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本文引用的文献

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Minerals form a continuum phase in mature cancellous bone.矿物质在成熟的松质骨中形成连续相。
Calcif Tissue Int. 2011 May;88(5):351-61. doi: 10.1007/s00223-011-9462-8. Epub 2011 Jan 28.
2
The nano-morphological relationships between apatite crystals and collagen fibrils in ivory dentine.象牙质牙本质中磷灰石晶体与胶原原纤维的纳米形态关系。
Biomaterials. 2010 Jul;31(19):5275-86. doi: 10.1016/j.biomaterials.2010.03.025. Epub 2010 Apr 9.
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Functional grading of mineral and collagen in the attachment of tendon to bone.肌腱与骨附着处矿物质和胶原蛋白的功能分级
Biophys J. 2009 Aug 19;97(4):976-85. doi: 10.1016/j.bpj.2009.05.043.
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Mechanical properties of mineralized collagen fibrils as influenced by demineralization.脱矿作用对矿化胶原纤维力学性能的影响
J Struct Biol. 2008 Jun;162(3):404-10. doi: 10.1016/j.jsb.2008.02.010. Epub 2008 Mar 31.
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Microfibrillar structure of type I collagen in situ.原位I型胶原蛋白的微纤维结构。
Proc Natl Acad Sci U S A. 2006 Jun 13;103(24):9001-5. doi: 10.1073/pnas.0502718103. Epub 2006 Jun 2.
6
Sacrificial bonds and hidden length dissipate energy as mineralized fibrils separate during bone fracture.在骨折过程中,当矿化原纤维分离时,牺牲键和隐藏长度会消耗能量。
Nat Mater. 2005 Aug;4(8):612-6. doi: 10.1038/nmat1428. Epub 2005 Jul 17.
7
Atomic force microscopic studies on the structure of bovine femoral cortical bone at the collagen fibril-mineral level.在胶原纤维 - 矿物质水平上对牛股骨皮质骨结构的原子力显微镜研究。
J Mater Sci Mater Med. 2002 Mar;13(3):333-7. doi: 10.1023/a:1014079421895.
8
High-resolution AFM imaging of intact and fractured trabecular bone.完整和骨折的小梁骨的高分辨率原子力显微镜成像。
Bone. 2004 Jul;35(1):4-10. doi: 10.1016/j.bone.2004.02.024.
9
THE PROBLEM OF DEMINERALISATION IN THIN SECTIONS OF FULLY CALCIFIED BONE.完全钙化骨薄片中的脱矿质问题。
J Cell Biol. 1964 Jan;20(1):165-73. doi: 10.1083/jcb.20.1.165.
10
Size and shape of mineralites in young bovine bone measured by atomic force microscopy.通过原子力显微镜测量幼年牛骨中矿化物的尺寸和形状。
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骨的纳米级生理学:胶原-矿物质结构的空间建模和扫描透射电子显微镜研究。

The nanometre-scale physiology of bone: steric modelling and scanning transmission electron microscopy of collagen-mineral structure.

机构信息

Department of Mechanical Engineering and Materials Science, Washington University, Saint Louis, MO 63130, USA.

出版信息

J R Soc Interface. 2012 Aug 7;9(73):1774-86. doi: 10.1098/rsif.2011.0880. Epub 2012 Feb 16.

DOI:10.1098/rsif.2011.0880
PMID:22345156
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3385760/
Abstract

The nanometre-scale structure of collagen and bioapatite within bone establishes bone's physical properties, including strength and toughness. However, the nanostructural organization within bone is not well known and is debated. Widely accepted models hypothesize that apatite mineral ('bioapatite') is present predominantly inside collagen fibrils: in 'gap channels' between abutting collagen molecules, and in 'intermolecular spaces' between adjacent collagen molecules. However, recent studies report evidence of substantial extrafibrillar bioapatite, challenging this hypothesis. We studied the nanostructure of bioapatite and collagen in mouse bones by scanning transmission electron microscopy (STEM) using electron energy loss spectroscopy and high-angle annular dark-field imaging. Additionally, we developed a steric model to estimate the packing density of bioapatite within gap channels. Our steric model and STEM results constrain the fraction of total bioapatite in bone that is distributed within fibrils at less than or equal to 0.42 inside gap channels and less than or equal to 0.28 inside intermolecular overlap regions. Therefore, a significant fraction of bone's bioapatite (greater than or equal to 0.3) must be external to the fibrils. Furthermore, we observe extrafibrillar bioapatite between non-mineralized collagen fibrils, suggesting that initial bioapatite nucleation and growth are not confined to the gap channels as hypothesized in some models. These results have important implications for the mechanics of partially mineralized and developing tissues.

摘要

骨内胶原和生物磷灰石的纳米级结构决定了骨的物理性质,包括强度和韧性。然而,骨内的纳米结构组织还不为人知,存在争议。被广泛接受的模型假设磷灰石矿物(“生物磷灰石”)主要存在于胶原纤维内部:在相邻胶原分子之间的“间隙通道”内,以及在相邻胶原分子之间的“分子间空间”内。然而,最近的研究报告表明存在大量的纤维外生物磷灰石,这对该假设提出了挑战。我们通过扫描透射电子显微镜(STEM)使用电子能量损失光谱和高角度环形暗场成像研究了小鼠骨骼中生物磷灰石和胶原的纳米结构。此外,我们还开发了一种空间模型来估计间隙通道内生物磷灰石的堆积密度。我们的空间模型和 STEM 结果限制了骨内总生物磷灰石中分布在纤维内的部分,在间隙通道内小于或等于 0.42,在分子间重叠区域内小于或等于 0.28。因此,骨内相当大一部分生物磷灰石(大于或等于 0.3)必须存在于纤维之外。此外,我们在非矿化胶原纤维之间观察到纤维外生物磷灰石,这表明初始生物磷灰石成核和生长并不像一些模型中假设的那样局限于间隙通道。这些结果对部分矿化和发育组织的力学具有重要意义。