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Diss Factsheets

Toxicological information

Genetic toxicity: in vivo

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Administrative data

Endpoint:
in vivo mammalian germ cell study: cytogenicity / chromosome aberration
Type of information:
migrated information: read-across based on grouping of substances (category approach)
Adequacy of study:
key study
Study period:
1974-02-04 to 1974-09-10
Reliability:
2 (reliable with restrictions)
Rationale for reliability incl. deficiencies:
other: see 'Remark'
Remarks:
The study was conducted using methods comparable to OECD guideline 478 "Genetic Toxicology: Rodent Dominant Lethal Test". Not GLP. Results of mating are reported for each male, but not in detail for each female. A positive control was not included, but is not necessarily required according to the OECD guideline.
Cross-referenceopen allclose all
Reason / purpose for cross-reference:
reference to same study
Reason / purpose for cross-reference:
reference to other study

Data source

Reference
Reference Type:
study report
Title:
Unnamed
Year:
1974
Report date:
1974

Materials and methods

Test guideline
Qualifier:
equivalent or similar to guideline
Guideline:
OECD Guideline 478 (Genetic Toxicology: Rodent Dominant Lethal Test)
Deviations:
yes
Remarks:
Not GLP. Results of mating are reported for each male, but not in detail for each female. A positive control was not included, but is not necessarily required according to the OECD guideline.
GLP compliance:
no
Type of assay:
rodent dominant lethal assay

Test material

Constituent 1
Chemical structure
Reference substance name:
Disodium dihydrogen (1-hydroxyethylidene)bisphosphonate
EC Number:
231-025-7
EC Name:
Disodium dihydrogen (1-hydroxyethylidene)bisphosphonate
Cas Number:
7414-83-7
Molecular formula:
C2H8O7P2.2Na
IUPAC Name:
disodium dihydrogen (1-hydroxyethane-1,1-diyl)bis(phosphonate)
Constituent 2
Reference substance name:
(1-hydroxyethylidene)bisphosphonic acid, disodium salt
IUPAC Name:
(1-hydroxyethylidene)bisphosphonic acid, disodium salt
Test material form:
not specified
Details on test material:
CAS No. 7414-83-7
Disodium ethane-1-hydroxy-1,1-diphosphonate, purity, source not stated.

Test animals

Species:
mouse
Strain:
other: C3D2F1/J
Sex:
male
Details on test animals or test system and environmental conditions:
TEST ANIMALS
- Source: Jackson Laboratories, Bar Harbor, Maine
- Age at study initiation: sexually mature
- Weight at study initiation: N/A
- Assigned to test groups randomly: Yes, on the basis of body weight
- Fasting period before study: N/A
- Housing: N/A
- Diet (e.g. ad libitum): ad libitum
- Water (e.g. ad libitum): ad libitum
- Acclimation period: One week

ENVIRONMENTAL CONDITIONS
- Temperature (°C): N/A
- Humidity (%): N/A
- Air changes (per hr): N/A
- Photoperiod (hrs dark / hrs light): N/A

Administration / exposure

Route of administration:
oral: gavage
Vehicle:
- Vehicle(s)/solvent(s) used: Water
- Amount of vehicle (if gavage or dermal): 0.25 ml
Details on exposure:
Each of three groups of mice received the test substance (as a single oral daily dose in 0.25 ml volumes), at levels of 1000, 200, and 20 mg/kg bw for five days. One other group received water for five days. The fifth group received no treatment.
Duration of treatment / exposure:
5 d
Frequency of treatment:
once daily
Post exposure period:
N/A
Doses / concentrationsopen allclose all
Dose / conc.:
20 mg/kg bw/day (actual dose received)
Dose / conc.:
200 mg/kg bw/day (actual dose received)
Dose / conc.:
1 000 mg/kg bw/day (actual dose received)
No. of animals per sex per dose:
20
Control animals:
yes, concurrent no treatment
yes, concurrent vehicle
Positive control(s):
none

Examinations

Tissues and cell types examined:
total implants, resorptions and dead embryos
Details of tissue and slide preparation:
CRITERIA FOR DOSE SELECTION: The top dose for the dominant lethal assay was based on the maximum tolerated dose determined from a preliminary study (see below under additional information on results). The intermediate dosing level was arbitrarily set at 200 mg/kg and the lower test group received the human-usage level of 20 mg/kg bw.

TREATMENT AND SAMPLING TIMES ( in addition to information in specific fields): N/A

DETAILS OF SLIDE PREPARATION: N/A

METHOD OF ANALYSIS: N/A

OTHER: N/A
Evaluation criteria:
N/A
Statistics:
Data from experimental groups were compared to data from control groups using the Chi-square test for significant deviations (P<= 0.05, DF=1)

Results and discussion

Test results
Sex:
male/female
Genotoxicity:
negative
Toxicity:
no effects
Vehicle controls validity:
valid
Negative controls validity:
valid
Positive controls validity:
not examined
Additional information on results:
RESULTS OF RANGE-FINDING STUDY
- Dose range: 62.5-2000 mg/kg bw
- Solubility: N/A
- Clinical signs of toxicity in test animals: 2 out of 10 mice died at the 2000 mg/kg dose level.
- Evidence of cytotoxicity in tissue analyzed: N/A
- Rationale for exposure: To determine an LD50 and/or a maximum tolerated dose for mice.
- Harvest times: Animals were exposed daily for 5 consecutive days.
- High dose with and without activation: 2000 mg/kg without activation
- Other: An LD50 could not be calculated, but the maximum tolerated dose was chosen as 1000 mg/kg.


