首页> 外文期刊>Pesquisa Veterinária Brasileira >Mapping the sites of latency and reactivation by bovine herpesvirus 5 (BoHV-5) and a thymidine kinase-deleted BoHV-5 in lambs
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Mapping the sites of latency and reactivation by bovine herpesvirus 5 (BoHV-5) and a thymidine kinase-deleted BoHV-5 in lambs

机译:绘制绵羊疱疹病毒5(BoHV-5)和胸腺嘧啶激酶缺失的BoHV-5的潜伏期和再激活部位的图谱

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A thymidine kinase (tk)-deleted bovine herpesvirus 5 (BoHV-5tkΔ) was previously shown to establish latent infection and reactivate - even poorly - in a sheep model (Cadore et al. 2013). As TK-negative alphaherpesviruses are unlike to reactivate in neural tissue, this study investigated the sites of latency and reactivation by this recombinant in lambs. For this, groups of lambs were inoculated intranasally with the parental BoHV-5 strain (SV-507/99) or with the recombinant BoHV-5tkΔ. During latent infection (40 days post-inoculation, pi), the distribution of recombinant virus DNA in neural and non-neural tissues was similar to that of the parental virus. Parental and recombinant virus DNA was consistently detected by PCR in trigeminal ganglia (TGs); frequently in palatine and pharyngeal tonsils and, less frequently in the retropharyngeal lymph nodes. In addition, latent DNA of both viruses was detected in several areas of the brain. After dexamethasone (Dx) administration (day 40pi), the recombinant virus was barely detected in nasal secretions contrasting with marked shedding of the parental virus. In tissues of lambs euthanized at day 3 post-Dx treatment (pDx), reverse-transcription-PCR (RT-PCR) for a late viral mRNA (glycoprotein D gene) demonstrated reactivation of parental virus in neural (TGs) and lymphoid tissues (tonsils, lymph node). In contrast, recombinant virus mRNA was detected only in lymphoid tissues. These results demonstrate that BoHV-5 and the recombinant BoHV-5tkΔ do establish latent infection in neural and non-neural sites. Reactivation of the recombinant BoHV-5tkΔ, however, appeared to occur only in non-neural sites. In anyway, the ability of a tk-deleted strain to reactivate latent infection deserves attention in the context of vaccine safety.
机译:先前已证明,在绵羊模型中,缺失胸腺嘧啶激酶(tk)的牛疱疹病毒5(BoHV-5tkΔ)可建立潜伏感染并重新激活(甚至差)(Cadore等人,2013)。由于TK阴性α疱疹病毒在神经组织中不太可能重新激活,因此本研究调查了这种重组体在羔羊中潜伏和重新激活的部位。为此,将几组羔羊鼻内接种亲代BoHV-5株(SV-507 / 99)或重组BoHV-5tkΔ。在潜伏感染期间(接种后40天,pi),重组病毒DNA在神经组织和非神经组织中的分布与亲本病毒相似。通过PCR在三叉神经节(TGs)中始终检测到亲本和重组病毒DNA。常见于p扁桃体和咽扁桃体,少见于咽后淋巴结。此外,在大脑的多个区域还检测到了两种病毒的潜伏性DNA。地塞米松(Dx)给药后(第40pi天),与亲本病毒明显脱落形成鲜明对比的是,在鼻分泌物中几乎未检测到重组病毒。在Dx处理后第3天(pDx)安乐死的羔羊组织中,晚期病毒mRNA(糖蛋白D基因)的逆转录PCR(RT-PCR)显示神经细胞(TGs)和淋巴组织中的亲本病毒重新激活(扁桃体,淋巴结)。相反,仅在淋巴组织中检测到重组病毒mRNA。这些结果表明,BoHV-5和重组BoHV-5tkΔ确实在神经和非神经部位建立了潜在的感染。然而,重组BoHV-5tkΔ的再激活似乎仅在非神经部位发生。无论如何,在疫苗安全性的背景下,tk缺失菌株重新激活潜伏感染的能力值得关注。

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