首页> 外文期刊>Viruses >Deletion of CD2-Like (CD2v) and C-Type Lectin-Like (EP153R) Genes from African Swine Fever Virus Georgia-?9GL Abrogates Its Effectiveness as an Experimental Vaccine
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Deletion of CD2-Like (CD2v) and C-Type Lectin-Like (EP153R) Genes from African Swine Fever Virus Georgia-?9GL Abrogates Its Effectiveness as an Experimental Vaccine

机译:缺失非洲猪瘟病毒Georgia-α的CD2样(CD2V)和C型凝集素样(EP153R)基因 - 9GL废除其作为实验疫苗的有效性

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African swine fever virus (ASFV) is currently the most dreaded infectious disease affecting the global swine production industry. There is no commercial vaccine available, making the culling of infected animals the current solution to control outbreaks. Effective experimental vaccines have been developed by deleting virus genes associated with virulence. Deletion of the ASFV 9GL gene (?9GL) has resulted in the attenuation of different ASFV strains, although the degree of attenuation varies across isolates. Here, we investigated the possibility of the increased safety of the experimental vaccine strain ASFV-G-Δ9GL by deleting two additional virus genes involved in pathogenesis, CD2v, a CD2 like viral encoded gene from the EP402R open reading frame (ORF), and C-type lectin-like viral gene, encoded from the EP153R ORF. Two new recombinant viruses were developed, ASFV-G-Δ9GL/ΔCD2v and ASFV-G-Δ9GL/ΔCD2v/ΔEP153R, harboring two and three gene deletions, respectively. ASFV-G-Δ9GL/ΔCD2v/ΔEP153R, but not ASFV-G-Δ9GL/ΔCD2v, had a decreased ability to replicate in vitro in swine macrophage cultures when compared with parental ASFV-G-Δ9GL. Importantly, ASFV-G-Δ9GL/ΔCD2v and ASFV-G-Δ9GL/ΔCD2v/ΔEP153R induced almost undetectable viremia levels when inoculated into domestic pigs and failed to protect them against challenge with parental virulent ASFV-Georgia, while ASFV-G-Δ9GL offered robust protection during challenge. Therefore, the deletion of CD2-like and C-type lectin-like genes significantly decreased the protective potential of ASFV-G-Δ9GL as a vaccine candidate. This study constitutes an example of the unpredictability of genetic manipulation involving the simultaneous deletion of multiple genes from the ASFV genome.
机译:非洲猪瘟病毒(ASFV)是目前最可怕的传染病,影响了全球猪生产产业。没有可用的商业疫苗,使受感染动物的剔除当前的控制爆发。通过删除与毒力相关的病毒基因开发了有效的实验疫苗。缺失ASFV 9GL基因(α9GL)导致不同ASFV菌株的衰减,尽管衰减程度跨越分离株。在这里,我们通过删除了来自EP402R开放阅读框(ORF)和C的涉及涉及的涉及病症的两种额外病毒基因,CD2和C,研究了涉及病症的两种病毒基因的两种额外的病毒基因来提高实验疫苗菌株ASFV-G-Δ9GL的可能性。型凝集素样病毒基因,从EP153R ORF编码。发育了两种新的重组病毒,分别开发了ASFV-G-Δ9G1/ΔCD2V和ASFV-G-Δ9G1/ΔCD2V/ΔEP153R,分别覆盖了两种和三种基因缺失。与父母ASFV-G-Δ9GL相比,ASFV-G-Δ9G1/ΔCD2V/ΔEP153R具有降低的猪巨噬细胞培养物中体外复制的能力降低。重要的是,当接种到家畜时,ASFV-G-Δ9G1/ΔCD2V和ASFV-G-Δ9G1/ΔCD2V/ΔEP153R几乎不可检测的病毒血症水平,未能用父母毒力ASFV-GERGIA保护它们,而ASFV-G-Δ9GL提供在挑战期间的鲁棒保护。因此,CD2样和C型凝集素样基因的缺失显着降低了ASFV-G-Δ9GL的保护电位作为疫苗候选者。该研究构成了遗传操作的不可预测性的一个例子,涉及从ASFV基因组同时缺失多种基因。

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