Back to resultsAn International, Multi-centre, Prospective, Non-controlled, Open, Single-group, 8-week Trial in Adolescent Subjects
Primary Purpose
Psoriasis Vulgaris
Status
Completed
Phase
Phase 2
Locations
International
Study Type
Interventional
Intervention
LEO 80185 gel
Sponsored by
About this trial
This is an interventional treatment trial for Psoriasis Vulgaris
Eligibility Criteria
Inclusion Criteria (all subjects):
- Clinical signs of psoriasis vulgaris on both the scalp and body (trunk and/or limbs)
At SV2 and Visit 1, a clinical diagnosis of scalp and body (trunk and/or limbs) psoriasis which is:
- of an extent of 10 to 35% of the body surface area (excluding psoriatic lesions of the face and sensitive areas. Sensitive areas include armpits, groin, under the breasts and in other skin folds around the genitals and buttocks), and
- of at least moderate severity according to the investigator's global assessment of disease severity on the body.
- A serum albumin-corrected calcium level below the upper reference limit at SV2
Inclusion Criteria (for subjects performing HPA axis assessments):
At SV2 and Visit 1, a clinical diagnosis of scalp psoriasis which is:
- more than or equal to 20% of the scalp area, and
- of at least moderate severity according to the investigator's global assessment of disease severity on the scalp.
- Subjects with a normal HPA axis function at SV2 including serum cortisol concentration above 5 mcg/dl before ACTH challenge and serum cortisol concentration above 18 mcg/dl 30 minutes after ACTH challenge.
Inclusion Criteria (for subjects not performing HPA axis assessments):
At SV2 and Visit 1, a clinical diagnosis of scalp psoriasis which is:
- more than or equal to 10% of the scalp area, and
- of at least moderate severity according to the investigator's global assessment of disease severity on the scalp.
Exclusion Criteria (all subjects):
Systemic treatment with biological therapies (marketed or not marketed), with a possible effect on scalp and/or body psoriasis within the following time period prior to Visit 1 and during the trial:
- etanercept - within 4 weeks prior to Visit 1
- adalimumab, infliximab - within 2 months prior to Visit 1
- ustekinumab - within 4 months prior to Visit 1
- experimental products - within 4 weeks/5 half-lives (whichever is longer) prior to Visit 1
- Systemic treatment with therapies other than biologicals, with a possible effect on scalp and/or body psoriasis (e.g., retinoids, immunosuppressants, PUVA) within 4 weeks prior to Visit 1 (Day 0) or during the trial.
- UVB therapy within 2 weeks prior to Visit 1 or during the trial.
- Any topical treatment on the scalp and body (except for emollients and non-steroid medicated shampoos) within 2 weeks prior to Visit 1 or during the trial.
- Systemic calcium, vitamin D supplements, antacids, diuretics, antiepileptics, diphosphonates or calcitonin within 4 weeks prior to SV2 or during the trial.
- Planned initiation of, or changes to, concomitant medication that could affect psoriasis (e.g., betablockers, chloroquine, lithium, ACE inhibitors) during the trial.
- Current diagnosis of guttate, erythrodermic, exfoliative or pustular psoriasis.
- Subjects with any of the following conditions present on the treatment areas on scalp and/or body: viral (e.g., herpes or varicella) lesions of the skin, fungal and bacterial skin infections, parasitic infections, skin manifestations in relation to syphilis or tuberculosis, rosacea, acne vulgaris, acne rosacea, atrophic skin, striae atrophicae, fragility of skin veins, ichthyosis, ulcers and wounds.
- Other inflammatory skin diseases that may confound the evaluation of scalp and/or body psoriasis.
- Planned excessive exposure to sun during the trial that may affect scalp and/or body psoriasis.
- Known or suspected severe renal insufficiency or severe hepatic disorders.
- Known or suspected disorders of calcium metabolism associated with hypercalcaemia.
- Any clinically significant abnormality following review of screening laboratory tests (blood and urine samples), physical examination or blood pressure/heart rate measurement performed at SV2.
- Current participation in any other interventional clinical trial.
- Previously enrolled in this trial.
- Subjects who have received treatment with any non-marketed drug substance (i.e., an agent which has not yet been made available for clinical use following registration) within a month prior to SV1 or longer, if the class of substance required a longer wash-out as defined above (e.g., biological treatments).
- Subjects or parent(s) or legal guardian known or suspected of being unlikely to comply with the Clinical Trial Protocol (e.g., alcoholism, drug dependency or psychotic state).
- Females who are pregnant, or of child-bearing potential and wishing to become pregnant during the trial, or who are breast-feeding.
- Females of child-bearing potential with positive pregnancy test at SV2.
- Subject (or their partner) not using an adequate method of contraception according to national requirements.
Exclusion Criteria (for subjects performing HPA axis assessments)
- A history of serious allergy, allergic asthma or serious allergic skin rash.
