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Clinical Trial Summary

Burn patients very commonly develop abnormal scars after injury which can be red, raised or elevated, painful and very itchy. They can prevent normal movement of hands and other joints and lead to ugly deformities which makes physical and psychological recovery very difficult. This proposal seeks to test the usefulness of a cream called Nefopam to prevent and treat these bad scars after burns and other injury to the skin. Nefopam is a drug that has been used as a pain medicine in Europe but has been found to have anti-scarring properties in rats and pigs. It has been tested in healthy people and found to be well tolerated and safe. The study purposes to make a scratch in the hip skin in 60 adult burn patients at two burn unit sites, the University of Alberta and the University of California at Davis, Sacramento CA. Burn patients in the study will have a scratch wound in the skin of the each side of the hip, part way through the thickness of the skin which is shallow at first but gets deeper. This scratch is made with a special guide which precisely controls the length and depth of the scratch so that each scratch is the same. Part of the scratch heals without scar and the deeper part heals with a red raised scar over a small region less than 2 inches long. One side will be treated with the drug and the other with a control or placebo are in a white cream that is indistinguishable, where you cannot tell which side contains the drug. Once the wound is nearly healed, usually less than 21 days, the cream will be applied twice daily for three weeks. Measurements will be done about once per month for four months where the healing scratches will be photographed, measurements of the thickness made with ultrasound and mexameter for scar color or pigment and redness. Ultrasound is a painless probe that uses sound waves to measure scar thickness and mexameter is a painless probe on the surface of the scratch to measure color and redness. Both measurements take only minutes to complete. Patients will be asked to answer a scar assessment form about on how they feel each scratch during the treatment and the research staff will also the complete scar form as well. It is the aim of the study to find a cream the works to prevent and reduce scarring after burn injury in military or civilian patients. In the future, an useful cream for scarring in burn patients may also be helpful for other skin damage which leads to scarring.


