2001
DOI: 10.1002/jat.762
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Lack of adverse effects on fertility of female cd‐1 mice exposed to repetitive intravaginal gel–microemulsion formulation of a dual‐function anti‐HIV agent: aryl phosphate derivative of bromo‐methoxy‐zidovudine (compound WHI‐07)

Abstract: 5-bromo-6-methoxy-5,6-dihydro-3(')-azidothymidine-5(')-(p-bromophenyl) methoxyalaninyl phosphate (WHI-07), a novel bromo-methoxy-substituted aryl phosphate derivative of zidovudine (ZDV), is a potent dual-function contraceptive agent with anti-HIV activity. Its potential for reproductive toxicity was assessed in a series of experiments using CD-1 mice under the conditions of its intended use as an intravaginal microbicide. Female CD-1 mice were exposed intravaginally to a gel-microemulsion formulation containi… Show more

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Cited by 17 publications
(13 citation statements)
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“…Repeated intravaginal application of WHI-07 for up to 13 weeks did not cause local, systemic, or reproductive toxicity in mice (8,19). WHI-07 did not exhibit mucosal toxicity, maternal toxicity, fetotoxicity, embryotoxicity, or teratogenicity in mice or rabbits (7,9,18). Histological evaluation of rabbit vaginal tissues immediately after daily intravaginal application of 2% WHI-07 in gel-microemulsion for 10 consecutive days revealed lack of epithelial cell disruption, leukocyte influx, vaginal erythema, or submucosal edema (mean individual scores 0-2 out of 4; total scores 2-5 out of 16) (7).…”
Section: Discussionmentioning
confidence: 99%
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“…Repeated intravaginal application of WHI-07 for up to 13 weeks did not cause local, systemic, or reproductive toxicity in mice (8,19). WHI-07 did not exhibit mucosal toxicity, maternal toxicity, fetotoxicity, embryotoxicity, or teratogenicity in mice or rabbits (7,9,18). Histological evaluation of rabbit vaginal tissues immediately after daily intravaginal application of 2% WHI-07 in gel-microemulsion for 10 consecutive days revealed lack of epithelial cell disruption, leukocyte influx, vaginal erythema, or submucosal edema (mean individual scores 0-2 out of 4; total scores 2-5 out of 16) (7).…”
Section: Discussionmentioning
confidence: 99%
“…Furthermore, repeated intravaginal exposure of CD-1 mice to WHI-07 for up to 13 weeks had no adverse effects on ovulation response, mean number of eggs recovered, the percent of eggs fertilized and cleaved or their subsequent reproductive capability (8,9,19). In molecular genotoxicity studies, WHI-07 did not increase DEL recombination frequency in yeast and did not activate any of the DNA damage-associated promoters in human HepG2 cells using the CAT-Tox(L) assay.…”
Section: Introductionmentioning
confidence: 97%
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“…In animal toxicity studies performed in mice, rabbits, cats, and/or pigs, intravaginal administration of gelmicroemulsion with or without 2.0% WHI-07 was not associated with any mucosal, systemic, developmental, and/ or reproductive toxicity. [22][23][24][25][26][27][28] Consequently, the shelf-life/ stability of WHI-07-loaded gel-microemulsion at 3 controlled temperatures (4ºC, 25ºC, and 40-C) was determined using a validated high-performance liquid chromatography (HPLC) method for up to 24 weeks (6 months). soya lecithin) was from American Lecithin Co (Danbury, CT); and propylene glycol was obtained from Spectrum Quality Products Inc (New Brunswick, NJ).…”
Section: Introductionmentioning
confidence: 99%
“…WHI-07-containing gel microemulsion is a potent vaginal contraceptive in the rabbit model (12). In preclinical studies, repetitive intravaginal administration of 2% WHI-07 via a gel microemulsion corresponding to 5.7 ϫ 10 6 times its in vitro anti-HIV IC 50 and 5,700 times its spermicidal 50% effective concentration for up to 13 weeks was not associated with mucosal, systemic, or reproductive toxicity in test animal species (13)(14)(15)(16). Repeated intravaginal administration of WHI-07 during the period of major organogenesis at concentrations as high as 2% did not produce teratogenicity or other developmental toxicity in rodent and nonrodent species tested (16).…”
mentioning
confidence: 99%