1,3-dimethylimidazolidin-2-one

• General information
• Classification & Labelling & PBT assessment
• Manufacture, use & exposure
• Physical & Chemical properties
• Environmental fate & pathways
• Ecotoxicological information
• Toxicological information
• Analytical methods
• Guidance on safe use
• Assessment reports
• Reference substances

• Substance Identity
• Administrative Information

• GHS
• DSD - DPD
• PBT assessment

• Life Cycle description
  • No identified uses
  • Manufacture
  • Formulation
  • Uses at industrial sites
  • Uses by professional workers
  • Consumer Uses
  • Article service life
• Uses advised against
  • Formulation
  • Uses at industrial sites
  • Uses by professional workers
  • Consumer Uses

• 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
  • Nanomaterial porosity
  • Nanomaterial pour density
  • Nanomaterial photocatalytic activity
  • Nanomaterial radical formation potential
  • Nanomaterial catalytic activity

• Endpoint summary
• Stability
  • Endpoint summary
  • Phototransformation in air
  • Hydrolysis
  • Phototransformation in water
  • Phototransformation in soil
• Biodegradation
  • Endpoint summary
  • Biodegradation in water: screening tests
  • Biodegradation in water and sediment: simulation tests
  • Biodegradation in soil
  • Mode of degradation in actual use
• Bioaccumulation
  • Endpoint summary
  • Bioaccumulation: aquatic / sediment
  • Bioaccumulation: terrestrial
• Transport and distribution
  • Endpoint summary
  • Adsorption / desorption
  • Henry's Law constant
  • Distribution modelling
  • Other distribution data
• Environmental data
  • Endpoint summary
  • Monitoring data
  • Field studies
• 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
  • Endpoint summary
  • Toxicity to soil macroorganisms except arthropods
  • Toxicity to terrestrial arthropods
  • Toxicity to terrestrial plants
  • Toxicity to soil microorganisms
  • Toxicity to birds
  • Toxicity to other above-ground organisms
• Biological effects monitoring
• Biotransformation and kinetics
• Additional ecotoxological information

• Toxicological Summary
• Toxicokinetics, metabolism and distribution
  • Endpoint summary
  • Basic toxicokinetics
  • Dermal absorption
• Acute Toxicity
  • Endpoint summary
  • Acute Toxicity: oral
  • Acute Toxicity: inhalation
  • Acute Toxicity: dermal
  • Acute Toxicity: other routes
• Irritation / corrosion
  • Endpoint summary
  • Skin irritation / corrosion
  • Eye irritation
• Sensitisation
  • Endpoint summary
  • Skin sensitisation
  • Respiratory sensitisation
• Repeated dose toxicity
  • Endpoint summary
  • Repeated dose toxicity: oral
  • Repeated dose toxicity: inhalation
  • Repeated dose toxicity: dermal
  • Repeated dose toxicity: other routes
• Genetic toxicity
  • Endpoint summary
  • Genetic toxicity: in vitro
  • Genetic toxicity: in vivo
• Carcinogenicity
• Toxicity to reproduction
  • Endpoint summary
  • Toxicity to reproduction
  • Developmental toxicity / teratogenicity
  • Toxicity to reproduction: other studies
• Specific investigations
  • Neurotoxicity
  • Immunotoxicity
  • Endocrine disrupter mammalian screening – in vivo (level 3)
  • Specific investigations: other studies
  • Phototoxicity in vitro
• Exposure related observations in humans
  • Endpoint summary
  • Health surveillance data
  • Epidemiological data
  • Direct observations: clinical cases, poisoning incidents and other
  • Sensitisation data (human)
  • Exposure related observations in humans: other data
• Toxic effects on livestock and pets
• Additional toxicological data

Toxicological information

Endpoint summary

• Administrative data
• Description of key information
• Key value for chemical safety assessment
• Additional information
• Justification for classification or non-classification

Administrative data

Description of key information

Acute oral toxicity:   deaths occurred in rats at 2000 mg/kg bodyweight with no deaths seen at 300 mg/kg bodyweight.

Acute inhaled toxicity:  no data available.

Acute dermal toxicity:  no deaths seen in rats exposed at 2000 mg/kg

Key value for chemical safety assessment

Acute toxicity: via oral route

Link to relevant study records

Referenceopen allclose all

Reference 1

Endpoint:

acute toxicity: oral

Type of information:

experimental study

Adequacy of study:

disregarded due to major methodological deficiencies

Study period:

1988

Reliability:

4 (not assignable)

Rationale for reliability incl. deficiencies:

other: The study contains no details on test substance source, purity, composition, batch number or storage conditions. Although test results are reported there are significant deficiencies in experimental details such as the dose levels used.

