Division of Infectious Diseases, Department of Medicine, University of California, San Francisco, California, USA.
Chan Zuckerberg Biohub, San Francisco, California, USA.
J Virol. 2022 Sep 28;96(18):e0092122. doi: 10.1128/jvi.00921-22. Epub 2022 Aug 30.
The genus (family ) currently comprises seven viruses, four of which have demonstrated prior evidence of zoonotic capacity. These include the biosafety level 4 agents Hendra (HeV) and Nipah (NiV) viruses, which circulate naturally in pteropodid fruit bats. Here, we describe and characterize Angavokely virus (AngV), a divergent henipavirus identified in urine samples from wild, Madagascar fruit bats. We report the nearly complete 16,740-nucleotide genome of AngV, which encodes the six major henipavirus structural proteins (nucleocapsid, phosphoprotein, matrix, fusion, glycoprotein, and L polymerase). Within the phosphoprotein (P) gene, we identify an alternative start codon encoding the AngV C protein and a putative mRNA editing site where the insertion of one or two guanine residues encodes, respectively, additional V and W proteins. In other paramyxovirus systems, C, V, and W are accessory proteins involved in antagonism of host immune responses during infection. Phylogenetic analysis suggests that AngV is ancestral to all four previously described bat henipaviruses-HeV, NiV, Cedar virus (CedV), and Ghanaian bat virus (GhV)-but evolved more recently than rodent- and shrew-derived henipaviruses, Mojiang (MojV), Gamak (GAKV), and Daeryong (DARV) viruses. Predictive structure-based alignments suggest that AngV is unlikely to bind ephrin receptors, which mediate cell entry for all other known bat henipaviruses. Identification of the AngV receptor is needed to clarify the virus's potential host range. The presence of V and W proteins in the AngV genome suggest that the virus could be pathogenic following zoonotic spillover. Henipaviruses include highly pathogenic emerging zoonotic viruses, derived from bat, rodent, and shrew reservoirs. Bat-borne Hendra (HeV) and Nipah (NiV) are the most well-known henipaviruses, for which no effective antivirals or vaccines for humans have been described. Here, we report the discovery and characterization of a novel henipavirus, Angavokely virus (AngV), isolated from wild fruit bats in Madagascar. Genomic characterization of AngV reveals all major features associated with pathogenicity in other henipaviruses, suggesting that AngV could be pathogenic following spillover to human hosts. Our work suggests that AngV is an ancestral bat henipavirus that likely uses viral entry pathways distinct from those previously described for HeV and NiV. In Madagascar, bats are consumed as a source of human food, presenting opportunities for cross-species transmission. Characterization of novel henipaviruses and documentation of their pathogenic and zoonotic potential are essential to predicting and preventing the emergence of future zoonoses that cause pandemics.
该属(科)目前包括七种病毒,其中四种已证明具有先前的人畜共患能力。这些包括生物安全 4 级的亨德拉(HeV)和尼帕(NiV)病毒,它们在翼手目果蝠中自然循环。在这里,我们描述并表征了 Angavokely 病毒(AngV),这是一种从马达加斯加野生果蝠尿液样本中分离出来的具有差异的亨尼帕病毒。我们报告了 AngV 的几乎完整的 16740 个核苷酸基因组,该基因组编码六种主要的亨尼帕病毒结构蛋白(核衣壳、磷蛋白、基质、融合、糖蛋白和 L 聚合酶)。在磷蛋白(P)基因内,我们确定了一个替代起始密码子,该密码子编码 AngV 的 C 蛋白和一个推定的 mRNA 编辑位点,其中插入一个或两个鸟嘌呤残基分别编码额外的 V 和 W 蛋白。在其他副粘病毒系统中,C、V 和 W 是辅助蛋白,在感染过程中参与拮抗宿主免疫反应。系统发育分析表明,AngV 是之前描述的所有四种蝙蝠亨尼帕病毒-HeV、NiV、雪松病毒(CedV)和加纳蝙蝠病毒(GhV)的祖先,但比源自啮齿动物和鼩鼱的亨尼帕病毒(Mojiang(MojV)、Gamak(GAKV)和 Daeryong(DARV)病毒进化得更晚。基于预测结构的比对表明,AngV 不太可能结合 Ephrin 受体,而所有其他已知的蝙蝠亨尼帕病毒都通过 Ephrin 受体进入细胞。需要鉴定 AngV 的受体,以阐明该病毒的潜在宿主范围。AngV 基因组中存在 V 和 W 蛋白表明,该病毒在人畜共患病溢出后可能具有致病性。亨尼帕病毒包括源自蝙蝠、啮齿动物和鼩鼱的高致病性新兴人畜共患病病毒。蝙蝠传播的亨德拉(HeV)和尼帕(NiV)是最著名的亨尼帕病毒,目前尚未为人类描述有效的抗病毒药物或疫苗。在这里,我们报告了一种新型亨尼帕病毒——安加沃克利病毒(AngV)的发现和表征,该病毒从马达加斯加的野生果蝠中分离出来。AngV 的基因组特征分析揭示了与其他亨尼帕病毒致病性相关的所有主要特征,表明 AngV 可能在溢出到人类宿主后具有致病性。我们的工作表明,AngV 是一种古老的蝙蝠亨尼帕病毒,可能使用与之前描述的 HeV 和 NiV 不同的病毒进入途径。在马达加斯加,蝙蝠被当作人类食物的来源,这为跨物种传播提供了机会。对新型亨尼帕病毒的特性进行描述,并记录其致病和人畜共患潜力,对于预测和预防导致大流行的未来人畜共患疾病的出现至关重要。
