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脱髓鞘疾病的体内和体外模型。十二、潜伏期期间日冕JHM病毒功能在RN2-2雪旺瘤细胞中的持续存在和表达。

In vivo and in vitro models of demyelinating diseases. XII. Persistence and expression of corona JHM virus functions in RN2-2 Schwannoma cells during latency.

作者信息

Coulter-Mackie M, Adler R, Wilson G, Dales S

出版信息

Virus Res. 1985 Oct;3(3):245-61. doi: 10.1016/0168-1702(85)90049-8.

Abstract

The coronavirus JHMV persistently infects rat Schwannoma cells RN2-2 at 32.5 degrees C and enters a host-imposed reversible, latent state at 39.5 degrees C. JHMV can remain up to 20 days in the latent state and about 14 days before the cultures lose the capacity to resume virus production upon return to 32.5 degrees C. Although persistently and latently infected RN2-2 cells display resistance to superinfection by a heterologous agent VSV, these cells do not release detectable soluble mediators (e.g., interferon) of the antiviral state. Nevertheless, RN2-2 cells are competent to synthesize and release interferon when treated with the appropriate inducers. These observations suggest that interferon does not play any role or may not be the major factor in the control of latency in the Schwannoma cell. Hybridization with virus-specific cDNAs shows that all viral mRNAs are present during latency and that viral mRNAs are present in the polysomes of infected cells at 39.5 degrees C. Western immunoblotting with hybridoma antibodies demonstrates that viral specific proteins are produced at the restrictive temperature. These results suggest that despite the absence of production of infectious virus at 39.5 degrees C, there is active transcription and translation into virus-specified products.

摘要

冠状病毒JHMV在32.5摄氏度时持续感染大鼠雪旺细胞瘤细胞RN2-2,并在39.5摄氏度时进入宿主施加的可逆潜伏状态。JHMV可在潜伏状态下持续长达20天,在培养物恢复到32.5摄氏度后失去恢复病毒产生能力之前约持续14天。尽管持续和潜伏感染的RN2-2细胞对异源病毒VSV的超感染具有抗性,但这些细胞不会释放可检测到的抗病毒状态的可溶性介质(如干扰素)。然而,当用适当的诱导剂处理时,RN2-2细胞有能力合成并释放干扰素。这些观察结果表明,干扰素在雪旺细胞瘤细胞潜伏控制中不发挥任何作用或可能不是主要因素。与病毒特异性cDNA杂交表明,在潜伏期间所有病毒mRNA均存在,并且在39.5摄氏度时病毒mRNA存在于受感染细胞的多核糖体中。用杂交瘤抗体进行的蛋白质免疫印迹表明,在限制温度下产生病毒特异性蛋白质。这些结果表明,尽管在39.5摄氏度时没有产生感染性病毒,但仍有活跃的转录和翻译成病毒指定产物的过程。

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The biology of coronaviruses.冠状病毒的生物学特性。
J Gen Virol. 1983 Apr;64 (Pt 4):761-76. doi: 10.1099/0022-1317-64-4-761.

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