Registration Dossier
Registration Dossier
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EC number: 220-666-8 | CAS number: 2855-13-2
Biodegradation in soil
Administrative data
Link to relevant study record(s)
- Endpoint:
- biodegradation in soil: simulation testing
- Remarks:
- Prediction of degradation products using CATALOGIC 301 C v .09.13
- Type of information:
- (Q)SAR
- Adequacy of study:
- key study
- Study period:
- 2021
- 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:
- 1. SOFTWARE
OASIS Catalogic v5.11.19
2. MODEL (incl. version number)
CATALOGIC 301C v.09.13
3. SMILES OR OTHER IDENTIFIERS USED AS INPUT FOR THE MODEL
See section 'Test Material'.
4. SCIENTIFIC VALIDITY OF THE (Q)SAR MODEL
See attached QMRF.
5. APPLICABILITY DOMAIN
See attached QPRF.
6. ADEQUACY OF THE RESULT
- The model is scientifically valid (see attached QMRF).
- The model estimates the biodegradability of a substance Screening information on the ready biodegradability is required for substances manufactured or imported in quantities of 1 t/y or more. Depending on the results, further information may be required for substances manufactured or imported in quantities of 100 t/y or more (simulation testing on ultimate degradation in surface water/soil/sediment). Column 2 of REACH Annex VII provides exemptions for conducting the study. It does not need to be conducted if the substance is inorganic. According to column 2 of REACH Annex IX, testing is not required if the substance is highly insoluble in water, or the substance is readily biodegradable.
- See attached QPRF for reliability assessment. - Principles of method if other than guideline:
- Estimation of ready biodegradation and degradation products using OASIS Catalogic v5.11.19 BOD 28 days MITI (301 C v .09.13).
- GLP compliance:
- no
- Test type:
- other: QSAR
- Oxygen conditions:
- aerobic
- Remarks on result:
- other: The applied QSAR model was used to predict the identity and quantity of the degradation products of the substance.
- Transformation products:
- yes
- Endpoint:
- biodegradation in soil: simulation testing
- Data waiving:
- exposure considerations
- Justification for data waiving:
- the study does not need to be conducted because direct and indirect exposure of soil is unlikely
- Reason / purpose for cross-reference:
- data waiving: supporting information
Referenceopen allclose all
