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增强人血清中昆虫细胞来源的拉格朗日病毒的感染力。

Enhancement of infectivity of insect cell-derived La Crosse Virus by human serum.

机构信息

University of Central Florida, College of Medicine, Orlando, FL, 32827, United States.

University of Central Florida, College of Medicine, Orlando, FL, 32827, United States.

出版信息

Virus Res. 2021 Jan 15;292:198228. doi: 10.1016/j.virusres.2020.198228. Epub 2020 Nov 11.

Abstract

Given the dual life cycle of arboviruses in insect and animal hosts and the importance of serum factors as a first line antiviral defense, we have examined the outcome of interactions between the arbovirus La Crosse Virus (LACV) and human serum. To mimic the life cycle between species, we used LACV derived from insect (I-LACV) and human keratinocyte (HaCaT) cells. Incubation of I-LACV with normal human serum did not result in neutralization, but instead stabilized I-LACV virions and enhanced the amount of infectious virus. Enhanced infectivity was also seen with heat-inactivated serum devoid of complement activity and with serum from a range of animals including mouse, ferret, and non-human primates. Depletion of antibodies from serum resulted in loss of enhancement of infectivity and sucrose gradient sedimentation assays showed IgG co-sedimenting with I-LACV particles. In agreement with our results with I-LACV, HaCaT-derived LACV was not neutralized by complement or antibodies in normal human serum. However, in contrast to I-LACV, HaCaT-derived LACV infectivity was stable when incubated alone and treatment with serum did not enhance infectivity. Our results indicate that LACV derived from insect cells differs substantially from virus derived from human cells, with I-LACV being dependent on serum factors to enhance infectivity. These findings suggest that understanding differential composition of insect versus animal cell-derived LACV may form the foundation for potential new antiviral approaches.

摘要

鉴于虫媒病毒在昆虫和动物宿主中的双重生命周期,以及血清因子作为第一道抗病毒防御的重要性,我们研究了虫媒病毒(La Crosse 病毒,LACV)与人体血清之间相互作用的结果。为了模拟物种之间的生命周期,我们使用了源自昆虫(I-LACV)和人角质形成细胞(HaCaT)的 LACV。将 I-LACV 与正常人体血清孵育不会导致中和,但会稳定 I-LACV 病毒粒子并增加感染性病毒的数量。即使使用缺乏补体活性的热灭活血清和来自包括鼠、雪貂和非人类灵长类动物在内的一系列动物的血清,也可以看到增强的感染性。从血清中耗尽抗体导致丧失增强感染性的能力,蔗糖梯度沉淀分析表明 IgG 与 I-LACV 颗粒共沉淀。与我们用 I-LACV 得到的结果一致,正常人体血清中的补体或抗体不能中和源自 HaCaT 的 LACV。然而,与 I-LACV 相反,单独孵育 HaCaT 衍生的 LACV 时其感染性稳定,而血清处理不会增强感染性。我们的研究结果表明,源自昆虫细胞的 LACV 与源自人类细胞的病毒有很大不同,I-LACV 依赖于血清因子来增强感染性。这些发现表明,了解昆虫与动物细胞衍生的 LACV 的差异组成可能为潜在的新抗病毒方法奠定基础。

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