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长寿的小鼠骨细胞在幼年和老年动物的颅面骨骼中存在,而在老年时其在后颅骨骼中的数量会减少。

Long-lived murine osteocytes are embodied by craniofacial skeleton in young and old animals whereas they decrease in number in postcranial skeletons at older ages.

作者信息

Stigler Robert G, Becker Kathrin, Kloss Frank R, Gassner Robert, Lepperdinger Günter

机构信息

Department of Oral and Maxillofacial Surgery, Medical University Innsbruck, Innsbruck, Austria.

Department of Orthodontics, Universitätsklinikum Düsseldorf, Düsseldorf, Germany.

出版信息

Gerodontology. 2018 Dec;35(4):391-397. doi: 10.1111/ger.12362. Epub 2018 Jul 27.

Abstract

BACKGROUND

Osteocytes are engaged in life-enduring processes such as bone remodelling, fracture healing or osseointegration of implants. Over age, ossification processes and regenerative capacity can greatly differ in mandible and femur.

OBJECTIVE

Mesenchymal stem cells from cranial and postcranial bones are of different embryologic origin. This may be the reason why the regenerative capacity differs between cranial and postcranial bones in old patients. It was hypothesised that different ageing patterns, reflected by osteocyte density, lacunar density and osteoid formation, exist between murine mandibles and femurs.

MATERIAL AND METHODS

Mandible and femur of young (4 months) and old (34-36 months old) male C57Bl/6 mice were histologically investigated to determine the number of lacunae occupied with osteocytes. Osteoid formation was revealed by Masson-Goldner staining, and the spatial distribution of BMP-2 synthesis was examined.

RESULTS

Over lifetime, the number of lacunae occupied with osteocytes only showed a modest decrease in mandibular bone (old 85.63%/young 91.12%) while greatly diverging in the femur (old 55.99%/young 93.28%). In equal measure, old femur exhibited less osteoid formation and decreased BMP-2 expression.

CONCLUSION

Tissue-specific conduct of bone ageing is moulded by osteocytic activities, which was found to vary between postcranial and craniofacial skeleton. The latter harbours long-lived osteocytes also in old animals which assures lifelong bone integrity. Preliminary concurring findings from a human cadaver, also presented in this contribution, provided a rationale for recommending the translatability to humans.

摘要

背景

骨细胞参与诸如骨重塑、骨折愈合或植入物骨整合等持续终生的过程。随着年龄增长,下颌骨和股骨的骨化过程和再生能力差异很大。

目的

来自颅骨和颅后骨的间充质干细胞具有不同的胚胎起源。这可能是老年患者颅骨和颅后骨再生能力不同的原因。据推测,小鼠下颌骨和股骨之间存在由骨细胞密度、陷窝密度和类骨质形成所反映的不同衰老模式。

材料与方法

对年轻(4个月)和年老(34 - 36个月)雄性C57Bl/6小鼠的下颌骨和股骨进行组织学研究,以确定被骨细胞占据的陷窝数量。通过Masson - Goldner染色显示类骨质形成,并检测BMP - 2合成的空间分布。

结果

在整个生命周期中,下颌骨中被骨细胞占据的陷窝数量仅略有下降(老年85.63%/年轻91.12%),而在股骨中差异很大(老年55.99%/年轻93.28%)。同样,老年股骨的类骨质形成较少且BMP - 2表达降低。

结论

骨衰老的组织特异性表现由骨细胞活动塑造,发现其在颅后骨骼和颅面骨骼之间有所不同。后者在老年动物中也含有长寿的骨细胞,这确保了骨骼的终生完整性。本研究中还展示的来自人类尸体的初步一致发现为推荐其向人类的可转化性提供了理论依据。

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