Qualifier:

no guideline followed

Principles of method if other than guideline:

Sample given by gavage to Sprague-Dawley rats with observations for 14 days.

GLP compliance:

no

Species:

rat

Strain:

Sprague-Dawley

Sex:

male/female

Details on test animals or test system and environmental conditions:

200-300g

Route of administration:

oral: gavage

Vehicle:

unchanged (no vehicle)

Details on oral exposure:

Gavage

Doses:

3-5 doses unspecified concentration

No. of animals per sex per dose:

5/sex/each

Control animals:

not specified

Details on study design:

14 day observation period

Sex:

male

Dose descriptor:

LD50

Effect level:

1.01 - 1.39 mL/kg bw

Sex:

female

Dose descriptor:

LD50

Effect level:

0.89 - 1.69 mL/kg bw

Mortality:

lowest lethal dose = 1.00 ml/kg
death at 1-6 days

Clinical signs:

other: lethargy, kyphosis, piloerection, ptosis, red discharge(ocular, nasal), tremors, diarrhoea, emaciation and prostration;

Gross pathology:

red lungs, red stomachs, discoloured kidneys, slight testicular atrophy in 2 rats

LD50 1.23 (0.89 -1.69)

Reference 2

Endpoint:

acute toxicity: oral

Type of information:

experimental study

Adequacy of study:

key study

Reliability:

1 (reliable without restriction)

Rationale for reliability incl. deficiencies:

other: GLP study carried out in compliance with an internationally recognised guideline

Qualifier:

according to guideline

Guideline:

OECD Guideline 423 (Acute Oral toxicity - Acute Toxic Class Method)

Qualifier:

according to guideline

Guideline:

EU Method B.1 tris (Acute Oral Toxicity - Acute Toxic Class Method)

Qualifier:

according to guideline

Guideline:

EPA OPPTS 870.1100 (Acute Oral Toxicity)

Qualifier:

according to guideline

Guideline:

other: Japanese Ministry of Agriculture, Forestry and Fisheries, Test Data for Registration of Agricultural Chemicals, Acute oral toxicity (2-1-1), 12 Nousan No 8147, Agricultural Production Bureau, November 24, 2000.

GLP compliance:

yes (incl. QA statement)

Test type:

acute toxic class method

Limit test:

no

Species:

rat

Strain:

other: Crl:CD (SD) albino

Sex:

female

Details on test animals or test system and environmental conditions:

TEST ANIMALS
- Source: reputable supplier
- Age at study initiation: 8 to 12 weeks
- Weight at study initiation: 224 to 262 g
- Fasting period before study: no
- Housing: solid bottomed polycarbonate cages with a stainless steel mesh lid. Each cage contained a quantity of autoclaved softwood bark-free fibre bedding.
- Diet (e.g. ad libitum): free access to a standard rodent diet
- Water (e.g. ad libitum): Potable water taken from the public supply was freely available via polycarbonate bottles fitted with sipper tubes
- Acclimation period: no

ENVIRONMENTAL CONDITIONS
- Temperature (°C): 19 to 23C
- Humidity (%): 40 to 70%
- Air changes (per hr): not reported
- Photoperiod (hrs dark / hrs light): Artificial lighting was controlled to give a cycle of 12 hours continuous light and 12 hours continuous dark per 24 hours.

IN-LIFE DATES: From: To: 7 February to 7 March 2013

Route of administration:

oral: gavage

Vehicle:

water

Details on oral exposure:

VEHICLE
- Concentration in vehicle: 30 and 200 mg/mL
- Amount of vehicle (if gavage): 10ml
- Justification for choice of vehicle: solubility

MAXIMUM DOSE VOLUME APPLIED: 10mL

CLASS METHOD (if applicable)
- Rationale for the selection of the starting dose: the dose levels for the study were chosen in compliance with the study guidelines. As no reliable previous toxicological information was available the initial dose level was 300 mg/kg.

Doses:

300 mg/kg and 2000mg/kg

No. of animals per sex per dose:

3

Control animals:

no

Details on study design:

- Duration of observation period following administration: 14 days
- Frequency of observations and weighing: clinical - twice daily; bodyweight - Days 1, 8, and 15
- Necropsy of survivors performed: yes


There were no deviations from protocol.

Sex:

female

Dose descriptor:

LD50

Effect level:

300 - 2 000 mg/kg bw

Based on:

test mat.

Mortality:

2000 mg/kg one animal on Day 3 and one on Day 4. The test was terminated on Day 4 for the remaining animal on humane grounds.

