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妊娠期蛋白质限制下的下颌骨发育:细胞和分子机制。

Mandible development under gestational protein restriction: cellular and molecular mechanisms.

机构信息

Fetal Programming and Hydroelectrolyte Metabolism Laboratory, Department of Internal Medicine, FCM, Campinas State University (UNICAMP), Campinas, SP, Brazil.

Department of Restorative Dentistry, Dental Materials Division, Piracicaba Dental School, UNICAMP, Piracicaba, SP, Brazil.

出版信息

J Mol Histol. 2024 Oct;55(5):937-953. doi: 10.1007/s10735-024-10242-0. Epub 2024 Aug 6.

Abstract

Insufficient evidence regarding how maternal undernutrition affects craniofacial bone development persists. With its unique focus on the impact of gestational protein restriction on calvaria and mandible osteogenesis, this study aims to fill, at least in part, this gap. Female mice were mated and randomized into NP (normal protein) or LP (low protein) groups. On the 18th gestational day (GD), male embryos were collected and submitted to microtomography (µCT), scanning electron microscopy (SEM), energy-dispersive X-ray spectroscopy (EDS), PCR, and autophagy dynamic analyses. The study shows that the LP offspring exhibited lower body mass than the NP group, with µCT analysis revealing no volumetric differences in fetus's head. EDS analysis showed lower calcium and higher phosphorus percentages in mandibles and calvaria. SEM assessment evidenced higher hydroxyapatite crystal-like (HC) deposition on the calvaria surface in LP fetus. Conversely, lower HC deposition was observed on the mandible surface, suggesting delayed matrix mineralization in LP fetuses with a higher percentage of collagen fibers in the mandible bone. The autophagy process was reduced in the mesenchyme of LP fetuses. PCR array analysis of 84 genes revealed 27 genes with differential expression in the LP progeny-moreover, increased mRNA levels of Akt1, Mtor, Nfkb, and Smad1 in the LP offspring. In conclusion, the results suggest that gestational protein restriction anticipated bone differentiation in utero, before 18GD, where this process is reduced compared to the control, leading to the reduction in bone area at 15 postnatal day previously observed. These findings provide insights into the molecular and cellular mechanisms of mandible development and suggest potential implications for the Developmental Origins of Health and Disease (DOHaD).

摘要

关于母体营养不良如何影响颅面骨发育的证据仍然不足。本研究特别关注妊娠期蛋白质限制对颅骨和下颌骨骨生成的影响,旨在部分填补这一空白。将雌性小鼠交配并随机分为 NP(正常蛋白)或 LP(低蛋白)组。在第 18 天妊娠期(GD),收集雄性胚胎并进行微 CT(µCT)、扫描电子显微镜(SEM)、能谱分析(EDS)、PCR 和自噬动态分析。研究表明,LP 后代的体重低于 NP 组,µCT 分析显示胎儿头部体积无差异。EDS 分析显示下颌骨和颅骨中的钙百分比降低,磷百分比升高。SEM 评估表明 LP 胎儿颅骨表面羟磷灰石晶体样(HC)沉积较高。相反,下颌骨表面观察到 HC 沉积较低,表明 LP 胎儿的基质矿化延迟,下颌骨中的胶原纤维百分比较高。LP 胎儿间充质中的自噬过程减少。对 84 个基因的 PCR 阵列分析显示 LP 后代中有 27 个基因表达差异——此外,LP 后代中 Akt1、Mtor、Nfkb 和 Smad1 的 mRNA 水平升高。总之,结果表明,妊娠期蛋白质限制在宫内提前于 18GD 预期骨分化,与对照组相比,该过程减少,导致之前观察到的 15 日龄后骨面积减少。这些发现提供了对下颌骨发育的分子和细胞机制的深入了解,并暗示了发育起源的健康和疾病(DOHaD)的潜在影响。

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