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缺氧诱导因子在新生鼠磨牙牙髓发育中的作用:表达模式、定位和代谢途径的研究。

Hypoxia-inducible factors in postnatal mouse molar dental pulp development: insights into expression patterns, localisation and metabolic pathways.

机构信息

Institute of Animal Physiology and Genetics, Czech Academy of Sciences, Brno, Czech Republic.

Department of Histology and Embryology, Faculty of Medicine, Masaryk University, Brno, Czech Republic.

出版信息

Pflugers Arch. 2024 Sep;476(9):1411-1421. doi: 10.1007/s00424-024-03003-1. Epub 2024 Aug 5.

Abstract

Hypoxia is relevant to several physiological and pathological processes and this also applies for the tooth. The adaptive response to lowering oxygen concentration is mediated by hypoxia-inducible factors (HIFs). Since HIFs were shown to participate in the promotion of angiogenesis, stem cell survival, odontoblast differentiation and dentin formation, they may play a beneficial role in the tooth reparative processes. Although some data were generated in vitro, little is known about the in vivo context of HIFs in tooth development. In order to contribute to this field, the mouse mandibular first molar was used as a model.The expression and in situ localisation of HIFs were examined at postnatal (P) days P0, P7, P14, using RT-PCR and immunostaining. The expression pattern of a broad spectrum of hypoxia-related genes was monitored by customised PCR Arrays. Metabolic aspects were evaluated by determination of the lactate level and mRNA expression of the mitochondrial marker Nd1.The results show constant high mRNA expression of Hif1a, increasing expression of Hif2a, and very low expression of Hif3a during early postnatal molar development. In the examined period the localisation of HIFs in the nuclei of odontoblasts and the subodontoblastic layer identified their presence during odontoblastic differentiation. Additionally, the lower lactate level and higher expression of mitochondrial Nd1 in advanced development points to decreasing glycolysis during differentiation. Postnatal nuclear localisation of HIFs indicates a hypoxic state in specific areas of dental pulp as oxygen demands depend on physiological events such as crown and root dentin mineralization.

摘要

缺氧与几种生理和病理过程相关,这也适用于牙齿。对氧浓度降低的适应性反应是由缺氧诱导因子(HIFs)介导的。由于 HIFs 被证明参与了血管生成、干细胞存活、成牙本质细胞分化和牙本质形成的促进,它们可能在牙齿修复过程中发挥有益的作用。虽然已经在体外生成了一些数据,但关于 HIFs 在牙齿发育中的体内背景知之甚少。为了对此领域做出贡献,本研究使用小鼠下颌第一磨牙作为模型。通过 RT-PCR 和免疫染色,在出生后(P)第 0、7、14 天(P)检测 HIFs 的表达和原位定位。通过定制的 PCR 阵列监测广泛的缺氧相关基因的表达模式。通过测定乳酸水平和线粒体标记物 Nd1 的 mRNA 表达来评估代谢方面。结果表明,在早期磨牙发育过程中,Hif1a 的 mRNA 表达持续高,Hif2a 的表达增加,而 Hif3a 的表达非常低。在检查期间,HIFs 在成牙本质细胞和亚成牙本质层的细胞核中的定位确定了它们在成牙本质细胞分化过程中的存在。此外,在分化过程中,较低的乳酸水平和更高的线粒体 Nd1 表达表明糖酵解减少。出生后 HIFs 的核定位表明牙髓特定区域处于缺氧状态,因为氧气需求取决于生理事件,如冠和根牙本质矿化。

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