- Known or suspected hypersensitivity to any component of CORTROSYN® (including ACTH/cosyntropin/tetracosactide)
- Systemic treatment with corticosteroids (including inhaled and nasal steroids) within 12 weeks prior to SV2 or during the trial.
- Topical treatment with corticosteroids within 2 weeks prior to SV2 or during the trial.
- Oestrogen therapy (including contraceptives) or any other medication known to affect cortisol levels levels or HPA axis integrity within 4 weeks prior to SV2 or during the trial.
- Enzymatic inductors (e.g., barbiturates, phenytoin, rifampicin) within 4 weeks prior to SV2 or during the trial.
- Systemic or topical cytochrome P450 inhibitors (e.g., ketoconazole, itraconazole, metronidazole) within 4 weeks prior to SV2 or during the trial. Topical ketoconazole 2 weeks prior to SV2.
- Hypoglycemic sulfonamides within 4 weeks prior to SV2 or during the trial.
- Antidepressive medications within 4 weeks prior to SV2 or during the trial.
- Known or suspected endocrine disorder that may affect the results of the ACTH challenge test.
- Clinical signs or symptoms of Cushing's disease or Addison's disease.
- Subjects with diabetes mellitus.
- Known or suspected cardiac condition.
- Not following nocturnal sleep patterns.
Sites / Locations
- Rady's Children Hospital
- Clinical Research Center, Morsani Center for Advanced Healthcare
- Indiana University
- Skin Specialists, PC
- St. Luke's Roosevelt Hospital
- Clinical Partners
- Dermatology and Laser Center of Charleston, PA
- Clinical Trials of Texas, Inc.
- Winnipeg Clinic
- Adult, Pediatric and Laser Derma
- Lynderm Research Inc.
- Skin Centre for Dermatology
- CHU de Nice
- Cabinet Medical
- CHI de Cornouaille
- Charite Berlin
- Uniklinik Bonn
- Uniklinik Frankfurt
- Katholisches Kinderkrankenhaus
- Endo - Med. Centrum Medyczne Clinic
- NZOZ Med.-Laser Clinic
- Specjalistyczny Ofrodek Leczniczo Clinic
- Medycyna Kliniczna Clinic
- Derm Medica Sp.zo.o. Clinic
- Policlinica de Diagnostic Rapid S.A. Clinic
- Spitalul Clinic "Colentina"
- Spitalul Clinic Judetean de Urgenta Cluj-Napoca
- Cabinet Medical Individual Tatu G. Alin Laurentiu
- Iasiprest SRL Dermato-Venerology
- Spitalul Clinic Judetean Mures
- Spitalul Clinic Municipal de Urgenta Timisoara
- Manchester Royal Infirmary
- Monklands Hospital
- Whipps Cross University Hospital
- St. Woolos Hospital
Arms of the Study
Arm 1
Arm Type
Experimental
Arm Label
LEO 80185 gel
Arm Description
Outcomes
Primary Outcome Measures
Adverse Drug Reactions (ADRs)
Number of Adverse Drug Reactions (ADRs)
Subjects With Serum Cortisol Concentration of ≤18 mcg/dl at 30 Minutes After ACTH-challenge at Week 4
Number of subjects with serum cortisol concentration of ≤18 mcg/dl at 30 minutes after ACTH-challenge at Week 4
Subjects With Serum Cortisol Concentration of ≤18 mcg/dl at 30 Minutes After ACTH-challenge at Week 8
Number of subjects with serum cortisol concentration of ≤18 mcg/dl at 30 minutes after ACTH-challenge at Week 8
Change in Albumin-corrected Serum Calcium From Baseline to Week 4
Change in albumin-corrected serum calcium from baseline to Week 4
Change in Albumin-corrected Serum Calcium From Baseline to Week 8
Change in albumin-corrected serum calcium from baseline to Week 8
Change in Albumin-corrected Serum Calcium From Baseline to End of Treatment
Change in albumin-corrected serum calcium from baseline to end of treatment, defined as the last value recorded after baseline up to and including Week 8.
Change in 24-hour Urinary Calcium Excretion From Baseline to Week 4
Change in 24-hour urinary calcium excretion from baseline to Week 4
Change in 24-hour Urinary Calcium Excretion From Baseline to Week 8
Change in 24-hour urinary calcium excretion from baseline to Week 8
Change in 24-hour Urinary Calcium Excretion From Baseline to End of Treatment
Change in 24-hour urinary calcium excretion from baseline to end of treatment, defined as the last value recorded after baseline up to and including Week 8.
