tert-butyl 2-ethylperoxyhexanoate

Administrative data

Description of key information

The test item was tested for skin sensitization to guinea pig in an in vivo Buehler test. Due to the irritation noted in both the test and challenge control animals, challenge with tert.-Butylperoxy- 2-ethylhexanoat was considered ambiguous. Following rechallenge with 2% tert.-Butylperoxy- 2-ethylhexanoat, slight evidence of sensitization was observed and tert.-Butylperoxy- 2-ethylhexanoat considered to be a possible weak sensitiser.

Key value for chemical safety assessment

Skin sensitisation

Link to relevant study records

Reference

Endpoint:

skin sensitisation: in vivo (non-LLNA)

Type of information:

experimental study

Adequacy of study:

key study

Study period:

1995-10-05 to 1996-01-23

Reliability:

2 (reliable with restrictions)

Rationale for reliability incl. deficiencies:

test procedure in accordance with national standard methods with acceptable restrictions

Qualifier:

equivalent or similar to guideline

Guideline:

OECD Guideline 406 (Skin Sensitisation)

Principles of method if other than guideline:

NA

GLP compliance:

yes

Type of study:

Buehler test

Justification for non-LLNA method:

The study was conducted in 1996 when the LLNA was not yet an established testing approach.

Species:

guinea pig

Strain:

Hartley

Sex:

male/female

Details on test animals and environmental conditions:

TEST ANIMALS
- Source: Harlan Sprague Dawley, Inc., Haslett, MI.
- Age at study initiation: Young adult
- Housing: individually in suspended stainless steel cages.
- Diet: ad libitum, Purina Certified Pig Chow
- Water: ad libitum, municipal tap water
- Acclimation period: for a minimum of five years


ENVIRONMENTAL CONDITIONS
- Temperature: 17.8 - 25.6 °C
- Humidity: 28 - 73 %
- Air changes (per hr): 10 - 15 air changes/hour
- Photoperiod (hrs dark / hrs light): 12-hour light/ 12-hour dark

Route:

epicutaneous, occlusive

Vehicle:

other: mineral oil

Concentration / amount:

25 % w/v t-Butyl Peroctoate

Route:

epicutaneous, occlusive

Vehicle:

other: mineral oil

Concentration / amount:

25 % w/v t-Butyl Peroctoate

No. of animals per dose:

10 male, 10 female

Details on study design:

RANGE FINDING TESTS:
Dosing: On the day prior to dose administration, four topical range-finding guinea pigs were weighed and the hair removed from the right and left side of the animals with a small animal clipper. Care was taken to avoid abrading the skin during clipping procedures. On the following day, four concentrations of the test article were prepared and each concentration was applied to the clipped area of each topical range-finding animal.
Following patch application, the trunk of each animal was wrapped with elastic wrap which was secured with adhesive tape to prevent removal of the patches and the animal was returned to its cage. Approximately six hours after patch application, the elastic wrap, tape and patches were removed. The test sites were then wiped with gauze moistened in distilled water to remove test article residue and the animals returned to their cages.


MAIN STUDY
A. INDUCTION EXPOSURE
On the day prior to the first induction dose administration, the hair was removed from the left side of the 20 test animals with a small animal clipper. Care was taken to avoid abrading the skin during clipping procedures. On the following day (day 0), the appropriate concentration of the test article was prepared and applied to the clipped area of the animals.
Following patch application, the trunk of each animal was wrapped with elastic wrap which was secured with adhesive tape to prevent removal of the patch and the animal was returned to its cage. Approximately 6 hours after patch application, the elastic wrap, tape and patches were removed. The test sites were then wiped with gauze moistened in distilled water to remove test article residue and the animals returned to their cages.

Dermal Observations: The test sites were graded for dermal irritation at approximately 24 and 48 hours following patch application using the Dermal Grading System.

The induction procedure was repeated on study day 7 and on study day 14 so that a total of three consecutive induction exposures were made to the 20 test animals.


B. CHALLENGE EXPOSURE
On the day prior to challenge dose administration, the hair was removed from the right side of the 19 test and 10 control animals with a small animal clipper. Care was taken to avoid abrading the skin during clipping procedures. On the following day (day 28), the appropriate concentration of the test article was prepared and applied to a naive site within the clipped area of the animals.
Following patch application, the trunk of each animal was wrapped with elastic wrap which was secured with adhesive tape to prevent removal of the patch and the animal was returned to its cage. Approximately 6 hours after patch application, the elastic wrap, tape and patches were removed. The test sites were then wiped with gauze moistened in distilled water to remove test article residue and the animals returned to their cages.

Dermal Observations: The test sites were graded for dermal irritation at approximately 24 and 48 hours following patch application using the Dermal Grading System.


