细菌的冷冻替代研究

Lori L. Graham
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引用次数: 38

摘要

通常,细菌结构模型将从细胞群体的大量分析中获得的生化数据与单个细胞的电子显微镜观察相结合。生物电子显微镜专用的低温技术的最新发展已经开始取代常规的程序,如传统的薄切片。其中一种冷冻技术,冷冻替代,结合了超快速冷冻和标准显微切片方法的优点。这种技术特别适合于细菌结构的检查,并产生了与生化数据一致的额外超微结构信息,但通常挑战传统显微镜方法获得的细胞结构模型。除了更准确地保留细胞成分的空间分布外,冷冻替代已成功地与免疫化学标记技术相结合,并使细胞内和细胞表面的特定分子的鉴定和定位成为可能。在这篇综述中,我描述了目前对细菌超微结构的看法,并根据最近冷冻替代研究获得的新数据进行了修改。
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Freeze-substitution studies of bacteria

Typically, models of bacterial structure combine biochemical data obtained from bulk analyses of cell populations with electron microscopic observation of individual cells. Recent development of a battery of cryotechniques specific for biological electron microscopy have begun to supercede routine procedures such as conventional thin sectioning. One of these cryotechniques, freeze-substitution, combines the advantages of ultrarapid freezing with standard microtomy methods. This technique is particularly well suited to the examination of bacterial structure and has yielded additional ultrastructural information consistent with biochemical data but often challenging models of cell structure obtained from conventional microscopical methods. In addition to retaining more accurately the spatial distribution of cell components, freeze-substitution has been successfully combined with immunochemical labelling techniques and has enabled identification and localization of specific molecules both within the cell and on the cell surface. In this review, I describe current ideas on bacterial ultrastructure, modified in accordance with new data obtained from recent freeze-substitution studies.

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