Secondary Outcome Measures
Adverse Events (AEs)
Number of Adverse Events (AEs)
Subjects With Serum Cortisol Concentration of ≤18 mcg/dl at Both 30 and 60 Minutes After ACTH-challenge at Week 4
Number of subjects with serum cortisol concentration of ≤18 mcg/dl at both 30 and 60 minutes after ACTH-challenge at Week 4
Subjects With Serum Cortisol Concentration of ≤18 mcg/dl at Both 30 and 60 Minutes After ACTH-challenge at Week 8
Number of subjects with serum cortisol concentration of ≤18 mcg/dl at both 30 and 60 minutes after ACTH-challenge at Week 8
Change in Urinary Calcium:Creatinine Ratio From Baseline to Week 4
Change in urinary calcium:creatinine ratio from baseline to Week 4
Change in Urinary Calcium:Creatinine Ratio From Baseline to Week 8
Change in urinary calcium:creatinine ratio from baseline to Week 8
Change in Serum Alkaline Phosphatase From Baseline to Week 4
Change in serum alkaline phosphatase from baseline to Week 4
Change in Serum Alkaline Phosphatase From Baseline to Week 8
Change in serum alkaline phosphatase from baseline to Week 8
Pharmacokinetic Evaluation AUC(0-t)
AUC(0-t) values for betamethasone dipropionate, betamethasone 17-propionate, calcipotriol, and MC1080. Betamethasone dipropionate was only detected above lower limit of quantification in 5 samples from 4 subjects, and no subjects had enough positive samples to allow calculation AUC(0-t) for betamethasone dipropionate. Betamethasone 17-propionate was only detected in 12 samples from 5 subjects, and only 2 subjects had enough positive samples to calculate AUC(0-t). The mean value of AUC(0-t) for these 2 subjects is presented for betamethasone 17-propionate. Calcipotriol and MC1080 were never detected above lower limit of quantification, therefore no PK parameters could be calculated and no data have been entered for calcipotriol and MC1080.
Pharmacokinetic Evaluation AUC(0-infinity)
AUC(0-infinity) values for betamethasone dipropionate, betamethasone 17-propionate, calcipotriol, and MC1080. Betamethasone dipropionate was only detected above lower limit of quantification in 5 samples from 4 subjects, and no subjects had enough positive samples to allow calculation AUC(0-infinity) for betamethasone dipropionate. Betamethasone 17-propionate was only detected in 12 samples from 5 subjects, and only 2 subjects had enough positive samples to calculate AUC(0-infinity). The mean value of AUC(0-infinity) for these 2 subjects is presented for betamethasone 17-propionate. Calcipotriol and MC1080 were never detected above lower limit of quantification, therefore no PK parameters could be calculated and no data have been entered for calcipotriol and MC1080.
The terms AUC(0-infinity) and AUC(all) are interchangeable, AUC(0-infinity) was used in the protocol whereas AUC(all) was used in the report. AUC(0-infinity) has been used here to be consistent with the protocol.
Pharmacokinetic Evaluation C(Max)
C(max) values for betamethasone dipropionate, betamethasone 17-propionate, calcipotriol, and MC1080. Betamethasone dipropionate was only detected above lower limit of quantification in 5 samples from 4 subjects and betamethasone 17-propionate was only detected in 12 samples from 5 subjects, therefore pharmacokinetic profiles could not be calculated. Presented C(max) values for betamethasone dipropionate and betamethasone 17-propionate are the the single highest concentrations measured in any sample at any time. Calcipotriol and MC1080 were never detected above lower limit of quantification, therefore no PK parameters could be calculated and no data have been entered for calcipotriol and MC1080.
Pharmacokinetic Evaluation T(Max)
T(max) values for betamethasone dipropionate, betamethasone 17-propionate, calcipotriol, and MC1080. Betamethasone dipropionate was only detected above lower limit of quantification in 5 samples from 4 subjects and betamethasone 17-propionate was only detected in 12 samples from 5 subjects. Therefore it was not possible to calculate T(max) for betamethasone dipropionate and betamethasone 17-propionate. Calcipotriol and MC1080 were never detected above lower limit of quantification, therefore no PK parameters could be calculated and no data have been entered for calcipotriol and MC1080.
Pharmacokinetic Evaluation T(½)
T(½) values for betamethasone dipropionate, betamethasone 17-propionate, calcipotriol, and MC1080. Betamethasone dipropionate was only detected above lower limit of quantification in 5 samples from 4 subjects and betamethasone 17-propionate was only detected in 12 samples from 5 subjects, therefore it was not possible to calculate T(½) for betamethasone dipropionate or betamethasone 17-propionate. Calcipotriol and MC1080 were never detected above lower limit of quantification, therefore no PK parameters could be calculated and no data have been entered for calcipotriol and MC1080.
Subjects With "Controlled Disease" According to the Investigator's Global Assessment of Disease Severity on the Body at End of Treatment
Subjects with "Controlled disease" (i.e., "Clear" or "Almost clear" for subjects with at least "Moderate" disease at baseline, "Clear" for subjects with "Mild" disease at baseline) according to the investigator's global assessment of disease severity on the body at end of treatment, defined as the last value recorded up to and including Week 8.
