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EC number: 932-185-7 | CAS number: 1187742-72-8
- Life Cycle description
- Uses advised against
- Endpoint summary
- Appearance / physical state / colour
- Melting point / freezing point
- Boiling point
- Density
- Particle size distribution (Granulometry)
- Vapour pressure
- Partition coefficient
- Water solubility
- Solubility in organic solvents / fat solubility
- Surface tension
- Flash point
- Auto flammability
- Flammability
- Explosiveness
- Oxidising properties
- Oxidation reduction potential
- Stability in organic solvents and identity of relevant degradation products
- Storage stability and reactivity towards container material
- Stability: thermal, sunlight, metals
- pH
- Dissociation constant
- Viscosity
- Additional physico-chemical information
- Additional physico-chemical properties of nanomaterials
- Nanomaterial agglomeration / aggregation
- Nanomaterial crystalline phase
- Nanomaterial crystallite and grain size
- Nanomaterial aspect ratio / shape
- Nanomaterial specific surface area
- Nanomaterial Zeta potential
- Nanomaterial surface chemistry
- Nanomaterial dustiness
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- Nanomaterial pour density
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- Nanomaterial radical formation potential
- Nanomaterial catalytic activity
- Endpoint summary
- Stability
- Biodegradation
- Bioaccumulation
- Transport and distribution
- Environmental data
- Additional information on environmental fate and behaviour
- Ecotoxicological Summary
- Aquatic toxicity
- Endpoint summary
- Short-term toxicity to fish
- Long-term toxicity to fish
- Short-term toxicity to aquatic invertebrates
- Long-term toxicity to aquatic invertebrates
- Toxicity to aquatic algae and cyanobacteria
- Toxicity to aquatic plants other than algae
- Toxicity to microorganisms
- Endocrine disrupter testing in aquatic vertebrates – in vivo
- Toxicity to other aquatic organisms
- Sediment toxicity
- Terrestrial toxicity
- Biological effects monitoring
- Biotransformation and kinetics
- Additional ecotoxological information
- Toxicological Summary
- Toxicokinetics, metabolism and distribution
- Acute Toxicity
- Irritation / corrosion
- Sensitisation
- Repeated dose toxicity
- Genetic toxicity
- Carcinogenicity
- Toxicity to reproduction
- Specific investigations
- Exposure related observations in humans
- Toxic effects on livestock and pets
- Additional toxicological data
Endpoint summary
Administrative data
Description of key information
Skin sensitisation: not sensitising
Read-across based on grouping of substances (category approach) considering all available data on skin sensitisation in the Alkyl Ether Sulfates (AES) category in a Weight-of-Evidence approach.
Key value for chemical safety assessment
Skin sensitisation
Link to relevant study records
- Endpoint:
- skin sensitisation: in vivo (non-LLNA)
- Type of information:
- read-across based on grouping of substances (category approach)
- Adequacy of study:
- key study
- Justification for type of information:
- Please refer to the category justification provided in the category object.
- Key result
- Group:
- negative control
- Remarks on result:
- other: No skin sensitisation potential identified for Alkyl Ether Sulfates (AES) based on all available relevant data in the category.
- Key result
- Group:
- test chemical
- Remarks on result:
- other: No skin sensitisation potential identified for Alkyl Ether Sulfates (AES) based on all available relevant data in the category.
- Key result
- Group:
- positive control
- Remarks on result:
- other: No skin sensitisation potential identified for Alkyl Ether Sulfates (AES) based on all available relevant data in the category.
- Interpretation of results:
- other: CLP/EU GHS criteria not met, no classification required according to Regulation (EC) No 1272/2008
- Conclusions:
- Applying read-across based on grouping of substances (category approach), no skin sensitisation potential is predicted for the target substance.
- Executive summary:
The available data on skin sensitisation in the Alkyl Ether Sulfates (AES) category indicate no skin sensitisation potential for the target substance. As explained in the category justification, the differences in molecular structure and composition between the target substance and the members of the AES category are unlikely to lead to differences in the skin sensitisation potential.
