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A Phase 2 Maximal Use Systemic Exposure (MUSE) study evaluating the safety and efficacy of LEO 90100 used once daily in subjects with extensive psoriasis vulgaris.
The purpose of the present study is to assess the systemic safety of LEO 90100. Although LEO 90100 contains the same active ingredients in the same concentration as DAIVOBET/DOVOBET/TACLONEX ointment, the degree of absorption of the active ingredients from the new formulation may differ. Systemic safety will be assessed through the effect of LEO 90100 on calcium metabolism and HPA axis function under maximum use conditions (i.e., in subjects with very extensive psoriasis on the trunk, limbs and scalp, using up to 120g per week of LEO 90100 for up to 4 weeks). Data from this study, together with the measurements of albumin-corrected serum calcium and the calcium:creatinine ratio in spot urine samples in the planned phase 2 and 3 studies in the development program for LEO 90100, are expected to provide adequate information with respect to the systemic safety of LEO 90100.
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| Label | Type | Description | Intervention Names |
|---|---|---|---|
| LEO 90100 | Experimental |
|
| Name | Type | Description | Arm Group Labels | Other Names |
|---|---|---|---|---|
| LEO 90100 | Drug | Calcipotriol 50 mcg/g (as hydrate) and betamethasone 0.5 mg/g (as dipropionate) |
|
| Measure | Description | Time Frame |
|---|---|---|
| Subjects With Serum Cortisol Concentration of ≤18 mcg/dl at 30 Minutes After Adrenocorticotrophic Hormone-challenge (ACTH-challenge) | HPA-axis testing by means of the rapid standard-dose cosyntropin test (ACTH-challenge test) for detection of adrenal suppression. | Day 28 |
| Change in Albumin-corrected Serum Calcium From Baseline to Day 28 | The effect of LEO 90100 on calcium metabolism was evaluated based on change in albumin-corrected serum calcium from Baseline to Day 28. | Baseline and Day 28 |
| Change in 24-hour Urinary Calcium Excretion From Baseline to Day 28 | The effect of LEO 90100 on calcium metabolism was evaluated based on change in 24-hour urinary calcium excretion from Baseline to Day 28 in 24-hour. | Baseline and Day 28 |
| Change in 24-hour Urinary Calcium:Creatinine Ratio From Baseline to Day 28 | The effect of LEO 90100 on calcium metabolism was evaluated based on change in urinary calcium:creatinine ratio from Baseline to Day 28. | Baseline and Day 28 |
| Measure | Description | Time Frame |
|---|---|---|
| Number of Subjects With Serum Cortisol Concentration of ≤18 mcg/dl at 30 and 60 Minutes After ACTH-challenge at Day 28 | Serum cortisol concentrations at 30 and 60 minutes after injection were measured in order to assess the maximum stimulated cortisol level achieved. Potential adrenal suppression was indicated if the serum cortisol concentration is ≤18mcg/dl at 30 minutes after the injection. | Day 28 |
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Inclusion Criteria:
Signed and dated informed consent obtained prior to any trial related activities (including any washout period)
Age 18 years or above
Either sex
Any race or ethnicity
Any skin type
Attending a hospital out-patient clinic or the private practice of a dermatologist for treatment of psoriasis vulgaris
At SV2 and Day 0 (Visit 1), a clinical diagnosis of psoriasis vulgaris of at least 6 months duration involving the trunk and/or limbs and the scalp which is;
At SV2, a normal HPA axis function including a serum cortisol concentration above 5 mcg/dl before ACTH-challenge and above 18 mcg/dl 30 minutes after ACTH-challenge
At SV2, an albumin-corrected serum calcium below the upper reference range limit
At SV2, females of child-bearing potential must have a negative urine pregnancy result
Females of child-bearing potential must agree to use a highly effective method of contraception during the study. A highly effective method of birth control is defined as one which results in a low failure rate (less than 1% per year)
Able to communicate with the investigator and understand and comply with the requirements of the study
Exclusion Criteria:
A history of allergic asthma, serious allergy or serious allergic skin rash
Known or suspected hypersensitivity to component(s) of LEO 90100 or CORTROSYN (including cosyntropin/tetracosactide)
Systemic treatment with corticosteroids (including inhaled and nasal steroids) within 12 weeks prior to SV2
Systemic treatment with biological therapies (whether marketed or not marketed), with a possible effect on psoriasis vulgaris within the following time period prior to Day 0 (Visit 1);
Subjects who have received treatment with any non-marketed drug substance (i.e. a drug which has not yet been made available for clinical use following registration) within 4 weeks/5 half-lives (whichever is longer) prior to Day 0 (Visit 1)
Systemic treatment with all other therapies with a possible effect on psoriasis vulgaris (e.g. retinoids, methotrexate, cyclosporine and other immunosuppressants) within 4 weeks prior to Day 0 (Visit 1)
PUVA therapy within 4 weeks prior to Day 0 (Visit 1)
UVB therapy within 2 weeks prior to day 0 (Visit 1).
