Attenuated NIX in impaired mitophagy contributes to exacerbating cellular senescence in experimental periodontitis under hyperglycemic conditions.

The FEBS journal Pub Date : 2024-12-24 DOI:10.1111/febs.17352

Danni Song, Beibei Chen, Tianfan Cheng, Lijian Jin, Jiangfeng He, Yongming Li, Chongshan Liao

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Abstract

Premature accumulation of senescent cells results in tissue destruction, and it is one of the potential primary mechanisms underlying the accelerated progression of diabetes and periodontitis. However, whether this characterized phenomenon could account for periodontal pathogenesis under hyperglycemic conditions remains unclear. In this study, we assessed the senescent phenotypic changes in experimental periodontitis under hyperglycemic conditions. Next, we investigated the mitochondrial function and the potential mitophagy pathways in cellular senescence in vitro and in vivo. Our findings showed that significant senescence occurred in the gingival tissues of diabetic periodontitis mice with increased expression of senescence-related protein p21^Cip1 and the senescence-associated secretory phenotype response as well as the decreased expression of NIP3-like protein X (NIX), a mitochondrial receptor. Likewise, we showed that mitochondrial dysfunction (e.g., reduction of mitochondrial membrane potential and accumulation of reactive oxygen species) was attributed to cellular senescence in: human periodontal ligament cells (hPDLCs) through hyperglycemia-induced and Porphyromonas gingivalis lipopolysaccharide (P.g-LPS)-induced oxidative stresses. Notably, the resulting reduced NIX expression was reversed by the use of the mitochondrial reactive oxygen species (ROS) scavenger N-acetyl-l-cysteine (NAC), thus correcting the mitochondrial dysfunction. We further verified the expression of inflammatory mediators and senescence-related factors in mice gingival tissues and identified the possible regulatory pathways. Taken together, our work demonstrates the critical role of cellular senescence and mitochondrial dysfunction in periodontal pathogenesis under hyperglycemic conditions. Hence, restoration of mitochondrial function may be a potential novel therapeutic approach to tackling periodontitis in diabetic patients.

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在高血糖条件下实验性牙周炎中，线粒体自噬受损的NIX减弱有助于加剧细胞衰老。

衰老细胞的过早积累导致组织破坏，这是糖尿病和牙周炎加速发展的潜在主要机制之一。然而，这种特征现象是否可以解释在高血糖条件下牙周发病机制尚不清楚。在这项研究中，我们评估了实验性牙周炎在高血糖条件下的衰老表型变化。接下来，我们在体外和体内研究了细胞衰老过程中线粒体的功能和可能的线粒体自噬途径。我们的研究结果表明，糖尿病牙周炎小鼠的牙龈组织发生了明显的衰老，衰老相关蛋白p21Cip1的表达增加，衰老相关的分泌表型反应增加，线粒体受体nip3样蛋白X （NIX）的表达减少。同样，我们发现，通过高血糖诱导和牙龈卟啉单胞菌脂多糖（P.g-LPS）诱导的氧化应激，人牙周韧带细胞（hPDLCs）的细胞衰老可导致线粒体功能障碍（例如，线粒体膜电位降低和活性氧积累）。值得注意的是，使用线粒体活性氧（ROS）清除剂n -乙酰-l-半胱氨酸（NAC）可以逆转NIX表达的降低，从而纠正线粒体功能障碍。我们进一步验证了炎症介质和衰老相关因子在小鼠牙龈组织中的表达，并确定了可能的调控途径。综上所述，我们的工作证明了细胞衰老和线粒体功能障碍在高血糖条件下牙周发病机制中的关键作用。因此，恢复线粒体功能可能是治疗糖尿病患者牙周炎的一种潜在的新治疗方法。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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