Clinical signs:

other: There were no clinical signs of reaction to treatment seen in any animal dosed at 300 mg/kg throughout the study. Prior to death - underactivity, hunched posture, tremors, partially closed eyelids and irregular breathing, vocalising in two animals, unste

Gross pathology:

Macroscopic examination of the decedents revealed congestion (characterised by darkened tissues/organs) of the subcutaneous tissue, heart and lungs, small (atrophy) spleen, stomach and caecum, pallor of kidneys and live, enlarge swollen stomach, gaseous distension of the caecum, brown yellow fluid content of the stomach, duodenum, small and large intestines, pale areas on the liver and kidneys.

At the macroscopic examination at study termination on Day 15 pallor and dark patches were seen on the lungs in one female dosed at 300 mg/kg, no abnormalities were noted in any of the remaining animals receiving 300 mg/kg.

Other findings:

- Other observations: a loss in bodyweight was noted for all decedents.

Interpretation of results:

other: Classified as Category 4 according to EU criteria.

Conclusions:

The acute median lethal oral dose (LD50) to rats of DMI was demonstrated to be between 300 and 2000 mg/kg bodyweight.

Endpoint conclusion

Endpoint conclusion:

adverse effect observed

Dose descriptor:

LD50

Value:

500 mg/kg bw

Quality of whole database:

Two available studies, one disregarded the other a well conducted study performed under GLP in accordance with a recognised guideline.

Acute toxicity: via inhalation route

Endpoint conclusion

Endpoint conclusion:

no study available

Quality of whole database:

One disregarded study.

Acute toxicity: via dermal route

Link to relevant study records

Reference

Endpoint:

acute toxicity: dermal

Type of information:

experimental study

Adequacy of study:

key study

Study period:

13 January 2005 - 28 April 2005

Reliability:

1 (reliable without restriction)

Rationale for reliability incl. deficiencies:

other: GLP compliant study conducted in accordance with international guidelines.

Qualifier:

according to guideline

Guideline:

OECD Guideline 434 (Acute Dermal Toxicity - Fixed Dose Procedure)

Deviations:

no

GLP compliance:

yes

Test type:

fixed dose procedure

Species:

rabbit

Strain:

not specified

Sex:

male

Details on test animals or test system and environmental conditions:

TEST ANIMALS
- Age at study initiation: 9 weeks (at the time of start of quarantine acclimation)
- Weight at study initiation: 1.79 – 2.21 kg (at the time of grouping)
- Housing: Stainless steel or aluminium cages. 1 rabbit/cage
- Diet (e.g. ad libitum): Solid fodder (CR-1, Lot No. R1024, available from CLEA Japan, Inc.) Approx. 120 g were given once a day.
- Water (e.g. ad libitum): The rabbits were allowed to freely drink the water conforming to the water standards under the water supply law through an automatic water supply device (available from Edstrom Industries, Inc.)
- Acclimation: Yes


ENVIRONMENTAL CONDITIONS
- Temperature (°C): Actual measurement values: 20.6 – 22.5°C; allowable range: 19 - 25°C
- Humidity (%): Actual measurement values: 43 – 77%; allowable range: 30 – 70%
- Air changes (per hr): 15
- Photoperiod (hrs dark / hrs light): 12 hours/day artificial lighting (06:00 – 19:00 lamp-lighting)

Type of coverage:

occlusive

Vehicle:

unchanged (no vehicle)

Details on dermal exposure:

TEST SITE
- Area of exposure: back area 12 cm x 14 cm
- Type of wrap if used: The applied area was covered with paraffin film and gauze and fixed with non-irritating tape and bandage

REMOVAL OF TEST SUBSTANCE
- Washing (if done): After the application, the applied area was wiped with gauze dipped in slightly warm water
- Time after start of exposure: 24 hours

Duration of exposure:

24 hours

Doses:

1000 and 2000mg/kg

No. of animals per sex per dose:

5

Control animals:

no

Details on study design:

- Frequency of observations and weighing: On the day of administration, 10 times a day (once before administration, once immediately after administration, once every 15 or 30 minutes after administration); 1 to 13 days after administration, twice a day; once on the day of autopsy (for Group 2, once a day from the day following the day of grouping to the day preceding the administration, in addition to the above times of administration)
- Necropsy of survivors performed: yes
- Other examinations performed: bodyweight, organ weights, other: the external surface, internal organs and tissues were visually observed.
Organs removed: Liver, kidneys (right and left) and administered section (skin of the back)

Statistics:

No statistical verification was carried out in this test.

Dose descriptor:

LD50

Effect level:

> 2 000 other: mg/kg

Based on:

test mat.

Mortality:

During the observation period, there was no death observed.

Clinical signs:

other: No abnormal signs were observed on the day of administration. Day after administration a decrease in stool volume at 1000 and 2000 mg/kg and decreased appetite at 2000mg/kg were observed.

Gross pathology:

In autopsy, no abnormality was observed in any of the animals of any group.

