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标记复制技术:冷冻断裂复制品中膜内颗粒的后阴影标记

Labelled-replica techniques: post-shadow labelling of intramembrane particles in freeze-fracture replicas.

作者信息

Rash J E, Johnson T J, Hudson C S, Giddings F D, Graham W F, Eldefrawi M E

出版信息

J Microsc. 1982 Nov;128(Pt 2):121-38. doi: 10.1111/j.1365-2818.1982.tb00444.x.

Abstract

Three methods are described for direct post-fracture, post-shadow labelling of individual classes of intramembrane particles (IMPs) in freeze-fracture replicas of biological membranes. The P-face IMPs corresponding to the acetylcholine receptor complexes (AChRs) of vertebrate neuroeffector junctions are identified by post-replication labelling with ferritin-antibody complexes and with neurotoxin-biotin-avidin-colloidal gold affinity ligands. (The freeze-etch nomenclature of Branton et al., 1975, is used in this report.) These post-shadow labelling techniques resemble conventional en bloc labelling techniques except that the labelling reagents must penetrate a thin but discontinuous layer of platinum superimposed on the molecules of interest. In the 'sectioned labelled-replica technique', the replicated and labelled tissues are stained, embedded in plastic and sectioned parallel to the replica-tissue interfaces. In the direct 'labelled-replica techniques', the replicated and labelled samples are freeze-dried or critical point dried, the labelled surfaces are stabilized by carbon coating, and the underlying tissues are dissolved, allowing the labelled-replicas to be examined as conventional freeze-fracture replicas. The unshadowed side of each AChR IMP is shown to retain sufficient biochemical information to permit both immunospecific and neurotoxin specific labelling despite formaldehyde fixation, freezing, fracturing, platinum shadowing, and thawing in aqueous media. A new mixed ferricyanide-osmium staining method reveals electron opaque structures spanning the membrane bilayer in the same size, number and distribution as the labelled IMPs. These experiments demonstrate the feasibility of identifying individual IMPs in freeze-fracture replicas and may allow the identification of specific membrane lesions in human disease.

摘要

本文描述了三种用于在生物膜冷冻断裂复制品中对单个膜内颗粒(IMP)类别进行骨折后、阴影后直接标记的方法。通过用铁蛋白 - 抗体复合物以及神经毒素 - 生物素 - 抗生物素蛋白 - 胶体金亲和配体进行复制后标记,可识别与脊椎动物神经效应器接头的乙酰胆碱受体复合物(AChR)相对应的P面IMP。(本报告采用了Branton等人1975年的冷冻蚀刻命名法。)这些阴影后标记技术类似于传统的整体标记技术,不同之处在于标记试剂必须穿透叠加在感兴趣分子上的一层薄但不连续的铂层。在“切片标记复制品技术”中,对复制并标记的组织进行染色,嵌入塑料中,并平行于复制组织界面进行切片。在直接的“标记复制品技术”中,对复制并标记的样品进行冷冻干燥或临界点干燥,通过碳涂层稳定标记表面,并溶解下面的组织,从而可以像传统冷冻断裂复制品一样检查标记复制品。结果表明,尽管经过甲醛固定、冷冻、断裂、铂阴影处理以及在水性介质中解冻,每个AChR IMP的未阴影面仍保留了足够的生化信息,以允许进行免疫特异性和神经毒素特异性标记。一种新的铁氰化铁 - 锇混合染色方法揭示了跨越膜双层的电子不透明结构,其大小、数量和分布与标记的IMP相同。这些实验证明了在冷冻断裂复制品中识别单个IMP的可行性,并可能有助于识别人类疾病中的特定膜损伤。

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