2,4-bis[N'-(4-methylphenyl)ureido]toluene

Administrative data

Endpoint:

basic toxicokinetics

Type of information:

other: Toxicokinetic Assessment

Adequacy of study:

key study

Study period:

January 06, 2004

Reliability:

2 (reliable with restrictions)

Rationale for reliability incl. deficiencies:

other: Toxicokinetic Assessment by a certified toxicologist.

Data source

Materials and methods

Objective of study:

other: Assessment of toxicokinetic behaviour

GLP compliance:

no

Test material

Results and discussion

Any other information on results incl. tables

The acute oral and dermal toxicity of KY-MA is low with an LD₅₀> 5000 mg/kg and an LD₅₀> 2000 mg/kg, respectively. The 28-day toxicity study also revealed that KY-MA has a low toxicity with a NOAEL of 1000 mg/kg/day. Therefore, an extensive toxicokinetic assessment is considered of limited value. Below, an assessment of the anticipated toxicokinetic behaviour of KY-MA is given. This assessment is considered relevant for all three components of KY-MA.

Dissolution of a compound is required for absorption from the gastro-intestinal tract into the blood. Based on the physico-chemical properties of KY-MA, the initial dissolution of both components is expected to be low. In the presence of gastric acid and/or bile salts, the solubility of KY-MA may be somewhat increased in the gastro-intestinal fluids. However, it is unlikely that the compound will be absorbed to a high extent from the gastro-intestinal tract (1). Although KY-MA shows a very low solubility in water, some dissolution may occur at low pH because of protonation of the urea groups.

In the gastro-intestinal tract, especially the colon, dissolved KY-MA may already be partly metabolised by amidases (2).

In case KY-MA is absorbed, it will be extensively metabolised by amidases, but also hydroxylation of the phenyl rings by cytochrome P450-mediated metabolism may occur. The formed hydroxy-metabolites will then probably be conjugated and excreted via urine or bile.

Although theoretically aniline-derivatives could be formed as metabolites, based on the toxicity studies, there are no indications that these compounds are formed after ingestion or dermal application of KY-MA.

KY-MA will show a high volume of distribution, because of the lipophilicity of the compound. It will be extensively distributed into peripheral tissue, especially fatty tissues. Some accumulation in fatty tissues is therefore anticipated. The plasma protein binding is expected to be high.Therefore, a volume of distribution exceeding that of total body water (> 40 l) is expected.

No uptake via inhalation is anticipated because of the relatively large particle size.

Since it is generally accepted that substances with log Po/w ranging from 0.1 to 6 penetrate the skin easily (3), it is to be expected KY-MA will be absorbed to some extent through the skin.

Based on the expected kinetic behaviour in the body, as described above, KY-MA will not accumulate in the body after prolonged exposure.

The anticipated toxicokinetic behaviour is supported by the acute and subacute oral and dermal toxicity data. No significant difference in toxicokinetic behaviour is expected between the three components.

Applicant's summary and conclusion

Conclusions:

Based on the expected kinetic behaviour in the body, as described above, KY-MA will not accumulate in the body after prolonged exposure.
It is unlikely, that the compound will be absorbed to a high extend from the gastro-intestinal tract. In the gastro-intestinal tract, but also is case KY-MA is absorbed, it will be extensively metabolised by amidases. No uptake by inhalation is anticipated because of the relatively large particle size. KY-MA will be absorbed to some extend through the skin.