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Administrative data

Description of key information

Disperse Red 302:1 is considered to be no skin sensitiser.

Key value for chemical safety assessment

Skin sensitisation

Link to relevant study records
Reference
Endpoint:
skin sensitisation: in vivo (LLNA)
Type of information:
experimental study
Adequacy of study:
key study
Study period:
2014-07-11 to 2014-10-24
Reliability:
1 (reliable without restriction)
Rationale for reliability incl. deficiencies:
guideline study
Qualifier:
according to guideline
Guideline:
OECD Guideline 429 (Skin Sensitisation: Local Lymph Node Assay)
Deviations:
no
Qualifier:
according to guideline
Guideline:
EU Method B.42 (Skin Sensitisation: Local Lymph Node Assay)
Deviations:
no
Qualifier:
according to guideline
Guideline:
EPA OPPTS 870.2600 (Skin Sensitisation)
Deviations:
no
GLP compliance:
yes (incl. QA statement)
Remarks:
(Bayerisches Landesamt für Gesundheit und Lebensmittelsicherheit, München, Germany)
Type of study:
mouse local lymph node assay (LLNA)
Species:
mouse
Strain:
CBA
Sex:
female
Details on test animals and environmental conditions:
- Full barrier in an air-conditioned room
- Temperature: 22 ± 3 °C
- Relative humidity: 55 ± 10 %
- Artificial light, sequence being 12 hours light, 12 hours dark
- Air change: at least 10 x / hour
- Free access to Altromin 1324 maintenance diet for rats and mice (prescreen test and main study: lot no. 1526)
- Free access to tap water, sulphur acidified to a pH value of approx. 2.8 (drinking water, municipal residue control, microbiological controls at regular intervals)
- The animals were kept in groups of 5 animals in IVC cages, type II L, polysulphone cages on Altromin saw fibre bedding (prescreen test and main study: lot no. 290114)
- Certificates of food, water and bedding are filed at BSL BIOSERVICE
- Adequate acclimatisation period (at least five days) under laboratory conditions
Vehicle:
dimethyl sulphoxide
Remarks:
Applichem, lot no. 2P003474, expiry date: 09/2014
Concentration:
The maximum technically applicable concentration of the test item in the vehicle was found to be 12.5 % in DMSO. Based on the results observed in the preliminary test the following test item concentrations were selected for the main study:
3 %, 6.25 % and 12.5 % (w/v)
DMSO was used as vehicle and served as negative control.
No. of animals per dose:
5 mice / group; 3 mice / prescreen test
Details on study design:
Preparation of the test item:
Based on the results observed in the prescreen test the following test item concentrations were selected for the main study: 3, 6.25 and 12.5 % (w/v). The preparations were made immediately prior to each dosing.

Preparation of the animals:
The animals were randomly selected. Identification was ensured by cage number and individual marking (tail).

Clinical observation:
Prior to the application and once a day thereafter all animals were observed in order to detect signs of toxicity, including dermal irritation at site of application.

Weight assessment:
The animals were weighed prior to the application and at the end of the test period (prior to the treatment with ³HTdR).

Dose groups:
3 test groups (3 different concentrations) and 1 negative control group (vehicle) were tested.

Test regime:
Topical application:
Each mouse was treated by topical application of 25 µL of the selected solution to the entire dorsal surface of each ear. Topical applications were performed once daily over three consecutive days.

Administration of ³H-Methyl thymidine:
Five days after the first topical application all mice were dosed with 20 µCi ³H-methyl thymidine by intravenous injection (tail vein) of 250 µL of 3H-methyl thymidine, diluted to a working concentration of 80 µCi/mL.

Preparation of cell suspension:
Approximately 5 hours after the injection of ³H-methyl thymidine all mice were sacrificed by cervical dislocation. The draining auricular lymph nodes were excised, individually pooled for each animal (2 lymph nodes per animal) and collected in phosphate buffered saline (PBS). A single cell suspension of pooled lymph node cells was prepared by gentle mechanical disaggregation through polyamide gauze (200 mesh size). After washing the gauze with PBS, the cell suspension was pelleted in a centrifuge. The supernatant was discarded, and the pellets were resuspended with PBS. This washing procedure was repeated. After the final wash each pellet was resuspended in approx. 1 mL 5 % TCA at approx. 4° C for approximately 18 hours for precipitation of macromolecules. Each precipitate was once washed again, resuspended in 1 mL 5 % TCA and 7 mL scintillation fluid was added. Then this solution was transferred into scintillation vials and stored at room temperature overnight.

