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Staining of macromolecules: possible mechanisms and examples

机译:大分子染色:可能的机理和实例

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This review is based on a presentation given at the Biological Stain Commission meeting in June 2008. I discuss staining as an interaction between dye, solvent, and biological macromolecules. Most staining takes place in water, where the physico-chemical properties of the macromolecules are particularly important. Staining from aqueous solution is summarized. The first step is diffusion-ion exchange, which builds up the dye ion concentration close to the appropriately charged tissue constituents. While charge interactions are important for selectivity and build-up of dye ions around specific tissue and cell constituents, they have in most cases little to do with actual dye binding. The next step, actual binding, is predominantly between aromatic and other non-polar parts of the dye and corresponding groups in the tissue constituent. This results in a reduction of the total hydrophobic area exposed to water, hence the term hydrophobic interaction. Because dye binding is predominantly by dispersive forces, the larger the aromatic dye system and the fewer the number of charges on the dye, the greater the substantivity or affinity. Some relatively straightforward anionic or cationic one-step staining systems are discussed also. These include amyloid staining with Congo red, elastin staining with orceins, collagen staining with picrofuchsin, DNA-RNA staining with methyl green-pyronin Y, acid heteroglycan staining with Alcian blue, and metachromatic staining.
机译:这篇综述基于2008年6月生物染色委员会会议上的演讲。我将染色作为染料,溶剂和生物大分子之间的相互作用进行讨论。大多数染色发生在水中,其中大分子的物理化学性质特别重要。总结了从水溶液中染色。第一步是扩散-离子交换,其建立的染料离子浓度接近适当带电的组织成分。虽然电荷相互作用对于特定组织和细胞成分周围染料离子的选择性和聚集很重要,但在大多数情况下,它们与实际的染料结合关系不大。下一步是实际结合,主要是在染料的芳香族和其他非极性部分与组织成分中的相应基团之间。这导致暴露于水的总疏水面积减少,因此称为疏水相互作用。因为染料的结合主要是由分散力引起的,所以芳族染料体系越大,染料上的电荷数越少,直接性或亲和性就越大。还讨论了一些相对简单的阴离子或阳离子一步染色系统。这些包括用刚果红进行的淀粉样蛋白染色,用海藻素进行的弹性蛋白染色,用微紫红质蛋白进行的胶原蛋白染色,用甲基绿吡喃宁Y进行的DNA-RNA染色,用阿尔辛蓝进行的酸性杂聚糖染色以及变色染色。

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