Hengameh Bakhtiar , Mohammad Reza Mousavi , Sarah Rajabi , Mohammad Pezeshki-Modaress , Alireza Ayati , Azin Ashoori , Mohammad Reza Ellini , Khadijeh Baaji , Amir Kamali , Zhila Abediasl , Amir Azarpazhooh , Anil Kishen
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This study aimed to fabricate and characterize a novel injectable human amniotic membrane (HAM) hydrogel scaffold crosslinked with genipin, enabling the proliferation of Dental Pulp Stem Cells (DPSCs) and optimizing pulp regeneration.</p></div><div><h3>Methods</h3><p>HAM extracellular matrix (ECM) hydrogels (15, 22.5, and 30 mg/ml) crosslinked with different genipin concentrations (0, 0.1, 0.5, 1, 5, and 10 mM) were evaluated for mechanical properties, tooth discoloration, cell viability, and proliferation of DPSCs. The hydrogels were subcutaneously injected in rats to assess their immunogenicity. 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引用次数: 0
摘要
目的研究可注射生物材料在牙髓再生中的应用前景。本研究旨在制备并表征一种新型可注射的人羊膜(HAM)水凝胶支架,该支架与genipin交联,可促进牙髓干细胞(DPSCs)的增殖并优化牙髓再生。方法用不同浓度的genipin(0、0.1、0.5、1、5和10 mM)交联sham细胞外基质(ECM)水凝胶(15、22.5和30 mg/ml),评价其力学性能、牙齿变色、细胞活力和DPSCs的增殖。大鼠皮下注射水凝胶,观察其免疫原性。将水凝胶应用于根管模型并皮下植入大鼠体内,观察其8周后的再生潜能,并进行组织学和免疫染色分析。结果低浓度genipin交联的水凝胶表现出较低的牙齿变色程度,但0.1 mM genipin交联的水凝胶由于力学性能不佳而被排除在外。与0.5 mM genipin交联的水凝胶降解率较低。30mg /ml-0.5 mM交联水凝胶呈微孔结构,弹性模量为1200pa。体外培养时,30mg /ml-0.5 mM交联水凝胶的细胞活力和增殖能力最高。所有组都引起了最小的免疫反应,在有/没有DPSCs的两组中,人牙根都形成了高度血管化的髓样组织。genipin交联改善了可注射的HAM水凝胶的生物降解性,并赋予了更高的生物相容性。用DPSCs包封的水凝胶可以支持干细胞的生存和增殖。此外,这种生物材料形成的高度血管化的牙髓样组织显示出牙髓再生的潜力。
Fabrication and characterization of a novel injectable human amniotic membrane hydrogel for dentin-pulp complex regeneration
Objective
Injectable biomaterials that can completely fill the root canals and provide an appropriate environment will have potential application for pulp regeneration in endodontics. This study aimed to fabricate and characterize a novel injectable human amniotic membrane (HAM) hydrogel scaffold crosslinked with genipin, enabling the proliferation of Dental Pulp Stem Cells (DPSCs) and optimizing pulp regeneration.
Methods
HAM extracellular matrix (ECM) hydrogels (15, 22.5, and 30 mg/ml) crosslinked with different genipin concentrations (0, 0.1, 0.5, 1, 5, and 10 mM) were evaluated for mechanical properties, tooth discoloration, cell viability, and proliferation of DPSCs. The hydrogels were subcutaneously injected in rats to assess their immunogenicity. The hydrogels were applied in a root canal model and subcutaneously implanted in rats to determine their regenerative potential for eight weeks, and histological and immunostaining analyses were performed.
Results
Hydrogels crosslinked with low genipin concentration demonstrated low tooth discoloration, but 0.1 mM genipin crosslinked hydrogels were excluded due to their unfavourable mechanical properties. The degradation ratio was lower in hydrogels crosslinked with 0.5 mM genipin. The 30 mg/ml-0.5 mM crosslinked hydrogel exhibited a microporous structure, and the modulus of elasticity was 1200 PA. In vitro, cell culture showed maximum viability and proliferation in 30 mg/ml-0.5 mM crosslinked hydrogel. All groups elicited minimum immunological responses, and highly vascularized pulp-like tissue was formed in human tooth roots in both groups with/without DPSCs.
Significance
Genipin crosslinking improved the biodegradability of injectable HAM hydrogels and conferred higher biocompatibility. Hydrogels encapsulated with DPSCs can support stem cell viability and proliferation. In addition, highly vascularized pulp-like tissue formation by this biomaterial displayed potential for pulp regeneration.
期刊介绍:
Dental Materials publishes original research, review articles, and short communications.
Academy of Dental Materials members click here to register for free access to Dental Materials online.
The principal aim of Dental Materials is to promote rapid communication of scientific information between academia, industry, and the dental practitioner. Original Manuscripts on clinical and laboratory research of basic and applied character which focus on the properties or performance of dental materials or the reaction of host tissues to materials are given priority publication. Other acceptable topics include application technology in clinical dentistry and dental laboratory technology.
Comprehensive reviews and editorial commentaries on pertinent subjects will be considered.
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