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首页> 外文期刊>Journal of Clinical Microbiology >Enzyme-Linked Immunosorbent Assay Specific to Dengue Virus Type 1 Nonstructural Protein NS1 Reveals Circulation of the Antigen in the Blood during the Acute Phase of Disease in Patients Experiencing Primary or Secondary Infections
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Enzyme-Linked Immunosorbent Assay Specific to Dengue Virus Type 1 Nonstructural Protein NS1 Reveals Circulation of the Antigen in the Blood during the Acute Phase of Disease in Patients Experiencing Primary or Secondary Infections

机译:特定于登革热病毒1型非结构蛋白NS1的酶联免疫吸附测定揭示了在原发或继发感染的疾病急性期中血液中抗原的循环

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During flavivirus infection in vitro, nonstructural protein NS1 is released in a host-restricted fashion from infected mammalian cells but not vector-derived insect cells. In order to analyze the biological relevance of NS1 secretion in vivo, we developed a sensitive enzyme-linked immunosorbent assay (ELISA) to detect the protein in the sera of dengue virus-infected patients. The assay was based on serotype 1 NS1-specific mouse and rabbit polyclonal antibody preparations for antigen immunocapture and detection, respectively. With purified dengue virus type 1 NS1 as a protein standard, the sensitivity of our capture ELISA was less than 1 ng/ml. When a panel of patient sera was analyzed, the NS1 antigen was found circulating from the first day after the onset of fever up to day 9, once the clinical phase of the disease is over. The NS1 protein could be detected even when viral RNA was negative in reverse transcriptase-PCR or in the presence of immunoglobulin M antibodies. NS1 circulation levels varied among individuals during the course of the disease, ranging from several nanograms per milliliter to several micrograms per milliliter, and peaked in one case at 50 μg/ml of serum. Interestingly, NS1 concentrations did not differ significantly in serum specimens obtained from patients experiencing primary or secondary dengue virus infections. These findings indicate that NS1 protein detection may allow early diagnosis of infection. Furthermore, NS1 circulation in the bloodstream of patients during the clinical phase of the disease suggests a contribution of the nonstructural protein to dengue virus pathogenesis.
机译:在体外黄病毒感染期间,非结构蛋白NS1以宿主限制性的方式从受感染的哺乳动物细胞中释放,但没有从载体来源的昆虫细胞中释放。为了分析体内NS1分泌的生物学相关性,我们开发了一种敏感的酶联免疫吸附测定(ELISA)方法来检测登革热病毒感染患者血清中的蛋白质。该测定分别基于血清型1 NS1特异性小鼠和兔多克隆抗体制剂进行抗原免疫捕获和检测。以纯化的1型登革热病毒NS1作为蛋白质标准品,我们捕获的ELISA的灵敏度小于1 ng / ml。当分析一组患者的血清时,发现NS1抗原从发烧后的第一天到第9天一直循环,直到疾病的临床阶段结束。即使在逆转录PCR-PCR中或在存在免疫球蛋白M抗体的情况下病毒RNA阴性时,也可以检测到NS1蛋白。在疾病过程中,NS1循环水平在个体之间变化,范围从每毫升几毫微克到每毫升几微克,在一种情况下在50μg/ ml的血清中达到峰值。有趣的是,从患有原发或继发登革热病毒感染的患者获得的血清样本中,NS1浓度没有显着差异。这些发现表明,NS1蛋白检测可以早期诊断感染。此外,在疾病的临床阶段,患者血液中的NS1循环表明非结构蛋白对登革热病毒发病机制的贡献。

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