Chewing-Activated TRPV4/PIEZO1–HIF-1α–Zn Axes in a Rat Periodontal Complex

IF 5.7 1区医学 Q1 DENTISTRY, ORAL SURGERY & MEDICINE

Journal of Dental Research Pub Date : 2025-01-29 DOI:10.1177/00220345241294001

Y. Wang, B.H. Lee, Z. Yang, T.J. Ho, H. Ci, B. Jackson, T. Pushon, B. Wang, J. Levy, S.P. Ho

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引用次数: 0

Abstract

The upstream mechanobiological pathways that regulate the downstream mineralization rates in periodontal tissues are limitedly understood. Herein, we spatially colocalized and correlated compression and tension strain profiles with the expressions of mechanosensory ion channels (MS-ion) TRPV4 and PIEZO1, biometal zinc, mitochondrial function marker ( MFN2), cell senescence indicator ( p16), and oxygen status marker hypoxia-inducible factor-1α ( HIF-1α) in rats fed hard and soft foods. The observed zinc and related cellular homeostasis in vivo were ascertained by TRPV4 and PIEZO1 agonists and antagonists on human periodontal ligament fibroblasts ex vivo. Four-week-old male Sprague-Dawley rats were fed hard ( n = 3) or soft ( n = 3) foods for 4 wk (in vivo). Significant changes in alveolar socket and root shapes with decreased periodontal ligament space and increased cementum volume fraction were observed in maxillae on reduced loads (soft food). Reduced loads impaired distally localized compression-stimulated PIEZO1 and mesially localized tension-stimulated TRPV4, decreased mitochondrial function ( MFN2), and increased cell senescence in mesial and distal periodontal regions. The switch in HIF-1α from hard food–distal to soft food–mesial indicated a plausible effect of shear-regulated blood and oxygen flows in the periodontal complex. Blunting or activating TRPV4 or PIEZO1 MS-ion channels by channel-specific antagonists or agonists in human periodontal ligament fibroblast cultures (in vitro) indicated a positive correlation between zinc levels and zinc transporters but not with MS-ion channel expressions. The effects of reduced chewing loads in vivo were analogous to TRPV4 and PIEZO1 antagonists in vitro. Study results collectively illustrated that tension-induced TRPV4 and compression-induced PIEZO1 activations are necessary for cell metabolism. An increased hypoxic state with reduced functional loads can be a conducive environment for cementum growth. From a practical standpoint, dose rate–controlled loads can modulate tension and compression-specific MS-ion channel activation, cellular zinc, and HIF-1α transcription. These mechanobiochemical events indicate the plausible catalytic role of biometal zinc in mineralization, periodontal maintenance, and dentoalveolar joint function.

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咀嚼激活大鼠牙周复合体TRPV4/ PIEZO1-HIF-1α-Zn轴

调控牙周组织下游矿化率的上游机械生物学途径尚不清楚。在此，我们将大鼠的压缩和拉伸应变曲线与机械感觉离子通道（MS-ion） TRPV4和PIEZO1、生物金属锌、线粒体功能标志物（MFN2）、细胞衰老指标（p16）和氧状态标志物缺氧诱导因子-1α (HIF-1α)的表达进行了空间共定位和关联。通过TRPV4和PIEZO1激动剂和拮抗剂对人牙周韧带成纤维细胞的体外作用，确定体内观察到的锌和相关的细胞稳态。4周龄雄性Sprague-Dawley大鼠分别饲喂硬（n = 3）或软（n = 3）食物4周（体内）。在减少负荷（软性食物）下，上颌牙骨质体积分数增加，牙周韧带间隙减小，牙槽窝和牙根形状发生显著变化。负荷减少损害了远端受压刺激的PIEZO1和近端受压刺激的TRPV4，降低了线粒体功能（MFN2），增加了近端和远端牙周区域的细胞衰老。HIF-1α从硬食物远端到软食物近端的转换表明，在牙周复合体中剪切调节的血液和氧气流动可能起作用。在体外培养的人牙周韧带成纤维细胞中，通过通道特异性拮抗剂或激动剂钝化或激活TRPV4或PIEZO1 ms离子通道表明锌水平与锌转运蛋白呈正相关，但与ms离子通道表达无关。减少咀嚼负荷在体内的作用类似于TRPV4和PIEZO1拮抗剂在体外的作用。研究结果共同表明，张力诱导的TRPV4和压缩诱导的PIEZO1激活是细胞代谢所必需的。增加的缺氧状态和减少的功能负荷可以是一个有利于牙骨质生长的环境。从实际的角度来看，剂量率控制负载可以调节张力和压缩特异性的ms离子通道激活、细胞锌和HIF-1α转录。这些机械生化事件表明生物金属锌在矿化、牙周维护和牙槽关节功能方面的催化作用。

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来源期刊

Journal of Dental Research 医学-牙科与口腔外科

CiteScore

15.30

自引率

3.90%

发文量

155

审稿时长

3-8 weeks

期刊介绍： The Journal of Dental Research (JDR) is a peer-reviewed scientific journal committed to sharing new knowledge and information on all sciences related to dentistry and the oral cavity, covering health and disease. With monthly publications, JDR ensures timely communication of the latest research to the oral and dental community.