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基于选择分析的猫冠状病毒基因的适应性进化。

Adaptive Evolution of Feline Coronavirus Genes Based on Selection Analysis.

机构信息

College of Animal Science and Veterinary Medicine, Shenyang Agricultural University, Shenyang 110866, China.

Department of Laboratory Medicine and Pathobiology, University of Toronto, Toronto, Ontario, Canada M5S 1A8.

出版信息

Biomed Res Int. 2020 Aug 13;2020:9089768. doi: 10.1155/2020/9089768. eCollection 2020.

Abstract

PURPOSE

We investigated sequences of the feline coronaviruses (FCoV), which include feline enteric coronavirus (FECV) and feline infectious peritonitis virus (FIPV), from China and other countries to gain insight into the adaptive evolution of this virus.

METHODS

Ascites samples from 31 cats with suspected FIP and feces samples from 8 healthy cats were screened for the presence of FCoV. Partial viral genome sequences, including parts of the nsp12-nsp14, S, N, and 7b genes, were obtained and aligned with additional sequences obtained from the GenBank database. Bayesian phylogenetic analysis was conducted, and the possibility of recombination within these sequences was assessed. Analysis of the levels of selection pressure experienced by these sequences was assessed using methods on both the PAML and Datamonkey platforms.

RESULTS

Of the 31 cats investigated, two suspected FIP cats and one healthy cat tested positive for FCoV. Phylogenetic analysis showed that all of the sequences from mainland China cluster together with a few sequences from the Netherlands as a distinct clade when analyzed with FCoV sequences from other countries. Fewer than 3 recombination breakpoints were detected in the nsp12-nsp14, S, N, and 7b genes, suggesting that analyses for positive selection could be conducted. A total of 4, 12, 4, and 4 positively selected sites were detected in the nsp12-nsp14, S, N, and 7b genes, respectively, with the previously described site 245 of the S gene, which distinguishes FIPV from FECV, being a positive selection site. Conversely, 106, 168, 25, and 17 negative selection sites in the nsp12-14, S, N, and 7b genes, respectively, were identified.

CONCLUSION

Our study provides evidence that the FCoV genes encoding replicative, entry, and virulence proteins potentially experienced adaptive evolution. A greater number of sites in each gene experienced negative rather than positive selection, which suggests that most of the protein sequence must be conservatively maintained for virus survival. A few of the sites showing evidence of positive selection might be associated with the more severe pathology of FIPV or help these viruses survive other harmful conditions.

摘要

目的

我们调查了来自中国和其他国家的猫冠状病毒(FCoV)序列,包括猫传染性肠炎冠状病毒(FECV)和猫传染性腹膜炎病毒(FIPV),以深入了解该病毒的适应性进化。

方法

对 31 只疑似 FIP 的猫的腹水样本和 8 只健康猫的粪便样本进行了 FCoV 检测。获得了部分病毒基因组序列,包括 nsp12-nsp14、S、N 和 7b 基因的部分序列,并与从 GenBank 数据库中获得的其他序列进行了比对。进行了贝叶斯系统发育分析,并评估了这些序列中重组的可能性。使用 PAML 和 Datamonkey 平台上的方法评估了这些序列所经历的选择压力水平。

结果

在所研究的 31 只猫中,两只疑似 FIP 的猫和一只健康的猫检测到 FCoV 阳性。系统发育分析显示,当与来自其他国家的 FCoV 序列进行分析时,来自中国大陆的所有序列与来自荷兰的少数序列一起形成一个独特的分支。在 nsp12-nsp14、S、N 和 7b 基因中检测到的重组断点少于 3 个,表明可以进行阳性选择分析。在 nsp12-nsp14、S、N 和 7b 基因中分别检测到 4、12、4 和 4 个阳性选择位点,其中先前描述的 S 基因 245 位区分 FIPV 和 FECV 的位点是一个阳性选择位点。相反,在 nsp12-14、S、N 和 7b 基因中分别鉴定到 106、168、25 和 17 个负选择位点。

结论

我们的研究提供了证据表明,编码复制、进入和毒力蛋白的 FCoV 基因可能经历了适应性进化。每个基因中经历负选择而非正选择的位点更多,这表明为了病毒的生存,必须保守地维持大部分蛋白质序列。一些表现出正选择证据的位点可能与 FIPV 更严重的病理学有关,或者帮助这些病毒在其他有害条件下生存。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9223/7453238/cf96d336258f/BMRI2020-9089768.001.jpg

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