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Design and characterization of an in vivo injectable hydrogel with effervescently generated porosity for regenerative medicine applications

自愈水凝胶 生物相容性 材料科学 再生医学 生物医学工程 多孔性 组织工程 体内 纳米技术 化学 复合材料 高分子化学 医学 生物 生物化学 生物技术 冶金 细胞
作者
Louise Griveau,Marianne Lafont,Héloïse Le Goff,Clémence Drouglazet,Baptiste Robbiani,Aurore Berthier,Dominique Sigaudo‐Roussel,Najma Latif,Catherine Le Visage,Vincent Gache,Romain Debret,Pierre Weiss,Jérôme Sohier
出处
期刊:Acta Biomaterialia [Elsevier]
卷期号:140: 324-337 被引量:34
标识
DOI:10.1016/j.actbio.2021.11.036
摘要

Injectable hydrogels that polymerize directly in vivo hold significant promises in clinical settings to support the repair of damaged or failing tissues. Existing systems that allow cellular and tissue ingrowth after injection are limited because of deficient porosity and lack of oxygen and nutrient diffusion inside the hydrogels. Here is reported for the first time an in vivo injectable hydrogel in which the porosity does not pre-exist but is formed concomitantly with its in situ injection by a controlled effervescent reaction. The hydrogel tailorable crosslinking, through the reaction of polyethylene glycol with lysine dendrimers, allows the mixing and injection of precursor solutions from a dual-chamber syringe while entrapping effervescently generated CO2 bubbles to form highly interconnected porous networks. The resulting structures allow preserving modular mechanical properties (from 12.7 ± 0.9 to 29.9 ± 1.7 kPa) while being cytocompatible and conducive to swift cellular attachment, proliferation, in-depth infiltration and extracellular matrix deposition. Most importantly, the subcutaneously injected porous hydrogels are biocompatible, undergo tissue remodeling and support extensive neovascularisation, which is of significant advantage for the clinical repair of damaged tissues. Thus, the porosity and injectability of the described effervescent hydrogels, together with their biocompatibility and versatility of mechanical properties, open broad perspectives for various regenerative medicine or material applications, since effervescence could be combined with a variety of other systems of swift crosslinking. A major challenge in hydrogel design is the synthesis of injectable formulations allowing easy handling and dispensing in the site of interest. However, the lack of adequate porosity inside hydrogels prevent cellular entry and, therefore, vascularization and tissue ingrowth, limiting the regenerative potential of a vast majority of injectable hydrogels. We describe here the development of an acellular hydrogel that can be injected directly in situ while allowing the simultaneous formation of porosity. Such hydrogel would facilitate handling through injection while providing a porous structure supporting vascularization and tissue ingrowth.
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