Percentage Change in PASI From Baseline to End of Treatment
Percentage change in Psoriasis area and severity index (PASI) score from baseline to end of treatment, defined as the last value recorded up to and including Week 8. Psoriasis area and severity index (PASI) assesses extent and severity of clinical signs of psoriasis vulgaris. Body surface is divided in 4 ares: head (incl. neck), arms (incl. hands), trunk (incl. flexures) and legs (incl. buttocks and feet). Each area is scored from 0-6 for extent of psoriasis and from 0-4 for redness, thickness, and scaliness, and an area PASI score is calculated. The total PASI score is calculated from each area's score. The PASI score ranges from 0 (clear skin) to 72 (maximum disease), a PASI score higher than 10 generally corresponds to moderate-to-severe disease.
Subjects With "Controlled Disease" According to the Patient's Global Assessment of Disease Severity on the Body at End of Treatment
Subjects with "Controlled disease" (i.e., "Clear" or "Almost clear" for subjects with at least "Moderate" disease at baseline, "Clear" for subjects with "Mild" disease at baseline) according to the patient's global assessment of disease severity on the body at end of treatment, defined as the last value recorded up to and including Week 8.
Full Information
1. Study Identification
Unique Protocol Identification Number
NCT02038569
Brief Title
An International, Multi-centre, Prospective, Non-controlled, Open, Single-group, 8-week Trial in Adolescent Subjects
Official Title
Effect of Calcipotriol Plus Betamethasone Dipropionate Gel on the HPA Axis and Calcium Metabolism in Adolescent Subjects (Aged 12 to 16 Years, 11 Months) With Scalp and Body Psoriasis
Study Type
Interventional
2. Study Status
Record Verification Date
October 2018
Overall Recruitment Status
Completed
Study Start Date
January 2014 (Actual)
Primary Completion Date
February 2018 (Actual)
Study Completion Date
February 13, 2018 (Actual)
3. Sponsor/Collaborators
Responsible Party, by Official Title
Sponsor
Name of the Sponsor
LEO Pharma
4. Oversight
Data Monitoring Committee
No
5. Study Description
Brief Summary
An international, multi-centre, prospective, non-controlled, open, single-group, 8-week trial in adolescent subjects (aged 12 to 16 years, 11 months) with scalp and body psoriasis.
Detailed Description
A phase 2 trial evaluating the safety and efficacy of once daily use of LEO 80185 gel containing calcipotriol 50 mcg/g plus betamethasone 0.5mg/g (as dipropionate) in adolescent subjects (aged 12 to 16 years, 11 months) with scalp and body psoriasis.
6. Conditions and Keywords
Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
Psoriasis Vulgaris
7. Study Design
Primary Purpose
Treatment
Study Phase
Phase 2
Interventional Study Model
Single Group Assignment
Masking
None (Open Label)
Allocation
N/A
Enrollment
125 (Actual)
8. Arms, Groups, and Interventions
Arm Title
LEO 80185 gel
Arm Type
Experimental
Intervention Type
Drug
Intervention Name(s)
LEO 80185 gel
Primary Outcome Measure Information:
Title
Adverse Drug Reactions (ADRs)
Description
Number of Adverse Drug Reactions (ADRs)
Time Frame
8 weeks
Title
Subjects With Serum Cortisol Concentration of ≤18 mcg/dl at 30 Minutes After ACTH-challenge at Week 4
Description
Number of subjects with serum cortisol concentration of ≤18 mcg/dl at 30 minutes after ACTH-challenge at Week 4
Time Frame
30 minutes after ACTH-challenge at Week 4
Title
Subjects With Serum Cortisol Concentration of ≤18 mcg/dl at 30 Minutes After ACTH-challenge at Week 8
Description
Number of subjects with serum cortisol concentration of ≤18 mcg/dl at 30 minutes after ACTH-challenge at Week 8
Time Frame
30 minutes after ACTH-challenge at Week 8
Title
Change in Albumin-corrected Serum Calcium From Baseline to Week 4
Description
Change in albumin-corrected serum calcium from baseline to Week 4
Time Frame
From baseline to Week 4
Title
Change in Albumin-corrected Serum Calcium From Baseline to Week 8
Description
Change in albumin-corrected serum calcium from baseline to Week 8
Time Frame
From baseline to Week 8
Title
Change in Albumin-corrected Serum Calcium From Baseline to End of Treatment
Description
Change in albumin-corrected serum calcium from baseline to end of treatment, defined as the last value recorded after baseline up to and including Week 8.
