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Persistent Herpes Simplex Virus Infection In Vitro with Cycles of Cell Destruction and Regrowth

Overview
Journal J Bacteriol
Publisher American Society for Microbiology
Specialty Microbiology
Date 1965 Jul 1
PMID 16562018
Citations 19
Authors
B Hampar
M L Copeland
Affiliations
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Abstract

Hampar, Berge (National Institute of Dental Research, Bethesda, Md.), and Mary Lou Copeland. Persistent herpes simplex virus infection in vitro with cycles of cell destruction and regrowth. J. Bacteriol. 90:205-212. 1965.-The susceptibility of two Chinese hamster cell lines to herpes simplex virus (HSV) was studied from the time of their initiation through successive subcultures. The cells' susceptibility to the cytocidal effects of HSV decreased as the number of cell passages increased. During the early cell passages, the decrease in cell susceptibility to HSV was characterized by an increased time after infection for complete cell destruction to occur, with a concomitant increase in the period when virus could be recovered from supernatant fluids. This was followed by a number of cell passages during which persistent HSV infections were established. The persistent infections were characterized by (i) cycles of virus synthesis and cell destruction followed by regrowth of the cells, (ii) initiation and maintenance under conditions optimal for cell growth in the absence of antibody, (iii) the cells' ability to be passaged while still maintaining their cycling patterns, (iv) a relationship between virus synthesis and cell proliferation, and (v) inability of long-term treatment with antibody to "cure" the persistent infections. The unique characteristics of this HSV infection were compared with other persistent in vitro viral infections.

Citing Articles

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Involvement of an early human cytomegalovirus function in reactivation of quiescent herpes simplex virus type 2.

Colberg-Poley A, Isom H, Rapp F J Virol. 1981; 37(3):1051-9.

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Analysis and characterization of herpes simplex virus after its persistence in a lymphoblastoid cell line for 15 months.

Roumillat L, Feorino P, Caplan D, Lukert P Infect Immun. 1980; 29(2):671-7.

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Persistence of herpes simplex virus genes in cells of neuronal origin.

Levine M, Goldin A, Glorioso J J Virol. 1980; 35(1):203-10.

PMID: 6251268 PMC: 288796. DOI: 10.1128/JVI.35.1.203-210.1980.

Herpes simplex virus persistence in mouse neuroblastoma (C 1300) cell cultures: role of interferon.

Dawson G, Mowshowitz S, Cohen R, Elizan T J Neural Transm. 1984; 59(4):309-17.

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