Abstract

Insecticides, fungicides, dinitrobenzenes, resorcinols, phenols and anilines are widely used in agricultural and industrial productions. However, their modes of toxic action are unclear in some nontarget organisms, such as worms and tadpoles. In this study, acute toxicity data was experimentally collected for Limnodrilus hoffmeisteri worms and Rana chensinensis tadpoles, respectively. Interspecies correlation and excess toxicity were calculated to determine modes of action (MOAs) between the two species for class-based compounds. The result showed that, although the interspecies correlation of toxicity between the tadpoles and worms is significant with a coefficient of determination (R2) of 0.83, tadpoles are more sensitive than the worms and toxicity values between these two species are not identical with an overall 0.43 log unit difference. Regression analysis revealed that the toxicity of nonpolar narcotics or baseline compounds is linearly related to hydrophobicity for both the tadpoles and worms and the two baseline models are parallel, suggesting that these nonpolar narcotics share the same MOA between the two species. The difference of baseline toxicities between the two species is attributed to differences in bioconcentration factors. Analysis of the excess toxicity calculated from the toxicity ratio (TR) suggested that phenols and anilines can be classified as polar narcotics, not only to fish, but also to the tadpoles and worms. These compounds are more toxic than the baseline compounds and quantitative structure-activity relationship (QSAR) models show that their toxicity is linearly related to chemical hydrophobicity and polarity. Analysis of the excess toxicity reveals that aminophenols and resorcinols can be classified as reactive compounds, and insecticides and fungicides can be classified as specifically-acting compounds for both species. These compounds exhibited significantly greater toxic effect to both the tadpoles and worms. QSAR models have been developed to describe the toxic mechanisms for nonpolar narcotics, polar narcotics, reactive chemicals and specifically-acting compounds, and a theoretical equation has been derived to explain the effect of bio-uptake and interaction of the chemical with target receptors for both tadpole and worm toxicity. Our study reveals that tadpole toxicity can be estimated from worm toxicity data and the two species can serve as surrogates for each other in the safety evaluation of organic pollutants.

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