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矿化组织中的胶原蛋白交联:其化学、功能及临床相关性综述

Collagen cross-links in mineralizing tissues: a review of their chemistry, function, and clinical relevance.

作者信息

Knott L, Bailey A J

机构信息

Collagen Research Group, Division of Molecular and Cellular Biology, University of Bristol, Langford, UK.

出版信息

Bone. 1998 Mar;22(3):181-7. doi: 10.1016/s8756-3282(97)00279-2.

Abstract

Bone collagen cross-links are now widely used to assess bone resorption levels in many metabolic bone diseases. The post-translational modifications of bone and other mineralizing collagens are significantly different from those of other type I collagen matrices, a fact that has been exploited during recent advances in the development of biochemical markers of bone resorption. The enzymatic collagen cross-linking mechanism is based upon aldehyde formation from specific telopeptide lysine or hydroxylysine residues. The immature ketoimine cross-links in bone form via the condensation of a telopeptide aldehyde with a helical lysine or hydroxylysine. Subsequent maturation to the pyridinoline and pyrrole cross-links occur by further reaction of the ketoimines with telopeptide aldehydes. In mineralizing tissues, a relatively low level of lysyl hydroxylation results in low levels of hydroxylysyl pyridinoline, and the occurrence of the largely bone specific lysyl pyridinoline and pyrrolic cross-links. The collagen post-translational modifications appear to play an integral role in matrix mineralization. The matrix of the turkey tendon only mineralizes after a remodeling of the collagen and the subsequent formation of a modified matrix more typical of bone than tendon. Further, disturbances in the post-translational modification of collagen can also affect the mineralization density and crystal structure of the tissue. In addition to their use as a convenient measure of matrix degradation, collagen cross-links are of significant importance for the biomechanical integrity of bone. Recent studies of osteoporotic bone, for example, have demonstrated that subtle perturbations in the pattern of lysine hydroxylation result in changes in the cross-link profile. These alterations, specifically changes in the level of the pyrrolic cross-link, also correlate with the strength of the bone. Further research into the biochemistry of bone collagen cross-links may expand current understanding and their clinical application in metabolic bone disease. This review also demonstrates the potential for further study into this area to provide more subtle information into the mechanisms and etiology of disease and aging of mineralizing tissues.

摘要

骨胶原交联现在被广泛用于评估许多代谢性骨病中的骨吸收水平。骨和其他矿化胶原的翻译后修饰与其他I型胶原基质的翻译后修饰显著不同,这一事实在骨吸收生化标志物开发的最新进展中得到了利用。酶促胶原交联机制基于特定端肽赖氨酸或羟赖氨酸残基形成醛。骨中未成熟的酮亚胺交联通过端肽醛与螺旋赖氨酸或羟赖氨酸的缩合形成。随后,酮亚胺与端肽醛进一步反应,使交联成熟为吡啶啉和吡咯交联。在矿化组织中,赖氨酸羟化水平相对较低导致羟赖氨酸吡啶啉水平较低,以及大量骨特异性赖氨酸吡啶啉和吡咯交联的出现。胶原翻译后修饰似乎在基质矿化中起着不可或缺的作用。火鸡肌腱的基质只有在胶原重塑并随后形成比肌腱更典型的骨样修饰基质后才会矿化。此外,胶原翻译后修饰的紊乱也会影响组织的矿化密度和晶体结构。除了用作基质降解的便捷指标外,胶原交联对骨的生物力学完整性也非常重要。例如,最近对骨质疏松性骨的研究表明,赖氨酸羟化模式的细微扰动会导致交联谱的变化。这些改变,特别是吡咯交联水平的变化,也与骨的强度相关。对骨胶原交联生物化学的进一步研究可能会扩展目前的认识及其在代谢性骨病中的临床应用。这篇综述还展示了在该领域进一步研究的潜力,以便为矿化组织的疾病和衰老机制及病因提供更细微的信息。

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