Exploratory Study of IFX-1 in Patients With Pyoderma Gangrenosum
- Registration Number
- NCT03971643
- Lead Sponsor
- InflaRx GmbH
- Brief Summary
The purpose of this study is to determine whether vilobelimab (development name: IFX-1) is safe and effective in the treatment of pyoderma gangrenosum.
- Detailed Description
Neutrophilic dermatoses are a spectrum of inflammatory disorders characterized by skin lesions resulting from a neutrophil-rich inflammatory infiltrate in the absence of infection. Pyoderma gangrenosum is associated with a neutrophilic leukocytosis, which is likely to be triggered by C5a. This study is set up based on the hypothesis that vilobelimab might be able to block C5a induced pro-inflammatory effects such as neutrophil activation and cytokine generation, potentially contributing to the local skin inflammation and tissue damage.
Recruitment & Eligibility
- Status
- COMPLETED
- Sex
- All
- Target Recruitment
- 19
- Diagnosis of an ulcerative form of pyoderma gangrenosum confirmed by the investigator
In addition, the subject must fulfill at least 3 of the following 6 criteria at screening:
History of
- Pathergy (ulcer occurring at the sites of trauma)
- Personal history of inflammatory bowel disease or inflammatory arthritis
- History of papule, pustule or vesicle that rapidly ulcerated
Clinical examination (or photographic evidence) of
- Peripheral erythema, undermining border, and tenderness at site of ulceration
- Multiple ulcerations (at least 1 occurring on the lower leg)
- Cribriform or "wrinkled paper" scar(s) at sites of healed ulcers
Subject has a minimum of 1 evaluable ulcer (≥2 cm2) on the lower extremity at screening
- Pyoderma gangrenosum target ulcer for more than 3 years before screening
- Surgical wound debridement within the previous 2 weeks before screening
- Use of intravenous antibacterials, antivirals, anti-fungals, or anti-parasitic agents within 30 days before screening
- Any drug treatment for pyoderma gangrenosum including corticosteroids (>10 mg), intralesional steroids, cyclosporine A, biologicals and immunosuppressives (with the exception of antibiotics for wound superinfection) used within a time of 5 half-lives of the drug before screening
Study & Design
- Study Type
- INTERVENTIONAL
- Study Design
- SINGLE_GROUP
- Arm && Interventions
Group Intervention Description vilobelimab 800 mg Q2W vilobelimab Dose finding with a total of 15 doses of vilobelimab. Vilobelimab: IV infusions of vilobelimab diluted in sodium chloride. All patients received vilobelimab 800 mg three times during the first week (Days 1, 4, and 8). Starting at Day 15: Group 1 (N=6) continued to receive vilobelimab 800 mg every 2 weeks (Q2W), with option to increase dose from Day 57 to 1600 mg every Q2W. vilobelimab 1600 mg Q2W vilobelimab Dose finding with a total of 15 doses of vilobelimab. Vilobelimab: IV infusions of vilobelimab diluted in sodium chloride. All patients received vilobelimab 800 mg three times during the first week (Days 1, 4, and 8). Starting at Day 15: Group 2 (N=6) received vilobelimab 1600 mg every 2 weeks (Q2W), with option to increase dose from Day 57 to 2400 mg every Q2W. vilobelimab 2400 mg Q2W vilobelimab Dose finding with a total of 15 doses of vilobelimab. Vilobelimab: IV infusions of vilobelimab diluted in sodium chloride. All patients received vilobelimab 800 mg three times during the first week (Days 1, 4, and 8). Starting at Day 15: Group 3 (N=7) received vilobelimab 2400 mg every Q2W.
- Primary Outcome Measures
Name Time Method Treatment-emergent Adverse Events (TEAEs), Related TEAEs, Serious TEAEs, and Adverse Events of Special Interest (AESIs) From treatment start until end of study (including observational visits), an average of 249 days Number of patients with treatment-emergent adverse events (TEAEs), related TEAEs, serious TEAEs, and adverse events of special interest (AESIs)
TEAEs are defined as adverse events that start at or after the first administration of study drug.
Related TEAEs are defined as all TEAEs considered by the investigator to have at least a 'possible' relationship with the study drug.
AESIs are defined as infusion-related reactions, including acute and delayed hypersensitivity and anaphylactic reactions during or after infusion; Meningitis; Meningococcal septicaemia; Invasive infection.
As adverse events will be reported in details in the safety section, no separate reporting on System Organ Class (SOC) or Preferred Term (PT) level etc. is done here.
- Secondary Outcome Measures
Name Time Method Number of Patients With Physician's Global Assessment (PGA) Score ≤3 (Investigator Assessment) From treatment start until V16 (Day 189) Efficacy endpoint: Proportion of patients with a clinical response, defined as Physician's Global Assessment (PGA) score ≤3 of target ulcer at Visit V4, V6, V10 and V16 (End of Treatment \[EOT\]) (SAF).
