A Standardized Plaque Reduction Assay for Determination of Drug Susceptibilities of Cytomegalovirus Clinical Isolates

Landry, Marie L.; Stanat, Sylvia C.; Biron, Karen K.; Brambilla, Donald; Britt, William J.; Jokela, Janet A.; Chou, Sunwen; Drew, W. Lawrence; Erice, Alejo; Gilliam, Bruce L.; Lurain, Nell S.; Manischewitz, Jody; Miner, Richard C.; Nokta, Mostafa; Reichelderfer, Patricia; Spector, Stephen A.; Weinberg, Adriana; Yen‐Lieberman, Belinda; Crumpacker, Clyde S.

doi:10.1128/aac.44.3.688-692.2000

Cited by 132 publications

(97 citation statements)

References 12 publications

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“…The two cases (600del and 597del3) where the current phenotypes are more GCV resistant (Table 1) than previously reported by plaque reduction assays (5, 13) reflect the same technical considerations as those for A591V. There are well-documented difficulties in the standardization of plaque assays across studies because of limited replicates of testing (often no more than three), compounded by variable operator expertise and culture conditions leading to fluctuating baseline and mutant EC 50 values that greatly affect calculated ratios (25). A secondary objective of this study was to compare the assay performance of a cloned retinal epithelial cell line overexpressing platelet-derived growth factor receptor alpha (PDGFR␣).…”

Section: Discussionmentioning

confidence: 67%

Differentiated Levels of Ganciclovir Resistance Conferred by Mutations at Codons 591 to 603 of the Cytomegalovirus UL97 Kinase Gene

2017

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Diagnostic mutations in the cytomegalovirus UL97 kinase gene are used to assess the level of associated ganciclovir resistance and therapeutic options. The best-known mutations at codons 460, 520, or 591 to 607 individually confer 5-to 10-fold-decreased ganciclovir susceptibility, except that a 3-fold decrease occurs in the case of the amino acid substitution C592G. Less common point and in-frame deletion mutations at codons 591 to 603 remain incompletely characterized. The ganciclovir susceptibilities of 17 mutants in this codon range were evaluated by use of the same recombinant phenotyping system and extensive assay replicates in two types of cell cultures. Amino acid substitutions K599E and T601M conferred no ganciclovir resistance, while A591V conferred 3.8-fold-decreased susceptibility. In-frame deletions of three or more codons conferred at least 8-fold-increased ganciclovir resistance, while the level of resistance conferred by one-or two-codon deletions varied from 4-to 10-fold, depending on their location. Measured levels of ganciclovir resistance were closely comparable when assays were performed in either fibroblasts or modified retinal epithelial cells. The significant revision of a few previously published resistance phenotypes and the new data strengthen the interpretation of genotypic testing for cytomegalovirus drug resistance.KEYWORDS cytomegalovirus, drug resistance mechanisms, ganciclovir P rolonged treatment of human cytomegalovirus (CMV) infection with ganciclovir (GCV) or its oral prodrug, valganciclovir, may result in antiviral drug resistance when viral replication is incompletely suppressed. Without the routine availability of susceptibility testing on CMV culture isolates, the laboratory diagnosis of drug resistance is dependent on the direct detection of characteristic viral mutations in clinical specimens (1, 2). GCV resistance mutations usually develop first in the UL97 kinase gene involved in the initial phosphorylation of GCV that is necessary for its antiviral action. One of seven UL97 mutations (M460V/I, H520Q, C592G, A594V, L595S, and C603W) is initially detected in Ͼ80% of cases of GCV resistance in clinical practice, with most of the remainder consisting of less common amino acid substitutions or in-frame deletions at codons 590 to 607 or of mutations in the UL54 DNA polymerase gene (2). The canonical UL97 mutations confer 5-to 10-fold increases in the GCV concentration required for 50% viral growth inhibition (50% effective concentration [EC 50 ]), except that C592G confers a 3-fold increase. Given the limited alternative treatment options, mutations conferring lower-grade resistance may be amenable to GCV dose escalation, according to consensus treatment guidelines (3). Therefore, accurate calibration of the levels of resistance conferred by specific mutations is desirable for treatment planning purposes

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Section: Discussionmentioning

confidence: 67%

Differentiated Levels of Ganciclovir Resistance Conferred by Mutations at Codons 591 to 603 of the Cytomegalovirus UL97 Kinase Gene

2017

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“…12 It is thought that prolonged exposure to ganciclovir, particularly at concentrations that do not fully suppress viral replication, may lead to resistance. 7,11,13,14 Ganciclovir resistance may be assessed by phenotypic analysis by plaque reduction assay 4,15 and by genotypic analysis, which demonstrates characteristic mutations in the UL97 region or the DNA polymerase gene. 4,[16][17][18] In the past, foscarnet has been the main agent utilized for therapy for ganciclovirresistant CMV in transplant recipients, 19 but its usefulness in transplant recipients is often limited by nephrotoxicity and electrolyte disturbances.…”

Section: Discussionmentioning

confidence: 99%

Use of leflunomide in an allogeneic bone marrow transplant recipient with refractory cytomegalovirus infection

Avery

Bolwell

Yen‐Lieberman

et al. 2004

Bone Marrow Transplant

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“…The in vitro assay determines the antiviral's ability to reduce the number of lytic plaques, which quantifies the cytopathic effect induced by the virus. This can be determined as a 50% inhibitory concentration (IC 50 ) (Chou et al, 1999;Landry et al, 2000). This is a difficult method that requires trained personnel and standard antiviral concentrations.…”

Section: Laboratory Methods For the Detection Of Antiviral Drugsmentioning

confidence: 99%

Point Mutations and Antiviral Drug Resistance

Arellano‐Galindo¹,

Barrón²,

Vargas-Infante³

et al. 2012

Point Mutation

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A Standardized Plaque Reduction Assay for Determination of Drug Susceptibilities of Cytomegalovirus Clinical Isolates

Cited by 132 publications

References 12 publications

Differentiated Levels of Ganciclovir Resistance Conferred by Mutations at Codons 591 to 603 of the Cytomegalovirus UL97 Kinase Gene

Differentiated Levels of Ganciclovir Resistance Conferred by Mutations at Codons 591 to 603 of the Cytomegalovirus UL97 Kinase Gene

Use of leflunomide in an allogeneic bone marrow transplant recipient with refractory cytomegalovirus infection

Point Mutations and Antiviral Drug Resistance

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