成骨不全如基因突变对生物材料强度的分子效应的原子性研究

D. K. Dubey, V. Tomar
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引用次数: 0

摘要

成骨不全症(Osteogenesis imperfecta, OI)是一种以骨骼极度脆弱为特征的遗传性疾病,与胶原蛋白(tropocollagen, TC)分子突变和羟基磷灰石(hydroxyapatite, HAP)矿物结构改变有关。TC的突变可以表现为多肽链的取代和残基的点突变两种方式。本研究利用三维原子模拟的方法,从机制角度探讨了TC中OI突变对两种不同矿物分布的TC- hap模型生物材料强度的影响。分析表明,侧链官能团数量较多的残基序列被取代,使TC-HAP生物材料具有更高的强度。结果表明,TC点突变对TC- hap生物材料强度的影响不显著。相反,矿物分布的变化对TC-HAP生物材料的整体强度有显著影响。总的来说,研究表明TC突变通过改变羟基磷灰石生长过程中矿物分布来表现。
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An atomistic investigation into the molecular effects of osteogenesis imperfecta like genetic mutations on biomaterial strength
Osteogenesis imperfecta (OI) is a genetic disease marked by extreme bone fragility and is associated with mutations in tropocollagen (TC) molecule and changes in hydroxyapatite (HAP) mineral texture. Mutations in TC can manifest in both ways, substitution of polypeptide chains and point mutations of residues. This study presents a mechanistic view on the effects of OI mutations in TC on strength of model TC-HAP biomaterials with two different mineral distributions using three dimensional atomistic simulations. Analysis points out that substitution of residue sequences with higher number of side chain functional groups impart higher strength to the TC-HAP biomaterials. Results show that the effect of TC point mutations on the strength of TC-HAP biomaterials is insignificant. Instead, change in mineral distribution showed significant impact on the overall strength of TC-HAP biomaterials. Overall, study suggests that TC mutations manifest themselves by altering the mineral distribution during hydroxyapatite ...
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