6-methyl-1,3,5-triazine-2,4-diyldiamine

Administrative data

Endpoint:

in vivo mammalian somatic cell study: cytogenicity / erythrocyte micronucleus

Remarks:

Type of genotoxicity: chromosome aberration

Type of information:

migrated information: read-across from supporting substance (structural analogue or surrogate)

Adequacy of study:

key study

Study period:

2000

Reliability:

2 (reliable with restrictions)

Rationale for reliability incl. deficiencies:

other: see 'Remark'

Remarks:

There is no data available on "in vitro mammalian chromosome aberration" or "in-vitro micronucleus" genetic toxicity studies with Acetoguanamine. According to Annex VIII of REACH regualtion before new tests are carried out to determine the listed enpoints of this Annex all available in-vitro data, in-vivo data, historical human data, validated (Q)SAR-data and data from structurally related substances (read-across approach) shall be assessed first. Therefore a literatur research was performed to find in-vitro data, in-vivo data or historical human data on genetic toxicity testing with Acetoguanamine. No records were found and in order to avoid unneccessary animal testing structurally related substances were searched. A structurally related substance is Benzoguanamine, for which further genetic toxicity data was found. Irrespective of metabolic activation Acetoguanamine was not able to induce reverse mutations in Salmonella typhimurium just as Benzoguanamine did not in the Ames test. The molecule structure of Acetoguanamine supports the negative effect. It is completely integrated in the structure of Benzoguanamine. There are no additional functional groups which could be relevant regarding structural alerts for mutagenicity. Since Benzoguanamine showed no obvious potential to impact genomic integrity it can be assumed that Acetoguanamine will show the same properties.

Data source

Materials and methods

GLP compliance:

yes (incl. QA statement)

Type of assay:

micronucleus assay

Test material

Test animals

Species:

mouse

Strain:

NMRI

Sex:

male/female

Administration / exposure

Route of administration:

oral: gavage

Duration of treatment / exposure:

24hr, 48hr

Results and discussion

Additional information on results:

This substance was not mutagenic in bacteria [OECD TG 471 & 472]. It induced chromosomal aberration in CHL/IU cells with and without an exogenous metabolic activation system even under the soluble concentrations. It also gave a positive response in the human lymphocytes tested [OECD TG 473] and the mouse lymphoma TK assay [OECD TG 476] but only under the insoluble dose levels. The cytogenetic effect observed in in vitro assays however, could not be reproduced in the micronucleus tests in vivo [OECD TG 474]. Based on the weight of evidence, it could be concluded that this substance was not genotoxic in vivo.

Any other information on results incl. tables

STATISTICAL RESULTS:
-The highest dose (300 mg/kg for males and 200 mg/kg b.w. for females)  was estimated by five 
pre-experiments to the suitable since higher  concentrations were lethal.  After treatment with 
the test item the  number of NCEs was not substantially increased as compared to the mean  value 
of NCEs of the vehicle control thus indicating that this substance  at the indicated concentrations 
had no cytotoxic effectiveness in the  bone marrow.
 There was no biologically and statistically relevant enhancement in the  frequency of the detected 
micronuclei after administration of the test  item at any dose level or sampling time as compared 
to vehicle controle.   40 mg/kg b.w. cyclophosphamide administered orally was used as positive  
control which showed a substantial increase of induced micronucleus  frequency.

-micronucleus test results
(A)Male animals

Test group  Dose      Sampling     Sampling       NCEs per
---        mg/kg b.w.  time (hr)   micronuclei(%)  2000 PCEs
vehicle        0         24          0.02          1566
BG            75         24          0.08          1562
BG           150         24          0.09          1814
BG           300         24          0.02          1582
CP            40         24          1.11          2033

Vehicle        0         48          0.01          1694
BG            75         48          0.02          1639
BG           150         48          0.08          1795
BG           300         48          0.07          1755

Vehicle        0         72          0.03          1610
BG            75         72          0.04          1417
BG           150         72          0.03          1549
BG           300         72          0.02          1645

(B)Female animals

Test group   Dose      Sampling    Sampling       NCEs per
---        mg/kg b.w.  time (hr)   micronuclei(%) 2000 PCEs
vehicle       0          24         0.03          1652
BG           50          24         0.03          1563
BG          100          24         0.09          1463
BG          200          24         0.04          1889
CP           40          24         0.98          1755

Vehicle       0          48         0.01          2113
BG           50          48         0.04          1727
BG          100          48         0.01          1628
BG          200          48         0.02          1945

Vehicle       0          72         0.02          1577
BG           50          72         0.02          1408
BG          100          72         0.04          1638
BG          200          72         0.01          1492
 
BG = benzoguanamine (2,4-diamino-6-phenyl-1,3,5-triazine)
CP = cyclo phosphamide

Applicant's summary and conclusion

Conclusions:

Interpretation of results (migrated information): negative
not genotoxic in vivo

Executive summary:

In a CD-1 mouse bone marrow micronucleus assay, 5 male and female were treated oral gavage with this substance at doses of 0, 75, 150, 300 mg/kg bw in male mice and 0, 50, 100, 200 mg/kg/bw.  Bone marrow cells were harvested at 24, 48, 72Hr post-treatment.  The vehicle was corn oil. 

 There were no signs of toxicity during the study. The positive control induced the appropriate response. There was not a significant increase in the frequency of micronucleated polychromatic erythrocytes in bone marrow after any treatment time.

This study satisfies the requirement for Test Guideline OECD 474 forin vivocytogenetic mutagenicity data.

As there is no data available on "in vitro mammalian chromosome aberration" or "in-vitro micronucleus" genetic toxicity studies (required by Annex VIII of REACH regulation) with Acetoguanamine this endpoint was read-acrossed from Benzoguanamine to Acetoguanamine. This was done in order to avoid unnecessary animal testing and to fulfill the claim of REACH regulation Annex VIII ("data from structurally related substances (read-across approach) should be assessed first before new tests are carried out). Justification for Read-Across see above in "Rationale for Reliability".