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用于组织工程应用的三维定制化胶原蛋白样蛋白水凝胶。

Three-dimensional tailor-made collagen-like proteins hydrogel for tissue engineering applications.

机构信息

Division of Biochemistry and Biotechnology, Council of Scientific and Industrial Research (CSIR) - Central Leather Research Institute, Chennai, Tamilnadu, India.

Division of Biochemistry and Biotechnology, Council of Scientific and Industrial Research (CSIR) - Central Leather Research Institute, Chennai, Tamilnadu, India; Academy of Scientific and Innovative Research (AcSIR), Ghaziabad- 201002, India.

出版信息

Biomater Adv. 2022 Aug;139:212997. doi: 10.1016/j.bioadv.2022.212997. Epub 2022 Jun 23.

Abstract

Despite the potential tunable properties of blank slate collagen-like proteins (CLP), an alternative to animal-originated collagen, assembling them into a stable 3D hydrogel to mimic extracellular matrix is a challenge. To address this constraint, the CLP (without hydroxyproline, CLPpro) and its variants encoding functional unnatural amino acids such as hydroxyproline (CLPhyp) and 3,4-dihydroxyphenylalanine (CLPdopa) were generated through genetic code engineering for 3D hydrogel development. The CLPhyp and CLPdopa were chosen to enhance the intermolecular hydrogen bond interaction through additional hydroxyl moiety and thereby facilitate the self-assembly into a fibrillar network of the hydrogel. Hydrogelation was induced through genipin as a cross-linker, enabling intermolecular cross-linking to form a hydrogel. Spectroscopic and rheological analyses confirmed that CLPpro and its variants maintained native triple-helical structure, which is necessary for its function, and viscoelastic nature of the hydrogels, respectively. Unlike CLPpro, the varients (CLPhyp and CLPdopa) increased pore size formation in the hydrogel scaffold, facilitating 3T3 fibroblast cell interactions. DSC analysis indicated that the stability of the hydrogels got increased upon the genetic incorporation of hydroxyproline (CLPhyp) and dopa (CLPdopa) in CLPpro. In addition, CLPdopa hydrogel was found to be relatively stable against collagenase enzyme compared to CLPpro and CLPhyp. It is the first report on 3D biocompatible hydrogel preparation by tailoring CLP sequence with non-natural amino acids. These next-generation tunable CLP hydrogels open a new venue to design synthetic protein-based biocompatible 3D biomaterials for tissue engineering applications.

摘要

尽管无定形胶原蛋白样蛋白 (CLP) 具有潜在的可调特性,是动物源胶原蛋白的替代品,但将其组装成稳定的 3D 水凝胶以模拟细胞外基质仍然具有挑战性。为了解决这一限制,通过遗传密码工程生成了不含羟脯氨酸的 CLP (CLPpro) 及其编码功能性非天然氨基酸(如羟脯氨酸 (CLPhyp) 和 3,4-二羟基苯丙氨酸 (CLPdopa))的变体,用于 3D 水凝胶开发。选择 CLPhyp 和 CLPdopa 是为了通过额外的羟基基团增强分子间氢键相互作用,从而促进水凝胶的自组装成纤维状网络。通过京尼平作为交联剂诱导水凝胶形成,实现分子间交联形成水凝胶。光谱和流变分析证实,CLPpro 及其变体保持了天然的三螺旋结构,这是其功能所必需的,以及水凝胶的粘弹性。与 CLPpro 不同,变体(CLPhyp 和 CLPdopa)增加了水凝胶支架中的孔形成,促进了 3T3 成纤维细胞的相互作用。DSC 分析表明,在 CLPpro 中遗传掺入羟脯氨酸 (CLPhyp) 和多巴 (CLPdopa) 后,水凝胶的稳定性增加。此外,与 CLPpro 和 CLPhyp 相比,CLPdopa 水凝胶发现对胶原酶的稳定性相对较高。这是首次通过用非天然氨基酸修饰 CLP 序列来制备 3D 生物相容性水凝胶的报道。这些新一代可调 CLP 水凝胶为设计基于合成蛋白质的生物相容性 3D 生物材料开辟了新途径,可用于组织工程应用。

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