Determination of incorporated ³H -Methyl thymidine:
The ³H-methyl thymidine – incorporation was measured in a ß-counter and expressed as the number of disintegrations per minute (DPM). Similarly, background 3H-methyl thymidine levels were also measured (5 % TCA). Determination of radioactivity was performed individually for each animal.

Evaluation of results:
The proliferative response of lymph node cells was expressed as the number of radioactive disintegrations per minute per lymph node (DPM/NODE) and as the ratio of ³H-methyl thymidine - incorporation into lymph node cells of test group animals relative to that recorded for control group animals (STIMULATION INDEX). Before DPM/NODE values were determined, background values were subtracted. EC3 values, calculated concentrations which induce stimulation indices of three, are determined by linear interpolation, EC3=c+[(3-d)/(b-d)]x(a c), between two points of the stimulation indices axis, one above (a,b) and one below (c,d) the stimulation index of three. If all measured points are above or below the stimulation index of three, no EC3 value can be stated.

A substance is regarded as a 'sensitiser' in the LLNA if at least one concentration of the test item results in a 3-fold or greater increase in ³H-methyl thymidine - incorporation into lymph node cells of the test group animals, relative to that recorded for the lymph nodes of control group animals (Stimulation Index equal to or greater than 3.0). On the basis of the test results, the test substance may be classified into one of the following categories in conformity with the criteria given in Commission Regulation (EU) No 286/2011 as well as in GHS - Globally Harmonised System of Classification and Labelling of Chemicals, fifth revised edition, 2013:

Skin sensitiser:
Category 1:
A substance is classified as a skin sensitiser
a) if there is evidence in humans that the substance can lead to sensitisation by skin contact in a substantial number of persons, or
b) if there are positive results from an appropriate animal test.
WARNING, exclamation mark. May cause an allergic skin reaction.

Sub-category 1A:
Substances showing a high frequency of occurrence in humans and/or a high potency in animals can be presumed to have the potential to produce significant sensitisation in humans. Severity of reaction may also be considered.
EC3 value ≤2 %
WARNING, exclamation mark. May cause an allergic skin reaction.

Sub-category 1B:
Substances showing a low to moderate frequency of occurrence in humans and/or a low to moderate potency in animals can be presumed to have the potential to produce sensitisation in humans. Severity of reaction may also be considered.
EC3 value >2 %
WARNING, exclamation mark. May cause an allergic skin reaction.
Positive control substance(s):
other: Phenylenediamine
Statistics:
Outlier tests according to Dixon, Grubbs and Nalimov were performed for the values measured for the number of disintegrations per minute (DPM).
If outliers were identified, these values were not included in the calculation of the stimulation indices. As at least four values per group are required for the evaluation of the results, the outlier test was not repeated to detect further outliers.
Positive control results:
The recent reliability check was performed in May 2014. The raw data of this study are kept in the BSL archives (BSL Project ID 142473 A).
Positive-control substance: P-Phenylenediamine (CAS 106-50-3, Sigma, purity >98 %; Lot No.: SLBC7171V) 1 %
Vehicle: DMSO
Species/strain: healthy CBA/CaOlaHsd mice
Source: Harlan Laboratories GmbH, 5800 AN Venray, The Netherlands
Concentrations: 1 % on three consecutive days

The Stimulation Index was 10.0.
Key result
Parameter:
SI
Value:
1
Test group / Remarks:
3 %
Key result
Parameter:
SI
Value:
1.2
Test group / Remarks:
6.25 %
Key result
Parameter:
SI
Value:
1.6
Test group / Remarks:
12.5 %

All animals survived throughout the test period without showing any adverse clinical signs.

All animals showed the expected weight development, which includes a weight loss of up to 2 g throughout the study.

