首页> 美国卫生研究院文献>The EMBO Journal >Neurofilament architecture combines structural principles of intermediate filaments with carboxy-terminal extensions increasing in size between triplet proteins.
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Neurofilament architecture combines structural principles of intermediate filaments with carboxy-terminal extensions increasing in size between triplet proteins.

机译:神经丝结构将中间丝的结构原理与羧基末端延伸结合在一起该羧基末端延伸在三重态蛋白之间增大。

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摘要

Mammalian neurofilament triplet proteins (68 K, 160 K and 200 K) have been correlated by a biochemical, immunological and protein chemical study. The 160 K and 200 K triplet proteins are intermediate filament proteins in their own right, since they reveal the alpha-helical coiled-coil rod domain analyzed in detail for the 68 K protein. Triplet proteins display two distinct arrays. Their amino-terminal region built analogously to non-neuronal intermediate filament proteins should allow a co-polymerization process via the interaction of coiled-coil domains. The extra mass of all triplet proteins is allocated to carboxy-terminally located extensions of increasing size and unique amino acid sequences. These may provide highly charged scaffolds suitable for interactions with other neuronal components. Such a domain of 68 K reveals, in sequence analysis, 47 glutamic acids within 106 residues. The epitope recognized by a monoclonal antibody reacting probably with all intermediate filament proteins has been mapped. It is located within the last 20 residues of the rods, where six distinct intermediate filament proteins point to a consensus sequence.
机译:哺乳动物神经丝三联体蛋白质(68 K,160 K和200 K)已通过生物化学,免疫学和蛋白质化学研究进行了关联。 160 K和200 K三重态蛋白本身就是中间丝蛋白,因为它们揭示了对68 K蛋白进行详细分析的α-螺旋卷曲螺旋棒结构域。三联体蛋白质显示两个不同的阵列。其类似于非神经元中间丝蛋白质构建的氨基末端区域应允许通过卷曲螺旋结构域的相互作用进行共聚过程。所有三重态蛋白质的额外质量均分配给位于羧基末端的大小不断增加的延伸和独特的氨基酸序列。这些可以提供适合与其他神经元组件相互作用的带高电荷的支架。在序列分析中,这种68 K的结构域揭示了106个残基内的47个谷氨酸。已经绘制了可能与所有中间细丝蛋白反应的单克隆抗体识别的表位。它位于杆的最后20个残基内,其中六个不同的中间细丝蛋白指向共有序列。

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