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Regulatory inhibition of biological tissue mineralization by calcium phosphate through post-nucleation shielding by fetuin-A

机译:胎球蛋白A的成核后屏蔽对磷酸钙对生物组织矿化的调节抑制作用

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摘要

In vertebrates, insufficient availability of calcium and inorganic phosphate ions in extracellular fluids leads to loss of bone density and neuronal hyper-excitability. To counteract this problem, calcium ions are usually present at high concentrations throughout bodily fluids—at concentrations exceeding the saturation point. This condition leads to the opposite situation where unwanted mineral sedimentation may occur. Remarkably, ectopic or out-of-place sedimentation into soft tissues is rare, in spite of the thermodynamic driving factors. This fortunate fact is due to the presence of auto-regulatory proteins that are found in abundance in bodily fluids. Yet, many important inflammatory disorders such as atherosclerosis and osteoarthritis are associated with this undesired calcification. Hence, it is important to gain an understanding of the regulatory process and the conditions under which it can go awry. In this manuscript, we extend mean-field continuum classical nucleation theory of the growth of clusters to encompass surface shielding. We use this formulation to study the regulation of sedimentation of calcium phosphate salts in biological tissues through the mechanism of post-nuclear shielding of nascent mineral particles by binding proteins. We develop a mathematical description of this phenomenon using a countable system of hyperbolic partial differential equations. A critical concentration of regulatory protein is identified as a function of the physical parameters that describe the system.
机译:在脊椎动物中,细胞外液中钙和无机磷酸根离子的利用率不足会导致骨密度降低和神经元过度兴奋。为了解决这个问题,钙离子通常在整个体液中都以高浓度存在-浓度超过饱和点。这种情况导致了相反的情况,可能发生不需要的矿物沉淀。值得注意的是,尽管有热力学驱动因素,但异位或异位沉积进入软组织的情况仍然很少。这个幸运的事实是由于体液中大量存在的自动调节蛋白的存在。然而,许多重要的炎症性疾病,例如动脉粥样硬化和骨关节炎与这种不希望的钙化有关。因此,重要的是要了解监管程序及其可能出现的状况。在本手稿中,我们扩展了簇生长的均值连续谱经典成核理论,以涵盖表面屏蔽。我们使用这种配方来研究通过结合蛋白对新生矿物质颗粒进行核后屏蔽的机制,从而研究磷酸钙盐在生物组织中的沉积调节。我们使用可数的双曲型偏微分方程组对此现象进行了数学描述。调节蛋白的临界浓度被确定为描述系统的物理参数的函数。

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