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Study of Coxsackie B viruses interactions with Coxsackie Adenovirus receptor and Decay-Accelerating Factor using Human CaCo-2 cell line

机译:使用人CaCo-2细胞系研究柯萨奇B病毒与柯萨奇腺病毒受体和衰变促进因子的相互作用

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BackgroundDecay Accelerating Factor (DAF) and Coxsackievirus-Adenovirus Receptor (CAR) have been identified as cellular receptors for Coxsackie B viruses (CV-B). The aim of this study is to elucidate the different binding properties of CV-B serotypes and to find out if there are any amino acid changes that could be associated to the different phenotypes.Twenty clinical CV-B isolates were tested on CaCo-2 cell line using anti-DAF (BRIC216) and anti-CAR (RmcB) antibodies. CV-B3 Nancy prototype strain and a recombinant strain (Rec, CV-B3/B4) were tested in parallel. The P1 genomic region of 12 CV-B isolates from different serotypes was sequenced and the Trans-Epithelial Electrical Resistance (TEER) along with the virus growth cycle was measured.ResultsInfectivity assays revealed clear differences between CV-B isolates with regard to their interactions with DAF and CAR. All tested CV-B isolates showed an absolute requirement for CAR but varied in their binding to DAF. We also reported that for some isolates of CV-B, DAF attachment was not adapted. Genetic analysis of the P1 region detected multiple differences in the deduced amino acid sequences.ConclusionWithin a given serotype, variations exist in the capacity of virus isolates to bind to specific receptors, and variants with different additional ligands may arise during infection in humans as well as in tissue culture.
机译:背景衰变促进因子(DAF)和柯萨奇病毒-腺病毒受体(CAR)已被确定为柯萨奇B病毒(CV-B)的细胞受体。这项研究的目的是阐明CV-B血清型的不同结合特性,并查明是否存在与不同表型有关的氨基酸变化。在CaCo-2细胞上测试了20种临床CV-B分离株使用抗DAF(BRIC216)和抗CAR(RmcB)抗体的品系。并行测试了CV-B3 Nancy原型菌株和重组菌株(Rec,CV-B3 / B4)。对12种不同血清型CV-B分离株的P1基因组区域进行了测序,并测量了跨上皮电阻(TEER)以及病毒的生长周期。结果感染力分析表明,CV-B分离株之间在与病毒的相互作用方面存在明显差异DAF和CAR。所有测试的CV-B分离株均显示出对CAR的绝对要求,但它们与DAF的结合却有所不同。我们还报告说,对于某些CV-B分离株,DAF附着没有适应。对P1区的遗传分析发现推导的氨基酸序列存在多个差异。结论在给定的血清型中,病毒分离株结合特定受体的能力存在差异,并且在人类以及人类感染期间可能会出现具有不同附加配体的变异在组织培养中。

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