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用于结构基因组学的高通量X射线吸收光谱法中的瓶颈与障碍

Bottlenecks and roadblocks in high-throughput XAS for structural genomics.

作者信息

Scott Robert A, Shokes Jacob E, Cosper Nathaniel J, Jenney Francis E, Adams Michael W W

机构信息

Department of Chemistry, University of Georgia, Athens, GA 30602, USA.

出版信息

J Synchrotron Radiat. 2005 Jan;12(Pt 1):19-22. doi: 10.1107/S0909049504028791. Epub 2004 Dec 23.

DOI:10.1107/S0909049504028791
PMID:15616360
Abstract

Structural and functional characterization of the entire protein complement (the proteome) of an organism can provide an infrastructure upon which questions about biological pathways and systems biology can be framed. The technology necessary to perform this proteome-level structural and functional characterization is under development in numerous structural genomics and functional genomics initiatives. Given the ubiquity of metal active sites in a proteome, it seems appropriate to ask whether comprehensive local structural characterization of metal sites within a proteome (metalloproteomics) is either a valid or obtainable goal. With a proteome-wide knowledge of the active-site structures of all metalloproteins, one could start to ask how metal insertion, cluster assembly and metalloprotein expression are affected by growth conditions or developmental status etc. High-throughput X-ray absorption spectroscopy (HTXAS) is being developed as a technology for investigating the metalloproteome. In creating a pipeline from genome to metalloproteome, several bottlenecks to high-throughput determination of metal-site structures must be overcome. For example, automation of arraying small samples for XAS examination must be invented, automation of rapid data collection of multiple low-volume low-concentration samples must be developed, automation of data reduction and analysis must be perfected. Discussed here are the promises and the pitfalls of HTXAS development, including the results of initial feasibility experiments.

摘要

对生物体的整个蛋白质组(蛋白质补体)进行结构和功能表征,可为构建有关生物途径和系统生物学问题的框架提供一个基础架构。众多结构基因组学和功能基因组学计划正在开发进行这种蛋白质组水平结构和功能表征所需的技术。鉴于蛋白质组中金属活性位点的普遍存在,那么追问蛋白质组内金属位点的全面局部结构表征(金属蛋白质组学)是否是一个合理或可实现的目标似乎是恰当的。有了蛋白质组范围内所有金属蛋白活性位点结构的知识,人们就可以开始探究金属插入、簇组装和金属蛋白表达是如何受到生长条件或发育状态等因素影响的。高通量X射线吸收光谱法(HTXAS)正在作为一种研究金属蛋白质组的技术而被开发。在构建从基因组到金属蛋白质组的流程时,必须克服高通量测定金属位点结构的几个瓶颈。例如,必须发明将小样品排列用于X射线吸收光谱检查的自动化方法,必须开发多个低体积低浓度样品的快速数据收集自动化方法,必须完善数据简化和分析的自动化方法。这里讨论的是HTXAS开发的前景和陷阱,包括初步可行性实验的结果。

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