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Cytoplasmic matrix in embedment-free electron microscopy: non-molecular biological histology.

机译:无嵌入电子显微镜中的细胞质基质:非分子生物学组织学。

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Embedment-free electron microscopy using polyethylene glycol as a transient embedment has revealed that slender strands, originally termed microtrabeculae and microtrabecular lattices, interconnect every organelle and conventional cytoskeletons as well as plasma membranes, resulting in the formation of 3-D meshworks in all portions of the cytoplasmic matrix of every cell. The microtrabeculae correspond well to the wispy components in the cytoplasmic matrix of conventionally epoxy-sectioned cell specimens that have been looked at but often neglected because of their poorly defined images due to the presence of embedding media having a substantial electron-scattering property. Because of the occurrence of similar meshworks in specimens that are supposed to be unstructured, such as the intramitochondrial matrix and blood plasma, together with the failure to detect any predictable changes of the microtrabecular lattices by experimental manipulation of cellular environments, it is inaccurate to conclude that all microtrabecular lattice represent structures equivalent to those in a living state of cells simply because of their clear appearance. Instead, three possible interpretations are newly proposed for the biological significance of the microtrabecular lattices. The first is that the appearance of lattices represents the presence of proteins, and that their approximate concentrations are speculated based on the compactness of the lattice. The second is that when an intracellular microdomain composed of more compact lattices is contiguous with another domain composed of looser lattices in a given cell, the former might represent the gelated state and the latter the solated state. Possible examples for these two interpretations are also proposed, possibly leading us to further elaborate the significance of microtrabecular lattices.
机译:使用聚乙二醇作为瞬时嵌入物的无嵌入电子显微镜显示,原本称为微骨小梁和微骨小梁晶格的细长链将每个细胞器和常规细胞骨架以及质膜相互连接,从而在3D网格的所有部分形成了3D网格。每个细胞的细胞质基质。细小梁很好地对应了传统的环氧切片细胞标本的细胞质基质中的细小成分,这些细小成分已被观察,但由于存在嵌入图像的电子散射性很差而图像清晰度不高,因此经常被忽略。由于在应该被认为是非结构化的标本中出现了类似的网状结构,例如线粒体内基质和血浆,并且由于无法通过实验操作细胞环境而无法检测到任何可预测的小梁网格变化,因此得出结论是不准确的仅仅因为它们清晰的外观,所有微骨小梁的晶格就代表了与细胞存活状态相同的结构。取而代之的是,针对小梁格的生物学意义,最近提出了三种可能的解释。首先是晶格的出现代表蛋白质的存在,并且根据晶格的紧密度推测其近似浓度。第二个是在给定的细胞中,当由更紧密的晶格组成的细胞内微结构域与另一个由较松散的晶格组成的结构域相邻时,前者可能代表胶凝状态,而后者可能代表胶凝状态。还提出了这两种解释的可能例子,可能使我们进一步阐述微骨小梁的重要性。

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