大鼠中枢神经系统中神经元被两种伪狂犬病病毒重组体进行特定回路的共感染。
Circuit-specific coinfection of neurons in the rat central nervous system with two pseudorabies virus recombinants.
作者信息
Kim J S, Enquist L W, Card J P
机构信息
Department of Physical Therapy, Taegu University, Taegu, South Korea.
出版信息
J Virol. 1999 Nov;73(11):9521-31. doi: 10.1128/JVI.73.11.9521-9531.1999.
Neurotropic alphaherpesviruses have become popular tools for transynaptic analysis of neural circuitry. It has also been demonstrated that coinfection with two viruses expressing unique reporters can be used to define more complicated circuitry. However, the coinfection studies reported to date have employed nonisogenic strains that differ in their invasive properties. In the present investigation we used two antigenically distinct recombinants of the swine pathogen pseudorabies virus (PRV) in single and double infections of the rat central nervous system. Both viruses are derivatives of PRV-Bartha, a strain with reduced virulence that is widely used for circuit analysis. PRV-BaBlu expresses beta-galactosidase, and PRV-D expresses the PRV membrane protein gI, the gene for which is deleted in PRV-BaBlu. Antibodies to beta-galactosidase identify neurons infected with PRV-BaBlu, and antibodies monospecific for PRV gI identify neurons infected with PRV-D. The ability of these strains to establish coinfections in neurons was evaluated in visual and autonomic circuitry in which the parental virus has previously been characterized. The following conclusions can be drawn from these experiments. First, PRV-D is significantly more neuroinvasive than PRV-Bartha or PRV-BaBlu in the same circuitry. Second, PRV-D is more virulent than either PRV-Bartha or PRV-BaBlu, and PRV-BaBlu is less virulent than PRV-Bartha. Third, in every model examined, PRV-D and PRV-BaBlu coinfect some neurons, but single infections predominate. Fourth, prior infection with one virus renders neurons less permissive to infection by another virus. Fifth, prior infection by PRV-D is more effective than PRV-BaBlu in reducing invasion and spread of the second virus. Collectively, the data define important variables that must be considered in coinfection experiments and suggest that the most successful application of this approach would be accomplished by using isogenic strains of virus with equivalent virulence.
嗜神经α疱疹病毒已成为用于神经回路跨突触分析的常用工具。研究还表明,同时感染两种表达独特报告基因的病毒可用于定义更复杂的神经回路。然而,迄今为止报道的共感染研究使用的是非同基因毒株,它们在侵袭特性上存在差异。在本研究中,我们使用了猪病原体伪狂犬病病毒(PRV)的两种抗原性不同的重组体,对大鼠中枢神经系统进行单感染和双感染。这两种病毒都是PRV-Bartha的衍生物,PRV-Bartha是一种毒力降低的毒株,广泛用于神经回路分析。PRV-BaBlu表达β-半乳糖苷酶,PRV-D表达PRV膜蛋白gI,PRV-BaBlu中该基因缺失。针对β-半乳糖苷酶的抗体可识别感染PRV-BaBlu的神经元,对PRV gI具有单特异性的抗体可识别感染PRV-D的神经元。在视觉和自主神经回路中评估了这些毒株在神经元中建立共感染的能力,此前已对亲代病毒在这些回路中的特性进行了表征。从这些实验中可以得出以下结论。第一,在相同的神经回路中,PRV-D的神经侵袭性明显高于PRV-Bartha或PRV-BaBlu。第二,PRV-D比PRV-Bartha或PRV-BaBlu的毒力更强,而PRV-BaBlu的毒力比PRV-Bartha弱。第三,在每个检测模型中,PRV-D和PRV-BaBlu可共感染一些神经元,但单感染占主导。第四,先前感染一种病毒会使神经元对另一种病毒的感染更不敏感。第五,先前感染PRV-D在减少第二种病毒的侵袭和传播方面比PRV-BaBlu更有效。总体而言,这些数据定义了共感染实验中必须考虑的重要变量,并表明该方法最成功的应用是使用具有同等毒力的同基因病毒株来实现。
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