Registration Dossier
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EC number: 229-059-2 | CAS number: 6408-50-0
Skin sensitisation
Administrative data
- Endpoint:
- skin sensitisation, other
- Type of information:
- (Q)SAR
- Adequacy of study:
- weight of evidence
- Reliability:
- 2 (reliable with restrictions)
- Rationale for reliability incl. deficiencies:
- results derived from a valid (Q)SAR model and falling into its applicability domain, with adequate and reliable documentation / justification
- Justification for type of information:
- DEREK (EC3, potency)
1 Substance
1.1 CAS number 6408-50-0
1.2 EC number 229-059-2
1.3 Chemical name 1-(methylamino)-4-[(3-methylphenyl)amino]anthraquinone
IUPAC 1-(methylamino)-4-[(3-methylphenyl)amino]anthraquinone
Other HSB-2651
Other
1.4 Structural formula
1.5 Structure codes
SMILES CNc3ccc(Nc1cccc(C)c1)c4c(=O)c2ccccc2c(=O)c34
InChI InChI=1S/C22H18N2O2/c1-13-6-5-7-14(12-13)24-18-11-10-17(23-2)19-20(18)22(26)16-9-4-3-8-15(16)21(19)25/h3-12,23-24H,1-2H3
Other
Stereochemical features Not applicable
2 General Information
2.1 Date of QPRF 29 March 2018
2.2 Author and contact details Jamie Marshall, Envigo, Shardlow Business Park
London Road, Shardlow, Derbyshire, DE72 2GD
Email: jamie.marshall@envigo.com
3 Prediction
3.1 Endpoint (OECD Principle 1)
Endpoint EC3
Dependent variable Not applicable
3.2 Algorithm (OECD Principle 2)
Model or submodel name Derek EC3 Model
Model version 1.0.6
Reference to QMRF The QMRF for skin sensitisation alert with the identifier Q13-34-36-315 is available from the JRC QMRF inventory (http://qsardb.jrc.it/qmrf/). No QMRF for the EC3 model available. Further details can be obtained from https://www.lhasalimited.org/products/EC3-predictions-for-skin-sensitisation.htm
Predicted values (model result) 0.77 % (strong sensitiser)
Predicted values (comments) Based on structures triggering Alert 837 Ortho or para amino- or hydroxy-aniline: 10/27 compounds used in calculation.
Input for prediction Smiles
Calculated descriptor values Alert and fingerprints used for selecting analogues
3.3 Applicability domain (OECD Principle 3)
Domains Based on structures triggering Alert 837 Ortho or para amino- or hydroxy-aniline: 10/27 compounds used in calculation
Structural analogues i. LLNA EC3 % Median: 0.60% (strong sensitiser), Similarity: 32%
CAS 2495-37-6 Saflufenacil, CAS: 372137-35-4
ii. LLNA EC3 % Median: 0.90% (strong sensitiser), Similarity: 31%
CAS 140-11-4 Budesonide, CAS: 51333-22-3
iii. LLNA EC3 % Median: 0.57% (strong sensitiser), Similarity: 29%
Methyl cinnamate Mometasone furoate, CAS: not available
iv. LLNA EC3 % Median: 5.9% (moderate sensitiser), similarity: 27%
Benzyl benzoate Tixocortol pivalate, CAS: not available
Consideration on structural analogues Structural similarity between the four most similar structures and the query structure (30%) is considered poor.
The lack of similarity however is due to the analogues being chosen for their similarity to the para-aminoaniline moiety in the molecule. All the substances are ortho or para substituted anilines which, as explained above, are the anticipated autoxidation products of the substance and thus their similarity is to those substances rather than the parent compound itself. Thus while this similarity value is poor, it should not necessarily lead to the conclusion of discounting this result.
3.4 The uncertainty of the prediction (OECD principle 4)
DEREK assessment: Skin sensitisation in mammal is PLAUSIBLE, i.e. The weight of evidence supports the proposition.
