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用于生物系统二维和三维分子成像的新型 SIMS 范式。

A new SIMS paradigm for 2D and 3D molecular imaging of bio-systems.

机构信息

Manchester Interdisciplinary Biocentre, School of Chemical Engineering and Analytical Science, The University of Manchester, Manchester, M1 7DN, UK.

出版信息

Anal Bioanal Chem. 2010 Jan;396(1):85-104. doi: 10.1007/s00216-009-2986-3. Epub 2009 Aug 12.

Abstract

With the implementation of focused primary ion beams, secondary ion mass spectrometry (SIMS) has become a significant technique in the rapidly emerging field of mass spectral imaging in the biological sciences. Liquid metal ion guns (LMIG) offered the prospect of sub-100 nm spatial resolution, however this aspiration has yet to be reached for molecular imaging. This brief review shows that using LMIG the limitations of the static limit and low ionization probability will restrict useful imaging to around 2 mum spatial resolution with high-yield molecules. The only prospect of going beyond this in the absence of factors of 100 increase in ionization probability is to use polyatomic ion beams such as C (60) (+) , for which bombardment induced damage is low. In these cases sub-micron imaging becomes possible, using voxels together with molecular depth profiling and 3D imaging. The discussion shows that conventional ToF-SIMS instrumentation then becomes a limitation in that the pulsed ion beam has a very low duty cycle which results in inordinately long analysis times, and pulsing the beam means that high-mass resolution and high spatial resolution are mutually incompatible. New instrumental configurations are described that allow the use of a dc ion beam and separate the mass spectrometry for the ion formation process. Early results from these instruments suggest that sub-micron analysis and imaging with high mass resolution and good ion yields are now realizable, although the low ion yield issue still needs to be solved.

摘要

随着聚焦初级离子束的实施,二次离子质谱(SIMS)已成为生物科学中快速发展的质谱成像领域的一项重要技术。液态金属离子枪(LMIG)提供了达到亚 100nm 空间分辨率的前景,然而,对于分子成像来说,这一目标尚未实现。这篇简短的综述表明,使用 LMIG,静态极限和低电离概率的限制将限制高产量分子的有用成像达到约 2µm 的空间分辨率。在不增加 100 倍电离概率的情况下,唯一有望超越这一限制的方法是使用多原子离子束,如 C(60)(+),其轰击诱导的损伤较低。在这些情况下,使用亚微米级成像成为可能,使用体素进行分子深度剖析和 3D 成像。讨论表明,传统的飞行时间二次离子质谱仪在这方面受到限制,因为脉冲离子束的占空比非常低,导致分析时间过长,而且脉冲化意味着高空间分辨率和高质量分辨率是相互不兼容的。本文描述了新的仪器配置,允许使用直流离子束,并将离子形成过程的质谱分析分开。这些仪器的早期结果表明,现在可以实现具有高质量分辨率和良好离子产率的亚微米级分析和成像,尽管离子产率低的问题仍需要解决。

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