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磷酸丝氨酸骨黏合剂的细胞相容性及生物活性离子释放曲线:从体外到体内的桥梁

Cytocompatibility and Bioactive Ion Release Profiles of Phosphoserine Bone Adhesive: Bridge from In Vitro to In Vivo.

作者信息

Vrchovecká Kateřina, Pávková-Goldbergová Monika, Engqvist Håkan, Pujari-Palmer Michael

机构信息

Department of Pathology Physiology, Faculty of Medicine, Masaryk University, 62500 Brno, Czech Republic.

Department of Materials Science and Engineering, Applied Material Science, Uppsala University, 75103 Uppsala, Sweden.

出版信息

Biomedicines. 2022 Mar 22;10(4):736. doi: 10.3390/biomedicines10040736.

Abstract

One major challenge when developing new biomaterials is translating in vitro testing to in vivo models. We have recently shown that a single formulation of a bone tissue adhesive, phosphoserine modified cement (PMC), is safe and resorbable in vivo. Herein, we screened many new adhesive formulations, for cytocompatibility and bioactive ion release, with three cell lines: MDPC23 odontoblasts, MC3T3 preosteoblasts, and L929 fibroblasts. Most formulations were cytocompatible by indirect contact testing (ISO 10993-12). Formulations with larger amounts of phosphoserine (>50%) had delayed setting times, greater ion release, and cytotoxicity in vitro. The trends in ion release from the adhesive that were cured for 24 h (standard for in vitro) were similar to release from the adhesives cured only for 5−10 min (standard for in vivo), suggesting that we may be able to predict the material behavior in vivo, using in vitro methods. Adhesives containing calcium phosphate and silicate were both cytocompatible for seven days in direct contact with cell monolayers, and ion release increased the alkaline phosphatase (ALP) activity in odontoblasts, but not pre-osteoblasts. This is the first study evaluating how PMC formulation affects osteogenic cell differentiation (ALP), cytocompatibility, and ion release, using in situ curing conditions similar to conditions in vivo.

摘要

开发新型生物材料时面临的一个主要挑战是将体外测试转化为体内模型。我们最近表明,一种骨组织粘合剂——磷酸丝氨酸改性水泥(PMC)的单一配方在体内是安全且可吸收的。在此,我们用三种细胞系:MDPC23成牙本质细胞、MC3T3前成骨细胞和L929成纤维细胞,筛选了许多新的粘合剂配方,以评估其细胞相容性和生物活性离子释放情况。通过间接接触测试(ISO 10993 - 12),大多数配方具有细胞相容性。磷酸丝氨酸含量较高(>50%)的配方凝固时间延迟,离子释放量更大,且在体外具有细胞毒性。固化24小时(体外标准)的粘合剂的离子释放趋势与仅固化5 - 10分钟(体内标准)的粘合剂的离子释放趋势相似,这表明我们或许能够使用体外方法预测材料在体内的行为。含有磷酸钙和硅酸盐的粘合剂与细胞单层直接接触7天均具有细胞相容性,且离子释放增加了成牙本质细胞中的碱性磷酸酶(ALP)活性,但对前成骨细胞没有影响。这是第一项使用与体内条件相似的原位固化条件,评估PMC配方如何影响成骨细胞分化(ALP)、细胞相容性和离子释放的研究。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fd3a/9044752/1dd4b2506c11/biomedicines-10-00736-g008.jpg

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