In the group to which a dose of 2000 mg/kg was given, the rabbits began to show a decline in appetite and a fall in the amount of feces after one day from the administration and continued to fall in body weight until after two days from the administration. A decline in appetite and a fall in the amount of feces continued up to four days from the administration in 4 animals (in one animal, a fall in the amount of feces alone was observed two days from the administration.)

No abnormality was observed after five days from the administration to the final day of observation.

In the group to which a dose of 1000 mg/kg was given, one animal showed a decline in appetite after one day from the administration, and two animals showed a decline in appetite and a fall in the amount of feces two days after the administration. With regard to the body weight, the body weight value decreased one day after the administration, compared with the before-test value,

and there was no abnormality after three days from the administration to the final day of observation.

Interpretation of results:

Category 5 based on GHS criteria

Conclusions:

On the basis of the results described above, it was judged under the conditions of the test that the single dermal DMI dose LD50 for rabbits was a dose higher than 2000 mg/kg.
Furthermore, the test substance was classified under “Category-5/Unclassified” according to the classification of acute toxicity under the Globally Harmonized System of Classification and Labelling of Chemicals.

Endpoint conclusion

Endpoint conclusion:

adverse effect observed

Dose descriptor:

LD50

Value:

2 000 mg/kg bw

Additional information

Acute oral toxicity

An acute toxicity test was performed to determine the acute toxicity by oral exposure to DMI. The study was conducted in accordance with a relevant test guideline and in compliance with GLP.

Two groups of three fasted female rats received a single oral gavage dose of the test substance, formulated in purified water, at a dose level of 300 mg/kg bodyweight. As results at this dose level indicated the acute (median) lethal oral dose of the test substance to be greater than 300 mg/kg bodyweight, in compliance with the study guidelines a further group of three fasted females were similarly dosed at 2000 mg/kg bodyweight to complete the study. At 2000 mg/kg one animal died on Day 3 and one on Day 4. The test was terminated on Day 4 for the remaining animal on humane grounds. There were no deaths and no clinical signs of reaction to treatment in any animal dosed at 300 mg/kg throughout the study. Clinical signs prior to death comprised underactivity, hunched posture, tremors, partially closed eyelids and irregular breathing seen in two females, vocalising, unsteady gait, increased body tone, reduced body temperature, loose faeces, fast breathing and thin build noted in one female and salivation, piloerection and red coloured urine seen in one female. All of these signs (except for salivation which was seen after dosing on Day 1) were seen from Day 3. No signs were observed for the female which was found dead on Day 3. At the macroscopic examination at study termination on Day 15 pallor and dark patches were seen on the lungs in one female dosed at 300 mg/kg, no abnormalities were noted in any of the remaining animals receiving 300 mg/kg.

The acute median lethal oral dose (LD50) to rats of DMI was demonstrated to be between 300 and 2000 mg/kg bodyweight.

Acute inhalation toxicity

No data available

Acute dermal toxicity

Doses of DMI of 2000 and 1000 mg/kg were given to each of five groups of rabbits at a single time. During the observation period, there was no death in any of the groups to which doses of 2000 or 1000 mg/kg were given. In the group to which a dose of 2000 mg/kg was given, the rabbits began to show a decline in appetite and a fall in the amount of feces after one day from the administration and continued to fall in body weight until after two days from the administration. A decline in appetite and a fall in the amount of feces continued up to four days from the administration in 4 animals (in one animal, a fall in the amount of feces alone was observed two days from the administration.) No abnormality was observed after five days from the administration to the final day of observation. In the group to which a dose of 1000 mg/kg was given, one animal showed a decline in appetite after one day from the administration, and two animals showed a decline in appetite and a fall in the amount of feces two days after the administration. With regard to the body weight, the body weight value decreased one day after the administration, compared with the before-test value, and there was no abnormality after three days from the administration to the final day of observation. No abnormality was observed in any of the animals of any group.

On the basis of the results described, it was judged under the conditions of the test that the single dermal DMI dose LD50 for rabbits was a dose higher than 2000 mg/kg.

 

Justification for selection of acute toxicity – oral endpoint

One valid study available.

Justification for selection of acute toxicity – dermal endpoint

Two available studies, one disregarded the other a well conducted study performed under GLP in accordance with a recognised guideline.

Justification for classification or non-classification

The acute toxicity results for DMI were reviewed with reference to the EU interpretation of CLP, EU Regulation 1272/2008. On the basis that the available tests confirmed the oral LD50 value to be greater than 300 mg/kg but less than 2000 mg/kg, and the dermal LD50 value to be greater than 2000 mg/kg bodyweight, DMI is classified as category 4 for oral exposure but does not require classification as toxic by dermal exposure.