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Epitope Identification and Application for Diagnosis of Duck Tembusu Virus Infections in Ducks

机译:表位的鉴定及其在鸭鸭坦布苏病毒感染中的诊断

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Duck Tembusu virus (DTMUV) causes substantial egg drop disease. DTMUV was first identified in China and rapidly spread to Malaysia and Thailand. The antigenicity of the DTMUV E protein has not yet been characterized. Here, we investigated antigenic sites on the E protein using the non-neutralizing monoclonal antibodies (mAbs) 1F3 and 1A5. Two minimal epitopes were mapped to 221 LD/NLPW 225 and 87 YAEYI 91 by using phage display and mutagenesis. DTMUV-positive duck sera reacted with the epitopes, thus indicating the importance of the minimal amino acids of the epitopes for antibody-epitope binding. The performance of the dot blotting assay with the corresponding positive sera indicated that YAEYI was DTMUV type-specific, whereas 221 LD/NLPW 225 was a cross-reactive epitope for West Nile virus (WNV), dengue virus (DENV), and Japanese encephalitis virus (JEV) and corresponded to conserved and variable amino acid sequences among these strains. The structure model of the E protein revealed that YAEYI and LD/NLPW were located on domain (D) II, which confirmed that DII might contain a type-specific non-neutralizing epitope. The YAEYI epitope-based antigen demonstrated its diagnostic potential by reacting with high specificity to serum samples obtained from DTMUV-infected ducks. Based on these observations, a YAEYI-based serological test could be used for DTMUV surveillance and could differentiate DTMUV infections from JEV or WNV infections. These findings provide new insights into the organization of epitopes on flavivirus E proteins that might be valuable for the development of epitope-based serological diagnostic tests for DTMUV.
机译:鸭Tembusu病毒(DTMUV)导致大量的鸡蛋掉落病。 DTMUV首先在中国被发现,并迅速传播到马来西亚和泰国。 DTMUV E蛋白的抗原性尚未鉴定。在这里,我们使用非中和性单克隆抗体(mAb)1F3和1A5研究了E蛋白上的抗原位点。通过噬菌体展示和诱变将两个最小表位定位到221 LD / NLPW 225和87 YAEYI 91。 DTMUV阳性鸭血清与表位反应,因此表明表位的最小氨基酸对于抗体-表位结合的重要性。用相应的阳性血清进行斑点印迹分析的结果表明,YAEYI是DTMUV类型特异性的,而221 LD / NLPW 225是西尼罗河病毒(WNV),登革热病毒(DENV)和日本脑炎的交叉反应性表位病毒(JEV),并对应于这些菌株中的保守氨基酸序列和可变氨基酸序列。 E蛋白的结构模型表明YAEYI和LD / NLPW位于结构域(D)II上,这证实DII可能包含类型特异性的非中和表位。基于YAEYI表位的抗原通过与从DTMUV感染的鸭子获得的血清样品高度特异性反应,显示出其诊断潜力。基于这些观察,基于YAEYI的血清学检测可用于DTMUV监测,并可将DTMUV感染与JEV或WNV感染区分开。这些发现为黄病毒E蛋白表位的组织提供了新的见解,这可能对开发基于表位的DTMUV血清学诊断测试有价值。

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