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野生型麻疹病毒的C蛋白在体外和猕猴体内生长的严格要求。

Stringent requirement for the C protein of wild-type measles virus for growth both in vitro and in macaques.

作者信息

Takeuchi Kaoru, Takeda Makoto, Miyajima Naoko, Ami Yasushi, Nagata Noriyo, Suzaki Yuriko, Shahnewaz Jamila, Kadota Shin-Ichi, Nagata Kyosuke

机构信息

Department of Infection Biology, Graduate School of Comprehensive Human Sciences and Institute of Basic Medical Sciences, University of Tsukuba, 1-1-1 Tennodai, Tsukuba, Ibaraki 305-8575, Japan.

出版信息

J Virol. 2005 Jun;79(12):7838-44. doi: 10.1128/JVI.79.12.7838-7844.2005.

Abstract

The P gene of measles virus (MV) encodes the P protein and three accessory proteins (C, V, and R). However, the role of these accessory proteins in the natural course of MV infection remains unclear. For this study, we generated a recombinant wild-type MV lacking the C protein, called wtMV(C-), by using a reverse genetics system (M. Takeda, K. Takeuchi, N. Miyajima, F. Kobune, Y. Ami, N. Nagata, Y. Suzaki, Y. Nagai, and M. Tashiro, J. Virol. 74:6643-6647). When 293 cells expressing the MV receptor SLAM (293/hSLAM) were infected with wtMV(C-) or parental wild-type MV (wtMV), the growth of wtMV(C-) was restricted, particularly during late stages. Enhanced green fluorescent protein-expressing wtMV(C-) consistently induced late-stage cell rounding and cell death in the presence of a fusion-inhibiting peptide, suggesting that the C protein can prevent cell death and is required for long-term MV infection. Neutralizing antibodies against alpha/beta interferon did not restore the growth restriction of wtMV(C-) in 293/hSLAM cells. When cynomolgus monkeys were infected with wtMV(C-) or wtMV, the number of MV-infected cells in the thymus was >1,000-fold smaller for wtMV(C-) than for wtMV. Immunohistochemical analyses showed strong expression of an MV antigen in the spleen, lymph nodes, tonsils, and larynx of a cynomolgus monkey infected with wtMV but dramatically reduced expression in the same tissues in a cynomolgus monkey infected with wtMV(C-). These data indicate that the MV C protein is necessary for efficient MV replication both in vitro and in cynomolgus monkeys.

摘要

麻疹病毒(MV)的P基因编码P蛋白和三种辅助蛋白(C、V和R)。然而,这些辅助蛋白在MV感染自然病程中的作用仍不清楚。在本研究中,我们通过反向遗传学系统(武田真、竹内健、宫岛直、小布施文、阿美洋、永田直、铃木洋、永井洋、田代正明,《病毒学杂志》74:6643 - 6647)构建了一种缺失C蛋白的重组野生型MV,称为wtMV(C-)。当用wtMV(C-)或亲本野生型MV(wtMV)感染表达MV受体SLAM的293细胞(293/hSLAM)时,wtMV(C-)的生长受到限制,尤其是在后期。在存在融合抑制肽的情况下,表达增强绿色荧光蛋白的wtMV(C-)持续诱导后期细胞变圆和细胞死亡,这表明C蛋白可以防止细胞死亡,并且是MV长期感染所必需的。针对α/β干扰素的中和抗体不能恢复wtMV(C-)在293/hSLAM细胞中的生长限制。当食蟹猴感染wtMV(C-)或wtMV时,胸腺中被MV感染的细胞数量,wtMV(C-)比wtMV少>1000倍。免疫组织化学分析显示,感染wtMV的食蟹猴的脾脏,淋巴结,扁桃体和喉部有强烈的MV抗原表达,但感染wtMV(C-)的食蟹猴的相同组织中表达显著降低。这些数据表明,MV C蛋白对于MV在体外和食蟹猴体内的有效复制都是必需的。

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