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内源性骨再生依赖于动态氧事件。

Endogenous bone regeneration is dependent upon a dynamic oxygen event.

作者信息

Sammarco Mimi C, Simkin Jennifer, Fassler Danielle, Cammack Alex J, Wilson Aaron, Van Meter Keith, Muneoka Ken

机构信息

Department of Cell and Molecular Biology, Tulane University, New Orleans, LA, USA.

出版信息

J Bone Miner Res. 2014 Nov;29(11):2336-45. doi: 10.1002/jbmr.2261.

Abstract

Amputation of the digit tip within the terminal phalangeal bone of rodents, monkeys, and humans results in near-perfect regeneration of bone and surrounding tissues; however, amputations at a more proximal level fail to produce the same regenerative result. Digit regeneration is a coordinated, multifaceted process that incorporates signaling from bioactive growth factors both in the tissue matrix and from several different cell populations. To elucidate the mechanisms involved in bone regeneration we developed a novel multi-tissue slice-culture model that regenerates bone ex vivo via direct ossification. Our study provides an integrated multi-tissue system for bone and digit regeneration and allows us to circumvent experimental limitations that exist in vivo. We used this slice-culture model to evaluate the influence of oxygen on regenerating bone. Micro-computed tomography (µCT) and histological analysis revealed that the regenerative response of the digit is facilitated in part by a dynamic oxygen event, in which mutually exclusive high and low oxygen microenvironments exist and vacillate in a coordinated fashion during regeneration. Areas of increased oxygen are initially seen in the marrow and then surrounding areas of vasculature in the regenerating digit. Major hypoxic events are seen at 7 days postamputation (DPA 7) in the marrow and again at DPA 12 in the blastema, and manipulation of oxygen tensions during these hypoxic phases can shift the dynamics of digit regeneration. Oxygen increased to 21% oxygen tension can either accelerate or attenuate bone mineralization in a stage-specific manner in the regenerative timeline. These studies not only reveal a circumscribed frame of oxygen influence during bone regeneration, but also suggest that oxygen may be one of the primary signaling influences during regeneration.

摘要

啮齿动物、猴子和人类的指骨末端指端截肢会导致骨骼和周围组织近乎完美的再生;然而,在更近端水平的截肢则无法产生相同的再生结果。指再生是一个协调的、多方面的过程,它整合了来自组织基质和几种不同细胞群的生物活性生长因子的信号。为了阐明骨再生所涉及的机制,我们开发了一种新型的多组织切片培养模型,该模型通过直接骨化在体外再生骨骼。我们的研究提供了一个用于骨和指再生的整合多组织系统,并使我们能够规避体内存在的实验限制。我们使用这个切片培养模型来评估氧气对再生骨的影响。微型计算机断层扫描(µCT)和组织学分析表明,指的再生反应部分是由一个动态氧气事件促进的,在这个事件中,相互排斥的高氧和低氧微环境存在,并在再生过程中以协调的方式波动。氧气增加的区域最初出现在骨髓中,然后出现在再生指的血管周围区域。主要的缺氧事件在截肢后7天(DPA 7)出现在骨髓中,在芽基中在DPA 12时再次出现,在这些缺氧阶段对氧气张力的操纵可以改变指再生的动态。在再生时间轴上,将氧气张力增加到21%可以以阶段特异性的方式加速或减弱骨矿化。这些研究不仅揭示了骨再生过程中氧气影响的限定框架,还表明氧气可能是再生过程中的主要信号影响因素之一。

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