565
    21 Schwichtenberg, Bremen, DE /ID# 241683 Bremen Germany 28779
    22 Praxis P. Hausler-Mehlhorn /ID# 241527 Chemnitz Germany 09130
    23 Derma Köln /ID# 241856 Cologne Germany 50737
    24 Praxis Dr. Sbornik /ID# 241818 Deggendorf Germany 94469
    25 Richter-Huhn, Dresden, DE /ID# 241822 Dresden Germany 01219
    26 Praxis Dr. Korge /ID# 241531 Dueren Germany 52349
    27 Praxis Dr. Mempel /ID# 241827 Elmshorn Germany 25335
    28 Praxis Dres. Freitag/Knoell /ID# 242278 Falkensee Germany 14612
    29 Praxis Dr. Hong-Weldemann /ID# 248844 Freiburg im Breisgau Germany 79098
    30 Kurzen, Freising, DE /ID# 241845 Freising Germany 85354
    31 Hautarztpraxis Friedberg Dr. med. Wilfried Jungkunz /ID# 248851 Friedberg (Hessen) Germany 61169
    32 Rotterdam, Gelsenkirchen, DE /ID# 241819 Gelsenkirchen Germany 45897
    33 Gemeinschaftspraxis Rietkoetter und Jablonka /ID# 241821 Gelsenkirchen Germany 45899
    34 Praxis Dr. Lange /ID# 241829 Gera Germany 07548
    35 Loth, Gernsbach, DE /ID# 241828 Gernsbach Germany 76593
    36 Hautarztpraxis Dr. Budihardja /ID# 241851 Gießen Germany 35392
    37 Brinkmann & Partner, Gladbeck, /ID# 241850 Gladbeck Germany 45964
    38 Herrmann, Greifswald, DE /ID# 241889 Greifswald Germany 17489
    39 Dermatologikum Hamburg GmbH /ID# 245431 Hamburg Germany 20354
    40 Hautarztpraxis Luetten/Sack /ID# 241534 Hamburg Germany 21109
    41 MVZ Prof. Dr. Ockenfels Haut- und Allergie-Praxisklinik GmbH /ID# 245395 Hanau Germany 63450
    42 Praxis Dres. Kaspari /Schenck /ID# 241688 Hannover Germany 30159
    43 Zentrum fuer Rheumatologie und Schmerzmedizin /ID# 244326 Hanover Germany 30159
    44 Gemeinschaftspraxis Dres. Anika Hünermund/Mario Pawlak /ID# 241908 Heilbad Heiligenstadt Germany 37308
    45 Praxis Dres. Bischoff/Danz /ID# 241852 Ilmenau Germany 98693
    46 Stockmeier, Ingoldstadt, DE /ID# 248877 Ingolstadt Germany 85049
    47 Hautarztpraxis Weidgang /ID# 248850 Juelich Germany 52428
    48 Derma Sana /ID# 241854 Karlsruhe Germany 76133
    49 Dermatologische Praxis Kempen /ID# 248852 Kempen Germany 47906
    50 Grossmann, Koblenz, DE /ID# 242992 Koblenz Germany 56068
    51 Dres. Jacobs & Kollegen /ID# 241989 Kulmbach Germany 95326
    52 Praxis Dr. Schwarz /ID# 242279 Langenau Germany 89129
    53 Praxis Dres. Wiemers/Wiemers /ID# 241602 Leipzig Germany 04317
    54 Haut- und Allergie-Zentrum Lippstadt /ID# 241929 Lippstadt Germany 59557
    55 Hagemeier, Loehne, DE /ID# 241886 Loehne Germany 32584
    56 Magdeburger Company for Medical Studies & Services GmbH /ID# 248849 Magdeburg Germany 39104
    57 Dermatologie Quist - BAG Dres. Quist PartG /ID# 243325 Mainz Germany 55128
    58 Beldio Research GmbH /ID# 245830 Memmingen Germany 87700
    59 HMS GmbH Zimmer /ID# 241657 Merzig Germany 66663
    60 Hautzentrum am Marienplatz /ID# 248847 Munich Germany 80331
    61 Quack, Munich, DE /ID# 241536 Munich Germany 81539
    62 Dr. Gißler-Walter /ID# 248876 Mutterstadt Germany 67112
    63 Dermatologie Moelln Praxis Dr. Bodo Segert /ID# 242280 Mölln Germany 23879
    64 ZENTderma /ID# 241539 Mönchengladbach Germany 41061
    65 MediCorium Zentrum fuer Dermatologie und Aesthetik /ID# 243328 Oberursel Germany 61440
    66 Hockmann, Oelde, DE /ID# 241906 Oelde Germany 59302
    67 Praxis Dr. Behnke /ID# 248870 Panketal Germany 16341
    68 Baumann & Lang, Plauen, DE /ID# 244325 Plauen Germany 08523
    69 Praxis Dr. Asadullah /ID# 243944 Potsdam Germany 14467
    70 Kramer/Mortazawi, Remscheid /ID# 241824 Remscheid Germany 42897
    71 Praxis Dr. Fränken /ID# 241853 Schwelm Germany 58332
    72 Haut- und Laserzentrum Hunsrück /ID# 243882 Simmern Germany 55469
    73 Karl, Soest, DE /ID# 241909 Soest Germany 59494
    74 Gemeinschaftspraxis fur Dermatologie /ID# 245831 Stadtroda Germany 07646
    75 Praxis Dr. Termeer /ID# 241662 Stuttgart Germany 70499
    76 Barnikol, Waltershausen, DE /ID# 241844 Waltershausen Germany 99880
    77 Praxis Dehmel / Brand-Opitzer /ID# 243884 Wasserburg A. Inn Germany 83512
    78 Dr. Barbara Kempkes, Werne /ID# 241910 Werne Germany 59368
    79 Hautarztpraxis Dr. med. Matthias Hoffmann /ID# 241907 Witten Germany 58453
    80 Albrecht, Wurzen, DE /ID# 241988 Wurzen Germany 04808

    Sponsors and Collaborators

    • AbbVie

    Investigators

    • Study Director: ABBVIE INC., AbbVie

    Study Documents (Full-Text)

    None provided.

    More Information

    Additional Information:

    Publications

    None provided.
    Responsible Party:
    AbbVie
    ClinicalTrials.gov Identifier:
    NCT05139836
    Other Study ID Numbers:
    • P21-705
    First Posted:
    Dec 1, 2021
    Last Update Posted:
    Jul 26, 2022
    Last Verified:
    Jul 1, 2022
    Individual Participant Data (IPD) Sharing Statement:
    Undecided
    Plan to Share IPD:
    Undecided
    Studies a U.S. FDA-regulated Drug Product:
    No
    Studies a U.S. FDA-regulated Device Product:
    No
    Product Manufactured in and Exported from the U.S.:
    No
    Keywords provided by AbbVie
    Atopic Dermatitis (AD)
    Upadacitinib
    RINVOQ
    Additional relevant MeSH terms:
    Dermatitis, Atopic
    Dermatitis
    Eczema

    Study Results

    No Results Posted as of Jul 26, 2022