Pathogenicity for Suckling Mice of Coxsackie Viruses Adapted to Human Amnion Cells

Overview

Journal J Exp Med

Specialties Allergy & Immunology
General Medicine

Date 1961 May 1

PMID 13760473

Citations 4

Authors

F Lehmann-Grube

J T SYVERTON

Affiliations

Soon will be listed here.

Abstract

Continuous passages in primary human amnion cell cultures of Coxsackie prototype viruses A-9, A-10, A-11, A-13, A-14, A-15, A-18, B-1, B-2, B-4, and B-5 increased the titers, hastened and enhanced cytopathic effect, and in varying degrees caused loss of virulence for newborn mice. Only B-3 behaved differently in that neither adaptation to cells in vitro nor attenuation with respect to the original animal host could be observed. Types A-15, B-1, B-2, and B-5 slowly regained virulence when passed in mice after high concentration passages in amnion cells whereas all other viruses reverted to their original virulence after only 1 or 2 passages in the animal host. When these strains, however, were purified by cloning procedures, they too showed markedly increased stability. In all stages of attenuation, viruses multiplied extensively in vivo as could be shown by titration in amnion cell cultures. It is suggested that a genetic mechanism is operative leading to virus populations in which the majority of the particles is qualitatively changed.

Citing Articles

Virological aspects of Coxsackie virus infections.

DOMOK I Arch Gesamte Virusforsch. 1963; 13:128-42.

PMID: 14028548

Propagation of group A Coxsackie viruses in tissue cultures. II. Some interactions between virus and mammalian cells.

Wenner H, LENAHAN M Yale J Biol Med. 1961; 34:421-38.

PMID: 14006144 PMC: 2605061.

Comparative susceptibility of mammalian cells in culture to prototype enteroviruses.

Lehmann-Grube F Arch Gesamte Virusforsch. 1961; 11:276-83.

PMID: 13760474 DOI: 10.1007/BF01241691.

Immunofluorescence studies on Coxsackie group A. I. Localization of viral antigen in infected primary human amnion cells.

ZALAN E, Kelen A, LABZOFFSKY N Arch Gesamte Virusforsch. 1965; 15(5):668-80.

PMID: 5323528

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