C. RECHALLENGE
A rechallenge was conducted in order to clarify the results of the challenge phase.
On the day prior to rechallenge dose administration, the hair was removed from the left side of the 19 test and 10 control animals with a small animal clipper. Care was taken to avoid abrading the skin during clipping procedures. On the following day (day 35), the appropriate concentration of the test article was prepared and applied to a naive site within the clipped area of the animals.
Following patch application, the trunk of each animal was wrapped with elastic wrap which was secured with adhesive tape to prevent removal of the patch and the animal was returned to its cage. Approximately 6 hours after patch application, the elastic wrap, tape and patches were removed. The test sites were then wiped with gauze moistened in distilled water to remove test article residue and the animals returned to their cages.

Dermal Observations: The test sites were graded for dermal irritation at approximately 24 and 48 hours following patch application using the Dermal Grading System.

Challenge controls:

see above at "Details on study design"

Positive control substance(s):

yes

Remarks:

Hexylcinnamaldehyde

Positive control results:

Using Hexylcinnamaldehyde as a mild to moderate positive control, Springborn Laboratories, Inc., Spencerville, Ohio, has compiled historical control data for contact sensitization to this agent utilizing the test system described herein (Modified Buehler Design). As indicated, 95% of animals induced with Hexylcinnamaldehyde elicited a contact sensitization response following challenge with Hexylcinnamaldehyde, thereby demonstrating the susceptibility of the test system to this sensitizing agent.

Key result

Reading:

1st reading

Hours after challenge:

24

Group:

test chemical

Dose level:

5 % t-Butyl Peroctoate

No. with + reactions:

9

Total no. in group:

19

Clinical observations:

Discrete or patchy erythema

Key result

Reading:

2nd reading

Hours after challenge:

48

Group:

test chemical

Dose level:

5 % t-Butyl Peroctoate

No. with + reactions:

3

Total no. in group:

19

Clinical observations:

Discrete or patchy erythema

Key result

Reading:

1st reading

Hours after challenge:

24

Group:

other: challenge control

Dose level:

5 % t-Butyl Peroctoate

No. with + reactions:

3

Total no. in group:

10

Clinical observations:

Discrete or patchy erythema

Key result

Reading:

2nd reading

Hours after challenge:

48

Group:

other: challenge control

Dose level:

5 % t-Butyl Peroctoate

No. with + reactions:

2

Total no. in group:

10

Clinical observations:

Discrete or patchy erythema

Key result

Reading:

rechallenge

Hours after challenge:

24

Group:

test chemical

Dose level:

2 % t-Butyl Peroctoate

No. with + reactions:

5

Total no. in group:

19

Clinical observations:

Discrete or patchy erythema

Key result

Reading:

rechallenge

Hours after challenge:

48

Group:

test chemical

Dose level:

2 % t-Butyl Peroctoate

No. with + reactions:

0

Total no. in group:

19

Clinical observations:

none

Key result

Reading:

rechallenge

Hours after challenge:

24

Group:

other: challenge control

Dose level:

2 % t-Butyl Peroctoate

No. with + reactions:

0

Total no. in group:

10

Clinical observations:

none

Key result

Reading:

rechallenge

Hours after challenge:

48

Group:

other: challenge control

Dose level:

2 % t-Butyl Peroctoate

No. with + reactions:

0

Total no. in group:

10

Clinical observations:

none

Group:

positive control

Remarks on result:

not measured/tested

Key result

Group:

negative control

Remarks on result:

not measured/tested

Interpretation of results:

Category 1 (skin sensitising) based on GHS criteria

Conclusions:

Due to the irritation noted in both the test and challenge control animals, challenge with tert.-Butylperoxy- 2-ethylhexanoat was considered to be ambiguous. Following rechallenge with 2% tert.-Butylperoxy- 2-ethylhexanoat, slight evidence of sensitization was observed in 5/19 test animals at the 24 hour scoring interval; however, the dermal responses did not persist to the 48 hour scoring interval. Therefore, based on the results of this study, tert.-Butylperoxy- 2-ethylhexanoat is considered to be a possible weak sensitizer in guinea pigs. The results of the Hexylcinnamaldehyde Historical Control demonstrates that the test design utilized by Springborn Laboratories, Inc., could detect potential mild to moderate contact sensitizers.

Executive summary:

The dermal sensitization potential of tert.-Butylperoxy- 2-ethylhexanoat was evaluated in Hartley-derived albino guinea pigs. Ten male and ten female guinea pigs were topically treated with 25 % w/v tert.-Butylperoxy- 2-ethylhexanoat in mineral oil, once per week, for 3 consecutive weeks. Following a two week rest period, a challenge was performed whereby the 19 test and 10 previously untreated (naive) challenge control guinea pigs were topically treated with 5 % w/v tert.-Butylperoxy- 2-ethylhexanoat in mineral oil. Challenge responses in the test animals were compared to those of the challenge control animals. Following a one week rest period, a rechallenge was performed whereby the 19 test and the 10 challenge control guinea pigs were topically treated with 2% w/v tert.-Butylperoxy- 2-ethylhexanoat in mineral oil. Rechallenge responses in the test animals were compared to those of the challenge control animals.

