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水凝胶抑制胚胎跖骨生长揭示准静态负荷与 mTOR 通路的相互作用。

Restraint upon Embryonic Metatarsal Growth by Hydrogel Reveals Interaction between Quasi-Static Load and the mTOR Pathway.

机构信息

Comparative Biomedical Sciences Department, Royal Veterinary College, London NW1 0TU, UK.

出版信息

Int J Mol Sci. 2021 Dec 8;22(24):13220. doi: 10.3390/ijms222413220.

Abstract

Mechanical cues play a vital role in limb skeletal development, yet their influence and underpinning mechanisms in the regulation of endochondral ossification (EO) processes are incompletely defined. Furthermore, interactions between endochondral growth and mechanics and the mTOR/NF-ĸB pathways are yet to be explored. An appreciation of how mechanical cues regulate EO would also clearly be beneficial in the context of fracture healing and bone diseases, where these processes are recapitulated. The study herein addresses the hypothesis that the mTOR/NF-ĸB pathways interact with mechanics to control endochondral growth. To test this, murine embryonic metatarsals were incubated in a hydrogel, allowing for the effects of quasi-static loading on longitudinal growth to be assessed. The results showed significant restriction of metatarsal growth under quasi-static loading during a 14-day period and concentration-dependent sensitivity to hydrogel-related restriction. This study also showed that hydrogel-treated metatarsals retain their viability and do not present with increased apoptosis. Metatarsals exhibited reversal of the growth-restriction when co-incubated with mTOR compounds, whilst it was found that these compounds showed no effects under basal culture conditions. Transcriptional changes linked to endochondral growth were assessed and downregulation of and was observed in hydrogel-treated metatarsi at day 7. Furthermore, cell cycle analyses confirmed the presence of chondrocytes exhibiting S-G2/M arrest. These data indicate that quasi-static load provokes chondrocyte cell cycle arrest, which is partly overcome by mTOR, with a less marked interaction for NF-ĸB regulators.

摘要

机械线索在肢体骨骼发育中起着至关重要的作用,但它们在调控软骨内骨化(endochondral ossification,EO)过程中的影响和潜在机制尚未完全明确。此外,软骨内生长与力学以及 mTOR/NF-κB 途径之间的相互作用仍有待探索。在骨折愈合和骨骼疾病等情况下,这些过程被重现,如果能了解机械线索是如何调节 EO 的,显然将非常有益。本文研究的假设是 mTOR/NF-κB 途径与力学相互作用,以控制软骨内生长。为了验证这一假设,本研究将鼠胚跖骨置于水凝胶中孵育,以评估准静态加载对纵向生长的影响。结果表明,在 14 天的时间内,准静态加载显著限制了跖骨的生长,并且对水凝胶相关限制具有浓度依赖性的敏感性。本研究还表明,水凝胶处理的跖骨保持其活力,不会增加细胞凋亡。当与 mTOR 化合物共同孵育时,跖骨的生长受限得到逆转,而在基础培养条件下,这些化合物没有表现出任何作用。本研究还评估了与软骨内生长相关的转录变化,发现水凝胶处理的跖骨在第 7 天 和 的表达下调。此外,细胞周期分析证实存在表现出 S-G2/M 期阻滞的软骨细胞。这些数据表明,准静态负荷会引起软骨细胞的细胞周期阻滞,而 mTOR 部分克服了这种阻滞,NF-κB 调节剂的相互作用则不那么明显。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1b13/8706285/3a0fd0818a2a/ijms-22-13220-g001.jpg

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