Reference
For a detailed assessment of the skin sensitisation potential of the Alkyl Ether Sulfates (AES) category, please refer to the category justification attached to the category object.
Endpoint conclusion
- Endpoint conclusion:
- no adverse effect observed (not sensitising)
- Additional information:
Skin sensitisation
No data on skin sensitisation are available for alcohols, C12-14 (even numbered), ethoxylated (<=2.5 moles EO), sulfated, monoisopropanolamine salt (CAS No. 1187742-72-8, EC No. 932-185-7). In order to assess the skin sensitising potential, studies in the database of the Alkyl Ether Sulfates (AES) category are considered in a read-across approach. Studies assessing skin sensitisation are available for the following AES substances:
Table 1: Database on skin sensitisation in the Alkyl Ether Sulfates (AES) category
CAS / EC Nos.
Substance
Study or Report No.
Study protocol (adopted in)
Concentration in test material [%]
Hazard conclusion
‘Linear’ subgroup
1471312-55-6 / 939-523-2
Alcohols, C8-10, ethoxylated, sulfates, sodium salts
121487
OECD 406 (GPMT)
98.7
Not sensitising
68585-34-2 / 500-223-8
Alcohols C10-16, ethoxylated (1-2,5 EO) sulphated, sodium salts
247/8409
Similar OECD 406 (GPMT)
Not reported
Not sensitising
4301
OECD 406 (GPMT)
10
Not sensitising
11182
Similar OECD 406 (GPMT)
Not reported
Not sensitising
11182
Similar OECD 406 (Buehler)
Not reported
Not sensitising
16604
Similar OECD 406 (Buehler)
31.4
Not sensitising
4309
Similar OECD 406 (GPMT)
Not reported
Sensitising
4303
Similar OECD 406 (GPMT)
Not reported
Sensitising
4289
Similar OECD 406 (GPMT)
Not reported
Sensitising
4304
Similar OECD 406 (GPMT)
Not reported
Sensitising
9731
Similar OECD 406 (Buehler)
Not reported
Sensitising
30449
Human data (HRIPT), Good clinical practices guideline 21 CFR parts 50 and 56
Not reported
Not sensitising
07-009A
Human data (HRIPT), Good clinical practices guideline 21 CFR parts 50 and 56
Not reported
Not sensitising
68891-38-3 / 500-234-8
Alcohols, C12-14, ethoxylated, sulfates, sodium salts
R770036
OECD 406 (GMPT)
28
Not sensitising
3170
OECD 406 (GPMT)
28
Not sensitising
861041D/UGF 19/SS
OECD 406 (GPMT)
70
Not sensitising
90/8507
Similar OECD 406 (GPMT)
Not reported
Not sensitising
89.0241
OECD 406 (GPMT)
27
Not sensitising
SM880964
Similar OECD 406 (GPMT)
27
Sensitising
174450-50-1 / 605-725-1
Alcohols C12-14 (even numbered), ethoxylated (< 2.5 EO), sulphated, triisopropanolamine salts
2399
OECD 406 (Buehler)
83.8
Not sensitising
‘Mixed branched & linear’ subgroup
160901-28-0 / 500-465-4
Alcohols, C9-11, branched and linear, ethoxylated, sulfates, sodium salts
221/7703
Similar OECD 406 (GPMT)
Not reported
Not sensitising
Evaluation of skin sensitisation as observed in studies
The available studies were performed with alcohols, C8-10, ethoxylated, sulfates, sodium salts (CAS No. 1471312-55-6, EC No. 939-523-2), alcohols C10-16, ethoxylated (1-2,5 EO) sulphated, sodium salts (CAS No. 68585-34-2, EC No. 500-223-8), alcohols, C12-14, ethoxylated, sulfates, sodium salts (CAS No. 68891-38-3, EC No. 500-234-8) and alcohols C12-14 (even numbered), ethoxylated (< 2.5 EO), sulphated, triisopropanolamine salts (CAS No. 174450-50-1, EC No. 605-725-1) from the ‘linear’ subgroup and with alcohols, C9-11, branched and linear, ethoxylated, sulfates, sodium salts (CAS No. 160901-28-0, EC No. 500-465-4) from the ‘mixed branched & linear’ subgroup. The concentration of the respective AES substances in the test material used in these studies varied from 10 - 98.7%, with water as the solvent in most test materials. For a number of studies no test material purity was reported. All in vivo animal studies followed the Buehler or GPMT protocol described in OECD guideline 406.
