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首页> 外文期刊>Polyhedron: The International Journal for Inorganic and Organometallic Chemistry >Compartmental control of mineral formation: adaptation of a biomineralization strategy for biomedical use
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Compartmental control of mineral formation: adaptation of a biomineralization strategy for biomedical use

机译:矿物质形成区室控制:生物矿化策略在生物医学中的应用

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A common biomineralization strategy is the use of lipid vesicle compartments to sequester ions, control ion transport, and to control the shape and size of inorganic mineral particles deposited within developing tissues. In this paper, we describe an adaptation of this bioinspired strategy for inducing rapid formation of calcium phosphates for potential medical and dental use. Calcium and inorganic phosphate salts were separately loaded into temperature-sensitive liposomes composed of 90% 1,2-bis(palmitoyl)-sn-glycero-3-phosphocholine and 10% 1,2-bis(myristoyl) -sn-glycero-3 -phosphocholine. Leakage of calcium and inorganic phosphate from liposomes stored at room temperature was negligible over a period of several weeks. Calcium-loaded liposomes released entrapped calcium when heated to 36-37 degrees C, while phosphate-loaded liposomes released entrapped inorganic phosphate (P-i) at slightly lower temperatures (33-34 degrees C). Release of entrapped ions at this temperature was due to increased permeability of phospholipid bilayers at the lipid chain melting temperature. Aqueous suspensions containing mixtures of calcium and P-i-loaded liposomes formed calcium phosphate mineral when heated to 37 degrees C, as indicated by a rapid drop in suspension pH from 7 to approximately 5. This result was consistent with diffusion of both calcium and phosphate ions out of the liposomes and their reaction to form calcium phosphate mineral. Such a strategy could be used in medical and dental procedures to induce rapid inorganic mineral formation from an injectable liposome-containing fluid. This was illustrated by applying a liposome suspension to warm human dentin and enamel surfaces, which resulted in deposition of calcium phosphate minerals onto the tissue substrates. (C) 2000 Elsevier Science Ltd All rights reserved. [References: 36]
机译:常见的生物矿化策略是使用脂质囊泡隔室隔离离子,控制离子传输并控制沉积在发育组织中的无机矿物颗粒的形状和大小。在本文中,我们描述了这种生物启发策略的适应性,可诱导快速形成潜在的医学和牙科用途的磷酸钙。将钙盐和无机磷酸盐分别装入温度敏感的脂质体中,该脂质体由90%1,2-双(棕榈酰基)-sn-甘油-3-磷酸胆碱和10%1,2-双(肉豆蔻酰基)-sn-甘油-3组成-磷酸胆碱。在室温下储存的脂质体中钙和无机磷酸盐的泄漏在几周内可以忽略不计。当加热到36-37摄氏度时,负载钙的脂质体释放出夹带的钙,而在稍低的温度(33-34摄氏度)下,负载磷的脂质体释放出夹带的无机磷酸盐(P-i)。在此温度下捕获的离子的释放是由于在脂链熔化温度下磷脂双层的渗透性增加。悬浮液的pH从7急剧下降到大约5时,含有钙和Pi脂质体混合物的水悬浮液在加热到37摄氏度时会形成磷酸钙矿物质。该结果与钙和磷酸根离子的扩散相一致。脂质体及其反应形成磷酸钙矿物质。可以将这种策略用于医学和牙科程序中,以从可注射的含脂质体的液体中快速形成无机矿物质。通过将脂质体悬浮液应用于温暖的人牙本质和牙釉质表面,可以说明磷酸钙矿物质沉积在组织基质上的情况。 (C)2000 Elsevier Science Ltd保留所有权利。 [参考:36]

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