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一种蜱传兰加特病毒突变体,其对温度敏感,在神经母细胞瘤细胞中宿主范围受限,且对免疫缺陷小鼠无神经侵袭性。

A tick-borne Langat virus mutant that is temperature sensitive and host range restricted in neuroblastoma cells and lacks neuroinvasiveness for immunodeficient mice.

作者信息

Rumyantsev Alexander A, Murphy Brian R, Pletnev Alexander G

机构信息

Laboratory of Infectious Diseases, National Institute of Allergy and Infectious Diseases/NIH, 12735 Twinbrook Parkway, Twinbrook 3, Room 3W13, MSC 8133, Bethesda, MD 20892-8133, USA.

出版信息

J Virol. 2006 Feb;80(3):1427-39. doi: 10.1128/JVI.80.3.1427-1439.2006.

Abstract

Langat virus (LGT), the naturally attenuated member of the tick-borne encephalitis virus (TBEV) complex, was tested extensively in clinical trials as a live TBEV vaccine and was found to induce a protective, durable immune response; however, it retained a low residual neuroinvasiveness in mice and humans. In order to ablate or reduce this property, LGT mutants that produced a small plaque size or temperature-sensitive (ts) phenotype in Vero cells were generated using 5-fluorouracil. One of these ts mutants, clone E5-104, exhibited a more than 10(3)-fold reduction in replication at the permissive temperature in both mouse and human neuroblastoma cells and lacked detectable neuroinvasiveness for highly sensitive immunodeficient mice. The E5-104 mutant possessed five amino acid substitutions in the structural protein E and one change in each of the nonstructural proteins NS3 and NS5. Using reverse genetics, we demonstrated that a Lys(46)-->Glu substitution in NS3 as well as a single Lys(315)-->Glu change in E significantly impaired the growth of LGT in neuroblastoma cells and reduced its peripheral neurovirulence for SCID mice. This study and our previous experience with chimeric flaviviruses indicated that a decrease in viral replication in neuroblastoma cells might serve as a predictor of in vivo attenuation of the neurotropic flaviviruses. The combination of seven mutations identified in the nonneuroinvasive E5-104 mutant provided a useful foundation for further development of a live attenuated TBEV vaccine. An evaluation of the complete sequence of virus recovered from brain of SCID mice inoculated with LGT mutants identified sites in the LGT genome that promoted neurovirulence/neuroinvasiveness.

摘要

兰加特病毒(LGT)是蜱传脑炎病毒(TBEV)复合体的自然减毒株,作为一种活TBEV疫苗在临床试验中进行了广泛测试,结果发现它能诱导产生保护性的、持久的免疫反应;然而,它在小鼠和人类中仍保留了低残留神经侵袭性。为了消除或降低这种特性,使用5-氟尿嘧啶产生了在Vero细胞中产生小噬斑大小或温度敏感(ts)表型的LGT突变体。其中一个ts突变体克隆E5-104在小鼠和人类神经母细胞瘤细胞的允许温度下复制减少了1000倍以上,并且对高度敏感的免疫缺陷小鼠缺乏可检测到的神经侵袭性。E5-104突变体在结构蛋白E中有五个氨基酸取代,在非结构蛋白NS3和NS5中各有一个变化。利用反向遗传学,我们证明NS3中的赖氨酸(46)→谷氨酸取代以及E中的单个赖氨酸(315)→谷氨酸变化显著损害了LGT在神经母细胞瘤细胞中的生长,并降低了其对SCID小鼠的外周神经毒力。这项研究以及我们之前对嵌合黄病毒的经验表明神经母细胞瘤细胞中病毒复制的减少可能作为嗜神经性黄病毒体内减毒的预测指标。在非神经侵袭性E5-104突变体中鉴定出的七个突变的组合为减毒活TBEV疫苗的进一步开发提供了有用的基础。对接种LGT突变体的SCID小鼠脑内回收病毒的完整序列进行评估,确定了LGT基因组中促进神经毒力/神经侵袭性的位点。

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