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Chemical Synthesis and In Vitro Evaluation of a Phage Display-Derived Peptide Active against Infectious Salmon Anemia Virus

机译:噬菌体展示衍生肽对传染性鲑鱼贫血病毒有活性的化学合成和体外评估

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Infectious salmon anemia virus (ISAV) is the etiological agent of the disease by the same name and causes major losses in the salmon industry worldwide. Epizootic ISAV outbreaks have occurred in Norway and, to a lesser degree, in Canada. In 2007, an ISAV outbreak in Chile destroyed most of the seasonal production and endangered the entire Chilean salmon industry. None of the existing prophylactic approaches have demonstrated efficacy in providing absolute protection from or even a palliative effect on ISAV proliferation. Sanitary control measures for ISAV, based on molecular epidemiology data, have proven insufficient, mainly due to high salmon culture densities and a constant presence of a nonpathogenic strain of the virus. This report describes an alternative treatment approach based on interfering peptides selected from a phage display library. The screening of a phage display heptapeptide library resulted in the selection of a novel peptide with significant in vitro antiviral activity against ISAV. This peptide specifically interacted with the viral hemagglutinin-esterase protein, thereby impairing virus binding, with plaque reduction assays showing a significant reduction in viral yields. The identified peptide acts at micromolar concentrations against at least two different pathogenic strains of the virus, without detectable cytotoxic effects on the tested fish cells. Therefore, antiviral peptides represent a novel alternative for controlling ISAV and, potentially, other fish pathogens.IMPORTANCE Identifying novel methods for the efficient control of infectious diseases is imperative for the future of global aquaculture. The present study used a phage display heptapeptide library to identify a peptide with interfering activity against a key protein of the infectious salmon anemia virus (ISAV). A piscine orthomyxovirus, ISAV is a continuous threat to the commercial sustainability of cultured salmon production worldwide. The complex epidemiological strategy of this pathogen has made prophylactic control extremely difficult. The identified antiviral peptide efficiently impairs ISAV infection in vitro by specifically blocking hemagglutinin-esterase, a pivotal surface protein of this virus. Peptide synthesis could further modify the primary structure of the identified peptide to improve specific activity and stability. The present results form the foundation for developing a new pharmacological treatment against ISAV.
机译:传染性鲑鱼贫血病毒(ISAV)是该病的病原体,并且在全球鲑鱼产业中造成重大损失。挪威爆发了流行性ISAV疫情,加拿大的疫情也有所减少。 2007年,智利的一次ISAV爆发摧毁了大部分季节性生产,并危及整个智利鲑鱼产业。现有的预防方法均未显示出对ISAV增殖提供绝对保护或免受姑息作用的功效。根据分子流行病学数据,对ISAV的卫生控制措施已被证明是不充分的,这主要是由于鲑鱼养殖密度高以及该病毒的非致病性菌株持续存在。该报告描述了一种基于选自噬菌体展示文库的干扰肽的替代治疗方法。噬菌体展示七肽文库的筛选导致选择了一种对ISAV具有显着的体外抗病毒活性的新型肽。该肽与病毒血凝素-酯酶蛋白特异性相互作用,从而削弱了病毒的结合,噬斑减少试验显示病毒产量显着降低。鉴定出的肽以微摩尔浓度作用于病毒的至少两种不同的致病菌株,对受试鱼细胞没有可检测的细胞毒性作用。因此,抗病毒肽代表了控制ISAV以及潜在的其他鱼类病原体的新选择。重要事项确定有效控制传染病的新方法对于全球水产养殖的未来至关重要。本研究使用噬菌体展示七肽文库来鉴定对传染性鲑鱼贫血病毒(ISAV)的关键蛋白具有干扰活性的肽。 ISAV是鱼正粘病毒,对世界范围内养殖鲑鱼生产的商业可持续性构成持续威胁。该病原体的复杂流行病学策略使得预防控制极为困难。鉴定出的抗病毒肽通过特异性阻断血凝素酯酶(一种该病毒的关键表面蛋白),在体外有效削弱ISAV感染。肽合成可以进一步修饰已鉴定肽的一级结构,以提高比活性和稳定性。目前的结果为开发针对ISAV的新药理疗法奠定了基础。

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