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A comparative analysis of deferoxamine treatment modalities for dermal radiation‐induced fibrosis

医学 去铁胺 纤维化 透皮 血管性 软组织 药理学 伤口愈合 放射治疗 药物输送 外科 病理 内科学 化学 有机化学
作者
Christopher V. Lavin,Darren Abbas,Evan J. Fahy,Daniel K. Lee,Michelle Griffin,Nestor M. Diaz Deleon,Shamik Mascharak,Kellen Chen,Arash Momeni,Geoffrey C. Gurtner,Michael T. Longaker,Derrick C. Wan
出处
期刊:Journal of Cellular and Molecular Medicine [Wiley]
卷期号:25 (21): 10028-10038 被引量:21
标识
DOI:10.1111/jcmm.16913
摘要

Abstract The iron chelator, deferoxamine (DFO), has been shown to potentially improve dermal radiation‐induced fibrosis (RIF) in mice through increased angiogenesis and reduced oxidative damage. This preclinical study evaluated the efficacy of two DFO administration modalities, transdermal delivery and direct injection, as well as temporal treatment strategies in relation to radiation therapy to address collateral soft tissue fibrosis. The dorsum of CD‐1 nude mice received 30 Gy radiation, and DFO (3 mg) was administered daily via patch or injection. Treatment regimens were prophylactic, during acute recovery, post‐recovery, or continuously throughout the experiment ( n = 5 per condition). Measures included ROS‐detection, histology, biomechanics and vascularity changes. Compared with irradiated control skin, DFO treatment decreased oxidative damage, dermal thickness and collagen content, and increased skin elasticity and vascularity. Metrics of improvement in irradiated skin were most pronounced with continuous transdermal delivery of DFO. In summary, DFO administration reduces dermal fibrosis induced by radiation. Although both treatment modalities were efficacious, the transdermal delivery showed greater effect than injection for each temporal treatment strategy. Interestingly, the continuous patch group was more similar to normal skin than to irradiated control skin by most measures, highlighting a promising approach to address detrimental collateral soft tissue injury following radiation therapy.
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