Aspects of Thymidine Metabolism and Function in Cultured Mammalian Cells Infected with Herpes Simplex Virus Type 1

Baybutt, Herbert; Murray, B. G.; Pearson, Colin K.

doi:10.1099/0022-1317-59-2-223

Cited by 8 publications

(1 citation statement)

References 27 publications

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“…Lending support to this hypothesis is the fact that HSV has a ribonucleotide reductase (8,25) and a thymidine kinase (48) (8,19). The expression of these enzymes has been implicated in the generation of nucleotide pool imbalances (1,18,40), and it is known that deregulation of intracellular levels of dNTPs can be mutagenic (24,33,58). In addition, the viral DNA polymerase (7) is known to be error prone during the replication of its own DNA (15 6,1986 on May 10, 2018 by guest http://mcb.asm.org/ Downloaded from mutations by increasing nucleotide misincorporation during cellular DNA replication.…”

Section: Resultsmentioning

confidence: 99%

Herpes simplex virus type 2 mutagenesis: characterization of mutants induced at the hprt locus of nonpermissive XC cells.

Pilon¹,

Langelier²,

Royal³

1986

Mol. Cell. Biol.

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. 66:259-265, 1985). A series of 17 independent mutants were isolated after viral infection together with 12 spontaneous noninfected mutants to characterize the nature of the mutations induced by the virus at the molecular level. The DNA of the mutants isolated after viral infection was probed with cloned HSV-2 fragments representing the entire genome. In these mutants, no authentic HSV-2 hybridization could be detected. This was indicative of a mechanism of mutagenesis which did not require the permanent integration of viral sequences in the host genome. The structure of the hprt gene was determined by the method of Southern (J. Mol. Biol. 98:503-517, 1975), and the level of hprt mRNA was analyzed by Northern blots. Except for the identification of one deletion mutant in each of the two groups, the HPRT-clones showed no evidence of alteration in their hprt gene. A total of 7 of 12 spontaneous mutants and 11 of 15 mutants isolated from the infected population transcribed an hprt mRNA of the same size and abundance as did the wild-type cells. Thus, the majority of the mutants seemed to have a point mutation in their hprt structural gene.Interestingly, the proportion of the different types of mutations was similar in the two groups of mutants. This analysis revealed that HSV-2 infection did not increase the frequency of rearrangements but rather that it probably induced a general increase of the level of mutations in the cells. This type of response is thought to be compatible with the biology of the virus, and the possible mechanisms by which HSV-2 induces somatic mutations in mammalian cells are discussed.Defined regions of the herpes simplex virus type 2 (HSV-2) genome can transform rodent cells in vitro (12,20), but the existence of a viral oncogene responsible for the maintenance of the transformed state has been questioned because of the lack of evidence that a specific viral sequence was retained in these cells (13). In addition, transformation by HSV is less efficient (13,20,21) than what is generally observed with viral oncogenes (3, 29). These considerations suggested that the role of the virus was transient and led to the hypothesis that HSV acts as a mutagen (13,17,42,61). The first evidence that HSV could cause mutations came from observations that infection often results in fragmentation and pulverization of cellular chromosomes (4,16,45,57). It was subsequently shown by Schlehofer and zur Hausen (41) that infection of human permissive rhabdomyosarcoma cells by inactivated HSV-1 could result in an increased mutation frequency at the hypoxanthine phosphoribosyltransferase (hprt) locus. In a previous report, we made use of the XC cell line, which is not permissive for HSV-2, to demonstrate that intact viral particles could increase the frequency of HPRT-mutants by factors ranging from 2.4 to 10.3 (38). Other DNA viruses such as simian virus 40 and adenovirus type 2 can cause mutations at several loci in nonpermissive infections (14,27,28,50,52,60). However, the nature of the virally induced mutations h...

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Section: Resultsmentioning

confidence: 99%

Herpes simplex virus type 2 mutagenesis: characterization of mutants induced at the hprt locus of nonpermissive XC cells.

Pilon¹,

Langelier²,

Royal³

1986

Mol. Cell. Biol.

