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胶原样肽的进化筛选促进羟基磷灰石晶体成核。

Evolutionary screening of collagen-like peptides that nucleate hydroxyapatite crystals.

机构信息

Department of Bioengineering, University of California, Berkeley, Berkeley, California 94720, USA.

出版信息

Langmuir. 2011 Jun 21;27(12):7620-8. doi: 10.1021/la104757g. Epub 2011 Feb 3.

Abstract

The biogenesis of inorganic/organic composite materials such as bone typically involves the process of templated mineralization. Biomimetic synthesis of bone-like materials therefore requires the development of organic scaffolds that mediate mineralization of hydroxyapatite (HAP), the major inorganic component of bone. Using phage display, we identified a 12-residue peptide that bound to single-crystal HAP and templated the nucleation and growth of crystalline HAP mineral in a sequence- and composition-dependent manner. The sequence responsible for the mineralizing activity resembled the tripeptide repeat (Gly-Pro-Hyp) of type I collagen, a major component of bone extracellular matrix. Using a panel of synthetic peptides, we defined the structural features required for mineralizing activity. The results support a model for the cooperative noncovalent interaction of the peptide with HAP and suggest that native collagen may have a mineral-templating function in vivo. We expect this short HAP-binding peptide to be useful in the synthesis of three-dimensional bone-like materials.

摘要

无机/有机复合材料的生物发生,如骨骼的形成,通常涉及模板矿化过程。因此,仿生合成骨样材料需要开发介导羟磷灰石(HAP)矿化的有机支架,HAP 是骨骼的主要无机成分。我们利用噬菌体展示技术鉴定了一个由 12 个残基组成的肽,该肽与单晶 HAP 结合,并以序列和组成依赖的方式模板化结晶 HAP 矿的成核和生长。负责矿化活性的序列类似于 I 型胶原蛋白的三肽重复(甘氨酸-脯氨酸-羟脯氨酸),这是骨骼细胞外基质的主要成分。我们使用一系列合成肽定义了矿化活性所需的结构特征。结果支持肽与 HAP 进行合作非共价相互作用的模型,并表明天然胶原蛋白在体内可能具有矿化模板功能。我们预计这种短的 HAP 结合肽将在三维骨样材料的合成中有用。

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