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Increased intra-cortical porosity reduces bone stiffness and strength in pediatric patients with osteogenesis imperfecta

机译:皮质内孔隙率的增加降低了成骨不全患儿的骨硬度和强度

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摘要

Osteogenesis imperfecta (OI) is a heritable disease occurring in one out of every 20,000 births. Although it is known that Type I collagen mutation in OI leads to increased bone fragility, the mechanism of this increased susceptibility to fracture is not clear. The aim of this study was to assess the microstructure of cortical bone fragments from patients with osteogenesis imperfecta (OI) using polarized light microscopy, and to correlate microstructural observations with the results of previously performed mechanical compression tests on bone from the same source. Specimens of cortical bone were harvested from the lower limbs of three (3) OI patients at the time of surgery, and were divided into two groups. Group 1 had been subjected to previous micro-mechanical compression testing, while Group 2 had not been subjected to any prior testing. Polarized light microscopy revealed disorganized bone collagen architecture as has been previously observed, as well as a large increase in the areal porosity of the bone compared to typical values for healthy cortical bone, with large (several hundred micron sized), asymmetrical pores. Importantly, the areal porosity of the OI bone samples in Group 1 appears to correlate strongly with their previously measured apparent Young's modulus and compressive strength. Taken together with prior nanoindentation studies on OI bone tissue, the results of this study suggest that increased intra-cortical porosity is responsible for the reduction in macroscopic mechanical properties of OI cortical bone, and therefore that in vivo imaging modalities with resolutions of ~ 100 μm or less could potentially be used to non-invasively assess bone strength in OI patients. Although the number of subjects in this study is small, these results highlight the importance of further studies in OI bone by groups with access to human OI tissue in order to clarify the relationship between increased porosity and reduced macroscopic mechanical integrity.
机译:成骨不全症(OI)是一种遗传性疾病,每20,000例出生中就有一个发生。尽管已知OI中的I型胶原蛋白突变会导致骨骼脆性增加,但这种骨折易感性增加的机制尚不清楚。这项研究的目的是使用偏振光显微镜评估成骨不全症(OI)患者的皮质骨碎片的微观结构,并将微观结构观察结果与先前对同一来源的骨骼进行机械压缩测试的结果相关联。在手术时从三(3)名OI患者的下肢采集皮质骨标本,并将其分为两组。第1组已进行过先前的微机械压缩测试,而第2组未进行过任何先前的测试。偏光显微镜显示,如先前观察到的那样,骨胶原结构紊乱,并且与具有健康的皮质骨的典型值(具有几百个微米大小)的不对称毛孔的典型值相比,骨的表面孔隙率大大增加。重要的是,第1组中OI骨样品的孔隙率似乎与它们先前测得的表观杨氏模量和抗压强度密切相关。结合先前对OI骨组织的纳米压痕研究,这项研究的结果表明,皮质内孔隙率的增加是OI皮质骨宏观力学性能下降的原因,因此,体内成像方式的分辨率约为100μm或更少的潜力可能被用于非侵入性评估OI患者的骨强度。尽管本研究的受试者人数很少,但这些结果凸显了通过接触人OI组织的人群对OI骨进行进一步研究的重要性,以阐明孔隙率增加与宏观机械完整性降低之间的关系。

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