Developmental toxicity of orally administered technical dimethoate in rats

## Abstract **BACKGROUND:** Artesunate has been reported to cause embryolethality and malformations when administered orally to rats during organogenesis. The purpose of this study was to determine the most sensitive period(s) for the induction of these effects in order to provide clues about possi

Pregnant CD ® rats were dosed cutaneously (530, 1600 or 4270 mg kg ؊1 day ؊1 ) or fed diets containing octoxynol-9 (70 or 340 mg kg ؊1 day ؊1 ) during the major period of organogenesis. Monitors for maternal toxicity included clinical observations, body weight, organ weight and food consumption. Fet

Pregnant rats were treated with a single intravenous or oral administration of indium chloride (InCl 3 ) on day 9 of pregnancy and their fetuses were examined for growth and malformation on day 20 of pregnancy. By intravenous administration, fetal weight was significantly decreased and the incidence

Developmental toxicity of indium was examined using rat embryo culture with reference to toxicokinetics. Rat embryos at day 9.5 of pregnancy were cultured for 48 h under various exposure conditions to indium trichloride. Indium was embryotoxic to cultured rat embryos at concentrations ranging from 2

This study was performed to evaluate the effects of prenatal development of rats exposed to Polnoks R, an antioxidant in elastomer processing. Pregnant female rats were exposed to Polnoks R by gavage every day on days 6-15 of gestation at doses of 170, 340, and 670 mgfkg body weight (b.w.) (6%, 13%,