Actinic Keratoses Clinical Trial
Official title:
A Randomized, Double-blind, Vehicle-controlled, Multicenter Phase III Study to Evaluate the Safety, Tolerability, and Efficacy of BF-200 ALA (Ameluz®) in the Field-directed Treatment of Actinic Keratosis on the Extremities and Neck/Trunk With Photodynamic Therapy (PDT) Using the BF-RhodoLED® XL or BF-RhodoLED® Lamp
The aim of this study is to test the safety. tolerability and efficacy of field-directed photodynamic therapy (PDT) with 10% aminolevulinic acid gel (Ameluz®, BF-200 ALA) in combination with one of the narrow spectrum red light RhodoLED lamps in comparison to vehicle treatment for actinic keratosis (AK) on the extremities and neck/trunk.
Status | Recruiting |
Enrollment | 165 |
Est. completion date | April 2025 |
Est. primary completion date | July 2024 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 18 Years and older |
Eligibility | Inclusion Criteria: 1. Willingness and ability of subjects to provide informed consent and sign the Health Insurance Portability and Accountability Act (HIPAA) form. A study-specific informed consent and HIPAA form must be obtained in writing prior to starting any study procedures. 2. 4 - 15 mild to moderate clinically confirmed AK lesions according to Olsen either on the extremities or on the neck/trunk with a diameter of = 4 mm that must be present in the treatment field (defined as AK target lesions). In addition, non-target AK lesions may be present in the treatment field, including up to two severe AK lesions = 4 mm. For each severe AK lesion (= 4 mm), a biopsy must be taken for confirmation of diagnosis. The treatment field (continuous or in several patches) totaling approx. either 80 cm², 160 cm² or 240 cm2 must be within one effective illumination area of the BF-RhodoLED® XL but may require up to three illuminations with the BF-RhodoLED®. All AK target lesions and, if applicable, severe AK lesions = 4 mm located in the treatment field should be clearly distinguishable, without restrictions on the distance between lesions, and should have a minimal distance of 1 cm to the border of the treatment field. 3. All sexes, = 18 years of age. 4. Willingness to undergo a 2 mm punch biopsy for each (up to two) severe AK lesion = 4 mm, if applicable, at the screening visit. 5. Willingness and ability to comply with study procedures, particularly willingness to receive up to 2 PDTs within approximately 12 weeks. 6. Subjects with good general health or with clinically stable medical conditions will be permitted to be included in the study. 7. Willingness to stop the use of moisturizers and any other non-medical topical treatments within the treatment field at least 24 h prior to the next clinical visit. 8. Acceptance to abstain from extensive sunbathing and the use of a solarium or tanning beds during the treatment phase. 9. For female subjects with reproductive potential: Negative serum pregnancy test. 10. For female subjects with reproductive potential: Effective contraception at screening visit and throughout the treatment phase of the study (until Visit 4 or Visit 6). Exclusion Criteria: 1. Any known history of hypersensitivity to ALA, porphyrins, or excipients of BF-200 ALA. 2. History of soy or peanut allergy. 3. Sunburn or other possible confounding skin conditions (e.g., wounds, irritations, bleeding, or skin infections) inside or in close proximity (< 2 cm distance) to the treatment field. 4. Clinically significant (cs) medical conditions making implementation of the protocol or interpretation of the study results difficult or impairing subject's safety such as: 1. Presence of photodermatoses or porphyria 2. Metastatic tumor or tumor with high probability of metastasis 3. Infiltrating skin neoplasia (suspected or known) 4. Unstable cardiovascular disease (New York Heart Association class III, IV) 5. Unstable hematologic (including myelodysplastic syndrome), hepatic, renal, neurologic, or endocrine condition 6. Unstable collagen-vascular condition 7. Unstable gastrointestinal condition 8. Immunosuppressive condition 9. Presence of clinically significant inherited or acquired coagulation defect 5. Clinical diagnosis of atopic dermatitis, Bowen´s disease (BD), basal cell carcinoma (BCC), eczema, psoriasis, rosacea, squamous cell carcinoma (SCC), other malignant or benign tumors inside or in close proximity (< 2 cm distance) to the treatment field. 6. Presence of strong artificial pigmentation (e.g., tattoos) or any other abnormality that may impact lesion assessment or light penetration in the treatment field. 7. Any physical therapy such as cryotherapy, laser therapy, electrodessication, microdermabrasion, surgical removal of lesions, curettage, or treatment with chemical peels such as trichloroacetic acid inside or in close proximity (< 10 cm distance) to the treatment field within 4 weeks prior to screening. 