Doxorubicin-Loaded Polymeric Meshes Prevent Local Recurrence After Sarcoma Resection While Avoiding Cardiotoxicity

心脏毒性 阿霉素 医学 肉瘤 软组织肉瘤 软组织 软骨肉瘤 化疗 外科 病理
作者
Eric Bressler,Ngoc-Quynh Chu,Robert C. Sabatelle,David A. Mahvi,Jeremy T Korunes-Miller,Fumiaki Nagashima,Fumito Ichinose,Rong Liu,Mark W. Grinstaff,Yolonda L. Colson,Chandrajit P. Raut
出处
期刊:Cancer Research [American Association for Cancer Research]
卷期号:82 (23): 4474-4484
标识
DOI:10.1158/0008-5472.can-22-0734
摘要

Surgery is the only potentially curative treatment for localized soft-tissue sarcomas. However, for sarcomas arising in the retroperitoneum, locoregional recurrence rates are 35% to 59% despite resection. Doxorubicin (DOX) is the standard first-line systemic chemotherapy for advanced soft-tissue sarcoma, yet its intravenous administration yields limited clinical efficacy and results in dose-limiting cardiotoxicity. We report the fabrication and optimization of a novel electrospun poly(caprolactone) (PCL) surgical mesh coated with layers of a hydrophobic polymer (poly(glycerol monostearate-co-caprolactone), PGC-C18), which delivers DOX directly to the operative bed following sarcoma resection. In xenograft models of liposarcoma and chondrosarcoma, DOX-loaded meshes (DoM) increased overall survival 4-fold compared with systemically administered DOX and prevented local recurrence in all but one animal. Importantly, mice implanted with DoMs exhibited preserved cardiac function, whereas mice receiving an equivalent dose systemically displayed a 23% decrease from baseline in both cardiac output and ejection fraction 20 days after administration. Collectively, this work demonstrates a feasible therapeutic approach to simultaneously prevent post-surgical tumor recurrence and minimize cardiotoxicity in soft-tissue sarcoma.A proof-of-principle study in animal models shows that a novel local drug delivery approach can prevent tumor recurrence as well as drug-related adverse events following surgical resection of soft-tissue sarcomas.
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