RESULTS OF DEFINITIVE STUDY
- Types of structural aberrations for significant dose levels (for Cytogenetic or SCE assay): N/A
- Induction of micronuclei (for Micronucleus assay): N/A
- Ratio of PCE/NCE (for Micronucleus assay): N/A
- Appropriateness of dose levels and route: Top dose was based on maximum tolerated dose.
- Statistical evaluation: N/A

Any other information on results incl. tables

Total litter losses occurred very rarely throughout the study and they showed no relationship to dosage of the test substance. Only two litters approached being totally lost in all test groups. One incident occurred in the untreated controls in which two to three implants in one female were dead and another occurred in the high dose group (1000 mg/kg) in which only one of five implants was alive at necropsy. Both litter losses originated during the third week of mating and were attributed to a malfunction in the individual animals and therefore were not considered test-related.

The number of deaths in females mated with males given the test substance did not differ significantly from those in concurrent controls for any of the mating periods.

Mating performance of all test groups compared favorably with the controls. As in the examination of individual female data, individual poor performance of the sire which was not test related could easily be detected. For example one male in the mid test group failed to impregnate a female until the fifth week of mating. In the final two weeks of the study, three of the four females mated with this male mouse conceived but only carried an average of six implants per pregnancy. The average number of implants for the rest of the group was 8.9 for the entire study and 9.0 for all other sires combined during the same two weeks of mating. The fact that eighteen implants sired by the male mouse mentioned above produced no fetal deaths provides additional evidence supporting the decision that the performance of this male was not test related.

When it came to conception rates, implants and fetal mortality, little variation occurred between test groups and controls for any of the parameters measured.

The mutagenic index was measured. It was a calculation based on two independent variables, fetal deaths and total implants, used as a convenient comparison of group to group performance. No significant differences (P= 0.05. D.F=1) were found when test group mutagenic indices were compared to either the vehicle or untreated controls.

Mating Performance and Uterine Content Evaluation by Groups 

 

Group

Percent Pregnant

Implants

Total / Average

Fetal Deaths

Total / Average

Percent Resorption

Untreated Control

83.3

1675 / 8.37

78 / 0.39

4.47

Vehicle Control

78.7

1635 / 8.65

64 / 0.37

3.66

EHDP 1.000 mg/kg

80.0

1618 / 8.42

74 / 0.39

4.14

EHDP 200 mg/kg

73.9

1545 / 8.78

66 / 0.38

4.27

EHDP 20 mg/kg

73.1

1543 / 8.82

53 / 0.30

3.30

 

EHDP Dominant Lethal Assay Mutagenic Indices

 

Week Treatment

Untreated Control

Vehicle Control

EHDP

 1000 mg/kg

EHDP

 200 mg/kg

EHDP

 20 mg/kg

1

3.88

4.76

4.27

4.18

4.13

2

2.37

4.10

3.85

5.85

2.94

3

4.37

4.78

5.70

3.83

5.43

4

5.57

4.10

3.66

4.49

3.76

5

5.15

2.80

7.41

2.81

2.61

6

6.15

3.16

3.41

5.21

2.69

 

 

Resorptions + Dead Embryos   x 100 = Mutagenic Index

       Total Implantations

Applicant's summary and conclusion

Conclusions:
The dominant lethal assay on EHDP proceeded very smoothly and gave no indication of any potential genetic hazard at test levels up to maximum tolerated doses. The test substance was tested in the dominant lethal assay using male mice that were orally dosed from 20 mg to 1000 mg/kg once daily for five days. No test substance related variations relative to control values in conception rates, total implant averages, fetal death averages, resorption percentage and mutagenic indices were observed. Under the conditions of the study, the test substance was considered negative in the dominant lethal assay.
Executive summary:

Phosphonic acid, P,'-(1 -hydroxyethylidene)bis-,sodium salt was administered orally (0.25 ml volumes) to male mice of the C3D2F1/J strain at three dose levels (1000, 200 and 20 mg/kg) for five consecutive days. The study also included a vehicle control (water) and an untreated group. 20 mice were assigned to each group.

Immediately following treatment, each male was caged with two untreated females for a period seven days and with two fresh females the following week. This procedure was continued for a total of six weeks, thereby encompassing the entire spermatogenic cycle of the mouse, which was purported to be 35 days.

Consequently, each male was mated to twelve females over a six-week period: A total of 240 matings per dose group.

On day 13 or 14 of gestation (as measured from the mid-week of presumptive mating), the females were sacrificed. Total implants, resorptions and dead embryos were enumerated and recorded.

Various parameters such as average number of implants per female, average number of fetal deaths/female, fetal deaths per sire, and percent pregnancy per group were subjected to statistical analysis.

The test substance produced data that were not significantly different from control values in conception rates, total implant averages, fetal death averages, resorption percentage and mutagenic indices.

Therefore, the test substance was considered to be non-mutagenic when administered orally at maximum tolerated doses in the test system employed.