[Preparation and Performance of a Novel Polyurethane Microporous Film on Polypropylene Medical Mesh Surface].

Q3 Medicine 四川大学学报(医学版) Pub Date : 2024-07-20 DOI:10.12182/20240760202
Chenxu Tian, Feng Luo, Jiehua Li, Xueling He
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Abstract

Objective: This study aims to develop a medical patch surface material featuring a microporous polyurethane (PU) membrane and to assess the material's properties and biological performance. The goal is to enhance the clinical applicability of pelvic floor repair patch materials.

Methods: PU films with a microporous surface were prepared using PU prepolymer foaming technology. The films were produced by optimizing the PU prepolymer isocyanate index (R value) and the relative humidity (RH) of the foaming environment. The surface morphology of the PU microporous films was observed by scanning electron microscopy, and the chemical properties of the PU microporous films, including hydrophilicity, were analyzed using infrared spectroscopy, Raman spectroscopy, and water contact angle measurements. In vitro evaluations included testing the effects of PU microporous film extracts on the proliferation of L929 mouse fibroblasts and observing the adhesion and morphology of these fibroblasts. Additionally, the effect of the PU microporous films on RAW264.7 mouse macrophages was studied. Immune response and tissue regeneration were assessed in vivo using Sprague Dawley (SD) rats.

Results: The PU films exhibited a well-defined and uniform microporous structure when the R value of PU prepolymer=1.5 and the foaming environment RH=70%. The chemical structure of the PU microporous films was not significantly altered compared to the PU films, with a significantly lower water contact angle ([55.7±1.5]° ) compared to PU films ([69.5±1.7]° ) and polypropylene (PP) ([ 104.3±2.5]°), indicating superior hydrophilicity. The extracts from PU microporous films demonstrated good in vitro biocompatibility, promoting the proliferation of L929 mouse fibroblasts. The surface morphology of the PU microporous films facilitated fibroblast adhesion and spreading. The films also inhibited the secretion of tumor necrosis factor-α (TNF-α) and interleukin (IL)-1β by RAW264.7 macrophages while enhancing IL-10 and IL-4 secretion. Compared to 24 hours, after 72 hours of culture, the expression levels of TNF-α and IL-1β were reduced in both the PU film and PU microporous film groups and were significantly lower than those in the PP film group (P<0.05), with the most notable decreases observed in the PU microporous film group. IL-10 and IL-4 levels increased significantly in the PU microporous film group, surpassing those in the PP film group (P<0.01), with the most pronounced increase in IL-4. The PU microporous film induced mild inflammation with no significant fibrous capsule formation in vivo. After 60 days of implantation, the film partially degraded, showing extensive collagen fiber growth and muscle formation in its central region.

Conclusion: The PU microporous film exhibits good hydrophilicity and biocompatibility. Its surface morphology enhances cell adhesion, regulates the function of RAW264.7 macrophages, and promotes tissue repair, offering new insights for the design of pelvic floor repair and reconstruction patch materials.

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[聚丙烯医用网表面新型聚氨酯微孔薄膜的制备与性能]。
研究目的本研究旨在开发一种具有微孔聚氨酯(PU)膜的医用补片表面材料,并评估该材料的特性和生物性能。目的是提高盆底修复贴片材料的临床适用性:方法:使用聚氨酯预聚物发泡技术制备了具有微孔表面的聚氨酯薄膜。通过优化聚氨酯预聚物异氰酸酯指数(R 值)和发泡环境的相对湿度(RH)制备了薄膜。通过扫描电子显微镜观察了聚氨酯微孔薄膜的表面形态,并利用红外光谱、拉曼光谱和水接触角测量分析了聚氨酯微孔薄膜的化学特性,包括亲水性。体外评估包括测试聚氨酯微孔薄膜提取物对 L929 小鼠成纤维细胞增殖的影响,以及观察这些成纤维细胞的粘附性和形态。此外,还研究了聚氨酯微孔薄膜对 RAW264.7 小鼠巨噬细胞的影响。使用 Sprague Dawley (SD) 大鼠对体内免疫反应和组织再生进行了评估:结果:当聚氨酯预聚物的 R 值=1.5,发泡环境的相对湿度=70% 时,聚氨酯薄膜呈现出清晰、均匀的微孔结构。与聚氨酯薄膜([69.5±1.7]°)和聚丙烯(PP)([104.3±2.5]°)相比,聚氨酯微孔薄膜的水接触角([55.7±1.5]°)明显较低,表明其亲水性较好。聚氨酯微孔薄膜提取物具有良好的体外生物相容性,可促进 L929 小鼠成纤维细胞的增殖。聚氨酯微孔薄膜的表面形态有利于成纤维细胞的粘附和扩散。薄膜还能抑制 RAW264.7 巨噬细胞分泌肿瘤坏死因子-α(TNF-α)和白细胞介素(IL)-1β,同时促进 IL-10 和 IL-4 的分泌。与 24 小时相比,培养 72 小时后,PU 膜组和 PU 微孔膜组的 TNF-α 和 IL-1β 表达水平均有所下降,且明显低于 PP 膜组(PPin vivo)。植入 60 天后,薄膜部分降解,其中心区域出现大量胶原纤维生长和肌肉形成:结论:聚氨酯微孔薄膜具有良好的亲水性和生物相容性。结论:聚氨酯微孔薄膜具有良好的亲水性和生物相容性,其表面形态可增强细胞粘附性,调节 RAW264.7 巨噬细胞的功能,促进组织修复,为盆底修复和重建补片材料的设计提供了新的思路。
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来源期刊
四川大学学报(医学版)
四川大学学报(医学版) Biochemistry, Genetics and Molecular Biology-Molecular Biology
CiteScore
0.70
自引率
0.00%
发文量
8695
期刊介绍: "Journal of Sichuan University (Medical Edition)" is a comprehensive medical academic journal sponsored by Sichuan University, a higher education institution directly under the Ministry of Education of the People's Republic of China. It was founded in 1959 and was originally named "Journal of Sichuan Medical College". In 1986, it was renamed "Journal of West China University of Medical Sciences". In 2003, it was renamed "Journal of Sichuan University (Medical Edition)" (bimonthly). "Journal of Sichuan University (Medical Edition)" is a Chinese core journal and a Chinese authoritative academic journal (RCCSE). It is included in the retrieval systems such as China Science and Technology Papers and Citation Database (CSTPCD), China Science Citation Database (CSCD) (core version), Peking University Library's "Overview of Chinese Core Journals", the U.S. "Index Medica" (IM/Medline), the U.S. "PubMed Central" (PMC), the U.S. "Biological Abstracts" (BA), the U.S. "Chemical Abstracts" (CA), the U.S. EBSCO, the Netherlands "Abstracts and Citation Database" (Scopus), the Japan Science and Technology Agency Database (JST), the Russian "Abstract Magazine", the Chinese Biomedical Literature CD-ROM Database (CBMdisc), the Chinese Biomedical Periodical Literature Database (CMCC), the China Academic Journal Network Full-text Database (CNKI), the Chinese Academic Journal (CD-ROM Edition), and the Wanfang Data-Digital Journal Group.
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