PGA values: 0 = Completely clear, 1 = Almost clear, 2 =Marked improvement, 3 = Moderate improvement, 4 = Slight improvement, 5 = No change from baseline, 6 = WorseTime to Complete Closure of Pyoderma Gangrenosum Target Ulcer (Investigator Assessment) [Days] From treatment start until end of study (including observational visits), an average of 249 days Efficacy endpoint: Kaplan-Meier analysis of time to first clinical remission (complete closure of target ulcer) defined as PGA score of ≤ 1,
PGA values: 0 = Completely clear, 1 = Almost clear, 2 =Marked improvement, 3 = Moderate improvement, 4 = Slight improvement, 5 = No change from baseline, 6 = WorsePercentage Change in Wound Healing (Wound Area) by Photographic Assessment From treatment start until V16 (Day 189) Efficacy endpoint: Percentage change in wound area \[percent change\] of target ulcer by photographic assessment between Visits V1 and V4, between Visits V1 and V6, between Visits V1 and V16, between Visits V6 and V10, between Visits V10 and V16.
Percentage Change in Wound Healing (Wound Volume) by Photographic Assessment From treatment start until V16 (Day 189) Efficacy endpoint: Percentage change in wound volume \[percent change\] of target ulcer by photographic assessment between Visits V1 and V4, between Visits V1 and V6, between Visits V1 and V16, between Visits V6 and V10, between Visits V10 and V16.
Rate of Change Per Day in Area of Target Ulcer by Photographic Assessment From V1 to V16 From treatment start until V16 (Day 189) Efficacy endpoint: Rate of change per day in area of target ulcer \[mm²/day\] between Visits V1 and V16 (photographic assessment)
Number of Patients With ≥ 50% Decrease in Area of Target Ulcer by Photographic Assessment at V16 From treatment start until V16 (Day 189) Efficacy endpoint: Number of patients with a decrease in area of target ulcer of ≥ 50% by photographic assessment at Visit V16 (EOT) compared to Baseline
Number of Patients With 100% Decrease in Area of Target Ulcer at V16 From treatment start until V16 (Day 189) Efficacy endpoint: Number of patients with a decrease in area of target ulcer of 100% at Visit V16 (EOT) compared to Baseline (remission) (photographic assessment)
Degree of Erythema of the Target Ulcer at V4, V6, V10 and V16 From treatment start until V16 (Day 189) Efficacy endpoint: Degree of erythema of the target ulcer at Visit V4, V6, V10 and V16 (EOT) (investigator assessment)
Border Elevation of the Target Ulcer at Visits V4, V6, V10 and V16 From treatment start until V16 (Day 189) Efficacy endpoint: Border elevation of the target ulcer at visits V4, V6, V10 and V16 (EOT) (investigator assessment)
Percentage Change in Pain by Numeric Rating Scale (NRS) at Visits V4, V6, V10 and V16 From treatment start until V16 (Day 189) Efficacy endpoint: Percentage change from Baseline in pain assessed by Numeric Rating Scale (NRS) \[percent change\] at visits V4, V6, V10 and V16 (EOT) Mean (SD)
The NRS is an 11-point scale (from 0 represent no pain to 10 representing the worst pain the subject can imagine).Percentage Change in Life Quality by DLQI at Visits V4, V6, V10, and V16 From treatment start until V16 (Day 189) Efficacy endpoint: Percentage change from Baseline in Dermatology Life Quality Index (DLQI) \[percent change\] at visits V4, V6, V10, and V16 (EOT)
The DLQI comprises 10 questions with single scores 0 (No effect on patient's life) to 3 (large effect on patient's life). The DLQI total score is calculated by summing up the score of each question resulting in a minimum of 0 (best) and a maximum of 30 (worst).
Trial Locations
- Locations (10)
InflaRx Site #08
🇺🇸Miami, Florida, United States
InflaRx Site #01
🇨🇦Richmond Hill, Ontario, Canada
InflaRx Site #07
🇺🇸Sacramento, California, United States
InflaRx Site #10
🇺🇸Saint Louis, Missouri, United States
InflaRx Site #03
🇺🇸Tampa, Florida, United States
InflaRx Site #12
🇺🇸Hershey, Pennsylvania, United States
InflaRx Site #09
🇺🇸Pittsburgh, Pennsylvania, United States
InflaRx Site #21
🇵🇱Rzeszów, Poland
InflaRx Site #20
🇵🇱Wrocław, Poland
InflaRx Site #05
🇺🇸Columbus, Ohio, United States