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Structural Requirements for the Antiviral Activity of the Human MxA Protein against Thogoto and Influenza A Virus

机译:对肺孢子和流感病毒的人MXA蛋白的抗病毒活性的结构要求

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The interferon-induced dynamin-like MxA protein has broad antiviral activity against many viruses, including orthomyxoviruses such as influenza A and Thogoto virus and bunyaviruses such as La Crosse virus. MxA consists of an N-terminal globular GTPase domain, a connecting bundle signaling element, and the C-terminal stalk that mediates oligomerization and antiviral specificity. We previously reported that the disordered loop L4 that protrudes from the compact stalk is a key determinant of antiviral specificity against influenza A and Thogoto virus. However, the role of individual amino acids for viral target recognition remained largely undefined. By mutational analyses, we identified two regions in the C-terminal part of L4 that contribute to an antiviral interface. Mutations in the proximal motif, at positions 561 and 562, abolished antiviral activity against orthomyxoviruses but not bunyaviruses. In contrast, mutations in the distal motif, around position 577, abolished antiviral activity against both viruses. These results indicate that at least two structural elements in L4 are responsible for antiviral activity and that the proximal motif determines specificity for orthomyxoviruses, whereas the distal sequence serves a conserved structural function.
机译:干扰素诱导的发动机样MXA蛋白具有广泛的抗病毒活性,其抗许多病毒,包括正交病毒,例如流感A和Thogoto病毒和兔克罗斯病毒等病毒。 MXA由N-末端球状GTP酶,连接束信号元件和介导低聚和抗病毒特异性的C末端茎秆组成。我们之前报道,从紧凑的茎突出的无序环L4是针对流感A和Thogoto病毒的抗病毒特异性的关键决定因素。然而,个体氨基酸对病毒靶标识的作用仍然很大程度上是未定义的。通过突变分析,我们确定了L4的C末端部分中的两个区域,其有助于抗病毒界面。近端基序的突变,在位置561和562处,废除抗病毒活性对正交病毒但不是兔酵母。相反,远端图案中的突变在577左右,消除了对两种病毒的抗病毒活性。这些结果表明,L4中的至少两个结构元素对抗病毒活性负责,并且近端基序决定了正交病毒的特异性,而远端序列是保守的结构功能。

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