8. Any of the topical treatments defined below within the designated periods prior to screening: 1. Topical treatment with ALA or ALA esters (e.g., methyl aminolevulinic acid (MAL)) inside the treatment field within 3 months. 2. Topical treatment with immunomodulatory, cytostatic, or cytotoxic drugs inside or in close proximity (< 10 cm distance) to the treatment field within 3 months. 3. Start of topical administration of a medication with hypericin or other drugs with phototoxic or photoallergic potential inside or in close proximity (< 10 cm distance) to the treatment field within 4 weeks. Subjects may, however, be eligible if such medication was applied for more than 4 weeks prior to screening without evidence of an actual phototoxic/photoallergic reaction. 9. Any use of the systemic treatments within the designated periods prior to screening: 1. Cytostatic or cytotoxic drugs within 6 months. 2. Immunosuppressive therapies or ALA or ALA esters (e.g., MAL) within 12 weeks. 3. Drugs known to have major organ toxicity within 8 weeks. 4. Interferon or glucocorticosteroids within 6 weeks. 5. Start of intake of medication with hypericin or drugs with phototoxic or photoallergic potential within 8 weeks prior to screening. Subjects may, however, be eligible if such medication was taken in for more than 8 weeks prior to the screening visit without evidence of an actual phototoxic/photoallergic reaction. 10. Breast feeding women. 11. Suspicion of drug or alcohol abuse. 12. Subjects 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. 13. A member of study site staff or sponsor staff directly involved in the conduct of the protocol or a close relative thereof. 14. Receipt of any investigational drug or medical product within 8 weeks before screening or simultaneous participation in another clinical study. Reassessment of subjects is allowed once in case exclusion criterion 3 is met and eligibility can be achieved within 4 weeks. Reassessment can be done on the day of the actual treatment. Dosing day exclusion criteria: At Visit 2 (baseline, PDT-1) Subjects with sunburn or other possibly confounding skin conditions (e.g., wounds, irritations, bleeding, or skin infections) inside or in close proximity (< 2 cm distance) to the treatment field. Reassessment of subjects is allowed once if the sunburn or other confounding skin conditions is/are expected to resolve within 2 weeks. At Visit 4 (PDT-2) Subjects with sunburn or other possibly confounding skin conditions (e.g., wounds, irritations, bleeding, or skin infections) inside or in close proximity (< 2 cm distance) to the treatment field. Rescheduling of PDT-2 can be performed once at the earliest possibility after resolution, but rescheduling should not exceed 2 weeks. |
Country | Name | City | State |
---|---|---|---|
United States | Clinical Research Center of the Carolinas | Charleston | South Carolina |
United States | Dermatology Associates PA of the Palm Beaches | Delray Beach | Florida |
United States | Dermatology Practice | Greenwood Village | Colorado |
United States | Austin Institute for Clinical Research | Houston | Texas |
United States | Laser and Skin Surgery Center of Indiana | Indianapolis | Indiana |
United States | Austin Institute for Clinical Research Inc. | Pflugerville | Texas |
United States | Alliance Dermatology & Mohs Center | Phoenix | Arizona |
United States | Medical Dermatology Specialists | Phoenix | Arizona |
United States | Skin Search of Rochester, Inc. | Rochester | New York |
United States | Gwinnett Clinical Research Center, Inc. | Snellville | Georgia |
United States | Rochester Dermatologic Surgery | Victor | New York |
Lead Sponsor | Collaborator |
---|---|
Biofrontera Bioscience GmbH |
United States,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Other | Subject recurrence rate | The percentage of subjects with all AK target lesions clinically cleared 12 weeks after the last PDT presenting with at least one recurrent lesion during follow-up, stratified by demographics, study sites, AK baseline parameters | On follow-up Visit 1 (6 months after last PDT) and follow-up Visit 2 (12 months after last PDT) | |
Other | Lesion recurrence rate | The percentage of AK target lesions showing recurrence in follow-up in relation to total number of clinically cleared AK target lesions 12 weeks after last PDT; overall and stratified by treatment area and AK severity at baseline (according to Olsen [mild, moderate, severe]) | On follow-up Visit 1 (6 months after last PDT) and follow-up Visit 2 (12 months after last PDT) | |
