Registration Dossier
Registration Dossier
Please be aware that this old REACH registration data factsheet is no longer maintained; it remains frozen as of 19th May 2023.
The new ECHA CHEM database has been released by ECHA, and it now contains all REACH registration data. There are more details on the transition of ECHA's published data to ECHA CHEM here.
Use of this information is subject to copyright laws and may require the permission of the owner of the information, as described in the ECHA Legal Notice.
EC number: 237-048-9 | CAS number: 13597-46-1
Endpoint summary
Administrative data
Description of key information
Zinc selenite:
Acute oral toxicity: LD50 of 50-500 mg/kg dw (Prinsen, 1996c)
Acute inhalation toxicity: LD50 of 1-5 mg/L air (Leuschner, 2010)
Dermal toxicity: waived
Key value for chemical safety assessment
Acute toxicity: via oral route
Endpoint conclusion
- Endpoint conclusion:
- adverse effect observed
- Dose descriptor:
- LD50
- Value:
- > 50 - < 500 mg/kg bw
- Quality of whole database:
- Literature data of good quality (Klimisch 2); effects between 200 and 500 mg/kg bw for males and between 50 and 200 mg/kg bw for females.
Acute toxicity: via inhalation route
Endpoint conclusion
- Endpoint conclusion:
- adverse effect observed
- Dose descriptor:
- LC50
- Value:
- > 1 - < 5 mg/L air
- Quality of whole database:
- Read-across from GLP study of hight quality (Klimisch 1)
Acute toxicity: via dermal route
Endpoint conclusion
- Endpoint conclusion:
- no study available
Additional information
- Se-metal (massive, powder)
- Disodium selenate
- Disodium selenite
- Selenium dioxide / selenious acid
- Zinc selenite
- Barium selenite
- Acute toxicity – oral
- Acute toxicity – inhalation
Additional information:
When no substance-specific data are available, a read-across category-approach is used for the assessment of the toxicological properties of selenium and selenium compounds. The following Se-substance are included in the category:
A detailed rationale for the read-across hypothesis has been outlined in the read-across report that was generated according to the principles laid out in the Read-Across Assessment Framework (RAAF). In summary, the physico-chemical behavior of elemental selenium (once it has formed an ion-from its metal state), disodium selenite, disodium selenate and selenium dioxide/selenious acid is the same with regard to their metabolic fate. All selenium compounds (organic and inorganic, including elemental selenium), do share the very same metabolic fate in that after their resorption, reduction to the selenide moiety [Se2-], which is the single common precursor for its further metabolic conversion, takes place.
Therefore, there seems to be good evidence that different selenium moieties will behave very similar also for their ability to form reactive species which may play a decisive role in the generation of cytotoxicity followed likewise by unspecific and secondary clastogenicity and read-across can be made from the available data for disodium selenite. It is concluded that additional testing for each individual member of the proposed Se-category is not necessary and scientifically not meaningful.
In the case of inorganic salts like barium selenite and zinc selenite, uptake is always associated with a dissolution of the substance, i.e. dissociation into the metal cation (Zn2+, Ba2+) and the selenite anion (SeO32-). It can safely be assumed that the selenium/selenite moiety of barium/zinc selenite is generally of higher toxicological relevance than the zinc/barium cations. Therefore, the subsequent assessment of the toxicity of barium/zinc selenite focuses on the selenium moiety. As no in vivo toxicokinetic data or in vitro bioaccessibility data are available for a comparative assessment of relative bioavailability of various selenite substances, water solubility is adopted as a surrogate for bioavailability. Disodium selenite is readily soluble, with a water solubility of 800-900 g/L at 20°C. Barium selenite and zinc selenite, on the other hand, are poorly soluble salts (water solubility at 20°C of 66.7 mg/L and 16 mg/L, respectively, i.e. a difference of four/five orders of magnitude). Based on that, an intrinsically very conservative read-across from highly soluble forms to the poorly soluble barium/zinc selenite is proposed as the latter are assumed to have a lower solubility. It should also be noted that selenite anions in the tests with disodium selenite are formed under most physiological relevant conditions (i.e. neutral pH), thus facilitating unrestricted read-across between the various substances. In slightly acid conditions (pKa:8.32) the hydrogen selenite ion (HSeO3-) is formed whereas in more acidic conditions (pKa:2.62) the formation of selenious acid is observed (H2SeO3). Based on such existing equilibrium conditions, read-across between selenites, hydrogen selenites and selenious acid (solubility of 1670 g/L at 20°C) is justified.