For a majority of the in vivo animal studies, no skin sensitising potential was reported. Mild to severe skin irritation effects (erythema and/or oedema) were observed following the epicutaneous and/or topical induction and were absent following the challenge phase.
Two studies of high quality were available within the category and are summarised below.
A study was performed with alcohols, C8-10, ethoxylated, sulfates, sodium salts (CAS No. 1471312-55-6, EC No. 939-523-2) according to the guinea pig maximisation test protocol described in OECD guideline 406 and under GLP conditions (Z&S, 2013). Ten female guinea pigs were included in the test group. The pure test substance (98.7%) was suspended in physiological saline for the intradermal induction, and in vaseline for the topical induction and challenge phases, respectively. On Day 0 the intradermal induction was performed with 2.5% test substance. The topical induction started on Day 6 with a 1.5% suspension, lasting for 48 h under occlusive conditions. On Day 20 the animals of the test and negative control groups were challenged with 0.5% test substance for 24 h under occlusive conditions. Skin reactions were scored 24 and 48 h after patch removal. The concentrations used in the main study were selected based on the results of a range-finding test with 10 animals. In the positive control group, 5 female guinea pigs were treated according to the same protocol as the test group with mercaptobenzothiazole. The intradermal and topical induction concentrations were 2% and 25%, respectively, while the challenge was performed with a 15% suspension in vaseline.
Following the intradermal induction, skin irritation was noted at the test sites of all animals. The topical induction did not cause skin irritation in any negative control or test group animals. Following the challenge, no skin irritation was observed in the negative control and test group animals. No adverse systemic effects of the treatment or significant body weight changes were noted in any animals. The 5 animals in the negative control group did not show any skin reactions following the challenge, while 5/5 animals in the positive control group showed a positive indication of skin sensitisation, indicating the controls were valid. The test substance showed no sensitising potential under the study conditions.
The study with alcohols C12-14 (even numbered), ethoxylated (< 2.5 EO), sulphated, triisopropanolamine salts (CAS No. 174450-50-1, EC No. 605-725-1) was performed according to the Buehler protocol described in OECD guideline 406 and under GLP conditions. Twenty female guinea pigs were included in the test group and ten in the negative control group. The pure test substance (83.8%) was suspended in deionised water for the topical induction and challenge phases. On Day 0 the first topical induction was performed with 50% test substance, lasting for 6 h under occlusive conditions. The second and third topical induction was performed on Day 7 and 14, respectively, with a 50% concentration. On Day 28 the animals of the test and negative control groups were challenged with 25% test substance for 6 h under occlusive conditions. Skin reactions were scored 24 and 48 h after patch removal. The concentrations used in the main study were selected based on the results of a range-finding test with 6 animals.
The dermal treatment during the first induction phase led to scarcely detectable skin irritation in 2/20 animals, 24 h after patch removal. After the second induction phase, 14/20 animals exhibited slight to well-defined erythema in combination with slight oedema 24 h after patch removal. Before the treatment in the third induction phase, these 14 animals, after shearing, still exhibited scaling in the administration area. The test substance was administered to intact skin. 24 h after the second induction phase, the administration area exhibited scarcely detectable erythema and oedema in 4/20 animals, well-defined erythema and oedema in 5/20 animals and moderate erythema and oedema in 2/20 animals, in 1 animal combined with necrotic spots on the skin. The control animals treated with the vehicle did not show irritation on the treated skin at any reading time point during the three induction phases. The challenge treatment did not cause any cutaneous reactions in the negative control and test group animals in the form of erythema or oedema 24 and 48 h after patch removal. No adverse systemic effects of the treatment or significant body weight changes were noted in any animals. A reliability check was performed regularly with 2-mercaptobenzothiazole. The test substance showed no sensitising potential under the conditions of the study.
