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从唾液中对寨卡病毒肽进行产后鉴定。

Postnatal Identification of Zika Virus Peptides from Saliva.

作者信息

Zuanazzi D, Arts E J, Jorge P K, Mulyar Y, Gibson R, Xiao Y, Bringel Dos Santos M, Machado Maria Aparecida A M, Siqueira W L

机构信息

1 Schulich Dentistry and Department of Biochemistry, Schulich School of Medicine & Dentistry, The University of Western Ontario, London, ON, Canada.

2 Department of Microbiology and Immunology, Schulich School of Medicine & Dentistry, The University of Western Ontario, London, ON, Canada.

出版信息

J Dent Res. 2017 Sep;96(10):1078-1084. doi: 10.1177/0022034517723325.

Abstract

We explored the potential to diagnose Zika virus (ZIKV) infection by analyzing peptides in saliva during a convalescent phase of infection, long after resolution of acute disease. A 25-y-old woman clinically diagnosed with Zika fever in the first trimester was enrolled with her dizygotic twins for a 3-mo postnatal sample of saliva (9-mo after maternal infection). The female baby (A) had microcephaly while the male baby (B) was born healthy. Peptidomic analysis was completed by mass spectrometry (MS/MS), and ZIKV peptides were identified using the National Institutes of Health Zika Virus Resource database, then aligned and mapped to the ZIKV polyprotein to determine proteome coverage and phylogenetic studies. A total of 423 (mother), 607 (baby A), and 183 (baby B) unique ZIKV peptides were identified in saliva by MS/MS, providing a coverage of 67%, 84%, and 45%, respectively, of the entire ZIKV polyprotein (>3,400 amino acids). All peptides were aligned to other flaviviruses that are circulating in Brazil (dengue and yellow fever) to discard false-positive matches. Nine peptides identified were highly conserved to dengue virus. Alignment of a contiguous peptide sequence for mother/babies with the 74 ZIKV sequences suggested that the virus may have entered the oral cavity through the salivary glands, leading to an infection that persists into the postnatal period (vertical transmission). Furthermore, we identified 9 sequence variations that were unique to the baby with microcephaly (not found in the mother or the twin). This sequence information could provide a template for future neuropathogenic studies. A much larger sample size is required to determine whether sequence variation in the envelope protein significantly associates with microcephaly. Finally, from a public health perspective, it will be important to determine whether viral replication is still taking place after birth and whether the virus can be transmitted through salivary contact.

摘要

我们通过分析感染恢复期(急性疾病消退很久之后)唾液中的肽段,探索了诊断寨卡病毒(ZIKV)感染的可能性。一名在孕早期临床诊断为寨卡热的25岁女性与其异卵双胞胎参与了研究,采集了产后3个月(母亲感染后9个月)的唾液样本。女婴(A)患有小头畸形,而男婴(B)出生时健康。通过质谱(MS/MS)完成了肽组学分析,使用美国国立卫生研究院寨卡病毒资源数据库鉴定寨卡病毒肽段,然后将其比对并映射到寨卡病毒多聚蛋白上,以确定蛋白质组覆盖范围并进行系统发育研究。通过MS/MS在唾液中分别鉴定出423条(母亲)、607条(婴儿A)和183条(婴儿B)独特的寨卡病毒肽段,分别覆盖了整个寨卡病毒多聚蛋白(超过3400个氨基酸)的67%、84%和45%。所有肽段都与在巴西流行的其他黄病毒(登革热和黄热病)进行比对,以排除假阳性匹配。鉴定出的9条肽段与登革热病毒高度保守。将母亲/婴儿的连续肽段序列与74条寨卡病毒序列进行比对,表明病毒可能通过唾液腺进入口腔,导致感染持续到产后阶段(垂直传播)。此外,我们鉴定出9个序列变异,这些变异是患小头畸形婴儿所特有的(在母亲或双胞胎中未发现)。该序列信息可为未来的神经病理学研究提供模板。需要更大的样本量来确定包膜蛋白中的序列变异是否与小头畸形显著相关。最后,从公共卫生角度来看,确定出生后病毒是否仍在复制以及病毒是否可通过唾液接触传播将非常重要。

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