Time Frame
From baseline to end of treatment
Title
Change in 24-hour Urinary Calcium Excretion From Baseline to Week 4
Description
Change in 24-hour urinary calcium excretion from baseline to Week 4
Time Frame
From baseline to Week 4
Title
Change in 24-hour Urinary Calcium Excretion From Baseline to Week 8
Description
Change in 24-hour urinary calcium excretion from baseline to Week 8
Time Frame
From baseline to Week 8
Title
Change in 24-hour Urinary Calcium Excretion From Baseline to End of Treatment
Description
Change in 24-hour urinary calcium excretion from baseline to end of treatment, defined as the last value recorded after baseline up to and including Week 8.
Time Frame
From baseline to end of treatment
Secondary Outcome Measure Information:
Title
Adverse Events (AEs)
Description
Number of Adverse Events (AEs)
Time Frame
8 weeks
Title
Subjects With Serum Cortisol Concentration of ≤18 mcg/dl at Both 30 and 60 Minutes After ACTH-challenge at Week 4
Description
Number of subjects with serum cortisol concentration of ≤18 mcg/dl at both 30 and 60 minutes after ACTH-challenge at Week 4
Time Frame
30 and 60 minutes after ACTH-challenge at Week 4
Title
Subjects With Serum Cortisol Concentration of ≤18 mcg/dl at Both 30 and 60 Minutes After ACTH-challenge at Week 8
Description
Number of subjects with serum cortisol concentration of ≤18 mcg/dl at both 30 and 60 minutes after ACTH-challenge at Week 8
Time Frame
30 and 60 minutes after ACTH-challenge at Week 8
Title
Change in Urinary Calcium:Creatinine Ratio From Baseline to Week 4
Description
Change in urinary calcium:creatinine ratio from baseline to Week 4
Time Frame
From baseline to Week 4
Title
Change in Urinary Calcium:Creatinine Ratio From Baseline to Week 8
Description
Change in urinary calcium:creatinine ratio from baseline to Week 8
Time Frame
From baseline to Week 8
Title
Change in Serum Alkaline Phosphatase From Baseline to Week 4
Description
Change in serum alkaline phosphatase from baseline to Week 4
Time Frame
From baseline to Week 4
Title
Change in Serum Alkaline Phosphatase From Baseline to Week 8
Description
Change in serum alkaline phosphatase from baseline to Week 8
Time Frame
From baseline to Week 8
Title
Pharmacokinetic Evaluation AUC(0-t)
Description
AUC(0-t) values for betamethasone dipropionate, betamethasone 17-propionate, calcipotriol, and MC1080. Betamethasone dipropionate was only detected above lower limit of quantification in 5 samples from 4 subjects, and no subjects had enough positive samples to allow calculation AUC(0-t) for betamethasone dipropionate. Betamethasone 17-propionate was only detected in 12 samples from 5 subjects, and only 2 subjects had enough positive samples to calculate AUC(0-t). The mean value of AUC(0-t) for these 2 subjects is presented for betamethasone 17-propionate. Calcipotriol and MC1080 were never detected above lower limit of quantification, therefore no PK parameters could be calculated and no data have been entered for calcipotriol and MC1080.
Time Frame
Week 4, blood samples taken before IMP was applied and 1, 3, and 5 hours after application of IMP
Title
Pharmacokinetic Evaluation AUC(0-infinity)
Description
AUC(0-infinity) values for betamethasone dipropionate, betamethasone 17-propionate, calcipotriol, and MC1080. Betamethasone dipropionate was only detected above lower limit of quantification in 5 samples from 4 subjects, and no subjects had enough positive samples to allow calculation AUC(0-infinity) for betamethasone dipropionate. Betamethasone 17-propionate was only detected in 12 samples from 5 subjects, and only 2 subjects had enough positive samples to calculate AUC(0-infinity). The mean value of AUC(0-infinity) for these 2 subjects is presented for betamethasone 17-propionate. Calcipotriol and MC1080 were never detected above lower limit of quantification, therefore no PK parameters could be calculated and no data have been entered for calcipotriol and MC1080.
The terms AUC(0-infinity) and AUC(all) are interchangeable, AUC(0-infinity) was used in the protocol whereas AUC(all) was used in the report. AUC(0-infinity) has been used here to be consistent with the protocol.
Time Frame
Week 4, blood samples taken before IMP was applied and 1, 3, and 5 hours after application of IMP
Title
Pharmacokinetic Evaluation C(Max)
Description
C(max) values for betamethasone dipropionate, betamethasone 17-propionate, calcipotriol, and MC1080. Betamethasone dipropionate was only detected above lower limit of quantification in 5 samples from 4 subjects and betamethasone 17-propionate was only detected in 12 samples from 5 subjects, therefore pharmacokinetic profiles could not be calculated. Presented C(max) values for betamethasone dipropionate and betamethasone 17-propionate are the the single highest concentrations measured in any sample at any time. Calcipotriol and MC1080 were never detected above lower limit of quantification, therefore no PK parameters could be calculated and no data have been entered for calcipotriol and MC1080.