-Concomitant predictions:
Not ready degradable
Primary Half Life = 9.24 days
Ultimae Half Life = 3m 27d
- Predicted value (model result): O2 -consumption (BOD) = 0.15 ± 0.0172
Predicted metabolites:
Table: QSAR prediction for CAS 2855-13-2 (3-aminomethyl-3,5,5-trimethylcyclohexylamine (IPDA) using CATALOGIC 301 C v .09.13 - June, 2016; metabolites with a quantity > 0. 1 % parent after 28 d are highlighted by bold type; metabolite no: according to (Q)SAR model Catalogic v09.13)
No | Metabolite no | Smiles | Level | Transformation no | Transformation name | Quantity (%) | Log Kow | BOD prediction % 80D (28 d) |
1 | 13 | CC1(C)CC(N)CC(C)(C(O )=O}C1 | 2 | 66 | Aldehyde Oxidation | 14,82 | -1,06 | 9 |
2 | Parent | CC1(C)CC(N)CC(C)(CN)C1 | 0 |
|
| 12,23 | 1,90 | 15 |
3 | 66 | CC(C)(CC(C)(C)C(O)=O)C(O)=O | 7 | 66 | Aldehyde Oxidation | 7,011 | 1,48 | 0 |
4 | 68 | CC(C)(CC(C)(CC(O)=O)C(O)=O)C(O)=O | 7 | 66 | Aldehyde oxidation | 10,56 | 0,73 | 0 |
5 | 57 | CC(C)(C)CC(C)(CO)C(O)=O | 6 | 346 | Decarboxylation | 6,41 | 1,84 | 1 |
6 | 35 | CC/C)/CC/C)/CC/0)=0)CN)C/0)=0 | 4 | 66 | Aldehvde Oxidation | 5,713 | -2,70 | 7 |
7 | 33 | CC/C)/CC/O)=OlCC/C)/CN)C/0)=0 | 4 | 66 | Aldehvde Oxidation | 5,713 | -2,70 | 22 |
8 | 46 | CC(C)(CC(C)(C)CN)C(O)=O | 5 | 346 | Decarboxylation | 4,54 | -1,37 | 8 |
9 | 45 | CC{C){C)CC{C){CN)C{O)=O | 5 | 346 | Decarboxylation | 4,54 | -1,37 | 22 |
10 | 107 | CC(C)(C)C(O)=O | 14 | 319 | Decarboxylation | 4,097 | 1,45 | 0 |
11 | 47 | CC(C)(CC(O)=O)CC(C)(CO)C(0)=O | 5 | 309 | Ester hydrolysis | 3,519 | 0,51 | 1 |
12 | 12 | CC1(C)CC(C)(CN)CC( =O) OC1 | 2 | 184 | Bayer-Villiger oxidation | 2,192 | 0,95 | 13 |
13 | 11 | CC1(C)CC(=O)OCC(C)(CN)C1 | 2 | 184 | Bayer-Villiger oxidation | 2,192 | 0,95 | 17 |
14 | 74 | CC/Cl/CC/Cl/CO)C/Ol=OlC/O)=O | 8 | 487 | Methvl arouo oxidation | 2,06 | 0,01 | 0 |
15 | 25 | CC1(C(O)=O)CC(N)CC(C)(CN)C1 | 3 | 66 | Aldehyde Oxidation | 1,751 | -2,54 | 18 |
16 | 38 | CC1(C)CC( C)(C(O)=O)CC( =O)OC1 | 4 | 184 | Bayer-Villiqer oxidation | 1,37 | 1,18 | 8 |
17 | 37 | CC1(C)CC(=O) OCC(C)(C(O)=O)C1 | 4 | 184 | Bayer-Villiqer oxidation | 1,37 | 1,18 | 5 |
18 | 73 | CC{CC{C){C)C)C{O)=O | 8 | 216 | Decarboxylation | 1,082 | 2,85 | 20 |
19 | 26 | CC1(C)CC(N)CC(CN)(C(O)=O)C1 | 3 | 66 | Aldehyde Oxidation | 0,8757 | -2,54 | 25 |
20 | 85 | CC(=CC(C)(C)C)C(0)=0 | 10 | 315 | Beta-oxidation | 0,8469 | 2,76 | 29 |
