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High resolution light microscopy of nanoforms

机译:纳米形态的高分辨率光学显微镜

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We developed a high resolution light imaging system. Diffraction gratings with 100 nm width lines as well as less than 100 nm size features of different-shaped objects are clearly visible on a calibrated microscope test slide (Vainrub et al., Optics Letters, 2006, 31, 2855). The two-point resolution increase results from a known narrowing of the central diffraction peak for the annular aperture. Better visibility and advanced contrast of the smallest features in the image are due to enhancement of high spatial frequencies in the optical transfer function. The imaging system is portable, low energy, and battery operated. It has been adapted to use in both transmitting and reflecting light. It is particularly applicable for motile nanoform systems where structure and functions can be depicted in real time. We have isolated micrometer and submicrometer particles, termed proteons, from human and animal blood. Proteons form by reversible seeded aggregation of proteins around proteon nucleating centers (PNCs). PNCs are comprised of l-2nm metallic nanoclusters containing 40-300 atoms. Proteons are capable of spontaneous assembling into higher nanoform systems assuming structure of complicated topology. The arrangement of complex proteon system mimics the structure of a small biological cell. It has structures that imitate membrane and nucleolus or nuclei. Some of these nanoforms are motile. They interact and divide. Complex nanoform systems can spontaneously reduce to simple proteons. The physical properties of these nanoforms could shed some light on the properties of early life forms or forms at extreme conditions.
机译:我们开发了高分辨率的光成像系统。在校准的显微镜测试载玻片上可以清晰地看到具有100 nm宽度线以及小于100 nm尺寸特征的不同形状物体的衍射光栅(Vainrub等人,Optics Letters,2006,31,2855)。两点分辨率的提高是由于环形孔的中心衍射峰变窄而导致的。图像中最小特征的更好的可见性和更高的对比度归因于光学传递函数中高空间频率的增强。该成像系统是便携式的,低能耗的,并且由电池供电。它适用于透射和反射光。它特别适用于可实时显示结构和功能的运动型纳米形式的系统。我们已经从人和动物的血液中分离出称为蛋白质的微米级和亚微米级颗粒。蛋白质是通过蛋白质成核中心(PNC)周围的种子的可逆种子聚集形成的。 PNC由包含40-300个原子的1-2 nm金属纳米簇组成。假设拓扑结构复杂,蛋白质可以自发组装成更高的纳米形式的系统。复杂蛋白系统的排列模仿了小型生物细胞的结构。它具有模仿膜和核仁或核的结构。这些纳米形式中的一些是可运动的。他们相互作用和分裂。复杂的纳米形式的系统可以自发地还原为简单的蛋白质。这些纳米形式的物理性质可以为早期生命形式或极端条件下的形式的性质提供一些启示。

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