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噬菌体fd外壳蛋白的化学修饰以及病毒粒子在组装和解组装过程中的取向

Chemical modification of the coat protein in bacteriophage fd and orientation of the virion during assembly and disassembly.

作者信息

Armstrong J, Hewitt J A, Perham R N

出版信息

EMBO J. 1983;2(10):1641-6. doi: 10.1002/j.1460-2075.1983.tb01638.x.

Abstract

The major (gene VIII) coat protein of bacteriophage fd was radiolabelled by treating the virus with methyl[3H]acetimidate without causing any loss of infectivity. Complete amidination of lysine-8 in the amino acid sequence of the protein was achieved but little or no modification of the lysine residues near the C terminus was observed. This supports the assumption that the coat protein is oriented in the viral filament with its N terminus on the outside and its C-terminal region abutting the DNA. Escherichia coli was co-infected with radiolabelled bacteriophage and with unlabelled miniphage, a shorter defective form of phage fd. Radiolabel was detected in the progeny miniphage, proving that individual coat protein subunits can be recycled and assembled onto progeny miniphage DNA. About 35% of the coat protein subunits of phage particles infecting E. coli were recycled in 1 h. These facts support a model of the assembly and disassembly of the virion at the bacterial membrane in which the end of the particle containing the minor adsorption (gene III) protein, which is presumably the first to disassemble during infection, is the last to assemble during morphogenesis.

摘要

通过用甲基[³H]乙亚胺处理噬菌体fd,对其主要(基因VIII)外壳蛋白进行放射性标记,且未导致任何感染性损失。实现了该蛋白氨基酸序列中赖氨酸-8的完全脒化,但未观察到C末端附近赖氨酸残基的修饰很少或没有修饰。这支持了这样一种假设,即外壳蛋白在病毒丝中的取向是其N末端在外部,C末端区域邻接DNA。用放射性标记的噬菌体和未标记的微型噬菌体(噬菌体fd的一种较短的缺陷形式)共同感染大肠杆菌。在子代微型噬菌体中检测到放射性标记,证明单个外壳蛋白亚基可以被循环利用并组装到子代微型噬菌体DNA上。在1小时内,感染大肠杆菌的噬菌体颗粒中约35%的外壳蛋白亚基被循环利用。这些事实支持了一种病毒粒子在细菌膜上组装和拆卸的模型,其中含有次要吸附(基因III)蛋白的粒子末端,推测在感染期间是第一个拆卸的,在形态发生期间是最后一个组装的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fd1d/555339/0f3b8a65a4bc/emboj00263-0024-a.jpg

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