21 | 90 | CC(C(O)C(C)(C)C)C(O)=O | 11 | 310 | Beta-oxidation | 0,7361 | 1,31 | 27 |
22 | 102 | CC/C/=O)C/C)/C)C)C/O)=O | 13 | 71 | Keto-enol tautomerism | 0,6399 | 0,80 | 41 |
23 | 77 | CC(CC(O)=O)(CC(C)(CN)C(O)=O)C(O)=O | 8 | 66 | Aldehyde oxidation | 0,4864 | -3,94 | 36 |
24 | 60 | CC(CC(O)=O)(CC{C)(CO)C(O)=O)CN | 6 | 309 | Ester hydrolysis | 0,4158 | -4,17 | 8 |
25 | 76 | CC(CC(O)=O)(CC(C)(CO)C(O)=O)C(O)=O | 8 | 487 | Methyl group oxidation | 0,3756 | -0,73 | 0 |
26 | 112 | CC/=C/O)C/C)(O)CC(O)=O)C/O)=O | 16 | 315 | Beta-oxidation | 0,3542 | -1,00 | 89 |
27 | 70 | CC(C)(CC(C)(CO)C(O)=O)CN | 7 | 346 | Decarboxylation | 0,3304 | -2,83 | 7 |
28 | 105 | CC(C)(C)CCC(O)=O | 13 | 319 | Decarboxylation | 0,2703 | 2,43 | 32 |
29 | 104 | CC(CC(C)(O)CC(O)=O)C(O)=O | 13 | 216 | Decarboxylation | 0,2699 | -0,44 | 66 |
30 | 79 | CC(C)(CC(CC(O)=O)(CN)C(O)=O)C(O)=O | 8 | 66 | Aldehyde oxidation | 0,2432 | -3,94 | 25 |
31 | 61 | CC(C)(CC(O)=O)CC(CN)(CO)C(O)=O | 6 | 309 | Ester hydrolysis | 0,2079 | -4,17 | 31 |
32 | 106 | CC(C)(CC(=O)CC(O)=O)C(O)=O | 13 | 340 | Decarboxylation | 0,1833 | -0,95 | 28 |
33 | 71 | CC(C)(C)CC(CN)(CO)C(0)=0 | 7 | 346 | Decarboxylation | 0,1652 | -2,83 | 32 |
34 | 50 | CC1{CN)CC{=O)OCC{C){C{O)=O)C1 | 5 | 184 | Bayer-Villiaer oxidation | 0,1618 | -3,49 | 11 |
35 | 49 | CC1/C/Ol=OlCC/=OlOCC/Cl/CNlC1 | 5 | 184 | Baver-Villiaer oxidation | 0,1618 | -3,49 | 28 |
36 | 110 | CC/C)/CO)C/O)=O | 15 | 487 | Methvl arouo oxidation | 0,157 | -0,02 | 0 |
37 | 101 | CC(C)CC(CC(O)=O)C(O)=O | 12 | 216 | Decarboxylation | 0,135 | 1,06 | 72 |
38 | 9 | CC1(C)CC(N)C(=O )OC(C)(CN)C1 | 1 | 747 | Bayer-Villiger oxidation | 0,1068 | -0,60 | 17 |
39 | 8 | CC1 (C )CC( C)( CN)CC( N)C( =0)01 | 1 | 747 | Bayer-Villiger oxidation | 0,1068 | -0,60 | 14 |
40 | 44 | CC(C)(CC(=O)CC(C){O)C=O)C(O)=O | 4 | 357 | Oxidative deamination and N-dealkylation | 0,0988 | -1,21 | 34 |
41 | 41 | CC(C)(O)CC(=O)CC{C){C=O)C{0)=0 | 4 | 357 | Oxidative deamination and N-dealkylation | 0,0988 | -1,21 | 68 |
42 | 21 | CC(C)(CC(N)CC(C)(O)CN)C(O)=O | 2 | 309 | Ester hydrolvsis | 0,09499 | -3,89 | 23 |
43 | 18 | CC(C)(O)CC( N)CC(C)(CN)C(O)=O | 2 | 309 | Ester hydrolvsis | 0,09499 | -3,89 | 39 |
44 | 100 | CC(C)(CC(O)(CC(O)=O)C(O)=O)C(O)=O | 12 | 164 | Beta-oxidation | 0,08658 | -0,61 | 25 |
45 | 52 | CC1(C)CC{CN){C/O)=O)CC/=O)OC1 | 5 | 184 | Bayer-Villiaer oxidation | 0,08092 | -3,49 | 31 |
