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替罗酶用于静脉性腿部溃疡清创的安全性和有效性的首次临床评估。

First clinical evaluation of the safety and efficacy of tarumase for the debridement of venous leg ulcers.

机构信息

SolasCure Limited, Wellington House, Cambridge, UK.

Óbudai Egészségügyi Centrum (OEC) KFT, Budapest, Hungary.

出版信息

Int Wound J. 2024 Mar;21(3):e14805. doi: 10.1111/iwj.14805.

Abstract

We report the first clinical evaluation of a new enzymatic wound debridement product containing tarumase in venous leg ulcer patients. As a first-in-human study, this was a prospective, open-label, multi-centre, dose escalation study across five dose cohorts and involving a total of 43 patients treated three times weekly for up to 4 weeks (12 applications). The primary and secondary endpoints of the study were to assess the systemic safety, local tolerability, and early proof of concept both for wound debridement and healing. Results indicated that the tarumase enzyme was well tolerated when applied topically to wounds, with no indications of systemic absorption, no evidence of antibody generation, and no systemic effects on coagulation pathways. Locally, there was no evidence of pain on application, no local itching, no increases in erythema, oedema, exudate or bleeding and only a few treatment emergent adverse events were reported. As the concentration of tarumase was escalated, trends towards faster and improved effectiveness of wound debridement were observed, especially in patients with significant slough at baseline. Trends towards faster rates of healing were also noted based on observations of increased granulation tissue, increased linear healing and reduction in surface area over the 4-week treatment period.

摘要

我们报告了一种新型酶清创产品(含 tarumase)在静脉性溃疡患者中的首次临床评估。作为首例人体研究,这是一项前瞻性、开放标签、多中心、剂量递增研究,涉及五个剂量组共 43 名患者,每周接受三次治疗,持续 4 周(12 次应用)。研究的主要和次要终点是评估全身性安全性、局部耐受性,以及在伤口清创和愈合方面的早期概念验证。结果表明,局部应用 tarumase 酶时具有良好的耐受性,无全身吸收迹象,无抗体产生证据,对凝血途径也无全身性影响。局部应用时无疼痛迹象,无局部瘙痒,红斑、水肿、渗出或出血无增加,仅报告了少数治疗时出现的不良事件。随着 tarumase 浓度的增加,观察到伤口清创的效果更快且改善,尤其是在基线时存在大量腐肉的患者中。基于肉芽组织增加、线性愈合增加和治疗 4 周期间表面积减少,观察到愈合速度加快的趋势。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f734/10883251/84e434422c76/IWJ-21-e14805-g002.jpg

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