School of Biological Sciences, The University of Auckland, Auckland, New Zealand.
Protein Sci. 2010 Apr;19(4):893-9. doi: 10.1002/pro.354.
Measles virus has a single-stranded RNA genome that is organized into a helical complex by the viral N protein. The resulting structure is termed the nucleocapsid and is traversed by the viral polymerase during RNA synthesis. The P protein, the noncatalytic subunit of the polymerase, provides the "legs and feet" that allow the polymerase to walk along its protein-RNA template. The polymerase feet are very simple three-helix bundles, only 50 amino acids in size. Previously, we have shown that these feet grasp the viral N protein during movement by attaching to a short sequence (amino acids 487-503) within the disordered and surface-exposed tail of N, causing it to fold into a helix. The result is a weak-affinity complex with a short lifetime, which would allow the polymerase to take rapid steps forward. The structure of the complex was determined using X-ray crystallography. This simple model of binding was challenged by a paper in this journal, claiming that a downstream sequence in the tail of N (amino acids 517-525) was also critical for the association. Its presence was reported to enhance the overall affinity of the polymerase feet for N by three orders of magnitude. We have, therefore, examined binding of the polymerase foot domain to amino acids 477-525 of N using quantitative biophysical techniques, and compared the results to our previous binding studies, performed using amino acids 477-505 of N. We find no evidence that the sequence downstream of amino acid 505 influences binding, validating the original single-site binding model.
麻疹病毒的单链 RNA 基因组由病毒 N 蛋白螺旋排列形成。这种结构被称为核衣壳,在 RNA 合成过程中,病毒聚合酶贯穿其中。P 蛋白是聚合酶的非催化亚基,它提供了“腿和脚”,使聚合酶能够沿着其蛋白-RNA 模板移动。聚合酶的“脚”是非常简单的三螺旋束,只有 50 个氨基酸大小。此前,我们已经表明,这些“脚”通过附着在 N 蛋白无规卷曲和暴露于表面的尾部内的短序列(氨基酸 487-503)来抓住病毒 N 蛋白,从而导致其折叠成螺旋。结果是形成一个弱亲和力的短暂复合物,这将允许聚合酶快速向前移动。该复合物的结构是通过 X 射线晶体学确定的。这一简单的结合模型受到了该杂志上一篇论文的挑战,该论文声称 N 蛋白尾部的下游序列(氨基酸 517-525)对聚合酶的结合也很关键。据报道,其存在将聚合酶“脚”与 N 的氨基酸 477-525 的结合总体亲和力提高了三个数量级。因此,我们使用定量生物物理技术研究了聚合酶脚结构域与 N 的氨基酸 477-525 的结合,并将结果与我们之前使用 N 的氨基酸 477-505 进行的结合研究进行了比较。我们没有发现氨基酸 505 下游的序列影响结合的证据,验证了原始的单结合位点模型。