Following induction 1 with 25 % w/v tert.-Butylperoxy- 2-ethylhexanoat in mineral oil, mild irritation was noted in the test animals. The dermal irritation increased slightly at induction 2 and 3. Following challenge with 5 % w/v tert-butyl 2-ethylperoxyhexanoate in mineral oil, dermal scores of 1 were noted in 9/19 test animals and 3/10 challenge control animals at the 48 hour scoring interval and in 3/19 test animals and 2/10 challenge control animals at the 48 hour scoring interval. Dermal scores of 0 were noted in the remaining test and challenge control animals. Group mean dermal scores were noted to be similar in the test animals as compared to the challenge control animals. Following rechallenge with 2 % w/v tert.-Butylperoxy- 2-ethylhexanoat in mineral oil, dermal scores of 1 were noted in 5/19 test animals at the 24 hour scoring interval. Dermal scores of 0 were noted in the remaining test and all challenge control animals. Group mean dermal scores were noted to be slightly higher in the test animals as compared to the challenge control animals.

One test animal (1431/F) was found dead on study day 27. Gross necropsy observations included dark red mandibular and axillary lymph nodes, an adhesion in the thoracic cavity, mottled lungs, mottled liver, enlarged spleen and congested meningeal vessels in the brain. The majority of sensitization study animals gained weight during the test period and generally appeared in good health.

Due to the irritation noted in both the test and challenge control animals, challenge with tert.-Butylperoxy- 2-ethylhexanoat was considered to be ambiguous. Following rechallenge with 2% tert-butyl 2-ethylperoxyhexanoate, slight evidence of sensitization was observed in 5/19 test animals at the 24 hour scoring interval; however, the dermal responses did not persist to the 48 hour scoring interval. Therefore, based on the results of this study, tert.-Butylperoxy- 2-ethylhexanoat is considered to be a possible weak sensitizer in guinea pigs.

Endpoint conclusion

Endpoint conclusion:

adverse effect observed (sensitising)

Additional information:

The dermal sensitization potential of tert.-Butylperoxy- 2-ethylhexanoat was evaluated in Hartley-derived albino guinea pigs. Ten male and ten female guinea pigs were topically treated with 25 % w/v tert.-Butylperoxy- 2-ethylhexanoat in mineral oil, once per week, for 3 consecutive weeks. Following a two week rest period, a challenge was performed whereby the 19 test and 10 previously untreated (naive) challenge control guinea pigs were topically treated with 5 % w/v tert.-Butylperoxy- 2-ethylhexanoat in mineral oil. Challenge responses in the test animals were compared to those of the challenge control animals. Following a one week rest period, a rechallenge was performed whereby the 19 test and the 10 challenge control guinea pigs were topically treated with 2% w/v tert.-Butylperoxy- 2-ethylhexanoat in mineral oil. Rechallenge responses in the test animals were compared to those of the challenge control animals.

Following induction 1 with 25 % w/v tert.-Butylperoxy- 2-ethylhexanoat in mineral oil, mild irritation was noted in the test animals. The dermal irritation increased slightly at induction 2 and 3. Following challenge with 5 % w/v tert.-Butylperoxy- 2-ethylhexanoat in mineral oil, dermal scores of 1 were noted in 9/19 test animals and 3/10 challenge control animals at the 48 hour scoring interval and in 3/19 test animals and 2/10 challenge control animals at the 48 hour scoring interval. Dermal scores of 0 were noted in the remaining test and challenge control animals. Group mean dermal scores were noted to be similar in the test animals as compared to the challenge control animals. Following rechallenge with 2 % w/v tert.-Butylperoxy- 2-ethylhexanoat in mineral oil, dermal scores of 1 were noted in 5/19 test animals at the 24 hour scoring interval. Dermal scores of 0 were noted in the remaining test and all challenge control animals. Group mean dermal scores were noted to be slightly higher in the test animals as compared to the challenge control animals.

One test animal (1431/F) was found dead on study day 27. Gross necropsy observations included dark red mandibular and axillary lymph nodes, an adhesion in the thoracic cavity, mottled lungs, mottled liver, enlarged spleen and congested meningeal vessels in the brain. The majority of sensitization study animals gained weight during the test period and generally appeared in good health.

Due to the irritation noted in both the test and challenge control animals, challenge with tert.-Butylperoxy- 2-ethylhexanoat was considered to be ambiguous. Following rechallenge with 2% tert.-Butylperoxy- 2-ethylhexanoat, slight evidence of sensitization was observed in 5/19 test animals at the 24 hour scoring interval; however, the dermal responses did not persist to the 48 hour scoring interval. Therefore, based on the results of this study, tert.-Butylperoxy- 2-ethylhexanoat was only considered to be a possible weak sensitizer in guinea pigs.

Respiratory sensitisation

Endpoint conclusion

Endpoint conclusion:

no study available

Justification for classification or non-classification

Classification, Labelling, and Packaging Regulation (EC) No 1272/2008
The available experimental test data are reliable and suitable for classification purposes under Regulation (EC) No 1272/2008. Based on available data on skin sensitization, the test item is classified and labelled as skin sensitizer Cat 1 (H317: "May cause an allergic skin reaction") according to Regulation (EC) No 1272/2008 (CLP), as amended for the tenth time in Regulation (EU) No 2017/776.