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与大西洋鲑(Salmo salar)心脏和骨骼肌炎症(HSMI)相关的鱼类正呼肠孤病毒(PRV)基因组的序列分析。

Sequence analysis of the genome of piscine orthoreovirus (PRV) associated with heart and skeletal muscle inflammation (HSMI) in Atlantic salmon (Salmo salar).

机构信息

Department of Laboratory Services, National Veterinary Institute, Oslo, Norway.

出版信息

PLoS One. 2013 Jul 29;8(7):e70075. doi: 10.1371/journal.pone.0070075. Print 2013.

Abstract

Piscine orthoreovirus (PRV) is associated with heart- and skeletal muscle inflammation (HSMI) of farmed Atlantic salmon (Salmo salar). We have performed detailed sequence analysis of the PRV genome with focus on putative encoded proteins, compared with prototype strains from mammalian (MRV T3D)- and avian orthoreoviruses (ARV-138), and aquareovirus (GCRV-873). Amino acid identities were low for most gene segments but detailed sequence analysis showed that many protein motifs or key amino acid residues known to be central to protein function are conserved for most PRV proteins. For M-class proteins this included a proline residue in μ2 which, for MRV, has been shown to play a key role in both the formation and structural organization of virus inclusion bodies, and affect interferon-β signaling and induction of myocarditis. Predicted structural similarities in the inner core-forming proteins λ1 and σ2 suggest a conserved core structure. In contrast, low amino acid identities in the predicted PRV surface proteins μ1, σ1 and σ3 suggested differences regarding cellular interactions between the reovirus genera. However, for σ1, amino acid residues central for MRV binding to sialic acids, and cleavage- and myristoylation sites in μ1 required for endosomal membrane penetration during infection are partially or wholly conserved in the homologous PRV proteins. In PRV σ3 the only conserved element found was a zinc finger motif. We provide evidence that the S1 segment encoding σ3 also encodes a 124 aa (p13) protein, which appears to be localized to intracellular Golgi-like structures. The S2 and L2 gene segments are also potentially polycistronic, predicted to encode a 71 aa- (p8) and a 98 aa (p11) protein, respectively. It is concluded that PRV has more properties in common with orthoreoviruses than with aquareoviruses.

摘要

鱼类正呼肠孤病毒(PRV)与养殖大西洋鲑(Salmo salar)的心肌和骨骼肌炎症(HSMI)有关。我们对 PRV 基因组进行了详细的序列分析,重点是潜在编码蛋白,与哺乳动物(MRV T3D)和禽呼肠孤病毒(ARV-138)以及水产呼肠孤病毒(GCRV-873)的原型株进行了比较。大多数基因片段的氨基酸同一性较低,但详细的序列分析表明,许多已知对蛋白质功能至关重要的蛋白质结构域或关键氨基酸残基在大多数 PRV 蛋白中都得到了保守。对于 M 类蛋白,μ2 中的脯氨酸残基对于 MRV 来说,在病毒包含体的形成和结构组织以及影响干扰素-β信号和诱导心肌炎方面发挥着关键作用。预测的内芯形成蛋白 λ1 和 σ2 的结构相似性表明存在保守的核心结构。相比之下,预测的 PRV 表面蛋白 μ1、σ1 和 σ3 的氨基酸同一性较低,表明呼肠孤病毒属之间的细胞相互作用存在差异。然而,对于 σ1,对于 MRV 与唾液酸结合以及 μ1 中用于感染期间内体膜穿透的切割和豆蔻酰化位点至关重要的氨基酸残基部分或完全在同源 PRV 蛋白中保守。在 PRV σ3 中,唯一发现的保守元件是一个锌指结构域。我们提供的证据表明,编码 σ3 的 S1 片段还编码一个 124 个氨基酸(p13)的蛋白质,该蛋白质似乎定位于细胞内的高尔基样结构中。S2 和 L2 基因片段也可能是多顺反子,分别预测编码一个 71 个氨基酸(p8)和一个 98 个氨基酸(p11)的蛋白质。综上所述,PRV 与正呼肠孤病毒的共同特征多于与水产呼肠孤病毒。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/01cd/3726481/50553aefa7da/pone.0070075.g001.jpg

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