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Biodegradation of different synthetic hydrogels made of polyethylene glycol hydrogel/RGD-peptide modifications: an immunohistochemical study in rats.

机译:聚乙二醇水凝胶/ RGD肽修饰物制成的不同合成水凝胶的生物降解:在大鼠中的免疫组织化学研究。

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AIM: The aim of the present study was to investigate the pattern of biodegradation of different polyethylene glycol (PEG) hydrogel/RGD-peptide modifications in rats. MATERIAL AND METHODS: Two different hydrogels were employed: (i) a combination of four-arm PEG-thiol, M(n)=2.3 kDa, and eight-arm PEG-acrylate, M(n)=2.3 kDa (PEG1); and (ii) a combination of four-arm PEG-thiol, M(n)=2.3 kDa, and four-arm PEG-acrylate, M(n)=15 kDa (PEG2). Both PEG1 and PEG2 were either used alone or combined with a nine amino acid cys-RGD peptide (RGD). A non-cross-linked porcine type I and III collagen membrane [BioGide (BG)] served as control. Specimens were randomly allocated in unconnected subcutaneous pouches separated surgically on the back of 60 wistar rats, which were divided into six groups (1, 2, 4, 8, 16, and 24 weeks). Specimens were prepared for histological (tissue integration, foreign body reactions, biodegradation) and immunohistochemical (angiogenesis) analysis. RESULTS: All materials investigated revealed unimpeded and comparable tissue integration without any signs of foreign body reactions. While BG exhibited transmembraneous blood vessel formation at 1 week, all PEG specimens were just surrounded by a well-vascularized connective tissue. The hydrolytic disruption of PEG1 and PEG1/RGD specimens was associated with an ingrowth of blood vessels at 4 weeks. Biodegradation times were highest for PEG1 (24 weeks)>PEG1/RGD (16 weeks)>BG (4 weeks)>PEG2=PEG2/RGD (2 weeks). CONCLUSION: Within the limits of the present study, it was concluded that (i) all materials investigated revealed a high biocompatibility and tissue integration, and (ii) hydrogel biodegradation was dependent on PEG composition.
机译:目的:本研究的目的是研究大鼠体内不同聚乙二醇(PEG)水凝胶/ RGD肽修饰物的生物降解模式。材料与方法:采用两种不同的水凝胶:(i)四臂PEG-硫醇M(n)= 2.3 kDa和八臂PEG-丙烯酸酯M(n)= 2.3 kDa(PEG1)的组合; (ii)四臂PEG-硫醇M(n)= 2.3 kDa和四臂PEG-丙烯酸酯M(n)= 15 kDa(PEG2)的组合。 PEG1和PEG2均可单独使用,也可与九个氨基酸的cys-RGD肽(RGD)组合使用。非交联的猪I型和III型猪胶原膜[BioGide(BG)]用作对照。将标本随机分配到60只wistar大鼠背部经手术分离的未连接的皮下袋中,将其分为六组(1、2、4、8、16和24周)。制备标本用于组织学(组织整合,异物反应,生物降解)和免疫组织化学(血管生成)分析。结果:所有研究的材料均显示无阻碍且可比的组织整合,没有任何异物反应的迹象。尽管BG在第1周表现出跨膜血管形成,但所有PEG标本仅被血管良好的结缔组织包围。 PEG1和PEG1 / RGD标本的水解破坏与第4周血管的向内生长有关。 PEG1(24周)> PEG1 / RGD(16周)> BG(4周)> PEG2 = PEG2 / RGD(2周)的生物降解时间最高。结论:在本研究的范围内,得出的结论是:(i)所有研究的材料均显示出高的生物相容性和组织整合性;(ii)水凝胶的生物降解作用取决于PEG的组成。

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