Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
The aim of this study is to test the safety and efficacy of photodynamic therapy (PDT) for the medication Ameluz® performed with the PDT-lamp BF-RhodoLED® in comparison to the respective placebo treatment for moderate to severe Acne vulgaris.
Not provided
Not provided
Not provided
Not provided
Not provided
| Label | Type | Description | Intervention Names |
|---|---|---|---|
| 1h incubation BF-200 ALA | Experimental | Topical application of BF-200 ALA containing 7.8% 5-ALA (5-aminolevulinic acid) red light photodynamic therapy (PDT) utilizing BF-RhodoLED® after 1h incubation. |
|
| 3h incubation BF-200 ALA | Experimental | Topical application of BF-200 ALA containing 7.8% 5-ALA (5-aminolevulinic acid) red light photodynamic therapy (PDT) utilizing BF-RhodoLED® after 3h incubation. |
|
| 1h incubation vehicle | Placebo Comparator | Topical application of vehicle to BF-200 ALA red light photodynamic therapy (PDT) utilizing BF-RhodoLED® after 1h incubation. |
|
| 3h incubation vehicle | Placebo Comparator | Topical application of vehicle to BF-200 ALA red light photodynamic therapy (PDT) utilizing BF-RhodoLED® after 3h incubation. |
|
| Name | Type | Description | Arm Group Labels | Other Names |
|---|---|---|---|---|
| 1h Incubation Photodynamic therapy (PDT) (ALA-PDT, Ameluz®-PDT) | Combination Product | The treatment field (whole face excluding the periocular area) will be cleansed with gauze soaked with ethanol or isopropanol. Afterwards, approximately 1 tube of study medication will be applied as a thin layer. After drug application, subjects should stay inside for 1 hour. Post incubation, red light illumination with BF-RhodoLED® will be performed according to the lamps user manual until a total light energy of 37 J/cm2 was applied. To cover the whole face 2 illuminations will be required which can either be performed subsequentially or in parallel (with 2 lamps). Other Names: ALA-PDT, Ameluz®-PDT |
| Measure | Description | Time Frame |
|---|---|---|
| Relative change in the number of inflammatory lesions (relative change from baseline) 8 weeks after the last PDT as assessed by investigator. | Outcome 1 is the relative change in the number of inflammatory lesions at the final visit with respect to baseline as assessed by the investigator. | 8 weeks after the last PDT |
| Treatment success defined by a minimum improvement of the modified investigator global assessment (mIGA) score by at least 2 assessed 8 weeks after the last PDT and resulting in an mIGA score of 0 (clear) or 1 (almost clear). | Treatment success is defined as a minimum improvement of the mIGA score by at least 2 and resulting in an mIGA score of 0 (clear) or 1 (almost clear). | 8 weeks after the last PDT |
| Measure | Description | Time Frame |
|---|---|---|
| Absolute and/or percentage change from baseline in the number of lesions as assessed by investigator. | In particular, the following will be assessed:
|
| Measure | Description | Time Frame |
|---|---|---|
| Frequency and severity of adverse events (AEs), serious AEs (SAEs), AEs of special interest (AESI) and treatment-emerged adverse events (TEAEs). | TEAEs are defined as all AEs with onset or worsening after first treatment with IMP up to the last visit of the subject (approximately 8 weeks post last PDT). | from screening to study completion, over a duration of up to approximately 25 weeks |
Inclusion Criteria:
Exclusion Criteria:
Any known history of hypersensitivity to ALA, porphyrins or excipients of BF-200 ALA.
History of soy or peanut allergy.
Subjects with sunburn or other possible confounding skin conditions (e.g. wounds, irritations, bleeding or skin infections) within or in close proximity (< 5 cm distance) to treatment field. (Reassessment of subjects is allowed once if the sunburn or other confounding skin conditions is/are expected to resolve within the screening period.
Reassessment can be done on the day of the actual treatment.)
Clinical diagnosis of atopic dermatitis and other cutaneous conditions (e.g. lupus erythematosus), Bowen's disease, BCC, eczema, psoriasis, acne conglobate, acne fulminans, or secondary acne (steroid-induced acne, perioral dermatitis, acne rosacea), squamous cell carcinoma, other malignant or benign tumors in the treatment field.
