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L-组氨酸控制具有板状形态的羟基磷灰石矿化:浓度和介质的影响。

L-histidine controls the hydroxyapatite mineralization with plate-like morphology: Effect of concentration and media.

作者信息

Chauhan Neelam, Singh Yashveer

机构信息

Department of Chemistry, Indian Institute of Technology Ropar, Rupnagar, 140001, Punjab, India.

Department of Chemistry, Indian Institute of Technology Ropar, Rupnagar, 140001, Punjab, India.

出版信息

Mater Sci Eng C Mater Biol Appl. 2021 Jan;120:111669. doi: 10.1016/j.msec.2020.111669. Epub 2020 Oct 22.

Abstract

Hydroxyapatite (HA) is the main inorganic component of bone and dentin, and their non-stoichiometric compositions and plate-shaped morphology is responsible for their bioactivity and osteoconductive nature. Collagenous (CPs) and non-collagenous proteins (NCPs) facilitate mineralization and regulate structural properties of HA through their side-chains. The bioactivity of synthetic HA does not usually match with the HA found in bone and, therefore, there is a need to understand the role of biomolecules in bone mineralization in order to develop non-stoichiometric plate-shaped HA for bone grafts. Role of several amino acids has been investigated but the role of L-his has been rarely investigated under physiological conditions even though it is a part of HA inhibitor proteins, like albumin, amelogenin, and histidine-rich proteins. In this study, L-his and L-glu were used to modify the structural properties of HA in different experimental conditions and buffer systems (tris and hepes). The results showed that L-his was able to regulate the plate-shaped morphology of HA in every experimental condition, unlike the L-glu, where the crystal morphology was regulated by experimental conditions. Both amino acids behaved differently in DI water, tris, and hepes buffer, and the media used influenced the precipitation time and structural properties of HA. Hepes and tris buffers also influenced the HA precipitation process. Overall, the studies revealed that L-his may be used as an effective regulator of plate-shaped morphology of HA, instead of large NCPs/proteins, for designing biomaterials for bone regeneration applications and the choice of buffer system is important in designing and evaluating the systems for mineralization. In cell culture studies, mouse osteoblast precursor cells (MC3T3-E1) showed highest proliferation on the bone-like plate-shaped HA, among all the HA samples investigated.

摘要

羟基磷灰石(HA)是骨骼和牙本质的主要无机成分,其非化学计量组成和板状形态决定了它们的生物活性和骨传导性。胶原蛋白(CPs)和非胶原蛋白(NCPs)通过其侧链促进矿化并调节HA的结构特性。合成HA的生物活性通常与骨骼中的HA不匹配,因此,有必要了解生物分子在骨矿化中的作用,以便开发用于骨移植的非化学计量板状HA。已经研究了几种氨基酸的作用,但L-组氨酸的作用在生理条件下很少被研究,尽管它是HA抑制蛋白的一部分,如白蛋白、釉原蛋白和富含组氨酸的蛋白。在本研究中,L-组氨酸和L-谷氨酸用于在不同实验条件和缓冲系统(tris和hepes)下修饰HA的结构特性。结果表明,与L-谷氨酸不同,L-组氨酸能够在每种实验条件下调节HA的板状形态,L-谷氨酸的晶体形态受实验条件调节。两种氨基酸在去离子水、tris和hepes缓冲液中的行为不同,所用介质影响HA的沉淀时间和结构特性。Hepes和tris缓冲液也影响HA的沉淀过程。总体而言,研究表明,L-组氨酸可作为HA板状形态的有效调节剂,而不是大的NCPs/蛋白质,用于设计骨再生应用的生物材料,缓冲系统的选择在设计和评估矿化系统中很重要。在细胞培养研究中,在所有研究的HA样品中,小鼠成骨细胞前体细胞(MC3T3-E1)在骨样板状HA上的增殖最高。

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