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Please be aware that this old REACH registration data factsheet is no longer maintained; it remains frozen as of 19th May 2023.

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Diss Factsheets

Ecotoxicological information

Long-term toxicity to fish

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Administrative data

Link to relevant study record(s)

Reference
Endpoint:
fish early-life stage toxicity
Data waiving:
study scientifically not necessary / other information available
Justification for data waiving:
other:
Reason / purpose for cross-reference:
reference to other study
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reference to other study
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reference to other study
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reference to other study
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Conclusions:
Testing for long-term toxicity to fish is not considered necessary because:
- Short-term toxicity to fish is low.
- The risk characterisation ratios (RCR) based on PNECfreshwater derived from the acute data are <1.

Description of key information

Key value for chemical safety assessment

Additional information

Testing for long-term toxicity to fish is not considered necessary because:

No long-term aquatic data are available for the registered substance, which has a hydrolysis half-life of 40-80 hours at pH 7 and 20-25°C. Due to this moderate hydrolysis rate, the assessment entity for the aquatic compartment is the parent substance. Long-term aquatic toxicity testing for the silanol hydrolysis product is therefore not appropriate. Long-term aquatic toxicity testing for the parent substance, S2, is not required for the following reasons:

In accordance with Column 2 of REACH Annex IX, there is no need to further investigate the effects of this substance in a long-term aquatic toxicity to fish study because, as indicated in guidance R.7.8.4.3 (ECHA 2017), the quantitative chemical safety assessment (conducted according to Annex I of REACH) indicates that the Risk Characterisation Ratio is well below 1, even with due consideration of contributing uncertainties, and therefore the risk is already adequately controlled and further testing is not justifiable. The parent substance has a low solubility in water, is not bioaccumulative (based on BCF = 146 to 715 (see IUCLID Section 5.3 for further details) and there is no reason to expect any specific mechanism of toxicity beyond narcosis. Therefore, the occurrence of toxic effects that were not expressed at, or below the limit of solubility (that were not attributed to physical effects of undissolved test substance or precipitated by-products) would be considered unlikely. Based on the short-term aquatic data set for the parent substance, the most sensitive trophic level is algae, which has a 72-hour EL50 value of 700 mg/l. This value is above the limit of solubility for the parent substance (0.014 mg/l at 20°C), however a PNEC has been derived for the purpose of chemical safety assessment, using this value as a starting point. An assessment factor of 1000 was applied to derive the freshwater PNEC. For a narcotic chemical without a specific mode of toxic action, it is unlikely that the aquatic PNEC would be significantly over-estimated using this method.

Based on the highest freshwater RCR available for the parent substance, S2 (0.077), with a corresponding Predicted Environmental Concentration (PEC) of 0.054 mg/l, the PNECaquatic (freshwater) value would need to be ≤0.054 mg/l to result in RCR values ≥1. This value is 13 times lower than the current PNECaquatic (freshwater), based on the short-term dataset (0.7 mg/l). A PNECaquatic (freshwater) value of ≤0.054 mg/l would correspond to a long-term EC10 or NOEC value of ≤2.7 mg/l when applying an assessment factor of 50, indicating high toxicity which was not observed in the short-term dataset.

Additionally, the parent substance is highly insoluble and any effects observed in the short-term aquatic dataset are attributable to physical effects of undissolved test substance or precipitated by-products, rather than intrinsic toxicity. The test media preparation is extremely difficult for this substance, due to the low water solubility of the substance, its potential to hydrolyse and the condensation of the hydrolysis products to insoluble oligomers. As a consequence, there is the likelihood that in long-term aquatic tests, dissolved and undissolved phases of the parent substance will be present simultaneously potentially causing physical effects and that hydrolysis product will also be present. Additionally, preparation of a test medium containing a pre-hydrolysed form of the substance for testing is not technically achievable due to the formation of different chemical species and different phases and this would not assess the parent substance.

Overall it is concluded that the risk characterisation conclusion is sufficiently conservative in respect of any uncertainties and therefore further in vivo testing is not considered necessary or justified on ethical grounds. Details on how the PNEC and the risk characterisation ratio have been derived can be found in IUCLID Section 6, CSR Section 7.0 and Chapters 9 and 10 of the Chemical Safety Report, respectively.