46 | 51 | CC1(C)CC(=O)OCC(CN)(C(O)=O)C1 | 5 | 184 | Bayer-Villiaer oxidation | 0,08092 | -3,49 | 29 |
47 | 86 | CC(CC(C)(CO)C(O)=O)(CO)C(O)=O | 10 | 487 | Methyl ciroup oxidation | 0,07865 | -1,04 | 0 |
48 | 91 | CC(CC(C)(CC(O)=O)C(O)=O)C(O)=O | 11 | 216 | Decarboxylation | 0,07059 | 0,28 | 34 |
49 | 64 | CC(C)(C)CC(C)(O)C=O | 6 | 357 | Oxidative deamination and N-dealkylation | 0,06711 | 1,09 | 25 |
50 | 63 | CC(C)(O)CC(C)(C)C=O | 6 | 357 | Oxidative deamination and N-dealkylation | 0,06711 | 1,09 | 8 |
51 | 109 | CC(=CC(C)(O)CC(O)=O)C(O)=O | 14 | 164 | Beta-oxidation | 0,0613 | -0,53 | 70 |
52 | 32 | CC( C)( CC(=O) CC(C)(0)CN)C( 0)=0 | 3 | 356 | Oxidative deamination and N-dealkylation | 0,05934 | -4,39 | 23 |
53 | 29 | CC( C)( O)CC( =O)CC(C)( CN)C( 0)=0 | 3 | 356 | Oxidative deamination and N-dealkylation | 0,05934 | -4,39 | 45 |
54 | 1 | CC1(C)CC(=O)CC(C)(CN)C1 | 1 | 762 | Oxidative deamination and N-dealkylation | 0,05626 | 1,40 | 28 |
55 | 111 | CC(C(O)C(C)(O)CC(O)=O)C(O)=O | 15 | 310 | Beta-oxidation | 0,05328 | -1,57 | 74 |
56 | 43 | CC(Cl{CC{O)=O)CC{Cl{O)CN | 4 | 123 | Decarboxvlation | 0,05073 | -2,83 | 20 |
57 | 42 | CC(C)(O)CC(C)(CC(O)=O)CN | 4 | 123 | Decarboxylation | 0,05073 | -2,83 | 12 |
58 | 54 | CC(C){C)CC(C)(O)CN | 5 | 346 | Decarboxylation | 0,04031 | 1,11 | 18 |
59 | 53 | CC(C)(O)CC(C)(C)CN | 5 | 346 | Decarboxylation | 0,04031 | 1,11 | 13 |
60 | 10 | CC1(C)CC(N)CC(C)(CN)OC1=O | 1 | 747 | Bayer-Villiger oxidation | 0,0316 | -0,60 | 25 |
61 | 7 | CC1(C)CC(N)CC(C)(CN)C(=0)01 | 1 | 747 | Bayer-Villiqer oxidation | 0,0316 | -0,60 | 44 |
62 | 6 | CC1 (C)CC( C)( CN)CC( N)OC1=O | 1 | 747 | Bayer-Villiqer oxidation | 0,0316 | 1,15 | 13 |
63 | 5 | CC1(C)CC(N)OC(=O)C(C)(CN)C1 | 1 | 747 | Bayer-Villiqer oxidation | 0,0316 | 1,15 | 24 |
64 | 20 | CC1(C)CC(=O)C(=O)OC(C)(CN)C1 | 2 | 356 | Oxidative deamination and N-dealkylation | 0,01975 | 0,93 | 24 |
65 | 19 | CC1(C)CC( C)(CN)CC(=O)C(=0)01 | 2 | 356 | Oxidative deamination and N-dealkylation | 0,01975 | 0,93 | 16 |
66 | 81 | CC(CC/CC/O)=O)/CO)C/O)=O)/CO)C/O)=O | 9 | 488 | Methvl arouo oxidation | 0,01467 | -1,49 | 0 |
67 | 80 | CC(CC(O)=O)(CC(CO)(CO)C(O)=O)C(O)=O | 9 | 488 | Methyl ciroup oxidation | 0,01467 | -1,79 | 0 |
68 | 99 | CC(C)(C)CC(C(O)=O)C(O)=O | 12 | 66 | Aldehyde oxidation | 0,004702 | 1,03 | 37 |
69 | 97 | CC(=CC(C)(CC(O)=O)C(O)=O)C(O)=O | 12 | 315 | Beta-oxidation | 0,0004693 | 0,20 | 62 |
