Turpentine, oil

Administrative data

Description of key information

Three major constituents of TOPP met the EU criteria for classification as skin irritants based on percentage cellular viability <50% in Episkinin vitrostudies (Maillet, 2010a, b and c).

Two major constituents of TOPP did not meet EU criteria for classification as eye irritants in GLP studies conducted in accordance with OECD Test Guideline 405 (Colas, 2010a and b). Turpentine (unspecified composition) was reported to cause adverse ocular effects following sub-conjunctival injection in a peer-reviewed publication.

TOPP also contains low concentrations of the sulfur-containing substances methyl mercaptan (typically 0.06%), dimethyl sulfide (typically 1.2%) and dimethyl disulfide (0.32%). The maximum total combined concentration of these constituents reported in commercial samples is 6% by weight expressed as sulfur. None of these is classified as irritant or corrosive in Annex VI of EC Regulation 1272/2008/EC. Data reported in IUCLID 2000 indicate that in OECD guideline studies dimethyl disulfide (CAS 624-92-0) did not meet the criteria for classification as skin or eye irritant. Slight effects are reported in non-guideline studies for dimethyl sulfide, but these are unlikely to meet the criteria for classification. Methyl mercaptan (CAS 74-93-1) is reported to be corrosive in IUCLID 2000, based on a test with sodium methyl mercaptide (pH 9.78). However, the validity of this read-across is questionable since the observed corrosive effects are most likely due to the high pH, which would not be relevant for neutral methyl mercaptan present in TOPP.

Overall, the sulfur-containing species present in TOPP would not contribute to a more severe classification for skin and eye irritation than the existing one.

Key value for chemical safety assessment

Skin irritation / corrosion

Link to relevant study records

Referenceopen allclose all

Reference 1

Endpoint:

skin irritation: in vitro / ex vivo

Type of information:

experimental study

Adequacy of study:

weight of evidence

Study period:

from June 22 to July 27, 2010

Reliability:

1 (reliable without restriction)

Rationale for reliability incl. deficiencies:

guideline study

Reason / purpose for cross-reference:

reference to same study

Reason / purpose for cross-reference:

reference to other study

Qualifier:

equivalent or similar to guideline

Guideline:

other: ECVAM protocol version 1.8 of February 2009

Deviations:

no

Principles of method if other than guideline:

Not applicable

GLP compliance:

yes (incl. QA statement)

Species:

human

Details on test animals or test system and environmental conditions:

Three-dimensional human epidermis model, supplied by SkinEthic Laboratories, Nice, France constituted by:
- a collagen type I matrix, coated with type IV collagen
- a differentiated and stratified epidermis model from human keratinocytes, obtained after 13-day culture period.
All biological components of the epidermis and the kit culture medium have been tested for the absence of viruses, bacteria and mycoplasma

Type of coverage:

open

Vehicle:

unchanged (no vehicle)

Controls:

other: not applicable

Amount / concentration applied:

TEST MATERIAL
- Amount(s) applied: 10 µL

Duration of treatment / exposure:

15 ± 0.5 min

Number of animals:

3 epidermis/product

Details on study design:

Before the beginning of the study, the non-specific MTT reduction by the test item was checked by incubating MTT solution and 10 µL test item for 3 hours ± 30 minutes and checking the colour of the solution.

Application of the test item and control:
- negative control: 10 µL of PBS+ to each epidermis surface
- positive control: 10 µL of SDS solution at 5% (w/v) in distilled water; after 7 minutes contact time, an intermediate re-spreading is done
- test substance: 10 µL of the test item, as supplied
- contact timepoint for all products: 15 ± 0.5 minutes at room temperature

Rinsing:
- epidermis rinsed thoroughly with 25 mL of PBS+
- remaining product removed with a cotton-bud

Incubation: plates incubated during 42 ± 1 hours in CO2 incubator with maintenance medium

MTT assay:
- epidermis incubated for 3 hours ± 5 minutes in MTT solution in the CO2 incubator
- formazan extraction in 500 µL of acidic isopropanol stored at 4 hours ± 30 minutes at room temperature, protected from light or during 70 ± 5 hours at 4 °C
- measurement of OD at 570 nm

Irritation / corrosion parameter:

other: other: viability % (MTT assay)

Value:

38.5

Remarks on result:

other:

Remarks:

Basis: mean. Time point: 15 min. Reversibility: no data. Remarks: ± 3.5.

Negative control (PBS+): mean OD = 0.821

Positive control (5% SDS): % viability (MTT assay) = 18.7 ± 3.0

Test item: % viability (MTT assay) = 38.5 ± 3.5

Table 1: MTT conversion assay in living epidermis

		O.D. 1	O.D. 2	Mean	Standard deviation	Viability %	Mean Viability %	Standard deviation
Negative control	Epidermis 1	0.768	0.808	0.788	0.028	96.0	100	0.044
	Epidermis 2	0.855	0.864	0.860	0.006	104.7
	Epidermis 3	0.819	0.811	0.815	0.006	99.3
Positive control	Epidermis 1	0.124	0.145	0.135	0.015	16.4	18.7	0.030
	Epidermis 2	0.158	0.131	0.145	0.019	17.6
	Epidermis 3	0.191	0.172	0.182	0.013	22.1
Test item	Epidermis 1	0.359	0.293	0.326	0.047	39.7	38.5	0.035
	Epidermis 2	0.301	0.267	0.284	0.024	34.6
	Epidermis 3	0.358	0.318	0.338	0.028	41.2

Interpretation of results:

Category 2 (irritant) based on GHS criteria

Conclusions:

Under the test conditions, beta-pinene is classified as irritating to the skin, R38, according to the criteria of Annex VI to the Directive 67/548/EEC and category 2 in CLP Regulation (EC) N° (1272-2008).

Executive summary:

A GLP study conducted in vitro with human epidermis model EPISKIN was performed to assess the irritancy potential of beta-pinene similarly to ECVAM protocol version 1.8 of February 2009. 10 µL of test item was applied directly on epidermis for 15 min on 3 epidermis. Positive control was 10 µL of 5% (w/v) SDS solution and negative control was 10 µL of PBS (each tested on 3 epidermis). MTT conversion assay was peformed to evaluate the percentage of cellular viability of the epidermis. Positive control had a percentage of cell viability of 18.7± 3.0 and test item 38.5 ± 3.5. As the percentage of viability is ≤ 50 %, the test item is considered to be irritating for skin. Under the test conditions, beta-pinene is classified as irritating to the skin, R38, according to the criteria of Annex VI to the Directive 67/548/EEC and category 2 in CLP Regulation (EC) N° (1272-2008).