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REACH

α-methyl-1H-imidazole-1-ethanol

EC number: 253-668-2 | CAS number: 37788-55-9

Life Cycle description
Uses advised against

Toxicological information

Endpoint summary

Administrative data

Key value for chemical safety assessment

Genetic toxicity in vitro

Description of key information

A study according to OECD 471 (Ames-test) was conducted. No significant increase of the number of revertant colonies in the treatments with and with-out metabolic activation could be observed. No concentration-related increase over the tested range was found. Therefore, the test item is stated as not mutagenic under the test conditions.

Link to relevant study records

Reference

Endpoint:: in vitro gene mutation study in bacteria
Type of information:: experimental study
Adequacy of study:: key study
Study period:: August 09, 2017 - August 17, 2017
Reliability:: 1 (reliable without restriction)
Qualifier:: according to guideline
Guideline:: OECD Guideline 471 (Bacterial Reverse Mutation Assay)
Qualifier:: according to guideline
Guideline:: EU Method B.13/14 (Mutagenicity - Reverse Mutation Test Using Bacteria)
GLP compliance:: yes (incl. QA statement)
Type of assay:: bacterial reverse mutation assay
Species / strain / cell type:: S. typhimurium TA 97
Species / strain / cell type:: S. typhimurium TA 98
Species / strain / cell type:: S. typhimurium TA 100
Species / strain / cell type:: S. typhimurium TA 102
Species / strain / cell type:: S. typhimurium TA 1535
Metabolic activation:: with and without
Test concentrations with justification for top dose:: In the first experiment, the test item (dissolved in DMSO) was tested up to concentrations of 5 µL/plate in the absence and presence of S9-mix in the strains TA97a, TA98, TA100, TA102 and TA1535 using the plate incorporation method. Based on the first experiment, the test item was tested up to concentrations of 5 μL/plate in the absence and presence of S9-mix in all bacteria strains using the pre-incubation method.
Vehicle / solvent:: solvent used: DMSO
Untreated negative controls:: yes
Remarks:: water and DMSO
Negative solvent / vehicle controls:: yes
Remarks:: water and DMSO
True negative controls:: yes
Remarks:: water and DMSO
Positive controls:: yes
Positive control substance:: sodium azide; benzo(a)pyrene; other: 4-Nitro-1,2-phenylene diamine; 2-Amino-anthracene
Details on test system and experimental conditions:: All Salmonella typhimurium strains were obtained from TRINOVA BioChem GmbH (batch: TA97a: 4997D, TA98: 5011D, TA100: 4996D, TA102: 4982D, TA1535: 5012D) and were stored as lyophilizates in the refrigerator at 2-8 °C.
The lyophilizates were used to prepare permanent cultures which were filled into vials and stored at < - 75 °C.
Evaluation criteria:: A substance is considered to have mutagenic potential, if a reproducible increase of re-vertant colonies per plate exceeding an increase factor of 2 in at least one strain can be observed. A concentration-related increase over the range tested is also taken as a sign of mutagenic activity.
: Key result
Species / strain:: S. typhimurium TA 97
Metabolic activation:: with and without
Genotoxicity:: negative
Cytotoxicity / choice of top concentrations:: not specified
Vehicle controls validity:: valid
Untreated negative controls validity:: valid
Positive controls validity:: valid
: Key result
Species / strain:: S. typhimurium TA 98
Metabolic activation:: with and without
Genotoxicity:: negative
Cytotoxicity / choice of top concentrations:: not specified
Vehicle controls validity:: valid
Untreated negative controls validity:: valid
Positive controls validity:: valid
: Key result
Species / strain:: S. typhimurium TA 100
Metabolic activation:: with and without
Genotoxicity:: negative
Cytotoxicity / choice of top concentrations:: not specified
Vehicle controls validity:: valid
Untreated negative controls validity:: valid
Positive controls validity:: valid
: Key result
Species / strain:: S. typhimurium TA 102
Metabolic activation:: with and without
Genotoxicity:: negative
Cytotoxicity / choice of top concentrations:: not specified
Vehicle controls validity:: valid
Untreated negative controls validity:: valid
Positive controls validity:: valid
: Key result
Species / strain:: S. typhimurium TA 1535
Metabolic activation:: with and without
Genotoxicity:: negative
Cytotoxicity / choice of top concentrations:: not specified
Vehicle controls validity:: valid
Untreated negative controls validity:: valid
Positive controls validity:: valid
Additional information on results:: Two test were conducted using the plate incorporation method in the first test and the pre-incubation method in the second test. In both test the maximum doese tested was 5 µL/plate for all strains. Nearly all determined values for the spontaneous revertants of the negative controls were in the normal range of the test laboratory. All positive controls (diagnostic mutagens) showed mu-tagenic effects with and without metabolic activation and nearly all were within the histori-cal control data ranges.
Conclusions:: No significant increase of the number of revertant colonies in the treatments with and with-out metabolic activation could be observed. No concentration-related increase over the tested range was found. Based on the results of this study it is concluded that N-(2-hydroxypropyl)imidazole is not mutagenic in the Salmonella typhimurium strains TA97a, TA98, TA100, TA102 and TA1535 in the absence and presence of metabolic activation under the experimental conditions in this study.

