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Analysis of Host Range Restriction Determinants in the Rabbit Model: Comparison of Homologous and Heterologous Rotavirus Infections

机译:兔模型中宿主范围限制决定因素的分析:同源和异源轮状病毒感染的比较

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摘要

The main limitation of both the rabbit and mouse models of rotavirus infection is that human rotavirus (HRV) strains do not replicate efficiently in either animal. The identification of individual genes necessary for conferring replication competence in a heterologous host is important to an understanding of the host range restriction of rotavirus infections. We recently reported the identification of the P type of the spike protein VP4 of four lapine rotavirus strains as being P[14]. To determine whether VP4 is involved in host range restriction in rabbits, we evaluated infection in rotavirus antibody-free rabbits inoculated orally with two P[14] HRVs, PA169 (G6) and HAL1166 (G8), and with several other HRV strains and animal rotavirus strains of different P and G types. We also evaluated whether the parental rhesus rotavirus (RRV) (P5B[3], G3) and the derived RRV-HRV reassortant candidate vaccine strains RRV × D (G1), RRV × DS-1 (G2), and RRV × ST3 (G4) would productively infect rabbits. Based on virus shedding, limited replication was observed with the P[14] HRV strains and with the SA11 Cl3 (P[2], G3) and SA11 4F (P6[1], G3) animal rotavirus strains, compared to the homologous ALA strain (P[14], G3). However, even limited infection provided complete protection from rotavirus infection when rabbits were challenged orally 28 days postinoculation (DPI) with 103 50% infective doses of ALA rabbit rotavirus. Other HRVs did not productively infect rabbits and provided no significant protection from challenge, in spite of occasional seroconversion. Simian RRV replicated as efficiently as lapine ALA rotavirus in rabbits and provided complete protection from ALA challenge. Live attenuated RRV reassortant vaccine strains resulted in no, limited, or productive infection of rabbits, but all rabbits were completely protected from heterotypic ALA challenge. The altered replication efficiency of the reassortants in rabbits suggests a role for VP7 in host range restriction. Also, our results suggest that VP4 may be involved in, but is not exclusively responsible for, host range restriction in the rabbit model. The replication efficiency of rotavirus in rabbits also is not controlled by the product of gene 5 (NSP1) alone, since a reassortant rotavirus with ALA gene 5 and all other genes from SA11 was more severely replication restricted than either parental rotavirus strain.
机译:轮状病毒感染的兔子和小鼠模型的主要局限性在于,人类轮状病毒(HRV)株不能在任何一只动物中有效复制。鉴定赋予异源宿主复制能力所必需的单个基因对于理解轮状病毒感染的宿主范围限制很重要。最近,我们报道了四种Lapin轮状病毒株的突触蛋白VP4的P型鉴定为P [14]。为了确定VP4是否参与兔的宿主范围限制,我们评估了口服接种两种P [14] HRV,PA169(G6)和HAL1166(G8)以及其他几种HRV株和动物的无轮状病毒抗体的兔子的感染情况不同P和G类型的轮状病毒株。我们还评估了亲代恒河猴轮状病毒(RRV)(P5B [3],G3)和衍生的RRV-HRV重配候选疫苗株RRV×D(G1),RRV×DS-1(G2)和RRV×ST3( G4)会感染兔子。基于病毒脱落,与同源ALA相比,在P [14] HRV菌株以及SA11 Cl3(P [2],G3)和SA11 4F(P6 [1],G3)动物轮状病毒株中观察到有限的复制。株(P [14],G3)。但是,当兔子在接种后28天(DPI)用10 3 50%感染剂量的ALA兔子轮状病毒进行口服攻击时,即使是有限的感染也能提供对轮状病毒感染的完全保护。尽管偶尔发生血清转化,但其他HRV并没有有效感染兔子,也没有提供有效的抗攻击保护。猿猴RRV在兔中的复制能力与高山ALA轮状病毒一样有效,并提供了针对ALA攻击的全面保护。减毒活的RRV重配疫苗株导致兔子无,有限或生产性感染,但所有兔子均受到完全保护,免受异型ALA攻击。重组子在兔中复制效率的改变表明VP7在宿主范围限制中的作用。同样,我们的结果表明,VP4可能参与了兔子模型中宿主范围的限制,但并非专门负责。轮状病毒在兔中的复制效率也不受基因5(NSP1)产物的控制,因为与任一亲本轮状病毒株相比,具有ALA基因5和SA11所有其他基因的重配轮状病毒受到更严格的复制限制。

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