The effect of acute maternal toxicity on fetal development in the mouse

Kavlock, Robert J.; Chernoff, Neil; Rogers, Ellen H.

doi:10.1002/tcm.1770050103

Cited by 127 publications

(63 citation statements)

References 10 publications

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“…These data seem to suggest a correlation between the severity of maternal toxicity and the effects on the conceptuses, however a definite relationship cannot be extrapolated because the concurrent role of the test compound in inducing the effects must be taken into account. The role of maternal toxicity in the induction of adverse effects on conceptuses is a very long standing problem that has been faced by a number of researchers (Chahoud et al, 1999;Chernoff et al, 1989;ECETOC, 2004;Kavlock et al, 1985;Khera, 1984Khera, , 1985Paumgartten, 2010;Rogers et al, 2005), apparently without a definite solution. First of all the definition of maternal toxicity is very poor.…”

Section: Introductionmentioning

confidence: 99%

The problem of maternal toxicity in developmental toxicity studies

Giavini

Menegola

2012

Regulatory Toxicology and Pharmacology

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Section: Introductionmentioning

confidence: 99%

The problem of maternal toxicity in developmental toxicity studies

Giavini

Menegola

2012

Regulatory Toxicology and Pharmacology

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“…Kavlock et al (1985) found a similar increase in supernumerary ribs with DMA V treatment in mice after maternal exposure on GD 8, and correlated these to the treatment-related retardation of maternal weight gain. In the rats at the lower DMA V dose levels, there were statistically significant intergroup differences in the incidences of some fetal skeletal variants but, due to lack of dose-relationship, none was considered indicative of a treatment effect.…”

Section: Dma Vmentioning

confidence: 60%

“…The authors found the latter effect to be correlated with the magnitude of the effect on maternal weight gain. The results reported by Kavlock et al (1985) are inappropriate for evaluating the risks of developmental effects in humans because (1) clearly maternally toxic, sometimes lethal doses were used, and (2) the numbers of dosage groups were not sufficient to enable evaluation of the dose-response relationship for DMA V (DeSesso et al, 1998;Jacobson et al, 1999;Holson et al, 2000). In a later study, Chernoff et al (1990) assessed a group of 16 pregnant Sprague-Dawley rats at term after oral administration of 40 mg/kg/day DMA V once daily during organogenesis (GD 6-15).…”

Section: Discussionmentioning

confidence: 90%

“…Hood (1998b) independently confirmed the greater sensitivity of rat embryos. Kavlock et al (1985) tested DMA V as one of a number of chemicals in a study investigating the relationship between maternal and developmental toxicity. These studies were of lesser value for assessing the potential for direct developmental effects of DMA V , because only maternally toxic doses were administered.…”

Section: Discussionmentioning

confidence: 99%

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Monomethylarsonic acid and dimethylarsinic acid: developmental toxicity studies with risk assessment

Irvine¹,

Boyer

DeSesso

2006

Birth Defects Research Pt B

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BACKGROUND:The toxicity of arsenic compounds is highly dependent on the valence and methylation state of the compound. Although there is extensive published literature on the potential developmental toxicity of inorganic arsenic compounds, little exists on organic arsenic compounds and, in particular, studies conducted in accordance with conventional regulatory guidelines appropriate for risk assessment are rare. The organic arsenic compounds, monomethylarsonic acid (MMA V ) and dimethylarsinic acid (DMA V , also called cacodylic acid), are the active ingredients in pesticide products that are used mainly for weed control. MMA V and DMA V are also metabolites of inorganic arsenic formed intracellularly by most living organisms (animals, plants and bacteria). In mammals, this occurs predominantly in liver cells. METHODS: Conventional developmental toxicity studies of orally administered MMA V and DMA V in the Sprague-Dawley rat and New Zealand White rabbit were conducted in commercial contract laboratories in the late 1980s for regulatory compliance. The results of these studies are summarized and presented to broaden the data available in the public domain. RESULTS: In both species, data shows an absence of dose-related effects at organic arsenic exposures that were not maternally toxic. MMA V doses of 0, 10, 100, and 500 mg/kg/day (rat) and 0, 1, 3, 7, and 12 mg/kg/day (rabbit) and DMA V doses of 0, 4, 12, and 36 mg/kg/day (rat) and 0, 3, 12, and 48 mg/kg/day (rabbit) were administered by oral gavage daily during organogenesis (Gestation Day [GD] 6-15, rat; GD 7-19, rabbit) and the litters examined at maternal sacrifice (GD 20, rat; GD 29, rabbit). After treatment with MMA V , maternal and fetal toxicity were observed at the highest doses of 500 mg/kg/day (rat) and 12 mg/kg/day (rabbit), but no treatment-related developmental toxicity at the lower doses, even in the presence of minimal maternal toxicity in the rat at 100 mg/kg/d. There was no evidence of teratogenicity associated with MMA V treatment. With DMA V , maternal and developmental toxicity were observed in the rat at 36 mg/kg/day, with a higher than spontaneous incidence of fetuses with diaphragmatic hernia. In the rabbit at 48 mg/kg/day, there was marked maternal toxicity, culminating for most females in abortion and with no surviving fetuses for evaluation. There was no treatment-related maternal or developmental toxicity in the rat or rabbit at 12 mg/kg/day. Based on pregnancy outcome, the developmental toxicity no observed adverse effect level (NOAEL) for orally administered MMA V were 100 and 7 mg/kg/day in the rat and rabbit, respectively, and for DMA V were 12 mg/kg/day in both species. CONCLUSIONS: Margins of exposure estimated based on conservative estimates of daily intakes of arsenic in all of its forms indicate that exposure to MMA V or DMA V at environmentally relevant exposure levels, by the oral route (the environmentally relevant route of exposure) is unlikely to pose a risk to pregnant women and their offspring. Birth Defects Res (Par...

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“…An increased incidence of supernumerary ribs was observed in both dinoseb-treated groups. The authors noted that increased incidence of supernumerary ribs may be a response to a non-specific disruption in maternal status (Kavlock et al, 1985). Administration of dinoseb to pregnant CD-1 mice by gavage on GDs 7-8 at 50 mg/kg bw/day in NaOH produced reduced fetal weight and increased incidence of fetuses with supernumerary ribs (71% in litters) without maternal death.…”

Section: Gavage Studies In Micementioning

confidence: 99%