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Optimal numbers of residues in linkers of DNA polymerase I, T7 primase and DNA polymerase IV

机译:DNA聚合酶I,T7引发酶和DNA聚合酶IV的接头中的残基的最佳数目

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DNA polymerase I (PolI), T7 primase and DNA polymerase IV (Dpo4) have a common feature in their structures that the two main domains are connected by an unstructured polypeptide linker. To perform their specific enzymatic activities, the enzymes are required to rearrange the position and orientation of one domain relative to the other into an active mode. Here, we show that the three enzymes share the same mechanism of the transition from the inert to active modes and use the minimum numbers of residues in their linkers to achieve the most efficient transitions. The transition time to the finally active mode is sensitively dependent on the stretched length of the linker in the finally active mode while is insensitive to the position and orientation in the initially inert state. Moreover, we find that for any enzyme whose two domains are connected by an unstructured flexible linker, the stretched length (L) of the linker in the finally active mode and the optimal number (Nopt) of the residues in the linker satisfy relation L?≈?αNopt, with α?=?0.24-0.27?nm being a constant insensitive to the system.
机译:DNA聚合酶I(PolI),T7引发酶和DNA聚合酶IV(Dpo4)在结构上具有一个共同特征,即两个主要域通过非结构化多肽接头连接。为了执行其特定的酶促活性,需要酶将一个结构域相对于另一个结构域的位置和方向重新排列为活性模式。在这里,我们表明这三种酶具有相同的机制,从惰性模式过渡到活性模式,并在其接头中使用最少数量的残基来实现最有效的过渡。到最终激活模式的过渡时间敏感地取决于在最终激活模式下连接子的延伸长度,而对最初处于惰性状态的位置和取向不敏感。此外,我们发现,对于任何两个通过非结构化柔性接头连接的结构域的酶,在最终活性模式下接头的延伸长度(L)和接头中残基的最佳数目(Nopt)都满足关系式L 1。 ≈ααNopt,αα=α0.24-0.27μnm是对系统不敏感的常数。

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