Radioactive Determination of the Test Substance Groups

POS CPM Test Item Conc. [%] Animal number DPM DPM- mean back- ground DPM/ Node Stimulation Index
16 1382.0

Negative 

Control

100 16 3672.0 3645.8
1822.9
 
17 760.0 17 1993.0 1966.8 983.4  
18 1144.0 18 2979.0 2952.8 1476.4  
19 1690.0 19 4479.0 4452.8 2226.4  
20 1050.0 20 2783.0 2756.8 1378.4  
MV 1205.2 MV 3181.2 3155.0 1577.5 1.0
SD 313.8 SD 841.0 841.0 420.5  
26 1681.0 FAT
93504/B TE
in DMSO
3 1 4516.0 4489.8 2244.9 1.4
27 1187.0 2 3103.0 3076.8 1538.4 1.0
28 777.0 3 2074.0 2047.8 1023.9 0.6
29 1167.0 4 3113.0 3086.8 1543.4 1.0
30 1402.0 5 3756.0 3729.8 1864.9 1.2
MV 1242.8 MV 3312.4 3286.2 1643.1 1.0
SD 297.7 SD 807.8 807.8 403.9 0.3
31 1227.0 FAT
93504/B TE
in DMSO
6.25 6 3266.0 3239.8 1619.9 1.0
32 1944.0 7 5178.0 5151.8 2575.9 1.6
33 1797.0 8 4717.0 4690.8 2345.4 1.5
34 1046.0 9 2757.0 2730.8 1365.4 0.9
35 1446.0 10 3873.0 3846.8 1923.4 1.2
MV 1492.0 MV 3958.2 3932.0 1966.0 1.2
SD 337.2 SD 893.6 893.6 446.8 0.3
36 1881.0 FAT
93504/B TE
in DMSO
12.5 11 5229.0 5202.8 2601.4 1.6
37 1974.0 12 5215.0 5188.8 2594.4 1.6
38 1883.0 13 4925.0 4898.8 2449.4 1.6
39 2886.0 14 7641.0 7614.8 3807.4 2.4
40 1051.0 15 2791.0 2764.8 1382.4 0.9
MV 1935.0 MV 5160.2 5134.0 2567.0 1.6
SD 581.9 SD 1538.2 1538.2 769.1 0.5
73 11.0 Background Szinti and TCA 28.0  
74 9.0 24.0  
75 10.0 25.0  
76 11.0 27.0  
77 11.0 27.0  
MV 10.4 MV 26.2 0.0 0.0 0.0
SD 0.8   SD 1.5      
Interpretation of results:
GHS criteria not met
Conclusions:
FAT 93504/B should not be regarded as a dermal sensitiser.

Executive summary:

The skin sensitising potential of FAT 93504/B was evaluated in a study conducted according to OECD Guideline 429. Mice of CBA/CaOlaHsd, each group containing 20 animals, were used for the test. Based on the results of the prescreen test the test item was assessed for sensitising properties at concentrations of 3 %, 6.25 % and 12.5 % (w/v), each diluted with DMSO (dimethyl sulfoxide). None of the three tested concentrations of the test item reached the stimulation index of 3. The stimulation index at a concentration of 3 % was 1.0 The stimulation index at a concentration of 6.25 % was 1.2. The stimulation index at a concentration of 12.5 % was 1.6. Hence, the EC3 value (derived by linear interpolation) could not be calculated as the stimulation indices of all concentrations were below 3. Consequently, according to OECD 429, the test item FAT 93504/B as described in this report is expected to have no sensitising properties and therefore should not be regarded as a dermal sensitiser.

Endpoint conclusion
Endpoint conclusion:
no adverse effect observed (not sensitising)
Additional information:

The skin sensitising potential of FAT 93504/B was evaluated in a study conducted according to OECD Guideline 429. Mice of CBA/CaOlaHsd, each group containing 20 animals, were used for the test. Based on the results of the prescreen test the test item was assessed for sensitising properties at concentrations of 3, 6.25 and 12.5 % (w/v), each diluted with DMSO (dimethyl sulfoxide). None of the three tested concentrations of the test item reached the stimulation index of 3. The stimulation index at a concentration of 3 % was 1.0. The stimulation index at a concentration of 6.25 % was 1.2. The stimulation index at a concentration of 12.5 % was 1.6. Hence, the EC3 value (derived by linear interpolation) could not be calculated as the stimulation indices of all concentrations were below 3. Consequently, according to OECD 429, FAT 93504/B, is expected to have no sensitising properties and therefore should not be regarded as a dermal sensitiser.

Respiratory sensitisation

Endpoint conclusion
Endpoint conclusion:
no study available

Justification for classification or non-classification

Disperse Red 302:1 is considered to be no skin sensitiser, hence it does not warrant classification according to the criteria set out by Regulation (EC) No. 1272/2008 (CLP).