Institute of Diagnostic Virology, Friedrich-Loeffler-Institut, Greifswald-Insel Riems, Germany.
J Gen Virol. 2024 Jun;105(6). doi: 10.1099/jgv.0.002005.
Schmallenberg virus (SBV) belongs to the Simbu serogroup within the family , genus and is transmitted by biting midges. Infection of naïve ruminants in a critical phase of gestation may lead to severe congenital malformations. Sequence analysis from viremic animals revealed a very high genome stability. In contrast, sequence variations are frequently described for SBV from malformed fetuses. In addition to S segment mutations, especially within the M segment encoding the major immunogen Gc, point mutations or genomic deletions are also observed. Analysis of the SBV_D281/12 isolate from a malformed fetus revealed multiple point mutations in all three genome segments. It also has a large genomic deletion in the antigenic domain encoded by the M segment compared to the original SBV reference strain 'BH80/11' isolated from viremic blood in 2011. Interestingly, SBV_D281/12 showed a marked replication deficiency in cells (KC cells), but not in standard baby hamster kidney cells (BHK-21). We therefore generated a set of chimeric viruses of rSBV_D281/12 and wild-type rSBV_BH80/11 by reverse genetics, which were characterized in both KC and BHK-21 cells. It could be shown that the S segment of SBV_D281/12 is responsible for the replication deficit and that it acts independently from the large deletion within Gc. In addition, a single point mutation at position 111 (S to N) of the nucleoprotein was identified as the critical mutation. Our results suggest that virus variants found in malformed fetuses and carrying characteristic genomic mutations may have a clear 'loss of fitness' for their insect hosts . It can also be concluded that such mutations lead to virus variants that are no longer part of the natural transmission cycle between mammalian and insect hosts. Interestingly, analysis of a series of SBV sequences confirmed the S111N mutation exclusively in samples of malformed fetuses and not in blood from viremic animals. The characterization of these changes will allow the definition of protein functions that are critical for only one group of hosts.
沙尔贝病毒(SBV)属于布姆病毒科、黄病毒属、披膜病毒科,通过吸血蠓传播。处于妊娠关键阶段的初感反刍动物感染 SBV 可能导致严重的先天性畸形。对病毒血症动物的序列分析显示其基因组非常稳定。相比之下,从畸形胎儿中经常可以发现 SBV 序列变异。除 S 片段突变外,尤其是编码主要免疫原 Gc 的 M 片段编码区,还观察到点突变或基因组缺失。对来自畸形胎儿的 SBV_D281/12 分离株的分析显示,所有三个基因组片段都存在多个点突变。与 2011 年从病毒血症血液中分离到的原始 SBV 参考株“BH80/11”相比,它在 M 片段编码的抗原结构域中还具有一个大的基因组缺失。有趣的是,与标准仓鼠肾细胞(BHK-21)相比,SBV_D281/12 在 KC 细胞(仓鼠肾细胞)中表现出明显的复制缺陷。因此,我们通过反向遗传学生成了一组 rSBV_D281/12 和野生型 rSBV_BH80/11 的嵌合病毒,并在 KC 和 BHK-21 细胞中对其进行了表征。结果表明,SBV_D281/12 的 S 片段负责复制缺陷,并且该缺陷独立于 Gc 内的大片段缺失起作用。此外,还鉴定出核蛋白位置 111 处(S 到 N)的单点突变是关键突变。我们的结果表明,在畸形胎儿中发现的并携带特征性基因组突变的病毒变体可能对其昆虫宿主的适应性明显降低。还可以得出结论,这种突变导致的病毒变体不再是哺乳动物和昆虫宿主之间自然传播循环的一部分。有趣的是,对一系列 SBV 序列的分析仅在畸形胎儿样本中证实了 S111N 突变,而在病毒血症动物的血液中没有发现该突变。对这些变化的分析将允许定义仅对一组宿主至关重要的蛋白功能。
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