Clinical Trial Description

Background: Fibroproliferative disorders (FPD) are common and serious disorders involving many human tissues and are a leading cause of mortality and reported as high a 45% of annual deaths. Hypertrophic scar (HTS) and keloids are the dermal equivalent of FPD and impose lower mortality but great morbidity, particularly following burn injury. In the US, 1.25 million people are treated for burns annually, 50,000 requiring hospitalization. Although the mortality rate for burn injury has improved, burn patients experience a prolonged hospitalization (mean 26.2 days) and rehabilitation, requiring an average of 12.7 weeks off work for patients with thermal injuries >30% of the TBSA. Much of the rehabilitation relates to functional and cosmetic limitations imposed by HTS, including a reduction in range of motion of the extremities and the intense pruritus and heat intolerance making early return to work prohibitive, until remodelling of the HTS has occurred. Although risk factors for HTS include sex, age, racial or genetic factors, and wound location, HTS develops after prolonged inflammation of slowly healing burn wounds with a very high frequency especially in deep dermal wounds independent of other factors in up to 75% of burn patients. Unfortunately, HTS and keloid are known to respond poorly to current forms of therapy, including pressure garments, topically applied silicone and intralesional steroids, usually slowly over months or years, often incompletely. Advances in the immunology of FPD including HTS and keloids, reveal many common features, such that novel advances in therapy for these disorders may provide far reaching benefits to many patients and military personnel suffering from severe scarring after burn injury. Drug Information: NEFOPAM HCL has been found safe and effective for the reduction of dermal scarring following standardized human dermal wounds of critical depth that produces HTS in normal human volunteers. NEFOPAM HCl was first developed as a non-narcotic analgesic drug and it is currently marketed primarily in Europe, New Zealand and parts of Asia for oral, intramuscular or intravenous use for acute or chronic pain. NEFOPAM HCl has over 30 years of human safety data. It is considered generally safe with mild side effects including nausea, sweating, dry mouth and tachycardia. NEFOPAM reformulated into a cream and topically administered has been shown to reduce the amount of scar tissue formed during wound healing in mice and the red Duroc pig model of hypertrophic scarring. Most recently, a phase I safety and efficacy study was conducted in human volunteers using a standardized progressively deeper dermal wound (0-1.6 mm in depth over 6 cm) made with a sterile jig in each hip, where normotrophic (negative control) and HTS (positive control) develop in the superficial and deep regions of the scratch. 24 patients have been studied over 104 days where the preliminary results demonstrate that NEFOPAM cream has very few adverse side effects, low immunogenicity and encouraging antifibrotic effects on the healing wounds. Purpose/ Hypothesis: To re-assess the safety, local tolerability and efficacy of NEFOPAM Cream in burn patients when applied to bilateral deep dermal wounds using a standardized dermal scratch model of hypertrophic scarring. Objectives: To assess the efficacy of NEFOPAM Cream versus placebo (vehicle) in reducing scar size following artificially induced dermal wounds in each lateral hip region of burn patients. To determine the efficacy on wound closure of NEFOPAM Cream versus placebo (vehicle) in burn patients. To assess the satisfaction of burn patients and investigators in the scar rating and appearance after topical application of NEFOPAM Cream versus placebo (vehicle). To determine the efficacy of NEFOPAM Cream versus placebo on the gene and protein expression of fibrotic molecules including type I and type III collagen, β-catenin target gene (AXIN-2), TGF- β1, and decorin, quantitative measures of collagen orientation index (COI), immunohistochemistry of a-SMA (smooth muscle actin) and β -catenin in scar tissue. Research Method/Procedures: This study will be a double blind, placebo-controlled, randomized multicenter Phase II study in which burn patients will be randomized to receive NEFOPAM Cream or placebo. Qualifying subjects will be randomized to receive 2.0 mL of NEFOPAM Cream or placebo (vehicle) on Day -1 on intact skin in an area on the upper hip not intended for the incision. On Day 0 burn patients who are free of adverse events will enter the treatment phase of the study. Consenting burn patients requiring skin graft surgery will be scratch-wounded under aseptic conditions on the lateral hip of each lower extremity while under local anesthesia or general anesthesia for their wound debridement as previously described. To create small standardized depth uniform wounds, a jig fitted with a sterile No.11 surgical scalpel blade will be used to create a wound that is 6 cm in length and from 0 to approximately 1.6 mm maximum depth into the deep dermis of the lateral hip mid-distance between the anterior superior iliac spine and the lateral trochanter of the hip. Two identical wounds will be made, one on each hip and subjects will be randomized to receive treatment with NEFOPAM Cream or placebo on each wound. Wounds will be followed until >90% re-epithelialized before the wounds will be cleaned and the cream will be applied twice a day for the next 21 days. The wounds will be covered with an occlusive dressing until Day 21 of treatment (Tegaderm ™). Once the treatment is completed and the wounds are fully healed, the wound/scar will be left uncovered and treated with a moisturizing cream (Glaxal™) if necessary. Burn patients randomized to receive active treatment will have one wound treated with NEFOPAM Cream (treatment wound site) and the other wound site treated with placebo cream/vehicle (control wound site) according to the randomization schedule and dosing instructions. All study team members and subjects will be blinded to all treatments. Subjects will receive two applications of treatment to each wound per day for 21 days after the wounds are 90% healed. Wound evaluations will be performed daily through the treatment period. Digital photography of the wound/scar will occur following wounding and on Day 6 (+/- 2), Day 13 (+/- 2), Day 20 (+/- 3), Day 27 (+/- 2), Day 48 (+/- 7) Day 76 (+/-14), Day 104 (+/- 15). Modified VBSA and POSAS scale, vascularity and pigmentation via Mexameter® and ultrasound evaluations of the scar will commence after the dermal scratch is completed and thereafter when the wound is healed (defined as >90% epithelialization of the wound with no exudate - approximately 1-3 weeks following wounding) and repeated on Day 20 (+/- 3), Day 27 (+/- 2), Day 48 (+/- 7) Day 76 (+/-14), Day 104 (+/- 15). Two punch biopsies will be performed on the maximally thick region of each scar on Day 28 and day 104 for immunohistochemistry analysis of a-SMA (smooth muscle actin) and β-catenin, collagen orientation, and RT-qPCR analysis of type I and type III collagen, the β-catenin target gene (AXIN-2), TGF- β1 and decorin. Subjects may request that the scar be completely excised on or after D104 under local anesthetic (1% xylocaine with epinephrine 1:100,000) and repaired using 4(0) monocril suture in the subcuticular plain to produce a fine linear scar. Tissue removed from this procedure will be used for immunohistochemistry analysis of β-catenin and RT-qPCR analysis of type I and type III collagen, the β-catenin target gene (AXIN-2), TGF- β1 and decorin. Plan for Data Analysis: All calculations and analyses will be performed using SAS version 9.4 or higher resident on the HP Unix (HPUX B.11.11 or higher. The continuous data will be summarized via PROC UNIVARIATE - mean, standard deviation, median, minimum, and maximum. The Safety Population will be used for analysis of adverse events, tolerability reactions, clinical evaluations, and laboratory tests. The ITT Population will be used for all other analyses. For any assessments that are not performed per hip (e.g. adverse event reporting), results will be grouped by treatment (NEFOPAM 3.0% and placebo, placebo alone). For assessments that are performed separately on each hip (e.g. tolerability, POSAS scale), results will be grouped two ways: (1) By within-subject differences between hips grouped by the 3 treatment groups; and (2) By overall group mean value by treatment applied. Tolerability is assessed separately for each hip by the investigator using a 5-point scale that ranges from 0 (No visible reaction) to 4 (Severe erythema with induration, vesicles or pustules and/or erosion/ulceration). While Likert scales are ordinal in nature, parametric methods are still robust and appropriate for analysis (43). Thus, for the assessment of tolerability, an ANCOVA model will be used to compare the within-subject difference between active and placebo hips (or, for placebo-only subjects, between left and right hips) in average tolerability. The average tolerability for each subject-hip will be calculated across all non-missing scheduled visits. ;


Study Design


Related Conditions & MeSH terms


NCT number NCT04685577
Study type Interventional
Source University of Alberta
Contact Nidhi Gupta, PhD
Phone 780-407-6979
Email nidhi2@ualberta.ca
Status Recruiting
Phase Phase 2
Start date July 10, 2022
Completion date December 2025

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