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Interaction between echovirus 7 and its receptor decay-accelerating factor (CD55): evidence for a secondary cellular factor in A-particle formation.

机译：回声病毒7及其受体衰变加速因子（CD55）之间的相互作用：A粒子形成中次生细胞因子的证据。

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摘要

Soluble forms of decay-accelerating factor (DAF) (CD55), the receptor for echovirus 7, were synthesized in the yeast Pichia pastoris. Purified recombinant protein containing SCR domains 2, 3, and 4, but lacking the serine/threonine rich region, was shown to block infection of susceptible cells by echovirus 7. In contrast to the situation with poliovirus and its receptor, the neutralization of echovirus 7 by soluble DAF was completely reversible and did not lead to the formation of 135S A-particles. Binding of virus to susceptible cells, by contrast, did lead to the formation of A particles, mainly from virus that had been internalized. The data suggest that a secondary factor(s) may contribute to A-particle formation and uncoating of echovirus 7.

机译：在酵母巴斯德毕赤酵母中合成了可溶性形式的衰减加速因子（DAF）（CD55），即回声病毒7的受体。含有SCR结构域2、3和4的纯化重组蛋白，但缺少富含丝氨酸/苏氨酸的区域，被证明可以阻止回声病毒7感染易感细胞。与脊髓灰质炎病毒及其受体的情况相反，回声病毒7的中和可溶性DAF的作用是完全可逆的，并且不会导致135S A颗粒的形成。相比之下，病毒与易感细胞的结合确实导致了A颗粒的形成，主要是由已被内在化的病毒形成的。数据表明，次要因素可能有助于回声病毒7的A颗粒形成和脱壳。

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期刊名称 Journal of Virology
作者
R M Powell; T Ward; D J Evans; J W Almond;
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年(卷),期 1997(71),12
年度 1997
页码 9306–9312
总页数 7
原文格式 PDF
正文语种
中图分类人体病毒学（致病病毒）;病毒（滤过性病毒）;
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专利

1. Two clusters of mutations map distinct receptor-binding sites of echovirus 11 for the decay-accelerating factor (CD55) and for canyon-binding receptors. [J] . Rezaikin AV, Novoselov AV, Sergeev AG Virus Research: An International Journal of Molecular and Cellular Virology . 2009,第1期

机译：两个突变簇将回声病毒11的不同受体结合位点映射为衰减加速因子（CD55）和峡谷结合受体。
2. Human Diffusely Adhering Escherichia coli Expressing Afa/Dr Adhesins That Use Human CD55 (Decay-Accelerating Factor) as a Receptor Does Not Bind the Rodent and Pig Analogues of CD55 [J] . Sylvie Hudault, O. Brad Spiller, B. Paul Morgan, Infection and immunity . 2004,第8期

机译：表达以人CD55（衰变促进因子）为受体的Afa / Dr粘附素的人弥散性粘附大肠杆菌不结合啮齿类动物和猪的CD55类似物
3. Afa/Dr Diffusely Adhering Escherichia coli Infection in T84 Cell Monolayers Induces Increased Neutrophil Transepithelial Migration, Which in Turn Promotes Cytokine-Dependent Upregulation of Decay-Accelerating Factor (CD55), the Receptor for Afa/Dr Adhesins [J] . Fréderic Bétis, Patrick Brest, Véronique Hofman, Infection and immunity . 2003,第4期

机译：Afa / Dr在T84细胞单层中弥漫性粘附大肠杆菌感染导致嗜中性粒细胞上皮迁移增加，进而促进细胞因子依赖性上调衰变促进因子（CD55）的上调，该衰变促进因子是Afa / Dr粘附素的受体。
4. Coordinated Dysregulation of Cellular Receptors, Proangiogenic Factors and Intracellular Pathways in Acute leukemia [C] . N. Barbarroja, Ch. Lopez-Pedrera, P. Buendia, International Congress on Thrombosis . 2004

机译：急性白血病细胞受体，雌激素因子和细胞内途径的协调诱导
5. Identification of decay-accelerating factor (CD55) as a HeLa cell receptor for enterovirus 70. [D] . Karnauchow, Timothy M. 1997

机译：鉴定衰变促进因子（CD55）作为肠病毒70的HeLa细胞受体。
6. Interaction between Echovirus 7 and Its Receptor Decay-Accelerating Factor (CD55): Evidence for a Secondary Cellular Factor in A-Particle Formation [O] . Robert M. Powell, Trevor Ward, David J. Evans, 1998

机译：Echovirus 7及其受体衰变加速因子（CD55）之间的相互作用：A颗粒形成中次级细胞因子的证据。
7. Interaction between Echovirus 7 and Its Receptor, Decay-Accelerating Factor (CD55): Evidence for a Secondary Cellular Factor in A-Particle Formation [O] . Robert M. Powell, Trevor Ward, David J. Evans, 1998

机译：Echovirus 7及其受体之间的相互作用，衰减加速因子（CD55）：α-粒子形成中的次生细胞因子的证据

Interaction between echovirus 7 and its receptor decay-accelerating factor (CD55): evidence for a secondary cellular factor in A-particle formation.

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