首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Functional characterization of the C—C chemokine-like molecules encoded by molluscum contagiosum virus types 1 and 2
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Functional characterization of the C—C chemokine-like molecules encoded by molluscum contagiosum virus types 1 and 2

机译:软体动物感染1型和2型CC趋化因子样分子的功能表征

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摘要

Many viruses have evolved mechanisms for evading the host immune system by synthesizing proteins that interfere with the normal immune response. The poxviruses are among the most accomplished at deceiving their hosts’ immune systems. The nucleotide sequence of the genome of the human cutaneous poxvirus, molluscum contagiosum virus (MCV) type 1, was recently reported to contain a region that resembles a human chemokine. We have cloned and expressed the chemokine-like genes from MCV type 1 and the closely related MCV type 2 to determine a potential role for these proteins in the viral life cycle. In monocyte chemotaxis assays, the viral proteins have no chemotactic activity but both viral proteins block the chemotactic response to the human chemokine, macrophage inflammatory protein (MIP)-1α. Like MIP-1α, both viral proteins also inhibit the growth of human hematopoietic progenitor cells, but the viral proteins are more potent in this activity than the human chemokine. These viral chemokines antagonize the chemotactic activity of human chemokines and have an inhibitory effect on human hematopoietic progenitor cells. We hypothesize that the inhibition of chemotaxis is an immune evasion function of these proteins during molluscum contagiosum virus infection. The significance of hematopoietic progenitor cell inhibition in viral pathogenesis is uncertain.
机译:通过合成干扰正常免疫反应的蛋白质,许多病毒已经进化出逃避宿主免疫系统的机制。在欺骗宿主的免疫系统方面,痘病毒是最成功的病毒之一。最近报道了人类皮肤痘病毒,软体动物感染性1型皮肤疣病毒(MCV)的基因组核苷酸序列,其包含一个类似于人趋化因子的区域。我们已经克隆并表达了MCV 1型和密切相关的MCV 2型趋化因子样基因,以确定这些蛋白在病毒生命周期中的潜在作用。在单核细胞趋化性测定中,病毒蛋白不具有趋化活性,但是两种病毒蛋白均阻断对人趋化因子巨噬细胞炎性蛋白(MIP)-1α的趋化反应。像MIP-1α一样,两种病毒蛋白也都抑制人造血祖细胞的生长,但是这种病毒蛋白比人趋化因子更有效。这些病毒趋化因子拮抗人类趋化因子的趋化活性,并对人类造血祖细胞具有抑制作用。我们假设对趋化性的抑制是这些蛋白在软体动物传染性葡萄球菌感染期间的免疫逃避功能。造血祖细胞抑制在病毒发病机制中的意义尚不确定。

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