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载双嘧达莫接枝共聚物电纺纳米纤维膜抑制腱周粘连。

Dipyridamole-grafted copolymer electrospun nanofiber membranes for suppression of peritendinous adhesions.

机构信息

Department of Orthopedics, Soochow University affiliated with Wuxi Ninth People's Hospital, Wuxi, China.

Department of Orthopaedics, Shanghai Sixth People's Hospital affiliated with Shanghai Jiao Tong University School of Medicine, 600 Yishan Rd, Shanghai 200233, China.

出版信息

Acta Biomater. 2024 Oct 15;188:197-211. doi: 10.1016/j.actbio.2024.09.031. Epub 2024 Sep 23.

DOI:10.1016/j.actbio.2024.09.031
PMID:39322044
Abstract

Post-traumatic tendon adhesions significantly affect patient prognosis and quality of life, primarily stemming from the absence of effective preventive and curative measures in clinical practice. Current treatment modalities, including surgical excision and non-steroidal anti-inflammatory drugs, frequently exhibit limited efficacy or result in severe side effects. Consequently, the use of anti-adhesive barriers for drug delivery and implantation at the injury site to address peritendinous adhesion (PA) has attracted considerable attention. Electrospun nanofiber membranes (ENMs) have been extensively employed as drug-delivery platforms. In this study, we fabricated a polylactic acid (PLA)-dipyridamole (DP)-graft copolymer ENM called PLC-DP. This membrane exhibits enzyme-sensitive features, allowing more controlled and sustained drug release compared with conventional drug-loaded ENMs. In experiments, PLC-DP implantation reduced tissue adhesion by 47 % relative to the control group while not adversely affecting tendon healing. Mechanistically, PLC-DP effectively activates the FXYD domain containing ion-transport regulator 2 (FXYD2) protein, thereby downregulating the fibroblast-transforming growth factor beta (TGF-β)/Smad3 signaling pathway. PLC-DP leverages the anti-adhesive properties of DP and the enzyme-sensitive characteristics of graft copolymers, providing a promising approach for the future clinical treatment and prevention of PA. STATEMENT OF SIGNIFICANCE: Peritendinous adhesions (PA) are a common and disabling condition that seriously affects the prognosis and quality of life of post-trauma patients. Current treatments often have limited efficacy or severe side effects, leaving a serious gap in clinical practice. We developed a significant biomaterial, poly(lactic acid)-dipyridamole graft copolymer electrospun nanofibrous membrane (PLC-DP), specifically for PA inhibition. In addition, this study uniquely combines dipyridamole, an anti-adhesive agent, and enzyme-sensitive copolymers in electrospun nanofibrous membrane. Unlike conventional drug-loaded electrospun nanofibrous membranes, PLC-DPs have enzyme-sensitive drug properties that allow for sustained drug release on demand. Our experiments showed that implantation of PLC-DP was effective in reducing tissue adhesions by 47 % without affecting tendon healing. We elucidated the mechanism behind this phenomenon, suggesting that PCD activates FXYD2 to inhibit TGF-β-induced expression of Col III, which is a key factor in PA development.

摘要

创伤后肌腱粘连严重影响患者的预后和生活质量,主要源于临床实践中缺乏有效的预防和治疗措施。目前的治疗方法,包括手术切除和非甾体抗炎药,常常疗效有限或导致严重的副作用。因此,在损伤部位使用抗粘连屏障进行药物输送和植入以解决腱周粘连 (PA) 引起了广泛关注。电纺纳米纤维膜 (ENM) 已被广泛用作药物输送平台。在这项研究中,我们制备了一种聚乳酸 (PLA)-双嘧达莫 (DP)-接枝共聚物 ENM,称为 PLC-DP。与传统的载药 ENM 相比,这种膜具有酶敏感特性,可实现更可控和持续的药物释放。在实验中,与对照组相比,PLC-DP 的植入使组织粘连减少了 47%,同时不会对肌腱愈合产生不利影响。在机制上,PLC-DP 可有效激活 FXYD 域包含的离子转运调节剂 2 (FXYD2) 蛋白,从而下调成纤维细胞转化生长因子β (TGF-β)/Smad3 信号通路。PLC-DP 利用 DP 的抗粘连特性和接枝共聚物的酶敏感特性,为未来临床治疗和预防 PA 提供了一种有前景的方法。

意义声明

腱周粘连 (PA) 是一种常见且致残的疾病,严重影响创伤后患者的预后和生活质量。目前的治疗方法往往疗效有限或副作用严重,在临床实践中存在严重的差距。我们开发了一种重要的生物材料,即聚乳酸-双嘧达莫接枝共聚物电纺纳米纤维膜 (PLC-DP),专门用于抑制 PA。此外,这项研究还将抗粘连剂双嘧达莫和酶敏感共聚物独特地结合到电纺纳米纤维膜中。与传统的载药电纺纳米纤维膜不同,PLC-DP 具有酶敏感的药物特性,可以按需持续释放药物。我们的实验表明,PLC-DP 的植入可有效减少 47%的组织粘连,而不影响肌腱愈合。我们阐明了这一现象背后的机制,表明 PCD 激活 FXYD2 抑制 TGF-β诱导的 Col III 表达,Col III 是 PA 发展的关键因素。

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