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首页> 外文期刊>Archives of virology >Simultaneous mutation of G275A and P276A in the matrix protein of Newcastle disease virus decreases virus replication and budding
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Simultaneous mutation of G275A and P276A in the matrix protein of Newcastle disease virus decreases virus replication and budding

机译:新城疫病毒基质蛋白中G275A和P276A同时突变可减少病毒复制和出芽

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摘要

The matrix (M) protein of Newcastle disease virus (NDV) is a highly conserved hydrophobic viral protein. In some paramyxoviruses (measles virus and Sendai virus), the paired glycine (G) near the C terminus of the M protein may form a turn that mediates the specific interaction with the cell membrane. Similar amino acids (glycine-proline [GP], at position 275-276) exist in the M protein of NDV. However, the role of these residues in the replication and pathogenicity of NDV is unknown. In this study, recombinant NDV with the sequence GP/AA or LGP/GGL in the M protein was generated to investigate the role of this conserved sequence. Budding experiments on the mutant viruses revealed that the GP/AA mutation reduced virus budding and virus replication in DF-1 cells; biological characterization revealed attenuated virulence and pathogenicity in chickens, indicating that the GP sequence plays a critical role in the life cycle of the virus.
机译:新城疫病毒(NDV)的基质(M)蛋白是高度保守的疏水性病毒蛋白。在某些副粘病毒(麻疹病毒和仙台病毒)中,M蛋白C末端附近的配对甘氨酸(G)可能形成转弯,介导与细胞膜的特异性相互作用。 NDV的M蛋白中存在相似的氨基酸(甘氨酸-脯氨酸[GP],位置275-276)。然而,这些残基在NDV的复制和致病性中的作用尚不清楚。在这项研究中,产生了在M蛋白中具有序列GP / AA或LGP / GGL的重组NDV,以研究此保守序列的作用。对突变病毒的萌芽实验表明,GP / AA突变减少了DF-1细胞中的病毒出芽和病毒复制。生物学特性揭示了鸡的毒力和致病性减弱,表明GP序列在病毒的生命周期中起着至关重要的作用。

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