The role of palmitoylation modifications in the regulation of bone cell function, bone homeostasis, and osteoporosis.

IF 4.7 2区 医学 Q2 CELL & TISSUE ENGINEERING
Ximeng Wang, Yuxuan Zhang, Zhidi Lin, Hongli Wang, Guangyu Xu, Xiaosheng Ma
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Abstract

Osteoporosis a is a metabolic bone disease caused by an imbalance in bone homeostasis, which is regulated by osteoblasts and osteoclasts. Protein palmitoylation modification is a post-translational modification that affects protein function, localization, and targeting by attaching palmitoyl groups to specific amino acid residues of proteins. Recent studies have shown that protein palmitoylation is involved in the regulation of osteoclast overproduction, osteoblast migration, osteogenic differentiation, dysfunctional autophagy, and endocrine hormone membrane receptors in osteoporosis. Exactly to what extent palmitoylation modifications can regulate osteoporosis, and whether palmitoylation inhibition can delay osteoporosis, is a key question that needs to be investigated urgently. In this review, we observed that palmitoylation modifications act mainly through two target cells - osteoblasts and osteoclasts - and that the targets of palmitoylation modifications are focused on plasma membrane proteins or cytosolic proteins of the target cells, which tend to assume the role of receiving extracellular signals. We also noted that different palmitoyl transferases acting on different substrate proteins exert conflicting regulation of osteoblast function. We concluded that the regulation of osteocyte function, bone homeostasis, and osteoporosis by palmitoylation modifications is multidimensional, diverse, and interconnected. Perfecting the palmitoylation modification network can enhance our ability to utilize post-translational modifications to resist osteoporosis and lay the foundation for targeting palmitoyl transferases to treat osteoporosis in the future.

棕榈酰化修饰在骨细胞功能、骨稳态和骨质疏松的调节中的作用。
骨质疏松症是由成骨细胞和破骨细胞调节的骨稳态失衡引起的代谢性骨病。蛋白棕榈酰化修饰是一种翻译后修饰,通过将棕榈酰基团连接到蛋白质的特定氨基酸残基上,影响蛋白质的功能、定位和靶向性。最近的研究表明,蛋白棕榈酰化参与了骨质疏松症中破骨细胞过度产生、成骨细胞迁移、成骨分化、功能失调的自噬和内分泌激素膜受体的调节。棕榈酰化修饰究竟能在多大程度上调控骨质疏松,抑制棕榈酰化是否能延缓骨质疏松,是亟待研究的关键问题。在这篇综述中,我们观察到棕榈酰化修饰主要通过两种靶细胞-成骨细胞和破骨细胞起作用,并且棕榈酰化修饰的靶点主要集中在靶细胞的质膜蛋白或细胞质蛋白上,这些蛋白往往承担接收细胞外信号的作用。我们还注意到,不同的棕榈酰转移酶作用于不同的底物蛋白,对成骨细胞功能的调节相互矛盾。我们得出结论,棕榈酰化修饰对骨细胞功能、骨稳态和骨质疏松的调节是多维的、多样的和相互关联的。完善棕榈酰化修饰网络可以增强我们利用翻译后修饰抵抗骨质疏松的能力,为今后靶向棕榈酰转移酶治疗骨质疏松奠定基础。
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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来源期刊
Bone & Joint Research
Bone & Joint Research CELL & TISSUE ENGINEERING-ORTHOPEDICS
CiteScore
7.40
自引率
23.90%
发文量
156
审稿时长
12 weeks
期刊介绍: The gold open access journal for the musculoskeletal sciences. Included in PubMed and available in PubMed Central.
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