Other | Recurrence rate of severe lesions | The percentage of severe AK lesions (according to Olsen [mild, moderate, severe]) showing recurrence in follow-up in relation to total number of clinically cleared severe AK lesions 12 weeks after last PDT; overall and stratified by treatment area | On follow-up Visit 1 (6 months after last PDT) and follow-up Visit 2 (12 months after last PDT) | |
Other | Esthetic appearance at follow-up visits assessed by the investigator | The esthetic outcome at follow-up visits as assessed by the subject according to a 4-point scale ranging from 0 (=very good) to 3 (=unsatisfactory); overall and stratified by treatment area | On follow-up Visit 1 (6 months after last PDT) and follow-up Visit 2 (12 months after last PDT) | |
Other | Esthetic outcome at follow-up visits assessed by the subject | The esthetic outcome at follow-up visits as assessed by the subject according to a 4-point scale ranging from 0 (=very good) to 3 (=unsatisfactory); overall and stratified by treatment area | On follow-up Visit 1 (6 months after last PDT) and follow-up Visit 2 (12 months after last PDT) | |
Other | Satisfaction with PDT at follow-up visits | Satisfaction with PDT treatment after the last PDT as assessed by the subject via questionnaire, 1. if they would chose PDT treatment in the future in case of recurrence or similar disease (yes/no) and 2. how they would rate the PDT treatment in comparison to other treatment modalities, if applicable (better than/ similar/ worse). The treatment modalities should be documented, if applicable); overall and stratified by treatment area | On follow-up Visit 1 (6 months after last PDT) and follow-up Visit 2 (12 months after last PDT) | |
Other | Any SAE and relevant AE | Relevant AEs include AEs or conditions affecting skin health in the treatment field which may impair proper assessment of the recurrence rate of the treated AK lesions, or other clinically relevant events at the investigator's discretion as well as any SAE that has occurred since the final visit of the treatment phase (Visit 4 or Visit 6); overall and stratified by demographics and treatment area | Entire follow-up duration, approx. 40 weeks | |
Other | New lesions inside the treatment field during follow-up | New lesions: AK, non-melanoma skin cancer [NMSC, including BCC, SCC or BD] or melanoma | On follow-up Visit 1 (6 months after last PDT) and follow-up Visit 2 (12 months after last PDT) | |
Primary | Overall subject complete response rate | Percentage of subjects with all AK target lesions clinically cleared after last PDT | 12 weeks after the last PDT (Visit 4 or Visit 6) | |
Secondary | Overall subject complete response rate for subjects with lesions treated on extremities | Percentage of subjects with all AK target lesions on extremities clinically cleared after last PDT | 12 weeks after the last PDT (Visit 4 or Visit 6) | |
Secondary | Overall subject complete response rate for subjects with lesions treated on neck/trunk | Percentage of subjects with all AK target lesions on neck/trunk clinically cleared after last PDT | 12 weeks after the last PDT (Visit 4 or Visit 6) | |
Secondary | Lesion complete response rate | Percentage of clinically cleared individual AK target lesions in relation to total number of AK target lesions at baseline (Visit 2) after the last PDT, overall and stratified by treatment area and AK severity at baseline (according to Olsen) | 12 weeks after the last PDT (Visit 4 or Visit 6) | |
Secondary | Complete response rate for severe lesions | Percentage of clinically cleared individual severe AK lesions in relation to total number of severe AK lesions at baseline (according to Olsen; Visit 2) after the last PDT, overall and stratified by treatment area | 12 weeks after the last PDT (Visit 4 or Visit 6) | |
Secondary | Subject complete response rate after PDT-1 | Percentage of subjects with all AK target lesions clinically cleared after PDT-1, overall and stratified by AK baseline parameters | 12 weeks after PDT-1 (Visit 4) | |
Secondary | Lesion complete response rate after PDT-1 | Percentage of clinically cleared individual AK target lesions in relation to total number of AK target lesions at baseline (Visit 2) after PDT-1, overall and stratified by treatment area and AK severity at baseline (according to Olsen [mild, moderate, severe]) | 12 weeks after PDT-1 (Visit 4) | |
Secondary | Complete response rate for severe lesions after PDT-1 | Percentage of clinically cleared individual severe AK lesions in relation to total number of severe AK lesions at baseline (according to Olsen [mild, moderate, severe]; Visit 2) after PDT-1, overall and stratified by treatment area | 12 weeks after PDT-1 (Visit 4) | |