In the in vivo studies 4309, 4303, 4289, 4304 and 9731 performed with alcohols C10-16, ethoxylated (1-2,5 EO) sulphated, sodium salts (CAS No. 68585-34-2, EC No. 500-223-8), as well as study No. SM880964 performed with alcohols, C12-14, ethoxylated, sulfates, sodium salts (CAS No. 68891-38-3, EC No. 500-234-8), it was concluded that the test material caused skin sensitisation. However, for all these studies the information on the irritating skin effect following epicutaneous and/or topical induction was missing. In most studies for which this information was reported, the induction application caused skin irritation. Therefore, the skin effects observed following the challenge phase in these studies are likely to have been skin irritation, rather than skin sensitisation.
Two Human Repeated Insult Patch Tests (study No. 30449 and 07-009A) were performed with alcohols C10-16, ethoxylated (1-2,5 EO) sulphated, sodium salts (CAS No. 68585-34-2, EC No. 500-223-8). Some skin irritation was noted during the induction phases in a majority of the volunteers. Both studies concluded that the test substance showed no skin sensitising potential in the human volunteers.
Data on counter ions
The effects of monoisopropanolamine (MIPA) on human health are clearly dominated by its corrosive properties. MIPA is listed in Annex VI of the CLP Regulation (EC) No. 1272/2008 as Skin Corr. 1B, H314. Further information indicates that MIPA is moderately toxic after dermal application, leading to a classification for Acute Tox. 4, H312. There is no indication of a skin sensitising potential of MIPA. Therefore, any contribution of MIPA to the endpoint skin sensitisation is considered to be negligible.
There is experimental data on substances with the counter ions sodium (Na+) and triisopropanolamine (TIPA), showing negative results for skin sensitisation. This indicates that these counter ions will not have a skin sensitising potential.
Magnesium (Mg2+) and ammonium (NH4+) are both considered not to show a skin sensitising potential based on the available data (primarily on their salts).
For a detailed evaluation of a potential effect of the counter ions on the toxicological profiles of the AES member substances, please refer to the category justification attached to the category object.
Conclusion on skin sensitisation potential of substances in the AES category
The WoE analysis based on the in vivo studies and HIRPTs indicates that AES substances in general do not show a skin sensitising potential. The conclusion is fully supported by the OECD QSAR Toolbox profiling results. This applies to all AES substances in the category, whether they belong to the ‘linear’, ‘unsaturated’ or ‘mixed branched & linear’ subgroups and regardless of their counter ion. The outcome of this WoE evaluation is used for the hazard assessment and to conclude on classification and labelling of all AES substances in the category. This evaluation is considered sufficient for the hazard assessment and classification and labelling of the AES substances. For a detailed evaluation of the skin sensitising potential of the substances in the AES category, please refer to the category justification attached to the category object.
Respiratory sensitisation
Endpoint conclusion
- Endpoint conclusion:
- no study available
Justification for classification or non-classification
The available data on skin sensitisation obtained with members of the Alkyl Ether Sulfates (AES) category do not meet the criteria for classification according to the CLP Regulation (EC) No. 1272/2008, and are therefore conclusive but not sufficient for classification. Based on grouping of substances (category approach), alcohols, C12-14 (even numbered), ethoxylated (<=2.5 moles EO), sulfated, monoisopropanolamine salt (CAS No. 1187742-72-8, EC No. 932-185-7) is predicted not to fulfil the classification criteria and is consequently not classified for skin sensitisation.
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