The Table below gives an overview of reliable acute oral toxicity studies for various Se-compounds. The table reports the test substance, test species, test result and reference.
Acute oral toxicity of different Se-compounds: available data
Test substance
| Test Species
| Result
| Reference
|
Disodium selenite | rat | LD50: 7 mg/kg bw | Cummins and Kimura, 1971 |
Se-metal (powder) | rat | LD0: 5000 mg/kg bw | Prinsen, 1996a |
Se-metal (crude) | rat | LD0: 5000 mg/kg bw | Prinsen, 1996b |
SeO2 | rat | LD50: 68.1 mg/kg bw | Sing and Junnarkar, 1991 |
SeO2 | mice | LD50: 23.3 mg/kg bw | Sing and Junnarkar, 1991 |
Zn-selenite | rat | LD50: 50-500 mg/kg bw | Prinsen, 1996c |
No data are available for disodium selenate. Information on fate and speciation of selenate in mammals shows that adsorbed selenate is rapidly transformed to selenide (via selenite as intermediate speciation form) which is the relevant form of Se in mammals; it is therefore expected that acute effects that are observed with sodium selenite are also relevant for disodium selenate. The data that were generated by Cummins and Kimura (1971) for disodium selenite can therefore be used for assessing the acute oral toxicity of disodium selenate.
Zinc selenite and Se-metal were significantly less toxic than disodium selenite. This is likely related to their lower solubility which is respectively 4 to 8 orders of magnitude lower than that of disodium selenite.
The table below gives an overview of reliable acute inhalation toxicity studies for various Se-compounds. The table reports the test substance, test species, test result and reference.
Acute inhalation toxicity of different Se-compounds: available data
Test substance | Test Species | Result | Reference |
Disodium selenate | rat | LD50: 0.052 – 0.51 mg/L air | Nagy, 2012 |
Se-metal | rat | LD0: 5.67 mg/L air | Bennick, 1996 |
Zinc selenite | rat | LD50: 1 – 5 mg/L air | Leuchner, 2010 |
No data for: Disodium selenite, selenium dioxide
No data are available for disodium selenite. Information on fate and speciation of inorganic Se-species shows that selenate is rapidly transformed to selenide (via selenite as intermediate speciation form) which is the relevant form of Se in mammals; it is therefore expected that acute effects that are observed with tests that are conducted with disodium selenate, also take into account the effects that are caused by the common transformation products of selenate/selenite.
Selenite was also assessed in a test with zinc selenite. The observed acute toxicity was about one order of magnitude less than sodium selenate. This difference, however, can be explained by the lower solubility of zinc selenite (compared to sodium selenate). Based on this finding there is no indication that the acute toxicity (via inhalation) of selenite would be higher than the acute toxicity for selenate.
In addition, skin irritation tests with disodium selenate and disodium selenite show a similar response (Cat.2, based on OECD 439, no irritation based on OECD 431; see further), suggesting that both substances show a similar reaction with biological tissues.
Justification for classification or non-classification
- Acute Tox. Cat.3 - H301 (oral)
- Acute Tox. Cat.3 - H331 (inhalation)
- Acute Tox. Cat.2 - H300 (oral)
- Acute Tox. Cat.3 - H331 (inhalation)
- Acute Tox. Cat.3 - H301 (oral)
- Acute Tox. Cat.3 - H331 (inhalation)
- Acute Tox. Cat.3 - H301 (oral)
- Acute Tox. Cat.3 - H331 (inhalation)
Selenium, disodium selenite and selenium compounds in general (incl zinc selenite) are subject to legally binding harmonised classifications. As included in the CLP Regulation (EC) No 1272/2008, Annex VI, Table 3.1, the following classifications with regard to acute toxicity are mandatory:
Selenium (Index-Nr 034 - 001 - 22 - 2):
Disodium selenite (Index-Nr 034 - 003 - 00 - 3)
Selenium compounds (general) (Index-Nr 034 - 002 - 00 - 8)
Based on the available data, and taking into account the harmonised classifications, the following substance-specific classification is determined for zinc selenite:
Information on Registered Substances comes from registration dossiers which have been assigned a registration number. The assignment of a registration number does however not guarantee that the information in the dossier is correct or that the dossier is compliant with Regulation (EC) No 1907/2006 (the REACH Regulation). This information has not been reviewed or verified by the Agency or any other authority. The content is subject to change without prior notice.
Reproduction or further distribution of this information may be subject to copyright protection. Use of the information without obtaining the permission from the owner(s) of the respective information might violate the rights of the owner.
