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BOTH PRE-S1 AND S DOMAINS OF HEPATITIS B VIRUS ENVELOPE PROTEINS INTERACT WITH THE CORE PARTICLE

机译:乙型肝炎病毒包膜蛋白的pre-S1和S域均与核心颗粒相互作用

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摘要

The three envelope proteins of the hepatitis B virus (HBV) are encoded by a single open reading frame in the genome containing three separate in-phase AUG codons. This organization defines three protein domains (pre-S1, pre-S2, S) which form the small (S), middle (M, pre-S2/S), and large (L, pre-S1/pre-S2/S) proteins. Mature virions are generated by the budding of preformed nucleocapsids through endoplasmic reticulum (ER) membranes containing S and L proteins, whereas the M protein is not necessary. This suggests an important function for the pre-S1 domain. To investigate the protein-protein interactions involved during the maturation process of the HBV virion, we studied in vitro the binding affinity to purified HBV core particles of various synthetic peptides identical to regions of the envelope proteins. Data previously obtained with deletion mutants were confirmed and refined. The 13 C-terminal amino acids of pre-S1 bound efficiently to core particles, whereas other pre-S domains did not. Moreover, the amino acid sequence 56-80 in the cytosolic loop of S bound efficiently to the HBV core. This double interaction between the HBV capside and both S and pre-S1 domains may be required for virion morphogenesis.
机译:乙型肝炎病毒(HBV)的三个包膜蛋白由基因组中包含三个独立的同相AUG密码子的单个开放阅读框编码。该组织定义了三个蛋白质结构域(pre-S1,pre-S2,S),分别形成小(S),中(M,S2-S2 / S)和大(L,S1 / pre-S2 / S) )蛋白质。成熟的病毒体是通过预先形成的核衣壳通过含有S和L蛋白的内质网(ER)膜出芽而生成的,而M蛋白不是必需的。这表明S1之前的域具有重要功能。为了研究HBV病毒体成熟过程中涉及的蛋白质相互作用,我们在体外研究了对与包膜蛋白区域相同的各种合成肽的纯化HBV核心颗粒的结合亲和力。先前用缺失突变体获得的数据得到确认和完善。 pre-S1的13个C末端氨基酸有效地结合到核心颗粒上,而其他pre-S结构域则没有。此外,S的胞质环中的氨基酸序列56-80有效结合至HBV核心。病毒粒子形态发生可能需要HBV帽侧与S和pre-S1域之间的这种双重相互作用。

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