2017
Toxicity of clomazone and its formulations to zebrafish embryos (Danio rerio)
STEVANOVIC, Marija, Slavica GASIC, Marek PÍPAL, Lucie BLÁHOVÁ, Dragica BRKIC et. al.Základní údaje
Originální název
Toxicity of clomazone and its formulations to zebrafish embryos (Danio rerio)
Autoři
STEVANOVIC, Marija (688 Srbsko), Slavica GASIC (688 Srbsko), Marek PÍPAL (203 Česká republika, domácí), Lucie BLÁHOVÁ (203 Česká republika, domácí), Dragica BRKIC (688 Srbsko), Nesko NESKOVIC (688 Srbsko) a Klára HILSCHEROVÁ (203 Česká republika, garant, domácí)
Vydání
Aquatic toxicology, AMSTERDAM, ELSEVIER SCIENCE BV, 2017, 0166-445X
Další údaje
Jazyk
angličtina
Typ výsledku
Článek v odborném periodiku
Obor
10617 Marine biology, freshwater biology, limnology
Stát vydavatele
Nizozemské království
Utajení
není předmětem státního či obchodního tajemství
Odkazy
Impakt faktor
Impact factor: 3.884
Kód RIV
RIV/00216224:14310/17:00100297
Organizační jednotka
Přírodovědecká fakulta
UT WoS
000403624000007
Klíčová slova anglicky
Clomazone; Formulations; Embryotoxicity; Embryo; Zebrafish
Příznaky
Mezinárodní význam, Recenzováno
Změněno: 9. 3. 2018 21:16, Mgr. Michaela Hylsová, Ph.D.
Anotace
V originále
Herbicides are the most widely used group of pesticides but after reaching water bodies they are able to cause adverse effects on non-target organisms. Different formulations using the same active ingredient are frequently available, which raises the issue of potential influence of different formulation types on herbicide toxicity. The present study evaluated the toxicity and teratogenic effects of the active ingredient clomazone and its two formulations (Rampe (R) EC and GAT Cenit 36 CS, both containing 360 g a.i./l of clomazone) on zebrafish embryos. The crucial difference between the two formulation types is the way of active substance release. This investigation is the first report on zebrafish embryotoxicity of both clomazone and its formulations. The technical active ingredient and formulations caused mortality and diverse teratogenic effects, showing different levels of toxicity. The LC50 values for the technical ingredient, Rampa (R) EC and GAT Cenit 36 CS were 61.4, 9.6 and 92.5 mg a.i./l, respectively. Spontaneous movements in 22 hpf embryos decreased under exposure to both the technical ingredient and formulations. A significant number of underdeveloped embryos was detected after exposure to clomazone and Rampe EC, while no underdevelopment was noted in embryos exposed to GAT Cenit 36 CS. Exposure to the technical ingredient and formulations led also to a series of morphological changes and interfered with the growth of zebrafish embryos. The EC50 based on detection of edemas, spine and tail tip deformations and gas bladder absence (120 hpf) was 12.1, 10.1 and 24.1 mg/l for technical clomazone, Rampe EC and GAT Cenit 36 CS, while teratogenicity index (TI) based on LC50/EC50 ratio was 5.1, 1 and 3.8, respectively. The data in this study showed that the emulsifiable concentrate formulation (Rampa. EC) caused statistically significantly higher toxicity, and the aqueous capsule suspension (GAT Cenit 36 CS) lower toxicity than technical clomazone. It indicates that different formulations with the same active ingredient may have different environmental impacts, which is why risk assessment based only on active ingredient toxicity might not be sufficient in terms of preventing formulation effects on the environment.
Návaznosti
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