Endpoint conclusion

Endpoint conclusion:: no adverse effect observed (negative)

Additional information

Justification for classification or non-classification

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.

Strain		TA97a	TA100	TA98	TA98	TA100	TA100	TA102	TA102	TA1535	TA1535
Induction		-S9	+S9	-S9	+S9	-S9	+S9	-S9	+S9	-S9	+S9
Demin. water	Mean	83	69	52	50	82	102	356	345	24	22
	sd	6.7	5.0	5.2	10.7	20.6	18.5	62.9	72.6	8.0	7.5
DMSO	Mean	85	78	43	39	110	101	257	324	21	21
	sd	5.6	13.6	5.5	11.9	6.0	21.2	26.6	20.8	0.6	5.3
Positive Controls*	Mean	343	657	560	487	404	1001	689	1083	265	132
	sd	35.9	24.1	146.0	123.3	17.4	0.0	60.2	400.0	59.5	15.2
	f(I)	4.04	8.42	13.02	12.49	4.93	9.91	2.68	3.34	11.04	6.29
5 μL/plate	Mean	83	83	40	40	84	115	411	425	23	24
	sd	15.3	2.0	10.1	13.2	2.0	28.7	44.1	62.0	2.6	1.2
	f(I)	0.98	1.06	0.93	1.03	0.76	1.14	1.60	1.31	1.10	1.14
1.5 μL/plate	Mean	84	76	51	34	94	130	343	417	25	24
	sd	7.6	14.5	3.0	0.6	14.0	15.0	23.4	26.6	4.7	4.0
	f(I)	0.99	0.97	1.19	0.87	0.85	1.29	1.33	1.29	1.19	1.14
0.5 μL/plate	Mean	62	77	34	38	119	122	361	313	19	19
	sd	8.6	10.1	5.3	4.5	5.8	3.5	81.2	35.9	1.0	3.6
	f(I)	0.73	0.99	0.79	0.97	1.08	1.21	1.40	0.97	0.90	0.90
0.15 μL/plate	Mean	79	82	37	43	108	117	303	285	21	24
	sd	23.1	11.0	2.5	4.5	30.0	19.6	53.3	36.1	2.0	0.6
	f(I)	0.93	1.05	0.86	1.10	0.98	1.16	1.18	0.88	1.00	1.14
0.5 μL/plate	Mean	88	94	50	38	112	126	331	327	20	21
	sd	6.1	22.0	2.5	1.2	36.2	3.5	89.9	56.6	1.0	3.5
	f(I)	1.04	1.21	1.16	0.97	1.02	1.25	1.29	1.01	0.95	1.00

Strain		TA97a	TA97a	TA98	TA98	TA100	TA100	TA102	TA102	TA1535	TA1535
Induction		-S9	+S9	-S9	+S9	-S9	+S9	-S9	+S9	-S9	+S9
Demin. water	Mean	80	117	38	37	97	101	292	303	16	17
	sd	16.9	6.1	3.5	8.9	23.5	21.9	40.6	66.5	3.5	8.9
DMSO	Mean	93	123	45	40	95	93	311	337	15	20
sd		12.2	3.1	9.3	7.0	26.0	18.1	19.7	73.8	4.7	8.3
Positive Controls*	Mean	656	607	477	421	413	531	1301	684	331	92
	sd	228.7	70.5	80.1	12.2	44.1	163.2	112.1	4.0	76.4	14.4
	f(I)	7.05	4.93	10.60	10.53	4.26	5.71	4.18	2.03	20.69	4.60
5 μL/plate	Mean	105	115	30	35	108	122	323	277	22	20
	sd	11.5	6.1	8.7	2.5	15.1	4.0	54.3	46.7	3.2	4.9
	f(I)	1.13	0.93	0.67	0.88	1.14	1.31	1.04	0.82	1.47	1.00
2.5 μL/plate	Mean	145	117	36	36	95	99	317	356	22	18
	sd	34.5	26.6	2.6	4.0	9.5	16.2	23.1	86.5	2.9	1.5
	f(I)	1.56	0.95	0.80	0.90	1.00	1.06	1.02	1.06	1.47	0.90
1.25 μL/plate	Mean	144	126	35	30	98	84	248	311	19	22
	sd	20.0	7.2	9.2	11.5	15.6	3.5	28.0	46.7	4.5	3.2
	f(I)	1.55	1.02	0.78	0.75	1.03	0.90	0.80	0.92	1.27	1.10
0.63 μL/plate	Mean	111	96	41	36	91	96	263	287	18	21
	sd	2.6	20.9	6.7	11.2	14.5	15.9	37.2	36.3	3.5	3.6
	f(I)	1.19	0.78	0.91	0.90	0.96	1.03	0.85	0.85	1.20	1.05
0.31 μL/plate	Mean	88	114	33	36	85	103	275	265	15	21
	sd	7.8	20.2	5.7	11.6	3.1	14.2	86.2	89.6	4.5	3.0
	f(I)	0.95	0.93	0.73	0.90	0.89	1.11	0.88	0.79	1.00	1.05
0.16 μL/plate	Mean	96	76	30	28	80	102	311	261	20	15
	sd	10.0	11.1	3.8	4.7	1.2	12.8	61.1	28.1	2.3	2.3
	f(I)	1.03	0.62	0.67	0.70	0.84	1.10	1.00	0.77	1.33	0.75