Clinically significant (CS) medical conditions making implementation of the protocol or interpretation of the study results difficult or impairing subject's safety such as:
Beard or other facial hair that might interfere with the study assessments unless subject agrees to be clean-shaven throughout the entire study period. (Reassessment of subjects is allowed once if assessment of acne lesions is impaired by facial hair at screening. Reassessment can be performed on the day of the actual treatment).
Facial procedures such as dermabrasion, chemical or laser peels as well as exposure to UV radiation (other than sunlight) at least 4 weeks prior to randomization visit (Visit 2, baseline).
Presence of strong artificial pigmentation (e.g. tattoos) or any other abnormality that may impact lesion assessment or light penetration in the treatment field.
Suspicion of drug or alcohol abuse.
Any topical medication of the skin prior to screening as defined below:
Any use of the below specified systemic treatments within the designated periods:
Breast feeding women.
Subject unlikely to comply with protocol, e.g. inability to return for visits, unlikely to complete the study, or inappropriate in the opinion of the investigator.
Prior randomization in the study.
A member of study site staff or sponsor staff directly involved in the conduct of the protocol or a close relative thereof.
Simultaneous participation in a further clinical study.
Four or more nodular acne lesions on the face.
Unwillingness or inability to limit sun exposure for 48 hours post PDT treatment.
Dosing Day exclusion criteria:
Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
| Name | Affiliation | Role |
|---|---|---|
| Mitchel P Goldman, MD | Dermatology Cosmetic Laser Medical Associates of La Jolla, Inc. | Principal Investigator |
| Facility | Status | City | State | ZIP | Country | Contacts |
|---|---|---|---|---|---|---|
| First OC Dermatology | Fountain Valley | California | 92708 | United States | ||
| Cosmetic Laser Dermatology |
Not provided
Not provided
Not provided
Not provided
Not provided
|
| 1h Incubation Photodynamic therapy (PDT) (vehicle to BF-200 ALA containing no active ingredient) | Combination Product | The treatment field (whole face excluding the periocular area) will be cleansed with gauze soaked with ethanol or isopropanol. Afterwards, approximately 1 tube of study medication will be applied as a thin layer. After drug application, subjects should stay inside for 1h. Post incubation, red light illumination with BF-RhodoLED® will be performed according to the lamps user manual until a total light energy of 37 J/cm2 was applied. To cover the whole face 2 illuminations will be required which can either be performed subsequentially or in parallel (with 2 lamps). |
|
| 3h Incubation Photodynamic therapy (PDT) (ALA-PDT, Ameluz®-PDT) | Combination Product | The treatment field (whole face excluding the periocular area) will be cleansed with gauze soaked with ethanol or isopropanol. Afterwards, approximately 1 tube of study medication will be applied as a thin layer. After drug application, subjects should stay inside for 3 hours. Post incubation, red light illumination with BF-RhodoLED® will be performed according to the lamps user manual until a total light energy of 37 J/cm2 was applied. To cover the whole face 2 illuminations will be required which can either be performed subsequentially or in parallel (with 2 lamps). Other Names: ALA-PDT, Ameluz®-PDT |
|
| 3h Incubation Photodynamic therapy (PDT) (vehicle to BF-200 ALA containing no active ingredient) | Combination Product | The treatment field (whole face excluding the periocular area) will be cleansed with gauze soaked with ethanol or isopropanol. Afterwards, approximately 1 tube of study medication will be applied as a thin layer. After drug application, subjects should stay inside for 3h. Post incubation, red light illumination with BF-RhodoLED® will be performed according to the lamps user manual until a total light energy of 37 J/cm2 was applied. To cover the whole face 2 illuminations will be required which can either be performed subsequentially or in parallel (with 2 lamps). |
|
| 4 or 8 weeks after the last PDT |
| Absolute and percentage change from baseline in the number of lesions as assessed by investigator. | In particular, the following will be assessed:
| 4 or 8 weeks after the last PDT |
| Absolute and percentage change from baseline in the number of lesions as assessed by investigator, only for responders at Visit 3 / 4 weeks after PDT-1. | In particular, the following will be assessed:
