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在登革热恢复期血清存在的情况下进行复制会影响寨卡病毒的中和敏感性和适应性。

Replication in the presence of dengue convalescent serum impacts Zika virus neutralization sensitivity and fitness.

机构信息

Translational Biology, Medicine, and Health Graduate Program, Virginia Tech, Roanoke, VA, United States.

Department of Biomedical Sciences and Pathobiology, Virginia Tech, Virginia-Maryland Regional College of Veterinary Medicine, Blacksburg, VA, United States.

出版信息

Front Cell Infect Microbiol. 2023 Mar 9;13:1130749. doi: 10.3389/fcimb.2023.1130749. eCollection 2023.

Abstract

INTRODUCTION

Flaviviruses like dengue virus (DENV) and Zika virus (ZIKV) are mosquito-borne viruses that cause febrile, hemorrhagic, and neurological diseases in humans, resulting in 400 million infections annually. Due to their co-circulation in many parts of the world, flaviviruses must replicate in the presence of pre-existing adaptive immune responses targeted at serologically closely related pathogens, which can provide protection or enhance disease. However, the impact of pre-existing cross-reactive immunity as a driver of flavivirus evolution, and subsequently the implications on the emergence of immune escape variants, is poorly understood. Therefore, we investigated how replication in the presence of convalescent dengue serum drives ZIKV evolution.

METHODS

We used an directed evolution system, passaging ZIKV in the presence of serum from humans previously infected with DENV (anti-DENV) or serum from DENV-naïve patients (control serum). Following five passages in the presence of serum, we performed next-generation sequencing to identify mutations that arose during passaging. We studied two non-synonymous mutations found in the anti-DENV passaged population (E-V355I and NS1-T139A) by generating individual ZIKV mutants and assessing fitness in mammalian cells and live mosquitoes, as well as their sensitivity to antibody neutralization.

RESULTS AND DISCUSSION

Both viruses had increased fitness in Vero cells with and without the addition of anti-DENV serum and in human lung epithelial and monocyte cells. In Aedes aegypti mosquitoes-using blood meals with and without anti-DENV serum-the mutant viruses had significantly reduced fitness compared to wild-type ZIKV. These results align with the trade-off hypothesis of constrained mosquito-borne virus evolution. Notably, only the NS1-T139A mutation escaped neutralization, while E-V335I demonstrated enhanced neutralization sensitivity to neutralization by anti-DENV serum, indicating that neutralization escape is not necessary for viruses passaged under cross-reactive immune pressures. Future studies are needed to assess cross-reactive immune selection in humans and relevant animal models or with different flaviviruses.

摘要

简介

登革热病毒(DENV)和寨卡病毒(ZIKV)等黄病毒是通过蚊子传播的病毒,会导致人类出现发热、出血和神经疾病,每年导致 4 亿例感染。由于它们在世界许多地区共同传播,黄病毒必须在针对血清学上密切相关病原体的已存在适应性免疫反应存在的情况下进行复制,这可能会提供保护或增强疾病。然而,预先存在的交叉反应性免疫作为黄病毒进化的驱动因素的影响,以及随后对免疫逃避变异体出现的影响,知之甚少。因此,我们研究了在存在恢复期登革热血清的情况下,ZIKV 的复制如何驱动其进化。

方法

我们使用定向进化系统,在先前感染 DENV(抗-DENV)的人类血清或 DENV 未感染患者的血清(对照血清)存在的情况下传代 ZIKV。在血清存在的情况下传代五次后,我们进行下一代测序以鉴定传代过程中出现的突变。我们通过生成单个 ZIKV 突变体并评估其在哺乳动物细胞和活体蚊子中的适应性以及对抗体中和的敏感性,研究了在抗-DENV 传代群体中发现的两个非同义突变(E-V355I 和 NS1-T139A)。

结果与讨论

两种病毒在添加或不添加抗-DENV 血清的情况下在 Vero 细胞以及人肺上皮细胞和单核细胞中均具有更高的适应性。在携带和不携带抗-DENV 血清的埃及伊蚊中-使用血液餐-突变病毒的适应性与野生型 ZIKV 相比显著降低。这些结果与受约束的蚊媒病毒进化的权衡假说一致。值得注意的是,只有 NS1-T139A 突变逃脱了中和,而 E-V335I 对中和的敏感性增强,表明在交叉反应性免疫压力下传代的病毒不需要逃避中和。未来的研究需要评估人类和相关动物模型或不同黄病毒中的交叉反应性免疫选择。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c118/10034770/4202b52a2ccb/fcimb-13-1130749-g001.jpg

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