Secondary | Esthetic appearance at the end of treatment phase assessed by the investigator | The esthetic appearance after the last PDT as assessed by the investigator as assessed by the subject according to a 4-point scale ranging from 0 (=very good) to 3 (=unsatisfactory); overall and stratified by treatment area | On final visit of the treatment phase, 12 weeks after the last PDT (Visit 4 or Visit 6) | |
Secondary | Esthetic outcome at the end of treatment phase assessed by the subject | The esthetic outcome after the last PDT as assessed by the subject according to a 4-point scale ranging from 0 (=very good) to 3 (=unsatisfactory); overall and stratified by treatment area | On final visit of the treatment phase, 12 weeks after the last PDT (Visit 4 or Visit 6) | |
Secondary | Satisfaction with PDT at the end of treatment phase | Satisfaction with PDT treatment after the last PDT as assessed by the subject via questionnaire, 1. if they would chose PDT treatment in the future in case of recurrence or similar disease (yes/no) and 2. how they would rate the PDT treatment in comparison to other treatment modalities, if applicable (better than/ similar/ worse). The treatment modalities should be documented, if applicable); overall and stratified by treatment area | On final visit of the treatment phase, 12 weeks after the last PDT (Visit 4 or Visit 6) | |
Secondary | Frequency and extent of adverse events (AEs), AEs of Special Interest (AESIs), serious AEs (SAEs) and treatment-emergent AEs (TEAEs) during treatment phase | Frequency and extent of AEs, AESIs, SAEs, and TEAEs, overall and stratified by demographics, skin type class (I-III and IV-VI), size of the treatment field, and treatment area.
TEAEs (including application site skin reactions and discomfort) are defined as all AEs with onset or worsening after treatment with IMP. |
Entire study duration, approx. 16 weeks for subjects requiring 1 PDT (until Visit 4) and approx. 28 weeks for subjects with 2 PDTs (until Visit 6) | |
Secondary | New lesions inside the treatment field during treatment phase | New lesions: AK, non-melanoma skin cancer [NMSC, including Basal Cell Carcinoma (BCC), Squamous Cell Carcinoma (SCC) or Bowen's Disease (BD)] or melanoma | All clinical visits throughout entire study duration, approx. 16 weeks for subjects requiring 1 PDT (until Visit 4) and approx. 28 weeks for subjects with 2 PDTs (until Visit 6) | |
Secondary | Assessment of application site reactions | Application site reactions (bleeding, burning, discharge, edema, erosion, erythema, exfoliation, hyperalgesia, induration, irritation, paraesthesia, pruritus, pustules, scabbing, or vesicles) will be assessed on a 4-point scale: grade 0 = none, grade 1 = mild, grade 2 = moderate, grade 3 = severe. | All visits (except screening, Visit 1) throughout entire study duration, approx. 16 weeks for subjects requiring 1 PDT (until Visit 4) and approx. 28 weeks for subjects with 2 PDTs (until Visit 6) | |
Secondary | Application site pain during illumination | Reported by the subjects assessed on an 11-point numeric rating scale ranging from 0 (no pain) to 10 (worst imaginable pain); overall and stratified by size of the treatment field and treatment area | During treatment (illumination) on treatment day for PDT-1 (Visit 2, up to 4 weeks after screening) and during treatment (illumination) on treatment day for PDT-2 (Visit 4; if applicable; 12 weeks after PDT-1) | |
Secondary | Number of patients with significant changes of vital signs | Number of patients with changes in blood pressure (systolic and diastolic) [mmHg] and changes in pulse rate [beats/min]. Findings which differ from reference range and are considered to be clinically significant are to be reported. | All clinical visits throughout entire study duration, approx. 16 weeks for subjects requiring 1 PDT (until Visit 4) and approx. 28 weeks for subjects with 2 PDTs (until Visit 6) | |
Secondary | Number of patients with significant changes in safety laboratory | Changes in clinical chemistry, in hematology and urinalysis parameters as defined in the protocol. Findings which differ from reference range and are considered to be clinically significant are to be reported. | All clinical visits throughout entire study duration, approx. 16 weeks for subjects requiring 1 PDT (until Visit 4) and approx. 28 weeks for subjects with 2 PDTs (until Visit 6) | |
Secondary | Number of patients with abnormal findings in physical examination | Physical examination of head, neck, skin, lymph nodes, thorax including heart and lungs, abdomen, and musculoskeletal, peripheral vascular and nervous system status will be performed. Abnormal findings, considered to be clinically significant, are to be reported. | At screening (up to 4 weeks before treatment) and 12 weeks after the last PDT (Visit 4 or Visit 6) |
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