3.5 The chemical and biological mechanisms according to the model underpinning the predicted result (OECD principle 5)
Hapten, binding to epidermal proteins via a range of reactive intermediates, ethier radical cations or Michael acceptors [Aptula et al]
This alert describes skin sensitisation of anilines substituted with hydroxyl or amino groups in ortho or para positions.
A range of reactive intermediates and oligomeric derivatives able to bind to epidermal proteins, have been proposed. The presence of an amino or hydroxy group in the para (or ortho) position to the aniline moiety makes this chemical class very effective at stabilising free radicals. Enzymatic or autoxidation of ortho and para amino or hydroxy substituted anilines lead to the formation of Wurster salt radical cations, quinone diimines and/or quinoneimines. Wurster salt-type intermediates are reactive, for example, at the exocyclic nitrogen while quinone diimine and quinoneimines are Michael acceptors..
4 Adequacy (Optional)
4.1 Regulatory purpose Skin sensitisation endpoint for assessing the skin sensitisation potency with in silico methods according to ECHA Guidance, Chapter R.7a, 2016.
4.2 Approach for regulatory interpretation of the model result
Result is directly applicable since no conversion of the result is required.
4.3 Outcome Using the average of the lowest values as reported for each structure in the DEREK report results in a conservative EC3 of 0.77 %.
4.4 Conclusion The prediction is considered reliable and will be used together with predictions from other models in a weight of evidence conclusion.
Data source
Reference
- Reference Type:
- study report
- Title:
- Unnamed
- Year:
- 2�018
Materials and methods
Test guideline
- Qualifier:
- no guideline followed
- Principles of method if other than guideline:
- - Principle of test:
QSAR prediciton of Skin senistisation
- Short description of test conditions: n/a
- Parameters analysed / observed: Skin senistisation
Test material
- Reference substance name:
- 1-(methylamino)-4-[(3-methylphenyl)amino]anthraquinone
- EC Number:
- 229-059-2
- EC Name:
- 1-(methylamino)-4-[(3-methylphenyl)amino]anthraquinone
- Cas Number:
- 6408-50-0
- Molecular formula:
- C22H18N2O2
- IUPAC Name:
- 1-(methylamino)-4-[(3-methylphenyl)amino]-9,10-dihydroanthracene-9,10-dione
- Test material form:
- solid: particulate/powder
- Details on test material:
- Identification: 1-(methylamino)-4-[(3-methylphenyl)amino] anthraquinone
Physical state/Appearance: dark red powder
Batch: 702W01
Purity: 99.4%
Expiry Date: 08 February 2020
Storage Conditions: room temperature in the dark
Intended use/Application: industrial chemical
Constituent 1
Results and discussion
In vitro / in chemico
Results
- Run / experiment:
- other: EC3 = 0.77%
- Parameter:
- other: Prediciton
- Remarks on result:
- positive indication of skin sensitisation
Any other information on results incl. tables
DEREK (EC3, potency) |
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1 |
Substance |
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1.1 |
CAS number |
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6408-50-0 |
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1.2 |
EC number |
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229-059-2 |
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1.3 |
Chemical name |
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1-(methylamino)-4-[(3-methylphenyl)amino]anthraquinone |
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IUPAC |
1-(methylamino)-4-[(3-methylphenyl)amino]anthraquinone |
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Other |
HSB-2651 |
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Other |
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1.4 |
Structural formula |
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1.5 |
Structure codes |
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SMILES |
CNc3ccc(Nc1cccc(C)c1)c4c(=O)c2ccccc2c(=O)c34 |
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InChI |
InChI=1S/C22H18N2O2/c1-13-6-5-7-14(12-13)24-18-11-10-17(23-2)19-20(18)22(26)16-9-4-3-8-15(16)21(19)25/h3-12,23-24H,1-2H3 |
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Other |
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Stereochemical features |
Not applicable |
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2 |
General Information |
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2.1 |
Date of QPRF |
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29 March 2018 |
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2.2 |
Author and contact details |
Jamie Marshall, Envigo, Shardlow Business Park London Road, Shardlow, Derbyshire, DE72 2GD Email: jamie.marshall@envigo.com |
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3 |
Prediction |
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3.1 |
Endpoint (OECD Principle 1) |
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Endpoint |
EC3 |
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Dependent variable |
Not applicable |
