INFLUENZA VIRUS MULTIPLICATION IN THE CHORIOALLANTOIC MEMBRANE IN VITRO: KINETIC ASPECTS OF INHIBITION BY 5, 6-DICHLORO-1-{beta}-D-RIBOFURANOSYLBENZIMIDAZOLE

doi:10.1084/jem.100.6.541

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The Journal of Experimental Medicine, Vol 100, 541-562, Copyright, 1954, by The Rockefeller Institute for Medical Research New York

ARTICLE

INFLUENZA VIRUS MULTIPLICATION IN THE CHORIOALLANTOIC MEMBRANE IN VITRO: KINETIC ASPECTS OF INHIBITION BY 5, 6-DICHLORO-1-ß-D-RIBOFURANOSYLBENZIMIDAZOLE

Igor Tamm M.D.¹ and David A. J. Tyrrell M.D.¹

¹ From the Hospital of The Rockefeller Institute for Medical Research

A procedure is described for kinetic studies on the multiplicationof Lee virus in the chorioallantoic membrane in vitro employingthe hemagglutination technique for measurement of virus concentration.A linear relationship was found between the logarithm of virusadsorbed and the amount of membrane used. Of the virus adsorbedless than 10 per cent could be recovered from the membrane.Of the recoverable virus 90 per cent was eliminated by specificimmune serum. Lee virus was adsorbed by the allantoic and chorioniclayers of the membrane to a similar degree. Multiplication occurredin both layers and to a similar extent. When 10^7.66 EID₅₀ ofLee virus was inoculated per 2.9 cm.² of chorioallantoic membrane,the ratio of infectivity to hemagglutination titer in the yieldwas low, although the rate of appearance of virus particleswas not diminished despite the large inocula.

Virus producedin membranes was liberated rapidly and continually into themedium. 5,6-Dichloro-1-ß-D-ribofuranosylbenzimidazole (DRB),0.000055 M, prolonged the latent period by more than 100 percent. The rate of increase during the period of rapid rise wassimilar in the presence or absence of DRB, but the yield wasmarkedly reduced at the end of this period in the presence ofDRB. The amount of the virus in the membranes continued to risein the presence of DRB and eventually approached the maximallevels reached much earlier in the controls. Measurement ofthe amount of virus in the media indicated a greater degreeof inhibition than did measurement in the membranes. Comparativestudies with two benzimidazole derivatives on the dependenceof the inhibitory effect on the time of addition of the compoundshowed that processes which could be inhibited by DRB were ofshorter duration than those inhibited by 2,5-dimethylbenzimidazole(MB). With MB the relationship between the time of additionand the inhibitory effect was similar both for virus and forsoluble complement-fixing antigen; with DRB the inhibitableprocesses were of shorter duration for the complement-fixingantigen than for virus particles. DRB was not only 35 timesmore active on a molar basis but also was more selective inits action than MB. DRB interfered with processes which precededthe emergence of either soluble complement-fixing antigen orvirus particles. Some of the implications of these findingsare discussed in relation to the mechanism of inhibition ofinfluenza virus multiplication by benzimidazole derivatives.

Submitted on July 29, 1954

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