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Search for multienzyme complexes of DNA precursor pathways in uninfected mammalian cells and in cells infected with herpes simplex virus type I

Harvey

Pearson

1988

Journal Cellular Physiology

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Confirmatory evidence for the existence of a multienzyme complex of DNA precursor pathways in mammalian cells was obtained. Using neutral sucrose gradient centrifugation of cell lysates we found that at least five enzymes involved in DNA precursor metabolism in uninfected. S-phase BHK-cell fibroblasts cosediment at a common rate, indicative of a multienzyme complex. The enzymes include DNA polymerase thymidine kinase, ribonucleotide reductase, dihydrofolate reductase, and NDP-kinase. This complex was partially, but not completely, disrupted when lysates from GO-phase cells were centrifuged. Using lysates from cells infected with herpes simplex virus (HSV) type I some of the virus-induced ribonucleotide reductase and a minor proportion of the HSV-thymidine kinase cosedimented rapidly. The virus-induced DNA polymerase sedimented independently near the middle of the gradient, in contrast to the behaviour of the host polymerase. The enzyme associations observed were disrupted by NaCl or by inclusion of ethylenediamine tetraacetic acid during the cell lysis procedure, instead of the usual EGTA. These results indicate the importance of ionic forces in maintaining the enzyme complexes. The bulk of the DNA and the RNA present in the lysates did not sediment at the same rate as the complexes, showing that the enzymes were not simply adhering nonspecifically to these polyanions. Newly synthesised radiolabeled DNA (15 min pulse with [3H]thymidine) was not preferentially associated with the enzymes, but some functional DNA was evident in the enzyme complex fraction from the uninfected S-phase cells. DNA polymerase activity in this fraction did not require, nor was it stimulated by, exogenous "activated" DNA. Added DNA primer-template was required, however, for maximal activity of the polymerase in gradient fractions derived from GO-phase cells and from HSV-infected cells. No evidence for channeling of ribonucleotide precursors into DNA of permeabilized cells (uninfected or HSV-infected) was detected. Most rCDP was incorporated into RNA. In the uninfected, S-phase cells about 10 pmol/10(6) cells/90 min of rCDP residues was incorporated into DNA compared with 120 pmol/10(6) cells/90 min when radiolabeled dCTP was used. Nonradioactive dCTP present in equimolar concentration in the incubation with labeled rCDP did not, however, diminish the incorporation of label from the ribonucleotide. In permeabilized HSV-infected cells incorporation of radiolabel from rCDP into DNA was barely detectable.

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Replication of thymidine kinase deficient herpes simplex virus type 1 in neuronal cell culture: Infection of the PC 12 cell

Rubenstein

Price

1983

Archives of Virology

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Replication of a thymidine kinase deficient (TK-) mutant of herpes simplex virus type 1 (HSV-1) was compared to replication of its parental TK+ strain in the PC 12 cell. This is a cell which ceases cell division and undergoes neuron-like morphological and physiological differentiation in the presence of nerve growth factor (NGF). No difference between mutant and parental strain replication was detected either when these cells were infected in the proliferative state or while maintained under the influence of NGF. Neither viral TK nor enhanced cellular TK activity was detected during TK- HSV-1 replication, which proceeded in the presence of selective antiviral drugs that inhibited TK+ HSV-1 viral replication. Moreover, thymidylate synthetase was inhibited early in TK- infection, and reutilization of thymine nucleotides derived from degraded cellular DNA was not detected. Under the conditions of these in vitro studies, increased production of dTTP as a result of enhanced TK activity did not appear to be rate-limiting, despite the non-dividing "differentiated" state of the PC 12 cell.

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Aspects of Thymidine Metabolism and Function in Cultured Mammalian Cells Infected with Herpes Simplex Virus Type 1

Cited by 8 publications

References 27 publications

Herpes simplex virus type 2 mutagenesis: characterization of mutants induced at the hprt locus of nonpermissive XC cells.

Herpes simplex virus type 2 mutagenesis: characterization of mutants induced at the hprt locus of nonpermissive XC cells.

Search for multienzyme complexes of DNA precursor pathways in uninfected mammalian cells and in cells infected with herpes simplex virus type I

Replication of thymidine kinase deficient herpes simplex virus type 1 in neuronal cell culture: Infection of the PC 12 cell

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