Physical and Life Sciences Directorate, Lawrence Livermore National Laboratory, Livermore, CA 94551, USA.
Proc Natl Acad Sci U S A. 2010 Jan 5;107(1):11-5. doi: 10.1073/pnas.0908205107. Epub 2009 Dec 14.
In vitro observations have revealed major effects on the structure, growth, and composition of biomineral phases, including stabilization of amorphous precursors, acceleration and inhibition of kinetics, and alteration of impurity signatures. However, deciphering the mechanistic sources of these effects has been problematic due to a lack of tools to resolve molecular structures on mineral surfaces during growth. Here we report atomic force microscopy investigations using a system designed to maximize resolution while minimizing contact force. By imaging the growth of calcium-oxalate monohydrate under the influence of aspartic-rich peptides at single-molecule resolution, we reveal how the unique interactions of polypeptides with mineral surfaces lead to acceleration, inhibition, and switching of growth between two distinct states. Interaction with the positively charged face of calcium-oxalate monohydrate leads to formation of a peptide film, but the slow adsorption kinetics and gradual relaxation to a well-bound state result in time-dependent effects. These include a positive feedback between peptide adsorption and step inhibition described by a mathematical catastrophe that results in growth hysteresis, characterized by rapid switching from fast to near-zero growth rates for very small reductions in supersaturation. Interactions with the negatively charged face result in formation of peptide clusters that impede step advancement. The result is a competition between accelerated solute attachment and inhibition due to blocking of the steps by the clusters. The findings have implications for control of pathological mineralization and suggest artificial strategies for directing crystallization.
体外观察揭示了对生物矿物相的结构、生长和组成的重大影响,包括无定形前体的稳定化、动力学的加速和抑制以及杂质特征的改变。然而,由于缺乏在生长过程中解析矿物表面分子结构的工具,这些影响的机制来源一直难以确定。在这里,我们报告了使用旨在最大化分辨率同时最小化接触力的系统进行原子力显微镜研究的结果。通过以单分子分辨率成像富天冬氨酸多肽对一水合草酸钙生长的影响,我们揭示了多肽与矿物表面的独特相互作用如何导致生长在两种不同状态之间的加速、抑制和切换。与一水合草酸钙的正电荷面相互作用导致多肽膜的形成,但由于吸附动力学缓慢且逐渐松弛到良好结合状态,导致时间依赖性效应。这些包括多肽吸附和阶跃抑制之间的正反馈,由数学突变描述,导致生长滞后,其特征是过饱和度非常小的降低导致快速从快速生长速率切换到接近零的生长速率。与带负电荷的面相互作用导致形成阻碍阶跃前进的肽簇。结果是由于簇阻碍台阶而导致溶质附着的加速和抑制之间的竞争。这些发现对控制病理性矿化具有意义,并为指导结晶提供了人工策略。