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使用微反应器制备羟基磷灰石纳米粒子及其蛋白质吸附特性。

Preparation of calcium hydroxyapatite nanoparticles using microreactor and their characteristics of protein adsorption.

机构信息

School of Chemistry, Osaka University of Education, 4-698-1Asahigaoka, Kashiwara-shi, Osaka 582-8582, Japan.

出版信息

J Phys Chem B. 2011 Feb 3;115(4):653-9. doi: 10.1021/jp110441e. Epub 2010 Dec 16.

DOI:10.1021/jp110441e
PMID:21162543
Abstract

The calcium hydroxyapatite Ca(10)(PO(4))(6)(OH)(2) (Hap) nanoparticles were prepared by using microreactor and employed these Hap nanoparticles to clarify the adsorption behavior of proteins. The size of Hap particles produced by the microreactor reduced in the order of a hardness of the reaction conditions for mixing Ca(OH)(2) and H(3)PO(4) aqueous solutions, such as flow rates of both solutions and temperature. Finally, the size of the smallest Hap nanoparticle became 2 × 15 nm(2), similar to that of BSA molecule (4 × 14 nm(2)). It is noteworthy that the smallest Hap nanoparticles still possesses rodlike shape, suggesting that particles are grown along c-axis even though the reactants mixed very rapidly in narrow channels of the microreactors. The X-ray diffraction patterns of the Hap nanoparticles revealed that the crystallinity of the materials produced by the microreactor is low. The FTIR measurement indicated that the Hap nanoparticles produced by microreactor were carbonate-substituted type B Hap, where the carbonate ions replace the phosphate ions in the crystal lattice. All the adsorption isotherms of acidic bovine serum albumin (BSA), neutral myoglobin (MGB), and basic lysozyme (LSZ) onto Hap nanoparticles from 1 × 10(-4) mol/dm(3) KCl solution were the Langmuirian type. The saturated amounts of adsorbed BSA (n(S)(BSA)) for the Hap nanoparticles produced by microreactor were decreased with decrease in the mean particle length, and finally it reduced to zero for the smallest Hap nanoparticles. Similar results were observed for the adsorption of LSZ; the saturated amounts of adsorbed LSZ (n(S)(LSZ)) also reduced to zero for the smallest Hap nanoparticles. However, in the case of MGB, the saturated mounts of adsorbed MGB (n(S)(MGB)) are also depressed with decreased in their particle size, but about half of MGB molecules still adsorbed onto the smallest Hap nanoparticles. This difference in the protein adsorption behavior was explained by the difference in the size and flexibility of three kinds of proteins. The reduction of n(S)(BSA) is due to the decrease in the fraction of C sites on the side face of each Hap nanoparticle; i.e., there is not enough area left on the nanoparticle surface to adsorb large BSA molecules even though the BSA molecules are soft and their conformations are alterable. The reduction of n(S)(LSZ) was explained by the reduction of P sites. Further, rigidity of the LSZ molecules was given another possibility of the depression of n(S)(LSZ) for the Hap nanoparticles. However, MGB molecules with small and soft structure were adsorbed on the Hap nanoparticle surface by changing their conformation. We could control the amounts of adsorbed proteins by changing the particle size of Hap in the nanometer range and kinds of proteins. These obtained results may be useful for developing biomimetic materials for bone grafts and successful surgical devices in the biochemical field.

摘要

羟基磷灰石 Ca(10)(PO(4))(6)(OH)(2)(Hap)纳米粒子是通过微反应器制备的,并将这些 Hap 纳米粒子用于澄清蛋白质的吸附行为。通过微反应器生产的 Hap 颗粒的尺寸按混合 Ca(OH)(2)和 H(3)PO(4)水溶液的反应条件的硬度顺序减小,例如两种溶液的流速和温度。最后,最小的 Hap 纳米颗粒的尺寸变为 2×15nm(2),与 BSA 分子(4×14nm(2))相似。值得注意的是,即使反应物在微反应器的狭窄通道中快速混合,最小的 Hap 纳米颗粒仍具有棒状形状,表明颗粒沿 c 轴生长。Hap 纳米粒子的 X 射线衍射图案表明,微反应器生产的材料的结晶度较低。FTIR 测量表明,微反应器生产的 Hap 纳米粒子为碳酸盐取代的 B 型 Hap,其中碳酸根离子取代晶格中的磷酸根离子。从 1×10(-4)mol/dm(3)KCl 溶液中吸附酸性牛血清白蛋白(BSA)、中性肌红蛋白(MGB)和碱性溶菌酶(LSZ)到 Hap 纳米粒子的所有吸附等温线均为 Langmuir 型。微反应器生产的 Hap 纳米粒子吸附 BSA 的饱和量(n(S)(BSA))随平均颗粒长度的减小而减小,最后对于最小的 Hap 纳米粒子减小到零。对于 LSZ 的吸附也观察到了类似的结果;吸附的 LSZ 的饱和量(n(S)(LSZ))也减小到零对于最小的 Hap 纳米粒子。然而,对于 MGB,吸附的 MGB 的饱和量(n(S)(MGB))也随其粒径的减小而减小,但仍有约一半的 MGB 分子吸附到最小的 Hap 纳米粒子上。这种蛋白质吸附行为的差异可以通过三种蛋白质的大小和灵活性的差异来解释。n(S)(BSA)的减少是由于每个 Hap 纳米粒子侧面 C 位的分数减少;也就是说,即使 BSA 分子柔软且构象可改变,纳米粒子表面上仍没有足够的区域来吸附大的 BSA 分子。n(S)(LSZ)的减少可以用 P 位的减少来解释。此外,LSZ 分子的刚性也使 Hap 纳米粒子上 n(S)(LSZ)的减少成为可能。然而,具有小而柔软结构的 MGB 分子通过改变其构象吸附在 Hap 纳米粒子表面上。通过改变 Hap 的粒径和蛋白质的种类,我们可以控制吸附的蛋白质的量。这些结果可能有助于开发用于骨移植和生化领域成功手术器械的仿生材料。

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