| 4 or 8 weeks after PDT-1 |
| Absolute and percentage change from baseline in the number of lesions as assessed by investigator, only for responders at Visit 4b / 4 weeks after PDT-2. | In particular, the following will be assessed:
| 4 or 8 weeks after PDT-2 |
| Absolute and percentage change in the number of lesions as assessed by investigator, only for responders at Visit 5b / 4 weeks after PDT-3. | In particular, the following be assessed:
| 4 or 8 weeks after PDT-3 |
| Change in the number of nodules & cysts | Absolute change and percentage change from baseline (Visit 2) as assessed by investigator. | 8 weeks after the last PDT |
| Treatment success defined by a minimum improvement of the IGA by at least 2. | Treatment success is defined as a minimum improvement of the IGA score by at least 2 (from baseline (Visit 2) as assessed by investigator). | 8 weeks after the last PDT |
| Improvement of the IGA. | As assessed by the investigator. | 8 weeks after the last PDT |
| Improvement of the mIGA. | As assessed by the investigator. | 8 weeks after the last PDT |
| Improvement of scar severity and overall esthetic appearance. | As assessed by the investigator via a physical global scale for acne scars (PGA) | 8 weeks after last PDT |
| Satisfaction regarding esthetic outcome and treatment. | As reported by the subject. | 8 weeks after the last PDT. |
| Application site skin reactions assessed by the investigator. | Application site skin reaction categories: discharge, erosion, erythema, exfoliation, fissure, induration, oedema, scabbing, skin flaking, ulceration, vesicles, other; severity of AE: mild, moderate or severe | from screening to study completion, over a duration of up to approximately 25 weeks |
| Application site discomfort reported by the subjects. | pplication site discomfort categories: burning, hyperaesthesia, pain, paraesthesia, pruritus, stinging, warmth, other; severity of AE: mild, moderate or severe | from screening to study completion, over a duration of up to approximately 25 weeks |
| Pain during illumination reported by the subject. | Assessed by the subjects using an 11-point numeric rating scale, where a score of 0 means "no pain" and a score of 10 means "worst imaginable pain". | from screening to study completion, over a duration of up to approximately 25 weeks |
| Changes in blood pressure | systolic & diastolic [mmHg] | at all clinic visits conducted over a duration of approximately 25 weeks |
| Changes in heart rate | [bpm] | at all clinic visits conducted over a duration of approximately 25 weeks |
| Investigation of clinical chemistry parameters | Findings which differ from reference range and are considered to be clinically significant are to be reported. | first and last visit conducted up to approximately 25 weeks apart |
| Investigation of hematology parameters | Findings which differ from reference range and are considered to be clinically significant are to be reported. | first and last visit conducted up to approximately 25 weeks apart |
| Investigation of urinalysis parameters | Findings which differ from reference range and are considered to be clinically significant are to be reported. | first and last visit conducted up to approximately 25 weeks apart |
| Physical examination of head, neck, skin, lymph nodes, thorax including heart and lungs, abdomen, and musculoskeletal, peripheral vascular and nervous system status | Abnormal findings, considered to be clinically significant, are to be reported. | first and last visit conducted up to approximately 25 weeks apart |
| San Diego |
| California |
| 92121 |
| United States |
| Dermatology Associates PA of the Palm Beaches | Delray Beach | Florida | 33445 | United States |
| ForCare Clinical Research | Tampa | Florida | 17033 | United States |
| DelRicht Research | Baton Rouge | Louisiana | 70809 | United States |
| Skin Search of Rochester, Inc | Rochester | New York | 14623 | United States |
| Clinical Research Center of the Carolinas | Charleston | South Carolina | 29407 | United States |
| DermResearch PA | Austin | Texas | 78759 | United States |
| Austin Institute for Clinical Research Inc. | Pflugerville | Texas | 78660 | United States |
| ID | Term |
|---|---|
| D000152 | Acne Vulgaris |
| ID | Term |
|---|---|
| D017486 | Acneiform Eruptions |
| D012871 | Skin Diseases |
| D017437 | Skin and Connective Tissue Diseases |
| D012625 | Sebaceous Gland Diseases |
Not provided
Not provided
| ID | Term |
|---|---|
| C008848 | 1-phenyl-3,3-dimethyltriazene |
Not provided
Not provided
Not provided