首页> 外文OA文献 >The Minor Receptor Group of Human Rhinovirus (HRV) Includes HRV23 and HRV25, but the Presence of a Lysine in the VP1 HI Loop Is Not Sufficient for Receptor Binding
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The Minor Receptor Group of Human Rhinovirus (HRV) Includes HRV23 and HRV25, but the Presence of a Lysine in the VP1 HI Loop Is Not Sufficient for Receptor Binding

机译:人类鼻病毒(HRV)的次要受体群包括HRV23和HRV25,但是VP1 HI环中赖氨酸的存在不足以与受体结合

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摘要

Like all 10 minor receptor group human rhinoviruses (HRVs), HRV23 and HRV25, previously classified as major group viruses, are neutralized by maltose binding protein (MBP)-V33333 (a soluble recombinant concatemer of five copies of repeat 3 of the very-low-density lipoprotein receptor fused to MBP), bind to low-density lipoprotein receptor in virus overlay blots, and replicate in intercellular adhesion molecule 1 (ICAM-1)-negative COS-7 cells. From phylogenetic analysis of capsid protein VP1-coding sequences, they are also known to cluster together with other minor group strains. Therefore, they belong to the minor group; there are now 12 minor group and 87 major group HRV serotypes. Sequence comparison of the VP1 capsid proteins of all HRVs revealed that the lysine in the HI loop, strictly conserved in the 12 minor group HRVs, is also present in 9 major group serotypes that are neutralized by soluble ICAM-1. Despite the presence of this lysine, they are not neutralized by MBP-V33333 and fail to replicate in COS-7 cells and in HeLa cells in the presence of an ICAM-1-blocking antibody. These nine serotypes are therefore “true” major group viruses.
机译:像所有十种次要受体群人类鼻病毒(HRV)一样,先前被归类为主要群病毒的HRV23和HRV25被麦芽糖结合蛋白(MBP)-V33333(一种由5个重复序列的5个重复序列组成的可溶性重组连接体中和)密度脂蛋白受体融合至MBP),在病毒覆盖印迹中与低密度脂蛋白受体结合,并在细胞间粘附分子1(ICAM-1)阴性的COS-7细胞中复制。从衣壳蛋白VP1编码序列的系统发育分析,它们也与其他次要菌株一起聚集。因此,他们属于少数群体;现在有12个次要组和87个主要组HRV血清型。所有HRV的VP1衣壳蛋白的序列比较显示,在HI环中的赖氨酸(在12个次要HRVs中严格保守)也存在于9个主要组血清型中,这些血清型被可溶性ICAM-1中和。尽管存在这种赖氨酸,但它们并未被MBP-V33333中和,并且在存在ICAM-1阻断抗体的情况下无法在COS-7细胞和HeLa细胞中复制。因此,这九种血清型是“真正的”主要群体病毒。

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