70 | 2 | CC1(C)CC(N)CC(C)(C=O)C1 | 1 | 357 | Oxidative deamination and N-dealkylation | 0,000395 | 1,88 | 12 |
71 | 36 | CC/C)/CC/C)/CC/O)=O)CN)C=O | 4 | 93 | Primarv hvdroxvl arouo oxidation | 0,0001756 | -2,37 | 10 |
72 | 34 | CC/C)/CC/O)=OlCC/C)/CN)C=O | 4 | 93 | Primarv hvdroxvl arouo oxidation | 0,0001756 | -2,37 | 26 |
73 | 23 | CC(C)(CC(C)(CC( O)=O)CN)CO | 3 | 309 | Ester hydrolvsis | 0,0001756 | -2,34 | 10 |
74 | 22 | CC(C)(CC(O)=O)CC(C)(CN)CO | 3 | 309 | Ester hydrolvsis | 0,0001756 | -2,34 | 26 |
75 | 58 | CC/Cl/CC/C)/CC/Ol=O)C/O)=O)C=O | 6 | 93 | Primarv hvdroxvl arouo oxidation | 0,0001097 | 0,48 | 5 |
76 | 48 | CC(C)(CC(C)(CC(O)=O)C(O)=O)CO | 5 | 309 | Ester hydrolvsis | 0,0001097 | 0,51 | 5 |
77 | 56 | CC(C)(CC(C)(C)C=O)C(O)=O | 6 | 357 | Oxidative deamination and N-dealkylation | 0,00007558 | 1,81 | 5 |
78 | 55 | CC(C)(C)CC(C)(C=O)C(0)=0 | 6 | 357 | Oxidative deamination and N-dealkylation | 0,00007558 | 1,81 | 30 |
79 | 96 | CC/=C/O)C/C)/C)C)C/O)=O | 12 | 315 | Beta-oxidation | 0,00004894 | 1,88 | 41 |
80 | 14 | CC1/C=O)CC/N)CC/C)/CN)C1 | 2 | 93 | Primarv hvdroxvl arouo oxidation | 0,00004668 | 0,41 | 21 |
81 | 3 | CC1(C O)CC( N)CC(C)( CN)C1 | 1 | 487 | Methyl i:iroup oxidation | 0,00004668 | 0,44 | 21 |
82 | 108 | CCC/O)=O | 14 | 319 | Decarboxylation | 0,00004254 | 0,58 | 100 |
83 | 15 | CC1/C)CC/ N)CC/CN)/C=O)C1 | 2 | 93 | Primarv hvdroxvl arouo oxidation | 0,00002334 | 0,41 | 28 |
84 | 4 | CC1(C)CC(N)CC(CN)(CO)C1 | 1 | 488 | Methyl i:iroup oxidation | 0,00002334 | 0,44 | 28 |
85 | 75 | CC(C)(CC(C)(CO)C(O)=O)C=O | 8 | 357 | Oxidative deamination and N-dealkylation | 0,00001591 | 0,35 | 5 |
86 | 69 | CC(CC(O)=O){CC(C)(CN)C=O)C(O)=O | 7 | 93 | Primary hydroxvl arouo oxidation | 0,00001296 | -4,19 | 39 |
87 | 59 | CC{CC(O)=O)(CC(C){CN)CO)C(O)=O | 6 | 309 | Ester hydrolvsis | 0,00001296 | -4,17 | 39 |
88 | 67 | CC{Cl/CC/Cl/CO)C/O)=O)CO | 7 | 487 | Mettwl arouo oxidation | 0,00001041 | 0,78 | 5 |
89 | 82 | CC(CC(O)=O)(CC(C)(C=O)C(O)=O)C(O)=O | 9 | 357 | Oxidative deamination and N-dealkylation | 0,000008098 | -0,76 | 54 |
90 | 65 | CC{C){C)CC{C){C{O)=O)C{O)=O | 7 | 66 | Aldehyde oxidation | 0,000007558 | 1,48 | 27 |
91 | 72 | CC(C){CC{CC{O)=O){CN)C{O)=O)C=O | 7 | 93 | Primary hydroxvl ciroup oxidation | 0,000006481 | -4,19 | 29 |
92 | 62 | CC(C)(CC(CC(O)=O)(CN)C(O)=O)CO | 6 | 309 | Ester hydrolysis | 0,000006481 | -4,17 | 29 |