Topical treatment with corticosteroids or vitamin D analogues on any body location within 2 weeks prior to SV2
Any topical treatment of psoriasis vulgaris on the trunk, limbs or scalp (except for emollients and non-medicated shampoos) within 2 weeks prior to Day 0 (Visit 1)
Planned initiation of, or changes to, concomitant medication that could affect psoriasis vulgaris (e.g., betablockers, antimalarials, lithium, ACE inhibitors) during the study
Oral calcium supplements, vitamin D supplements, bisphosphonates or calcitonin within 4 weeks prior to SV2. Note: Stable doses of oral vitamin D supplementation ≤400 IU/day is permitted provided there are no dose adjustments during the study period
Planned initiation of, or changes to concomitant medication that could affect calcium metabolism (e.g. antacids, thiazide and/or loop diuretics, antiepileptics) during the study
Planned excessive exposure of area(s) to be treated with study medication to either natural or artificial sunlight (including tanning booths, sunlamps etc.) during the study
Oestrogen therapy (including contraceptives), antidepressant medications and any other medication known to affect cortisol levels or HPA axis integrity within 4 weeks prior to SV2
Cytochrome P450 3A4 (CYP 3A4) inducers (e.g., barbiturates, phenytoin, rifampicin) within 4 weeks prior to SV2
Systemic cytochrome P450 3A4 (CYP 3A4) inhibitors (e.g., ketoconazole, itraconazole, metronidazole) within 4 weeks prior to SV2
Topical cytochrome P450 3A4 (CYP 3A4) inhibitors (e.g., ketoconazole) within 2 weeks prior to SV2
Non-nocturnal sleep patterns (e.g. night shift workers)
Any of the following conditions, whether known or suspected:
Any clinically significant abnormality following blood pressure/heart rate measurement or review of screening laboratory tests (blood and spot urine samples) collected at SV2
Any clinically significant abnormality following physical examination at SV1
Current diagnosis of guttate, erythrodermic, exfoliative or pustular psoriasis
Any of the following conditions present on the study treatment areas (trunk, limbs and scalp): 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, acne vulgaris, atrophic skin, striae atrophicae, fragility of skin veins, ichthyosis, ulcers and wounds
Other inflammatory skin disorders (e.g. seborrhoeic dermatitis and contact dermatitis) that may confound the evaluation of psoriasis vulgaris
Current participation in any other interventional clinical trial
Previously enrolled in this trial
Known or suspected of not being able to comply with the trial protocol (e.g., alcoholism, drug dependency or psychotic state)
Females who are pregnant, wishing to become pregnant during the study or who are breast-feeding
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| Name | Affiliation | Role |
|---|---|---|
| Vicki Taraska | Winnipeg Clinic | Principal Investigator |
| Facility | Status | City | State | ZIP | Country | Contacts |
|---|---|---|---|---|---|---|
| Guildford Dermatology Specialists | Surrey | British Columbia | V3R 6A7 | Canada | ||
| PerCuro Clinical Research |
| PubMed Identifier | Type | Citation | Retractions |
|---|---|---|---|
| Result | Taraska V, Tuppal R, Olesen M, Bang Pedersen C, Papp K. Fixed combination aerosol foam calcipotriene (Cal) 0.005% plus betamethasone 0.064% (as dipropionate; BD) exhibits no impact on the HPA axis and calcium homeostasis in patients with extensive psoriasis vulgaris: a multicenter, single-arm, Phase II, 4-week MUSE study. Semin Cutan Med Surg. 2015;34 S1:PA-29. | ||
| Result | Taraska V, Tuppal R, Olesen M, Bang Pedersen C, Papp K. Fixed combination aerosol foam calcipotriene 0.005% (Cal) plus betamethasone dipropionate 0.064% (BD) exhibits no impact on the HPA axis and calcium homeostasis in patients with extensive psoriasis vulgaris: a multicenter, single-arm, Phase II, 4-week MUSE study. Semin Cutan Med Surg 2014;33:abst PA-13. |
| Label | URL |
|---|---|
| Clinical Trials at LEO Pharma | View source |
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Subjects with extensive psoriasis vulgaris of at least moderate severity (according to the Investigators Global Assessment of Disease Severity; IGA) on the trunk, limbs and the scalp were enrolled.