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3.2 |
Algorithm (OECD Principle 2) |
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Model or submodel name |
Derek EC3 Model |
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Model version |
1.0.6 |
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Reference to QMRF |
The QMRF for skin sensitisation alert with the identifier Q13-34-36-315 is available from the JRC QMRF inventory (http://qsardb.jrc.it/qmrf/). No QMRF for the EC3 model available. Further details can be obtained from https://www.lhasalimited.org/products/EC3-predictions-for-skin-sensitisation.htm |
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Predicted values (model result) |
0.77 % (strong sensitiser) |
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Predicted values (comments) |
Based on structures triggering Alert 837 Ortho or para amino- or hydroxy-aniline: 10/27 compounds used in calculation. |
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Input for prediction |
Smiles |
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Calculated descriptor values |
Alert and fingerprints used for selecting analogues |
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3.3 |
Applicability domain (OECD Principle 3) |
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Domains |
Based on structures triggering Alert 837 Ortho or para amino- or hydroxy-aniline: 10/27 compounds used in calculation |
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Structural analogues |
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Consideration on structural analogues |
Structural similarity between the four most similar structures and the query structure (30%) is considered poor. The lack of similarity however is due to the analogues being chosen for their similarity to the para-aminoaniline moiety in the molecule. All the substances are ortho or para substituted anilines which, as explained above, are the anticipated autoxidation products of the substance and thus their similarity is to those substances rather than the parent compound itself. Thus while this similarity value is poor, it should not necessarily lead to the conclusion of discounting this result. |
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3.4 |
The uncertainty of the prediction (OECD principle 4) |
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DEREK assessment: Skin sensitisation in mammal is PLAUSIBLE, i.e. The weight of evidence supports the proposition. |
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3.5 |
The chemical and biological mechanisms according to the model underpinning the predicted result (OECD principle 5) |
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Hapten, binding to epidermal proteins via a range of reactive intermediates, ethier radical cations or Michael acceptors [Aptula et al] This alert describes skin sensitisation of anilines substituted with hydroxyl or amino groups in ortho or para positions. A range of reactive intermediates and oligomeric derivatives able to bind to epidermal proteins, have been proposed. The presence of an amino or hydroxy group in the para (or ortho) position to the aniline moiety makes this chemical class very effective at stabilising free radicals. Enzymatic or autoxidation of ortho and para amino or hydroxy substituted anilines lead to the formation of Wurster salt radical cations, quinone diimines and/or quinoneimines. Wurster salt-type intermediates are reactive, for example, at the exocyclic nitrogen while quinone diimine and quinoneimines are Michael acceptors.. |
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4 |
Adequacy (Optional) |
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4.1 |
Regulatory purpose |
Skin sensitisation endpoint for assessing the skin sensitisation potency with in silico methods according to ECHA Guidance, Chapter R.7a, 2016. |
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4.2 |
Approach for regulatory interpretation of the model result |
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Result is directly applicable since no conversion of the result is required. |
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4.3 |
Outcome |
Using the average of the lowest values as reported for each structure in the DEREK report results in a conservative EC3 of 0.77 %. |
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4.4 |
Conclusion |
The prediction is considered reliable and will be used together with predictions from other models in a weight of evidence conclusion. |
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Applicant's summary and conclusion
- Interpretation of results:
- Category 1A (indication of significant skin sensitising potential) based on GHS criteria
- Conclusions:
- Using the average of the lowest values as reported for each structure in the DEREK report results in a conservative EC3 of 0.77 %.
The prediction is considered reliable and will be used together with predictions from other models in a weight of evidence conclusion.
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.