93 | 103 | CC(CC(O)=O)C=C/C)C/O)=O | 13 | 216 | Decarboxylation | 0,000004688 | 0,98 | 71 |
94 | 84 | CC(C)(CC(CC(O)=O)(C=O)C(O)=O)C(O)=O | 9 | 357 | Oxidative deamination and N-dealkylation | 0,000004049 | -0,76 | 37 |
95 | 93 | CC(C)(C)CC(C=O)C(0)=0 | 11 | 93 | Primary hydroxvl ciroup oxidation | 0,00000275 | 1,36 | 40 |
96 | 88 | CC(C)(C)CC(CO)C(O)=O | 10 | 216 | Decarboxylation | 0,00000275 | 1,38 | 40 |
97 | 78 | CC(C)(C)CC(CO)(C=O)C(0)=0 | 8 | 357 | Oxidative deamination and N-dealkylation | 0,00000275 | 0,35 | 44 |
98 | 94 | CC(C)(CC(CC(O)=O)C/O)=O)C(0)=0 | 11 | 216 | Decarboxylation | 0,000002699 | 0,28 | 29 |
99 | 92 | CC(CC(O)=O)CC(C)(C(O)=O)C(O)=O | 11 | 216 | Decarboxylation | 0,000002699 | 0,28 | 62 |
100 | 28 | CC(C)(CC(C)(CC=O)CN)C(O)=O | 3 | 37 | Oxidative deamination and N-dealkylation | 0,000002531 | -2,37 | 10 |
101 | 27 | CC(C)(CC=O)CC( C)(CN)C(0)=0 | 3 | 37 | Oxidative deamination and N-dealkylation | 0,000002531 | -2,37 | 26 |
102 | 17 | CC/C)/CC/C)/CC/N)O) CN)C/ 0)=0 | 2 | 309 | Ester hvdrolvsis | 0,000002531 | -3,89 | 10 |
103 | 16 | CC/C)/CC/N)O)CC/C)/CN)C/O)=O | 2 | 309 | Ester hvdrolvsis | 0,000002531 | -3,89 | 26 |
104 | 31 | CC( C)( CC(=O) C(O)=O)CC( C)( O)CN | 3 | 309 | Ester hydrolysis | 0,000001581 | -0,96 | 24 |
105 | 30 | CC( C)( O)CC( C)( CC(=O)C(O)=O)CN | 3 | 309 | Ester hydrolysis | 0,000001581 | -0,96 | 16 |
106 | 83 | CC(C)(C)CC(CO)(C(O)=O)C(0)=0 | 9 | 66 | Aldehyde oxidation | 0,000000275 | 0,01 | 42 |
107 | 98 | CC(0)(CC(0)=O)CC(C)(C(0)=O)C(O)=O | 12 | 164 | Beta-oxidation | 2,699E-07 | -1,22 | 60 |
108 | 95 | CC(C)CC(CC(O)=O)(C(O)=O)C(O)=O | 11 | 216 | Decarboxylation | 0,000000135 | 0,28 | 56 |
109 | 24 | CC1(C)CC(=O)CC( C)(C(O)=O)C1 | 3 | 356 | Oxidative deamination and N-dealkylation | 2,5E-09 | 1,63 | 10 |
110 | 87 | CC/CC/O)=O)/CC/C\/C/O\=O)C/O)=O)C/O)=O | 10 | 66 | Aldehvde Oxidation | 8E-10 | -0,50 | 51 |
111 | 89 | CC(C)(CC(CC(O)=O)(C(O)=O)C(O)=O)C(O)=O | 10 | 66 | Aldehyde oxidation | 4E-10 | -0,50 | 34 |
112 | 39 | CC1(C(O)=O)CC(=O)CC(C)(CN)C1 | 4 | 356 | Oxidative deamination and N-dealkylation | 3E-10 | -3,04 | 22 |
113 | 40 | CC1(C)CC(=O)CC(CN)(C(O)=O)C1 | 4 | 356 | Oxidative deamination and N-dealkylation | 1E-10 | -3,04 | 33 |
Conclusion:
Overall predicted metabolites: 112 metabolits
40 metabolites: quantity > 0.1%; thereof: 4 RBD and 40 log Kow <3.