Time Frame
Week 4, blood samples taken before IMP was applied and 1, 3, and 5 hours after application of IMP
Title
Pharmacokinetic Evaluation T(Max)
Description
T(max) values for betamethasone dipropionate, betamethasone 17-propionate, calcipotriol, and MC1080. Betamethasone dipropionate was only detected above lower limit of quantification in 5 samples from 4 subjects and betamethasone 17-propionate was only detected in 12 samples from 5 subjects. Therefore it was not possible to calculate T(max) for betamethasone dipropionate and betamethasone 17-propionate. Calcipotriol and MC1080 were never detected above lower limit of quantification, therefore no PK parameters could be calculated and no data have been entered for calcipotriol and MC1080.
Time Frame
Week 4, blood samples taken before IMP was applied and 1, 3, and 5 hours after application of IMP
Title
Pharmacokinetic Evaluation T(½)
Description
T(½) values for betamethasone dipropionate, betamethasone 17-propionate, calcipotriol, and MC1080. Betamethasone dipropionate was only detected above lower limit of quantification in 5 samples from 4 subjects and betamethasone 17-propionate was only detected in 12 samples from 5 subjects, therefore it was not possible to calculate T(½) for betamethasone dipropionate or betamethasone 17-propionate. Calcipotriol and MC1080 were never detected above lower limit of quantification, therefore no PK parameters could be calculated and no data have been entered for calcipotriol and MC1080.
Time Frame
Week 4, blood samples taken before IMP was applied and 1, 3, and 5 hours after application of IMP
Title
Subjects With "Controlled Disease" According to the Investigator's Global Assessment of Disease Severity on the Body at End of Treatment
Description
Subjects with "Controlled disease" (i.e., "Clear" or "Almost clear" for subjects with at least "Moderate" disease at baseline, "Clear" for subjects with "Mild" disease at baseline) according to the investigator's global assessment of disease severity on the body at end of treatment, defined as the last value recorded up to and including Week 8.
Time Frame
End of treatment
Title
Percentage Change in PASI From Baseline to End of Treatment
Description
Percentage change in Psoriasis area and severity index (PASI) score from baseline to end of treatment, defined as the last value recorded up to and including Week 8. Psoriasis area and severity index (PASI) assesses extent and severity of clinical signs of psoriasis vulgaris. Body surface is divided in 4 ares: head (incl. neck), arms (incl. hands), trunk (incl. flexures) and legs (incl. buttocks and feet). Each area is scored from 0-6 for extent of psoriasis and from 0-4 for redness, thickness, and scaliness, and an area PASI score is calculated. The total PASI score is calculated from each area's score. The PASI score ranges from 0 (clear skin) to 72 (maximum disease), a PASI score higher than 10 generally corresponds to moderate-to-severe disease.
Time Frame
From baseline to end of treatment
Title
Subjects With "Controlled Disease" According to the Patient's Global Assessment of Disease Severity on the Body at End of Treatment
Description
Subjects with "Controlled disease" (i.e., "Clear" or "Almost clear" for subjects with at least "Moderate" disease at baseline, "Clear" for subjects with "Mild" disease at baseline) according to the patient's global assessment of disease severity on the body at end of treatment, defined as the last value recorded up to and including Week 8.
Time Frame
End of treatment
10. Eligibility
Sex
All
Minimum Age & Unit of Time
12 Years
Maximum Age & Unit of Time
17 Years
Accepts Healthy Volunteers
No
Eligibility Criteria
Inclusion Criteria (all subjects):
Clinical signs of psoriasis vulgaris on both the scalp and body (trunk and/or limbs)
At SV2 and Visit 1, a clinical diagnosis of scalp and body (trunk and/or limbs) psoriasis which is:
of an extent of 10 to 35% of the body surface area (excluding psoriatic lesions of the face and sensitive areas. Sensitive areas include armpits, groin, under the breasts and in other skin folds around the genitals and buttocks), and
of at least moderate severity according to the investigator's global assessment of disease severity on the body.
A serum albumin-corrected calcium level below the upper reference limit at SV2
Inclusion Criteria (for subjects performing HPA axis assessments):
At SV2 and Visit 1, a clinical diagnosis of scalp psoriasis which is:
more than or equal to 20% of the scalp area, and
of at least moderate severity according to the investigator's global assessment of disease severity on the scalp.
Subjects with a normal HPA axis function at SV2 including serum cortisol concentration above 5 mcg/dl before ACTH challenge and serum cortisol concentration above 18 mcg/dl 30 minutes after ACTH challenge.
Inclusion Criteria (for subjects not performing HPA axis assessments):
At SV2 and Visit 1, a clinical diagnosis of scalp psoriasis which is:
more than or equal to 10% of the scalp area, and
of at least moderate severity according to the investigator's global assessment of disease severity on the scalp.
