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通过电子显微镜观察失活流感病毒在道迪细胞中的命运。

Visualization of the fate of inactive influenza viruses in Daudi cells by electron microscopy.

作者信息

Weil-Hillman G, Gamliel H, Friedmann A, Zakay-Rones Z

出版信息

Scan Electron Microsc. 1985(Pt 4):1687-93.

PMID:3912969
Abstract

The replication of active and inactivated influenza viruses in Daudi lymphoma cells was studied by immunofluorescence and electron microscopy. In a previous study, we demonstrated that active and heat-inactivated X47 (H3N2) virus arrested Daudi cell growth by inhibiting cellular DNA synthesis while formalin-treated X47 virus did not. Transmission electron microscopic studies revealed that both the active and the heat-inactivated X47 virus penetrated into the cells. Only the active X47 (XA) virus replicated completely in Daudi cells and produced new viral particles by budding. The formalin-treated X47 virus did not damage or change the cells, and although the viral particles remained adsorbed to the cells, there was little penetration. The heat inactivated X47 virus (which was the most effective, non-virulent, oncolytic agent we studied) was visualized as large aggregates of particles adsorbed to the cell surface by electron microscopy. The cells themselves formed clumps. The viral aggregation and cell clumping likely resulted from the loss of viral neuraminidase activity due to heat treatment. The penetration of heat-inactivated viral particles was massive and involved numerous particles. Production of new viral particles was not demonstrated in this study even though nucleocapsids from the original virus were found in the cytoplasm. Thus, it appears that the massive penetration of the viral particles into cells damages the plasma membrane and may be responsible for the oncolytic potential of the heat-inactivated virus on Daudi cells.

摘要

通过免疫荧光和电子显微镜研究了活性和灭活流感病毒在Daudi淋巴瘤细胞中的复制情况。在先前的一项研究中,我们证明活性和热灭活的X47(H3N2)病毒通过抑制细胞DNA合成来阻止Daudi细胞生长,而经福尔马林处理的X47病毒则不会。透射电子显微镜研究显示,活性和热灭活的X47病毒均能侵入细胞。只有活性X47(XA)病毒能在Daudi细胞中完全复制,并通过出芽产生新的病毒颗粒。经福尔马林处理的X47病毒不会损伤或改变细胞,虽然病毒颗粒仍吸附在细胞上,但几乎没有侵入。热灭活的X47病毒(我们研究的最有效的非毒性溶瘤剂)在电子显微镜下可见为吸附在细胞表面的大量颗粒聚集体。细胞自身形成团块。病毒聚集和细胞团块可能是由于热处理导致病毒神经氨酸酶活性丧失所致。本研究中即使在细胞质中发现了原始病毒的核衣壳,也未证明有新病毒颗粒产生。因此,似乎病毒颗粒大量侵入细胞会损害质膜,这可能是热灭活病毒对Daudi细胞具有溶瘤潜力的原因。

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