寻找昆虫病毒通过水平基因转移获得的基因,特别是分析 ABC 转运体基因的转移。

IF 2.5 4区 医学 Q3 VIROLOGY
Takafumi N Sugimoto , Akiya Jouraku , Wataru Mitsuhashi
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引用次数: 0

摘要

尽管人们普遍认为大型DNA病毒通过水平基因转移(HGT)获得基因,但这种转移的具体方式尚未完全阐明。在这里,我们搜索了鞘翅目昆虫毒性病毒(EV)Anomala cuprea entomopoxvirus(ACEV)中可能通过水平基因转移获得的基因。我们将 HGT 的潜在来源生物分为三类:宿主杯状疟原虫;其他生物,包括与 EV 无关的病毒;以及宿主归属不确定的生物。在ACEV基因组的开放阅读框(ORF)中,2.1%被认为是ACEV或其最近的祖先通过HGT从宿主那里获得的;8.7%可能来自宿主以外的生物;3.7%可能是通过HGT从第三类生物那里获得的。分析表明,ACEV含有一些通过HGT获得的有趣的ORF,包括一个大的ATP结合盒蛋白(ABC转运体)ORF和一个tenascin ORF(ID分别为ACV025和ACV123)。我们随后对 ACEV 大 ABC 转运体 ORF(ACEV ORF 中最大的一个)的 HGT 进行了详细分析。我们对从病毒宿主 A. cuprea 幼虫的脂肪体(ACEV 复制场所)和中肠组织(ACEV 初次感染场所)中通过 RNA-seq 获得的 mRNA 序列进行了 BLAST 分析。脂肪体中的一种ABC转运体ORF和中肠组织中的两种ABC转运体ORF(其中一种与脂肪体中的相同)与ACEV的ABC转运体ORF具有最大的同一性。来自宿主的两种类型彼此具有高度的同一性(约 95% 的核苷酸序列同一性),这有力地表明由这两种类型组成的宿主 ABC 转运体群是 ACV025 的起源。随后,我们确定了包含杯状芽孢杆菌 ABC 转运体全长基因的序列(12,381 bp)。结果表明,它是在两种组织中发现的上述 mRNA 的转录模板。此外,我们还确定了仅在中肠组织中发现的 mRNA 的大部分(约 6.9 kb)模板序列。结果表明,ACEV ABC 转运体 ORF 缺失了与宿主 ABC 转运体基因内含子相对应的部分,这表明 ORF 很可能是以 mRNA 的形式通过 HGT 获得的。在 ACEV ABC 转运体基因附近没有观察到明确的重复序列--这是 LINE-1 逆转座子介导的 HGT 的迹象。为期约 2 个月的 ACV025 转录实验表明,该转运体序列被推测为具有持续功能。ACV025 的氨基酸序列表明,其产物可能具有调节宿主细胞膜磷脂的功能。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Search for genes gained by horizontal gene transfer in an entomopoxvirus, with special reference to the analysis of the transfer of an ABC transporter gene

Although it is generally believed that large DNA viruses capture genes by horizontal gene transfer (HGT), the detailed manner of such transfer has not been fully elucidated. Here, we searched for genes in the coleopteran entomopoxvirus (EV) Anomala cuprea entomopoxvirus (ACEV) that might have been gained by ACEV by HGT. We classified the potential source organisms for HGT into three categories: the host A. cuprea; other organisms, including viruses unrelated to EVs; and organisms with uncertain host attribution. Of the open reading frames (ORFs) of the ACEV genome, 2.1 % were suggested to have been gained from the host by ACEV or its recent ancestor via HGT; 8.7 % were possibly from organisms other than the host, and 3.7 % were possibly from the third category of organisms via HGT. The analysis showed that ACEV contains some interesting ORFs obtained by HGT, including a large ATP-binding cassette protein (ABC transporter) ORF and a tenascin ORF (IDs ACV025 and ACV123, respectively). We then performed a detailed analysis of the HGT of the ACEV large ABC transporter ORF—the largest of the ACEV ORFs. mRNA sequences obtained by RNA-seq from fat bodies—sites of ACEV replication—and midgut tissues—sites of initial infection—of the virus's host A. cuprea larvae were subjected to BLAST analysis. One type of ABC transporter ORF from the fat bodies and two types from the midgut tissues, one of which was identical to that in the fat bodies, had the greatest identity to the ABC transporter ORF of ACEV. The two types from the host had high levels of identity to each other (approximately 95 % nucleotide sequence identity), strongly suggesting that the host ABC transporter group consisting of the two types was the origin of ACV025. We then determined the sequence (12,381 bp) containing a full-length gene of the A. cuprea ABC transporter. It turned out to be a transcription template for the abovementioned mRNA found in both tissues. In addition, we determined a large part (ca. 6.9 kb) of the template sequence for the mRNA found only in the midgut tissues. The results showed that the ACEV ABC transporter ORF is missing parts corresponding to introns of the host ABC transporter genes, indicating that the ORF was likely acquired by HGT in the form of mRNA. The presence of definite duplicated sequences adjacent to the ACEV ABC transporter genes—a sign of LINE-1 retrotransposon-mediated HGT—was not observed. An approximately 2-month ACV025 transcription experiment suggested that the transporter sequence is presumed to be continuously functional. The amino acid sequence of ACV025 suggests that its product might function in the regulation of phosphatide in the host-cell membranes.

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来源期刊
Virus research
Virus research 医学-病毒学
CiteScore
9.50
自引率
2.00%
发文量
239
审稿时长
43 days
期刊介绍: Virus Research provides a means of fast publication for original papers on fundamental research in virology. Contributions on new developments concerning virus structure, replication, pathogenesis and evolution are encouraged. These include reports describing virus morphology, the function and antigenic analysis of virus structural components, virus genome structure and expression, analysis on virus replication processes, virus evolution in connection with antiviral interventions, effects of viruses on their host cells, particularly on the immune system, and the pathogenesis of virus infections, including oncogene activation and transduction.
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