All relevant predicted metabolites are neither PBT nor vP/vB
T: not assessed as no critical combination nRBD (~P/vP) plus log Kow >3 (~B/vB)
Description of key information
A simulation study according to OECD 303A revealed a biodegradation of 42% after 31 days in laboratory WWTP. No data are available on degradation rates in soil; therefore, the substance is regarded as P/vP from a precautionary point of view.
Degradation products were predicted using a QSAR model. 4 of 40 relevant degradation products are readily biodegradable.
Key value for chemical safety assessment
Additional information
QSAR-disclaimer:
In Article 13 of Regulation (EC) No 1907/2006, it is laid down that information on intrinsic properties of substances may be generated by means other than tests, provided that the conditions set out in Annex XI (of the same Regulation) are met.
According to Annex XI of Regulation (EC) No 1907/2006 (Q)SAR results can be used if (1) the scientific validity of the (Q)SAR model has been established, (2) the substance falls within the applicability domain of the (Q)SAR model, (3) the results are adequate for the purpose of classification and labelling and/or risk assessment and (4) adequate and reliable documentation of the applied method is provided.
For the assessment of the substance, (Q)SAR results were used for the prediction of potential degradation products. The criteria listed in Annex XI of Regulation (EC) No 1907/2006 are considered to be adequately fulfilled and therefore the endpoint(s) sufficiently covered and suitable for risk assessment.
Therefore, experimental simulation testing in soil is not provided.
Assessment:
A simulation study according to OECD 303A revealed a biodegradation of 42% after 31 days in laboratory WWTP.
According to REACH Annex IX, 9.2.1.3, column 1, a test on biodegradation in soil is only required for substances with a high potential for adsorption to soil. Since the test substance has a calculated log Koc of 2.97 at pH7 it is expected to have a low potential for adsorption to soil and sediment. According to a Mackay Level I model calculation, the main target compartment for isophorone diamine will be the hydrosphere (99.8 %), followed by sediment and soil with a percentage of just 0.08 % each. Therefore, no biodegradation test in soil is required.
The degradation products of IPDA are predicted via QSAR modelling of degradability and bioaccumulation for the PBT/vPvB assessment. None of the relevant degradation products has a high potential for adsorption to soil considering the calculated logKow.
Moreover, in accordance with Annex XI Section 3 and Annex IX 9.2.1.3, column 2, it is demonstrated in the risk assessment that the manufacture and all uses of the lifecycle of the substance do not pose an unacceptable risk for environmental compartments. In the chemical safety report operational conditions (OC) and risk mitigating measures (RMM) define how direct or indirect exposure into the environment is prevented and it is demonstrated that the risk characterization ratios (RCRs) of the chemical safety assessment are below 1 for all compartments (see Chemical Safety Report).
The degradation products of IPDA are predicted via QSAR modelling of degradability and bioaccumulation for the PBT/vPvB assessment. None of the relevant degradation products has a high potential for adsorption to soil considering the calculated logKow.
Moreover, in accordance with Annex XI Section 3 and Annex IX 9.2.1.4, column 2, it is demonstrated in the risk assessment that the manufacture and all uses of the lifecycle of the substance do not pose an unacceptable risk for environmental compartments. In the chemical safety report operational conditions (OC) and risk mitigating measures (RMM) define how direct or indirect exposure into the environment is prevented and it is demonstrated that the risk characterization ratios (RCRs) of the chemical safety assessment are below 1 for all compartments (see Chemical Safety Report).
For the persistence assessment, the substance itself is assessed to be P/vP from a precautionary point of view. Potentially forming degradation products have been predicted using a valid QSAR model (CATALOGIC 301 C v .09.13). The substance is within the applicability domain of the model. The model predicted 112 degradation products, of which 40 can be regarded as relevant based on their predicted quantity (see the corresponded endpoint study record). These relevant degradation products were evaluated with regard to their biodegradability and bioaccumulation potential based on QSAR data. 4 substances were readily biodegradable. Significant accumulation is not to be expected for all relevant biodegradation products as their logKow <3. Thus, they are neither PBT, nor vPvB.
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.