Screening: normal HPA axis function before and after ACTH-challenge test and albumin-corrected serum Ca lvl below the upper normal limit were required.
First Subject First Visit: 4-Jun-2012 Last Subject Last Visit: 2-May-2013
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| ID | Title | Description |
|---|---|---|
| FG000 | LEO 90100 | LEO 90100: Calcipotriol 50 mcg/g (as hydrate) and betamethasone 0.5 mg/g (as dipropionate) Once daily for up to 4 weeks |
| Title | Milestones | Reasons Not Completed | |||||
|---|---|---|---|---|---|---|---|
| Overall Study |
|
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| Number of Participants With an Adverse Drug Reaction (ADR) | Adverse drug reactions (ADRs) were defined as adverse events for which the investigator has not described the causal relationship to investigational medication as "not related". | Baseline to Day 28 |
| Change in Serum Phosphate From Baseline to Day 28 | The effect of LEO 90100 on calcium metabolism was evaluated based on change in serum phosphate from Baseline to Day 28. | Baseline and Day 28 |
| Change in 24-hour Urinary Phosphate Excretion From Baseline to Day 28 | The effect of LEO 90100 on calcium metabolism was evaluated based on change in 24-hour urinary phosphate excretion from Baseline to Day 28. | Baseline and Day 28 |
| Change in Urinary Phosphate: Creatinine Ratio From Baseline to Day 28 | The effect of LEO 90100 on calcium metabolism was evaluated based on change in urinary phosphate:creatinine ratio from Baseline to Day 28. | Baseline and Day 28 |
| Change in Serum Alkaline Phosphatase (ALP) From Baseline to Day 28 | The effect of LEO 90100 on calcium metabolism was evaluated based on change in serum ALP from Baseline to Day 28. | Baseline and Day 28 |
| Change in Plasma Parathyroid Hormone (PTH) From Baseline to Day 28 | The effect of LEO 90100 on calcium metabolism was evaluated based on change in plasma PTH from Baseline to Day 28. | Baseline and Day 28 |
| Change in Blood Pressure From Baseline to Day 28 | The effect of LEO 90100 on calcium metabolism was evaluated based on vital sign assessments (blood pressure). | Baseline and Day 28 |
| Change in Heart Rate From Baseline to Day 28 | The effect of LEO 90100 on calcium metabolism was evaluated based on vital sign assessments (heart rate). | Baseline and Day 28 |
| Number of Subjects Who Discontinued From the Study | Number of subjects who discontinued from the study due to adverse events. | Baseline to Day 28 |
| Pharmacokinetic Evaluation Cmax | The following PK parameters will be calculated, if possible, for each assayed compound based on the obtained plasma concentrations:
If it is not possible to calculate the above PK parameters, samples with plasma concentration above lower limit of quantification (LLOQ) will be presented. All subjects but 1 had plasma concentration of calcipotriol below the LLOQ (lower limit of quantification), and thus it was not possible to calculate group mean of the derived PK parameter based on one sample. Provided values for calcipotriol Cmax are derived from that 1 subject. | 4 weeks / 28 days |
| Pharmacokinetic Evaluation AUClast | The following PK parameters will be calculated, if possible, for each assayed compound based on the obtained plasma concentrations:
If it is not possible to calculate the above PK parameters, samples with plasma concentration above lower limit of quantification (LLOQ) will be presented. All subjects but 1 had plasma concentration of calcipotriol below the LLOQ (lower limit of quantification), and thus it was not possible to calculate group mean of the derived PK parameter based on one sample. Provided values for calcipotriol AUClast are derived from that 1 subject. | 4 weeks / 28 days |
| Pharmacokinetic Evaluation AUCinf | The following PK parameters will be calculated, if possible, for each assayed compound based on the obtained plasma concentrations:
If it is not possible to calculate the above PK parameters, samples with plasma concentration above lower limit of quantification (LLOQ) will be presented. | 4 weeks / 28 days |
| Pharmacokinetic Evaluation Tmax | The following PK parameters will be calculated, if possible, for each assayed compound based on the obtained plasma concentrations:
If it is not possible to calculate the above PK parameters, samples with plasma concentration above lower limit of quantification (LLOQ) will be presented. All subjects but 1 had plasma concentration of calcipotriol below the LLOQ (lower limit of quantification), and thus it was not possible to calculate group mean of the derived PK parameter based on one sample. Provided values for calcipotriol Tmax are derived from that 1 subject. | 4 weeks / 28 days |
| Pharmacokinetic Evaluation T1/2 | The following PK parameters will be calculated, if possible, for each assayed compound based on the obtained plasma concentrations:
If it is not possible to calculate the above PK parameters, samples with plasma concentration above lower limit of quantification (LLOQ) will be presented. | 4 weeks / 28 days |
| Efficacy Evaluation | The percentage of subjects who achieved 'controlled disease' (i.e., Clear or Almost clear) according to the Investigator's Global Assessment (IGA) of disease severity on the trunk, limbs and scalp at Days 28 (Visit 3) and End of treatment (EoT) were presented. | 4 weeks I 28 days and End of treatment |
| Victoria |
| British Columbia |
| V8V 3P9 |
| Canada |
| Winnipeg Clinic Dermatology Research | Winnipeg | Manitoba | R3C 0N2 | Canada |
| Maritime Medical Research Center | Bathurst | New Brunswick | E2A 4Z9 | Canada |
| Ultranova Skincare | Barrie | Ontario | L4M 6L2 | Canada |
| Co-Medica | Courtice | Ontario | L1E 3C3 | Canada |
| Mediprobe Research | London | Ontario | N5X 2P1 | Canada |
| The Centre for Dermatology | Richmond Hill | Ontario | L4B 1A5 | Canada |
| K. Papp Clinical Research | Waterloo | Ontario | N2J 1C4 | Canada |
| Centre de Dermatologie Maizerets | Québec | Quebec | G1J 1X7 | Canada |
| COMPLETED |
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| NOT COMPLETED |
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| ID | Title | Description |
|---|---|---|
| BG000 | LEO 90100 | LEO 90100: Calcipotriol 50 mcg/g (as hydrate) and betamethasone 0.5 mg/g (as dipropionate) |
| Units | Counts |
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| Participants |
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| Title | Description | Population Description | Parameter Type | Dispersion Type | Unit of Measure | Calculate Percentage | Denominator Units Selected | Denominators | Classes | ||||||||||||
|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|
| Age, Continuous | Mean | Standard Deviation | years |
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| Sex: Female, Male | Count of Participants | Participants |
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| Type | Title | Description | Population Description | Reporting Status | Anticipated Posting Date | Parameter Type | Dispersion Type | Unit of Measure | Calculate Percentage | Time Frame | Units Analyzed | Denominator Units Selected | Arm/Group Information | Denominators | Classes | Analyses | ||||||||||||||||||||
|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|
| Primary | Subjects With Serum Cortisol Concentration of ≤18 mcg/dl at 30 Minutes After Adrenocorticotrophic Hormone-challenge (ACTH-challenge) | HPA-axis testing by means of the rapid standard-dose cosyntropin test (ACTH-challenge test) for detection of adrenal suppression. | Per protocol analysis set. | Posted | Number | Subjects | Day 28 |
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| Primary | Change in Albumin-corrected Serum Calcium From Baseline to Day 28 | The effect of LEO 90100 on calcium metabolism was evaluated based on change in albumin-corrected serum calcium from Baseline to Day 28. | Posted | Mean | Standard Deviation | mmol/L | Baseline and Day 28 |
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| Primary | Change in 24-hour Urinary Calcium Excretion From Baseline to Day 28 | The effect of LEO 90100 on calcium metabolism was evaluated based on change in 24-hour urinary calcium excretion from Baseline to Day 28 in 24-hour. | Posted | Mean | Standard Deviation | mmol/24H | Baseline and Day 28 |
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| Primary | Change in 24-hour Urinary Calcium:Creatinine Ratio From Baseline to Day 28 | The effect of LEO 90100 on calcium metabolism was evaluated based on change in urinary calcium:creatinine ratio from Baseline to Day 28. | Posted | Mean | Standard Deviation | mmol/g | Baseline and Day 28 |
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| Secondary | Number of Subjects With Serum Cortisol Concentration of ≤18 mcg/dl at 30 and 60 Minutes After ACTH-challenge at Day 28 | Serum cortisol concentrations at 30 and 60 minutes after injection were measured in order to assess the maximum stimulated cortisol level achieved. Potential adrenal suppression was indicated if the serum cortisol concentration is ≤18mcg/dl at 30 minutes after the injection. | Posted | Number | Subjects | Day 28 |
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| Secondary | Number of Participants With an Adverse Drug Reaction (ADR) | Adverse drug reactions (ADRs) were defined as adverse events for which the investigator has not described the causal relationship to investigational medication as "not related". | Posted | Number | participants | Baseline to Day 28 |
