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前核簇在胶原蛋白磷酸钙矿化中的作用。

Involvement of prenucleation clusters in calcium phosphate mineralization of collagen.

机构信息

State Key Laboratory of Military Stomatology & National Clinical Research Center for Oral Diseases & Shaanxi Key Laboratory of Stomatology, Department of Prosthodontics, School of Stomatology, The Fourth Military Medical University, Xi'an, Shaanxi, China.

Department of Chemical and Biological Engineering, University of Colorado Boulder, Boulder, CO, USA.

出版信息

Acta Biomater. 2021 Jan 15;120:213-223. doi: 10.1016/j.actbio.2020.07.038. Epub 2020 Jul 22.

Abstract

Involvement of thermodynamically-stable prenucleation clusters (PNCs) in the biomineralization of collagen has been speculated since their existence was reported in mineralization systems. It has been hypothesized that intrafibrillar mineralization proceeds via nucleation of inhibitor-stabilized intermediates produced by liquid-liquid separation (aka. polymer-induced liquid precursors; PILPs). Here, the contribution of PNCs and PILPs to calcium phosphate intrafibrillar mineralization of collagen was examined in a model with a semipermeable membrane that excludes nucleation inhibitor-stabilized PILPs from reaching the collagen fibrils, using cryogenic electron microscopy of reconstituted fibrils and conventional transmission electron microscopy of collagen sponges. Molecular dynamics simulation with the Interface force field (IFF) was used to confirm the existence of PILPs with amorphous calcium phosphate and elucidate details of the dynamics. Furthermore, intrafibrillar mineralization of single collagen fibrils was experimentally observed with unstabilized PNCs when anionic/cationic polyelectrolytes were used to establish Donnan equilibrium across the semipermeable membrane. Molecular dynamics simulation verified PNC formation within the collagen intrafibrillar gap zones at the atomic scale and explained the role of external PILPs. The PILPs decrease the interfibrillar water content and increase the interfibrillar ionic concentration. Nevertheless, intrafibrillar mineralization of collagen sponges with PNCs alone was inefficacious, being constrained by competition from extrafibrillar mineral precipitation. STATEMENT OF SIGNIFICANCE: Compared with conventional PILP-based intrafibrillar mineralization, mineralization of collagen fibrils using unstabilized PNCs is constrained by competition from extrafibrillar mineral deposition. The narrow window of opportunity for PNCs to produce intrafibrillar mineralization provides a plausible explanation for the feasibility of nucleation inhibitor-free intrafibrillar apatite assembly during reconstitution of type I collagen.

摘要

自从在矿化系统中报道了热力学稳定的成核前团聚体(PNC)的存在以来,人们一直推测它们参与了胶原蛋白的生物矿化。有人假设,纤维内矿化是通过抑制剂稳定的中间体在液-液相分离(也称为聚合物诱导的液相前体;PILPs)作用下成核进行的。在这里,在一种使用半透膜的模型中,通过低温电子显微镜对重组纤维和胶原海绵的常规透射电子显微镜检查,研究了 PNC 和 PILP 对胶原蛋白纤维内磷酸钙矿化的贡献。使用界面力场(IFF)的分子动力学模拟来确认具有无定形磷酸钙的 PILP 的存在,并阐明动力学的细节。此外,当使用阴离子/阳离子聚电解质在半透膜上建立唐南平衡时,实验观察到未稳定的 PNC 对单根胶原蛋白纤维的纤维内矿化。分子动力学模拟在原子尺度上验证了 PNC 在胶原蛋白纤维内间隙区的形成,并解释了外部 PILP 的作用。PILP 降低了纤维间的含水量并增加了纤维间的离子浓度。然而,仅使用 PNC 的胶原蛋白海绵的纤维内矿化是无效的,因为受到纤维外矿化沉淀的竞争的限制。意义声明:与传统的基于 PILP 的纤维内矿化相比,使用未稳定的 PNC 进行胶原蛋白纤维矿化受到纤维外矿化沉积的竞争限制。PNC 产生纤维内矿化的机会窗口很窄,这为在 I 型胶原蛋白重建过程中无成核抑制剂的纤维内磷灰石组装的可行性提供了合理的解释。

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