Exclusion Criteria (all subjects):
Systemic treatment with biological therapies (marketed or not marketed), with a possible effect on scalp and/or body psoriasis within the following time period prior to Visit 1 and during the trial:
etanercept - within 4 weeks prior to Visit 1
adalimumab, infliximab - within 2 months prior to Visit 1
ustekinumab - within 4 months prior to Visit 1
experimental products - within 4 weeks/5 half-lives (whichever is longer) prior to Visit 1
Systemic treatment with therapies other than biologicals, with a possible effect on scalp and/or body psoriasis (e.g., retinoids, immunosuppressants, PUVA) within 4 weeks prior to Visit 1 (Day 0) or during the trial.
UVB therapy within 2 weeks prior to Visit 1 or during the trial.
Any topical treatment on the scalp and body (except for emollients and non-steroid medicated shampoos) within 2 weeks prior to Visit 1 or during the trial.
Systemic calcium, vitamin D supplements, antacids, diuretics, antiepileptics, diphosphonates or calcitonin within 4 weeks prior to SV2 or during the trial.
Planned initiation of, or changes to, concomitant medication that could affect psoriasis (e.g., betablockers, chloroquine, lithium, ACE inhibitors) during the trial.
Current diagnosis of guttate, erythrodermic, exfoliative or pustular psoriasis.
Subjects with any of the following conditions present on the treatment areas on scalp and/or body: viral (e.g., herpes or varicella) lesions of the skin, fungal and bacterial skin infections, parasitic infections, skin manifestations in relation to syphilis or tuberculosis, rosacea, acne vulgaris, acne rosacea, atrophic skin, striae atrophicae, fragility of skin veins, ichthyosis, ulcers and wounds.
Other inflammatory skin diseases that may confound the evaluation of scalp and/or body psoriasis.
Planned excessive exposure to sun during the trial that may affect scalp and/or body psoriasis.
Known or suspected severe renal insufficiency or severe hepatic disorders.
Known or suspected disorders of calcium metabolism associated with hypercalcaemia.
Any clinically significant abnormality following review of screening laboratory tests (blood and urine samples), physical examination or blood pressure/heart rate measurement performed at SV2.
Current participation in any other interventional clinical trial.
Previously enrolled in this trial.
Subjects who have received treatment with any non-marketed drug substance (i.e., an agent which has not yet been made available for clinical use following registration) within a month prior to SV1 or longer, if the class of substance required a longer wash-out as defined above (e.g., biological treatments).
Subjects or parent(s) or legal guardian known or suspected of being unlikely to comply with the Clinical Trial Protocol (e.g., alcoholism, drug dependency or psychotic state).
Females who are pregnant, or of child-bearing potential and wishing to become pregnant during the trial, or who are breast-feeding.
Females of child-bearing potential with positive pregnancy test at SV2.
Subject (or their partner) not using an adequate method of contraception according to national requirements.
Exclusion Criteria (for subjects performing HPA axis assessments)
A history of serious allergy, allergic asthma or serious allergic skin rash.
Known or suspected hypersensitivity to any component of CORTROSYN® (including ACTH/cosyntropin/tetracosactide)
Systemic treatment with corticosteroids (including inhaled and nasal steroids) within 12 weeks prior to SV2 or during the trial.
Topical treatment with corticosteroids within 2 weeks prior to SV2 or during the trial.
Oestrogen therapy (including contraceptives) or any other medication known to affect cortisol levels levels or HPA axis integrity within 4 weeks prior to SV2 or during the trial.
Enzymatic inductors (e.g., barbiturates, phenytoin, rifampicin) within 4 weeks prior to SV2 or during the trial.
Systemic or topical cytochrome P450 inhibitors (e.g., ketoconazole, itraconazole, metronidazole) within 4 weeks prior to SV2 or during the trial. Topical ketoconazole 2 weeks prior to SV2.
Hypoglycemic sulfonamides within 4 weeks prior to SV2 or during the trial.
Antidepressive medications within 4 weeks prior to SV2 or during the trial.
Known or suspected endocrine disorder that may affect the results of the ACTH challenge test.
Clinical signs or symptoms of Cushing's disease or Addison's disease.
Subjects with diabetes mellitus.
Known or suspected cardiac condition.
Not following nocturnal sleep patterns.
Overall Study Officials:
First Name & Middle Initial & Last Name & Degree
Lawrence Eichenfield, MD
Organizational Affiliation
Rady Chilidren's Hospital
Official's Role
Principal Investigator
Facility Information:
Facility Name
Rady's Children Hospital
City
San Diego
State/Province
California
ZIP/Postal Code
92132
Country
United States
Facility Name
Clinical Research Center, Morsani Center for Advanced Healthcare
City
Tampa
State/Province
Florida
ZIP/Postal Code
33612
Country
United States
Facility Name
Indiana University
City
Indianapolis
State/Province
Indiana
ZIP/Postal Code
46202
Country
United States
Facility Name
Skin Specialists, PC
City
Omaha
State/Province
Nebraska
ZIP/Postal Code
68144
Country
United States
Facility Name
St. Luke's Roosevelt Hospital
City
Forest Hills
State/Province
New York
ZIP/Postal Code
10025
Country
United States
Facility Name
Clinical Partners
City
Johnston
State/Province
Rhode Island
ZIP/Postal Code
12095
Country
United States
Facility Name
Dermatology and Laser Center of Charleston, PA
City
Charleston
State/Province
South Carolina
ZIP/Postal Code
29407
Country
United States
Facility Name
Clinical Trials of Texas, Inc.
