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含多糖纳米凝胶的聚乙二醇水凝胶在糖尿病模型中的免疫反应

Immunological response of polysaccharide nanogel-incorporating PEG hydrogels in an diabetic model.

作者信息

Bal Tugba, Karaoglu Ismail Can, Murat Fusun Sevval, Yalcin Esra, Sasaki Yoshihiro, Akiyoshi Kazunari, Kizilel Seda

机构信息

Chemical and Biological Engineering, Koc University, Istanbul, Sariyer, Turkey.

Biomedical Science and Engineering, Koc University, Istanbul, Sariyer, Turkey.

出版信息

J Biomater Sci Polym Ed. 2022 Oct;33(14):1794-1810. doi: 10.1080/09205063.2022.2077512. Epub 2022 May 19.

Abstract

Cell-based therapies hold significant advantages in comparison with the traditional drug-based or injection-based treatments. However, for long-term functional cellular implants, immune acceptance must be established. To accomplish the acceptance of the implanted cells, various biomaterial systems have been studied. Nanogels have shown great potential for modulation of cellular microenvironments, acting as a physical barrier between the immune system and the implant. However, internalization of nano-scale materials by implanted cells is not desirable and is yet to be overcome. In this study, we incorporated acrylate modified cholesterol-bearing pullulan (CHPOA) nanogels into poly (ethylene glycol) diacrylate (PEGDA) hydrogels through covalent crosslinking, where we used visible light-induced photopolymerization. We characterized morphology and swelling properties of CHPOA incorporated PEG composite hydrogels using FE-SEM and gravimetric analysis. Also, we investigated the biocompatibility properties of composite hydrogels , where we used both healthy and diabetic mice. We induced diabetes in mice using a low dose streptozotocin (STZ) injections and implanted composite hydrogels in both diabetic and healthy mice through subcutaneous route. Immune cell infiltration of the retrieved tissue was examined through histological analysis, where we observed minimum immune response levels of 0-2 rareness, according to ISO standard of biological evaluation of medical devices. Our observation suggests that the composite hydrogel developed here can be used to introduce nanostructured domains into bulk hydrogels and that this system has potential to be used as immunologically acceptable composite material in cellular therapy without internalization of nanoparticles.

摘要

与传统的基于药物或注射的治疗方法相比,基于细胞的疗法具有显著优势。然而,对于长期功能性细胞植入物,必须建立免疫耐受性。为了实现对植入细胞的耐受性,人们研究了各种生物材料系统。纳米凝胶在调节细胞微环境方面显示出巨大潜力,可作为免疫系统与植入物之间的物理屏障。然而,植入细胞对纳米级材料的内化是不可取的,并且尚未得到克服。在本研究中,我们通过共价交联将丙烯酸酯改性的含胆固醇支链淀粉(CHPOA)纳米凝胶掺入聚(乙二醇)二丙烯酸酯(PEGDA)水凝胶中,其中我们使用了可见光诱导的光聚合。我们使用场发射扫描电子显微镜(FE-SEM)和重量分析对掺入CHPOA的PEG复合水凝胶的形态和溶胀性能进行了表征。此外,我们研究了复合水凝胶的生物相容性,使用了健康小鼠和糖尿病小鼠。我们通过低剂量链脲佐菌素(STZ)注射诱导小鼠患糖尿病,并通过皮下途径将复合水凝胶植入糖尿病小鼠和健康小鼠体内。通过组织学分析检查回收组织中的免疫细胞浸润情况,根据医疗器械生物学评价的ISO标准,我们观察到最低免疫反应水平为0-2级罕见。我们的观察表明,这里开发的复合水凝胶可用于将纳米结构域引入块状水凝胶中,并且该系统有潜力在细胞治疗中用作免疫可接受的复合材料,而无需纳米颗粒的内化。

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