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EXTOXNET PIP - METHIDATHION Page 2 o <br /> dizziness,muscle twitching, difficulty breathing, blurred vision, and tightness in the chest [2]. High acute exposui <br /> may cause intense breathing problems, including paralysis of the respiratory muscles. <br /> . Chronic toxicity: Beagle dogs fed small doses of the compound for 2 years experienced no compound related <br /> effects at or below the dose of 0.10 mg/kg/day [2,8]. At doses of 0.4 mg/kg/day and above, the dogs experienced <br /> enzymatic changes and liver alterations. Inhibition of red blood cell cholinesterase, an enzyme, was observed onl) <br /> at the highest dose tested (1.6 mg/kg/day) [2]. Rats also have a low tolerance for the compound. Compound relate <br /> effects were first noted in the rats at doses of 2 mg/kg and above and included cholinesterase inhibition in the bloc <br /> and brain and some nerve related effects. At the highest dose of 5 mg/kg, the rats ate more food but had less body <br /> weight gain. They also developed skin lesions and foam in their lungs [2,8,81]. Rhesus monkeys fed small amoun <br /> of the compound developed changes in blood cholinesterase activity at doses of 1 mg/kg/day and above. Humans <br /> ingesting very small amounts of the compound at doses of 0.11 mg/kg/day for 6 weeks had no noticeable clinical <br /> effects [8]. A study of exposure levels of mixer/loaders of methidathion (Supracide applications) in California <br /> showed that the greatest exposure potential to the compound was through the skin (dermal) [82]. <br /> . Reproductive effects: Moderate amounts of methidathion caused a number of adverse reproductive effects. Whei <br /> male and female rats were fed moderate amounts of methidathion over two successive litters, the parents <br /> experienced tremors, decreased food consumption and decreased ovary weights at 1.25 mg/kg/day[2,8]. The low <br /> dose of 0.25 mg/kg/day disrupted mating behavior and also affected nursing offspring. At 2.5 mg/kg/day(the <br /> highest dose tested), stillbirths and decreased pup survival were observed [2]. Reproductive effects in humans as a <br /> result of methiciathion exposure are unlikely under normal circumstances. <br /> . Teratogenic effects: Small to moderate amounts of methidathion administered to pregnant rats and rabbits <br /> produced no birth defects in the offspring. The pregnant females experienced several compound related effects, <br /> most of which were typical of cholinesterase inhibition [2]. The compound is unlikely to pose a developmental ris <br /> to humans. <br /> . Mutagenic effects: Methidathion did not induce any genetic changes in a number of tests for gene mutation, <br /> chromosomal aberrations, and DNA damage. The various gene mutation studies were conducted on hamster bone <br /> marrow cells, in mammalian cells, and on several species of bacteria [2]. These data indicate that methidathion is <br /> not mutagenic. <br /> . Carcinogenic effects: Methidathion caused malignant and benign liver tumors (adenomas) in male mice fed 2.5 <br /> mg/kg/day for 2 years. Additional tumors (carcinomas)were found in the male mice fed 5 mg/kg/day over the sari <br /> period. This higher feeding level also produced numerous other signs of toxicity [2,8]. Since these results apply to <br /> only one sex in one species, the carcinogenic potential of methidathion is unclear. <br /> . Organ toxicity: Target organs in animal studies include the nervous system, liver, gall bladder, and ovaries. <br /> . Fate in humans and animals: Methidathion is rapidly absorbed, broken down, and eliminated in animals [8]. <br /> Following absorption of the compound, the majority is lost as a breakdown product through the lungs [2,6]. <br /> Between 30 and 50% of the ingested amount is eliminated (as breakdown products) in urine [2,6]. Half of the inti, <br /> amount of the compound is removed from mammals within 6 hours [2,6]. The breakdown products of the parent <br /> compound are not of toxicological concern [8]. Only very small amounts of various metabolic products of <br /> methidathion have been detected in milk from cows [6] and in chicken eggs [2]. <br /> Ecological Effects: <br /> . Effects on birds: Methidathion is highly toxic to birds following acute exposure. The reported oral LD50 values f <br /> the compound are 23 mg/kg to 33 mg/kg in mallards, 8.41 mg/kg in Canadian geese, 33.2 mg/kg in the ring-necke <br /> pheasant, and 225 mg/kg in the chukar partridge [8,6]. <br /> . Effects on aquatic organisms: The compound is very highly acutely toxic to aquatic organisms (both vertebrate <br /> and invertebrate); the reported LC50 values of the compound are 10 to 14 ug/L in rainbow trout and 2 to 9 ug/L in <br /> bluegill sunfish [13,72]. Tests on lobsters indicated that the combination ofinethidathion and another <br /> organophosphate insecticide, phosphamidon, was more toxic than either compound separately or than would be <br /> expected if the toxicities were added together [13]. Studies with bluegill sunfish indicate that there is only a slight <br /> ttp://extoxnet.orst.edu/pips/inethidat.htm 7/2/20( <br />