City
San Antonio
State/Province
Texas
ZIP/Postal Code
78229
Country
United States
Facility Name
Winnipeg Clinic
City
Winnipeg
State/Province
Manitoba
ZIP/Postal Code
R3C 0N2
Country
Canada
Facility Name
Adult, Pediatric and Laser Derma
City
St-John's
State/Province
Newfoundland and Labrador
ZIP/Postal Code
A1A 4Y3
Country
Canada
Facility Name
Lynderm Research Inc.
City
Markham
State/Province
Ontario
ZIP/Postal Code
L3P 1A8
Country
Canada
Facility Name
Skin Centre for Dermatology
City
Peterborough
State/Province
Ontario
ZIP/Postal Code
K9J 1Z2
Country
Canada
Facility Name
CHU de Nice
City
Nice
State/Province
Alpe-Maritimes
ZIP/Postal Code
06202
Country
France
Facility Name
Cabinet Medical
City
Martigues
State/Province
Bouches-du-Rhône
ZIP/Postal Code
13500
Country
France
Facility Name
CHI de Cornouaille
City
Quimper
State/Province
Finistère
ZIP/Postal Code
29107
Country
France
Facility Name
Charite Berlin
City
Berlin
ZIP/Postal Code
10117
Country
Germany
Facility Name
Uniklinik Bonn
City
Bonn
ZIP/Postal Code
53127
Country
Germany
Facility Name
Uniklinik Frankfurt
City
Frankfurt am Main
ZIP/Postal Code
60590
Country
Germany
Facility Name
Katholisches Kinderkrankenhaus
City
Hamburg
ZIP/Postal Code
22149
Country
Germany
Facility Name
Endo - Med. Centrum Medyczne Clinic
City
Karczew
ZIP/Postal Code
05-480
Country
Poland
Facility Name
NZOZ Med.-Laser Clinic
City
Lublin
ZIP/Postal Code
20-146
Country
Poland
Facility Name
Specjalistyczny Ofrodek Leczniczo Clinic
City
Ostróda
ZIP/Postal Code
14-100
Country
Poland
Facility Name
Medycyna Kliniczna Clinic
City
Warszawa
ZIP/Postal Code
00-660
Country
Poland
Facility Name
Derm Medica Sp.zo.o. Clinic
City
Wrocław
ZIP/Postal Code
51-318
Country
Poland
Facility Name
Policlinica de Diagnostic Rapid S.A. Clinic
City
Brasov
ZIP/Postal Code
500152
Country
Romania
Facility Name
Spitalul Clinic "Colentina"
City
Bucharest
ZIP/Postal Code
20125
Country
Romania
Facility Name
Spitalul Clinic Judetean de Urgenta Cluj-Napoca
City
Cluj-Napoca
ZIP/Postal Code
400006
Country
Romania
Facility Name
Cabinet Medical Individual Tatu G. Alin Laurentiu
City
Galati
ZIP/Postal Code
800101
Country
Romania
Facility Name
Iasiprest SRL Dermato-Venerology
City
Iasi
ZIP/Postal Code
700381
Country
Romania
Facility Name
Spitalul Clinic Judetean Mures
City
Targu-Mures
ZIP/Postal Code
800373
Country
Romania
Facility Name
Spitalul Clinic Municipal de Urgenta Timisoara
City
Timisoara
ZIP/Postal Code
300077
Country
Romania
Facility Name
Manchester Royal Infirmary
City
Manchester
State/Province
Greater Manchester
ZIP/Postal Code
M13 9WL
Country
United Kingdom
Facility Name
Monklands Hospital
City
Airdrie
State/Province
Lanarkshire
ZIP/Postal Code
ML6 OJ5
Country
United Kingdom
Facility Name
Whipps Cross University Hospital
City
Leytonstone
State/Province
London
ZIP/Postal Code
E11 1NR
Country
United Kingdom
Facility Name
St. Woolos Hospital
City
Stow Hill, Newport
State/Province
Monmouthshire
ZIP/Postal Code
NP20 4SZ
Country
United Kingdom
12. IPD Sharing Statement
Learn more about this trial
An International, Multi-centre, Prospective, Non-controlled, Open, Single-group, 8-week Trial in Adolescent Subjects
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