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细胞外被膜病毒在痘苗病毒体外和体内传播中的意义。

Significance of extracellular enveloped virus in the in vitro and in vivo dissemination of vaccinia.

作者信息

Payne L G

出版信息

J Gen Virol. 1980 Sep;50(1):89-100. doi: 10.1099/0022-1317-50-1-89.

Abstract

The significance of extracellular enveloped vaccinia (EEV) for the in vitro and in vivo dissemination of vaccinia virus was investigated. The quantity of in vitro released extracellular virus correlated very closely with the ability of 13 vaccinia strains to cause long-range spread of infection (comet formation) in cell cultures infected at low m.o.i. but was not correlated with plaque size. The kinetics of virus spread after low m.o.i. was related to the amount of virus released from primary infected cells but not to their content of intracellular naked vaccinia (INV). Most extracellular vaccinia virus from IHD-J-infected RK-13 cells banded in CsCl density gradients as EEV (88%) while very little banded as INV (2%). Antisera to the enveloped prevented comet formation while antisera to INV did not. CsCl centrifugation of blood-borne extracellular virus from rabbits infected intravenously with vaccinia virus after cyclophosphamide treatment revealed that 64% of the virus banded as EEV but only 11% as INV. High in vitro EEV-yielding vaccinia strains were able to spread from the respiratory tract to the brains of mice and cause death. Low in vitro EEV-yielding vaccinia strains were generally not able to disseminate in vivo or cause mouse mortality. The notable exception to this trend was strain WR, which, although releasing small amounts of virus in vitro, could nevertheless very effectively disseminate in vivo, causing a high rate of mouse mortality. Treatment with anti-envelope serum protected mice from a lethal vaccinia infection whereas antiserum to inactivated INV did not. These results indicate that the in vitro dissemination of vaccinia infection is mediated by EEV and implicate EEV as having a role in the in vivo dissemination.

摘要

研究了细胞外被膜痘苗病毒(EEV)在痘苗病毒体外和体内传播中的意义。体外释放的细胞外病毒量与13株痘苗病毒在低感染复数(m.o.i.)感染的细胞培养物中引起感染远距离传播(彗星形成)的能力密切相关,但与蚀斑大小无关。低m.o.i.后病毒传播的动力学与原代感染细胞释放的病毒量有关,而与细胞内裸露痘苗病毒(INV)的含量无关。来自IHD-J感染的RK-13细胞的大多数细胞外痘苗病毒在CsCl密度梯度中以EEV形式出现(88%),而以INV形式出现的很少(2%)。针对被膜的抗血清可阻止彗星形成,而针对INV的抗血清则不能。对环磷酰胺处理后静脉感染痘苗病毒的兔子血液中细胞外病毒进行CsCl离心,结果显示64%的病毒以EEV形式出现,但只有11%以INV形式出现。体外EEV产量高的痘苗病毒株能够从呼吸道传播到小鼠大脑并导致死亡。体外EEV产量低的痘苗病毒株通常不能在体内传播或导致小鼠死亡。这一趋势的显著例外是WR株,尽管它在体外释放少量病毒,但仍能在体内非常有效地传播,导致高小鼠死亡率。用抗被膜血清治疗可保护小鼠免受致命的痘苗感染,而针对灭活INV的抗血清则不能。这些结果表明,痘苗感染在体外的传播是由EEV介导的,并暗示EEV在体内传播中起作用。

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