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| Secondary | Change in Serum Phosphate From Baseline to Day 28 | The effect of LEO 90100 on calcium metabolism was evaluated based on change in serum phosphate from Baseline to Day 28. | Posted | Mean | Standard Deviation | mmol/L | Baseline and Day 28 |
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| Secondary | Change in 24-hour Urinary Phosphate Excretion From Baseline to Day 28 | The effect of LEO 90100 on calcium metabolism was evaluated based on change in 24-hour urinary phosphate excretion from Baseline to Day 28. | Posted | Mean | Standard Deviation | mmol/24H | Baseline and Day 28 |
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| Secondary | Change in Urinary Phosphate: Creatinine Ratio From Baseline to Day 28 | The effect of LEO 90100 on calcium metabolism was evaluated based on change in urinary phosphate:creatinine ratio from Baseline to Day 28. | Posted | Mean | Standard Deviation | mmol/g | Baseline and Day 28 |
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| Secondary | Change in Serum Alkaline Phosphatase (ALP) From Baseline to Day 28 | The effect of LEO 90100 on calcium metabolism was evaluated based on change in serum ALP from Baseline to Day 28. | Posted | Mean | Standard Deviation | IU/L | Baseline and Day 28 |
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| Secondary | Change in Plasma Parathyroid Hormone (PTH) From Baseline to Day 28 | The effect of LEO 90100 on calcium metabolism was evaluated based on change in plasma PTH from Baseline to Day 28. | Posted | Mean | Standard Deviation | pmol/L | Baseline and Day 28 |
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| Secondary | Change in Blood Pressure From Baseline to Day 28 | The effect of LEO 90100 on calcium metabolism was evaluated based on vital sign assessments (blood pressure). | Posted | Mean | Standard Deviation | mmHg | Baseline and Day 28 |
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| Secondary | Change in Heart Rate From Baseline to Day 28 | The effect of LEO 90100 on calcium metabolism was evaluated based on vital sign assessments (heart rate). | Posted | Mean | Standard Deviation | beats/min | Baseline and Day 28 |
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| Secondary | Number of Subjects Who Discontinued From the Study | Number of subjects who discontinued from the study due to adverse events. | Posted | Number | participants | Baseline to Day 28 |
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| Secondary | Pharmacokinetic Evaluation Cmax | The following PK parameters will be calculated, if possible, for each assayed compound based on the obtained plasma concentrations:
If it is not possible to calculate the above PK parameters, samples with plasma concentration above lower limit of quantification (LLOQ) will be presented. All subjects but 1 had plasma concentration of calcipotriol below the LLOQ (lower limit of quantification), and thus it was not possible to calculate group mean of the derived PK parameter based on one sample. Provided values for calcipotriol Cmax are derived from that 1 subject. | Plasma samples for PK assessment were collected from all 37 subjects however; PK samples from 2 subjects were only collected at screening (SV2) and at Day 14. Therefore these 2 subjects were excluded from PK analysis. Summary of PK parameters based on those subjects that had quantifiable plasma concentrations. | Posted | Mean | Full Range | pg/ml | 4 weeks / 28 days |
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| Secondary | Pharmacokinetic Evaluation AUClast | The following PK parameters will be calculated, if possible, for each assayed compound based on the obtained plasma concentrations:
If it is not possible to calculate the above PK parameters, samples with plasma concentration above lower limit of quantification (LLOQ) will be presented. All subjects but 1 had plasma concentration of calcipotriol below the LLOQ (lower limit of quantification), and thus it was not possible to calculate group mean of the derived PK parameter based on one sample. Provided values for calcipotriol AUClast are derived from that 1 subject. | Plasma samples for PK assessment were collected from all 37 subjects however; PK samples from 2 subjects were only collected at screening (SV2) and at Day 14. Therefore these 2 subjects were excluded from PK analysis. Summary of PK parameters based on those subjects that had quantifiable plasma concentrations | Posted | Mean | Full Range | pg/ml | 4 weeks / 28 days |
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| Secondary | Pharmacokinetic Evaluation AUCinf | The following PK parameters will be calculated, if possible, for each assayed compound based on the obtained plasma concentrations:
