Inhibition of Ganciclovir-Susceptible and -Resistant Human Cytomegalovirus Clinical Isolates by the Benzimidazole
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            -Riboside 1263W94

McSharry, James J.; McDonough, Ann; Olson, Betty; Talarico, Christine L.; Davis, M. R.; Biron, Karen K.

doi:10.1128/cdli.8.6.1279-1281.2001

Cited by 53 publications

(29 citation statements)

References 24 publications

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“…After application of GCV liposomes, the highest concentrations of GCV were found in the sclera and the cornea (1000-1500 ng/g), both of which are higher than the half maximal inhibitory concentration (IC 50 ) of GCV against CMV (900 ng/g). 16 The concentration s of GCV in the aqueous humor, lens, and vitreous humors in the liposome-treated group were found to be within the range of 100 to 500 ng/g, which were several times higher than those of the solution-treated group (30-300 ng/g). Because over 70% of À uid in vitreous humor moves toward the retina and exits the vitreous cavity through the retina, GCV concentration in vitreous humor could be used to evaluate the possible effectiveness of GCV against CMV retinitis.…”

Section: In Vivo Ocular Pharmacokinetics Studymentioning

confidence: 83%

Preparation and ocular pharmacokinetics of ganciclovir liposomes

Shen

2007

AAPS J

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Ophthalmic liposomes of ganciclovir (GCV) were prepared by the reverse phase evaporation method, and their ocular pharmacokinetics in albino rabbits were compared with those obtained after dosing with GCV solution. The in vitro transcorneal permeability of GCV liposomes was found to be 3.9-fold higher than that of the solution. After in vivo instillation in albino rabbits, no difference was found in the precorneal elimination rate of GCV from liposome vs solution dosing. The aqueous humor concentration-time pro¿ les of both liposomes and solution were well described by 2-compartmental pharmacokinetics with ¿ rst-order absorption. The area under the curve of the aqueous humor concentration-time pro¿ les of GCV liposomes was found to be 1.7-fold higher than that of GCV solution. Ocular tissue distribution of GCV from liposomes was 2 to 10 times higher in the sclera, cornea, iris, lens, and vitreous humor when compared with those observed after solution dosing. These results suggested that liposomes may hold some promise in ocular GCV delivery.

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Section: In Vivo Ocular Pharmacokinetics Studymentioning

confidence: 83%

Preparation and ocular pharmacokinetics of ganciclovir liposomes

Shen

2007

AAPS J

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“…Although we are unaware of previous studies of UL97 mutants in HCMV strains that encode full-length ULb=s, at least two reports have examined the effects of MBV on clinical isolates (5,69). The use of infected cells as inocula may explain why the authors did not find an increased requirement for UL97 in their assays with clinical isolates.…”

Section: Discussionmentioning

confidence: 99%

The ULb′ Region of the Human Cytomegalovirus Genome Confers an Increased Requirement for the Viral Protein Kinase UL97

Wang

Schauflinger³

et al. 2013

J Virol

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bWe report a requirement for the viral protein kinase UL97 in human cytomegalovirus (HCMV) replication that maps to the ULb= region of the viral genome. A UL97-null (⌬97) mutant of strain TB40/E, which encodes a full-length ULb= region, exhibited replication defects, particularly in production of cell-free virus, that were more severe than those seen with a ⌬97 mutant of laboratory strain AD169, which harbors extensive deletions in its ULb= region. These differences were recapitulated with additional HCMV strains by treatment with a UL97 kinase inhibitor, 1-(␤-L-ribofuranosyl)-2-isopropylamino-5,6-dichlorobenzimidazole (maribavir). We observed lower levels of viral DNA synthesis and an increased requirement for UL97 in viral late gene expression in strains with full-length ULb= regions. Analysis of UL97-deficient TB40/E infections by electron microscopy revealed fewer C-capsids in nuclei, unusual viral particles in the cytoplasmic assembly compartment, and defective viral nuclear egress. Partial inhibition of viral DNA synthesis caused defects in production of cell-free virus that were up to ϳ100-fold greater than those seen with cell-associated virus in strains TB40/E and TR, suggesting that UL97-dependent defects in cell-free virus production in strains with full-length ULb= regions were secondary to DNA synthesis defects. Accordingly, a chimeric virus in which the ULb= region of TB40/E was replaced with that of AD169 showed reduced effects of UL97 inhibition on viral DNA synthesis, late gene expression, and production of cell-free virus compared to parental TB40/E. Together, these results argue that the ULb= region encodes a factor(s) which invokes an increased requirement for UL97 during viral DNA synthesis.

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“…It is much more potent than ACV, and more importantly, it is very active against HCMV strains that are resistant to either of these drugs (42,64). Therefore, MBV is an excellent candidate to prevent and treat HCMV diseases in high-risk patients based on its efficacy and safety profile in phase 1 clinical trials (32,63).…”

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confidence: 99%