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Phospholipases of Mineralization Competent Cells and Matrix Vesicles: Roles in Physiological and Pathological Mineralizations

机译:矿化感受态细胞和基质囊泡的磷脂酶:在生理和病理学矿化中的作用

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摘要

The present review aims to systematically and critically analyze the current knowledge on phospholipases and their role in physiological and pathological mineralization undertaken by mineralization competent cells. Cellular lipid metabolism plays an important role in biological mineralization. The physiological mechanisms of mineralization are likely to take place in tissues other than in bones and teeth under specific pathological conditions. For instance, vascular calcification in arteries of patients with renal failure, diabetes mellitus or atherosclerosis recapitulates the mechanisms of bone formation. Osteoporosis—a bone resorbing disease—and rheumatoid arthritis originating from the inflammation in the synovium are also affected by cellular lipid metabolism. The focus is on the lipid metabolism due to the effects of dietary lipids on bone health. These and other phenomena indicate that phospholipases may participate in bone remodelling as evidenced by their expression in smooth muscle cells, in bone forming osteoblasts, chondrocytes and in bone resorbing osteoclasts. Among various enzymes involved, phospholipases A1 or A2, phospholipase C, phospholipase D, autotaxin and sphingomyelinase are engaged in membrane lipid remodelling during early stages of mineralization and cell maturation in mineralization-competent cells. Numerous experimental evidences suggested that phospholipases exert their action at various stages of mineralization by affecting intracellular signaling and cell differentiation. The lipid metabolites—such as arachidonic acid, lysophospholipids, and sphingosine-1-phosphate are involved in cell signaling and inflammation reactions. Phospholipases are also important members of the cellular machinery engaged in matrix vesicle (MV) biogenesis and exocytosis. They may favour mineral formation inside MVs, may catalyse MV membrane breakdown necessary for the release of mineral deposits into extracellular matrix (ECM), or participate in hydrolysis of ECM. The biological functions of phospholipases are discussed from the perspective of animal and cellular knockout models, as well as disease implications, development of potent inhibitors and therapeutic interventions.
机译:本综述旨在系统和批判性地分析磷脂酶的当前知识及其在矿化感受态细胞承担的生理和病理学矿化中的作用。细胞脂质代谢在生物矿化中起重要作用。在特定病理条件下,矿化的生理机制很可能发生在骨骼和牙齿以外的组织中。例如,肾功能衰竭,糖尿病或动脉粥样硬化患者的动脉血管钙化概括了骨形成的机制。骨质疏松症(一种骨吸收疾病)和源自滑膜炎症的类风湿关节炎也受到细胞脂质代谢的影响。由于饮食脂质对骨骼健康的影响,重点在于脂质代谢。这些现象和其他现象表明,磷脂酶可能参与骨骼重塑,正如其在平滑肌细胞,成骨成骨细胞,软骨细胞和骨吸收破骨细胞中的表达所证明的那样。在涉及的各种酶中,磷脂酶A1或A2,磷脂酶C,磷脂酶D,自分泌蛋白和鞘磷脂酶在矿化能力强的矿化和细胞成熟的早期阶段参与膜脂质重塑。许多实验证据表明,磷脂酶通过影响细胞内信号传导和细胞分化,在矿化的各个阶段发挥作用。脂质代谢产物(如花生四烯酸,溶血磷脂和1鞘氨醇)参与细胞信号传导和炎症反应。磷脂酶也是参与基质囊泡(MV)生物发生和胞吐作用的细胞机制的重要成员。它们可能有助于MV内部矿物质的形成,可能催化MV膜破裂,这是矿物质沉积物释放到细胞外基质(ECM)中所必需的,或参与ECM的水解。从动物和细胞敲除模型的角度讨论磷脂酶的生物学功能,以及疾病的影响,有效抑制剂的开发和治疗干预。

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