If it is not possible to calculate the above PK parameters, samples with plasma concentration above lower limit of quantification (LLOQ) will be presented. | Plasma samples for PK assessment were collected from all 37 subjects however; PK samples from 2 subjects were only collected at screening (SV2) and at Day 14. Therefore these 2 subjects were excluded from PK analysis. Summary of PK parameters based on those subjects that had quantifiable plasma concentrations | Posted | Mean | Full Range | pg/ml | 4 weeks / 28 days |
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| Secondary | Pharmacokinetic Evaluation Tmax | The following PK parameters will be calculated, if possible, for each assayed compound based on the obtained plasma concentrations:
If it is not possible to calculate the above PK parameters, samples with plasma concentration above lower limit of quantification (LLOQ) will be presented. All subjects but 1 had plasma concentration of calcipotriol below the LLOQ (lower limit of quantification), and thus it was not possible to calculate group mean of the derived PK parameter based on one sample. Provided values for calcipotriol Tmax are derived from that 1 subject. | Plasma samples for PK assessment were collected from all 37 subjects however; PK samples from 2 subjects were only collected at screening (SV2) and at Day 14. Therefore these 2 subjects were excluded from PK analysis. Summary of PK parameters based on those subjects that had quantifiable plasma concentrations | Posted | Median | Full Range | h | 4 weeks / 28 days |
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| Secondary | Pharmacokinetic Evaluation T1/2 | The following PK parameters will be calculated, if possible, for each assayed compound based on the obtained plasma concentrations:
If it is not possible to calculate the above PK parameters, samples with plasma concentration above lower limit of quantification (LLOQ) will be presented. | Plasma samples for PK assessment were collected from all 37 subjects however; PK samples from 2 subjects were only collected at screening (SV2) and at Day 14. Therefore these 2 subjects were excluded from PK analysis. Summary of PK parameters based on those subjects that had quantifiable plasma concentrations | Posted | Mean | Full Range | h | 4 weeks / 28 days |
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| Secondary | Efficacy Evaluation | The percentage of subjects who achieved 'controlled disease' (i.e., Clear or Almost clear) according to the Investigator's Global Assessment (IGA) of disease severity on the trunk, limbs and scalp at Days 28 (Visit 3) and End of treatment (EoT) were presented. | The percentage of subjects achieving controlled disease on Day 28 (n=35) was calculated from the full analysis set. The percentage of subjects achieving controlled disease at End of Treatment (n=37) was was calculated from the full analysis set using a last observation carried forward approach. | Posted | Number | percentage of subjects | 4 weeks I 28 days and End of treatment |
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| ID | Title | Description | Deaths (Affected) | Deaths (At Risk) | Serious Events (Affected) | Serious Events (At Risk) | Other Events (Affected) | Other Events (At Risk) |
|---|---|---|---|---|---|---|---|---|
| EG000 | LEO 90100 | LEO 90100: Calcipotriol 50 mcg/g (as hydrate) and betamethasone 0.5 mg/g (as dipropionate) | 0 | 37 | 4 | 37 |
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| Term | Organ System | Source Vocabulary | Assessment Type | Notes | Statistical Information |
|---|---|---|---|---|---|
| Fungal infection | Infections and infestations | MedDRA (15.1) |
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| Arthralgia | Musculoskeletal and connective tissue disorders | MedDRA (15.1) |
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| Headache | Nervous system disorders | MedDRA (15.1) |
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| Oropharyngeal pain | Respiratory, thoracic and mediastinal disorders | MedDRA (15.1) |
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| Upper-airway cough syndrome | Respiratory, thoracic and mediastinal disorders | MedDRA (15.1) |
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| Erythema | Skin and subcutaneous tissue disorders | MedDRA (15.1) | considered by the Investigator to be probably related to treatment (an adverse drug reaction (ADR)) |
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LEO acknowledges the investigators right to publish the entire results of the study, irrespective of outcome. LEO retains the right to have any publication submitted to LEO for review. Investigators must undertake not to submit any part of their individual data for publication without the prior consent of LEO.
| Title | Organization | Phone | Extension | |
|---|---|---|---|---|
| Clinical Trial Disclosure Manager | LEO Pharma A/S | +45 44945888 | ctr.disclosure@leo-pharma.com |
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