Reaction mass of cobalt and copper and iron

Administrative data

Endpoint:

developmental toxicity

Type of information:

experimental study

Adequacy of study:

key study

Reliability:

1 (reliable without restriction)

Rationale for reliability incl. deficiencies:

other: Already evaluated by the Competent Authorities for Biocides and Existing Substance Regulations.

Data source

Materials and methods

Test guidelineopen allclose all

GLP compliance:

yes

Remarks:

Self-certified laboratory

Limit test:

no

Test material

Test animals

Species:

rabbit

Strain:

New Zealand White

Details on test animals or test system and environmental conditions:

Source: Covance, Denver, Pennsylvania, USA.
Sex: Female.
Age at study initiation: approximately 5 months.
Weight at study initiation: 2988 to 4412 g (on day 0 of gestation).

Administration / exposure

Route of administration:

oral: gavage

Vehicle:

other: 0.5 % aqueous methylcellulose

Details on exposure:

Concentration in vehicle: 0, 6, 9, or 18 mg Cu/mL
Total volume applied: 1mL/kg bw

Analytical verification of doses or concentrations:

yes

Details on analytical verification of doses or concentrations:

Analysis of dose formulations confirmed stability, homogeneity and verified the accuracy of formulation. 

Details on mating procedure:

Mating period: Not specified.

Duration of treatment / exposure:

Duration of exposure: Day 7–28 of gestation.

No. of animals per sex per dose:

Number of animals per group: 22 females (1 rabbit of the high dose group was removed on day 7 of gestation, prior to dosing, due to a self-inflicted injury).

Control animals:

yes, concurrent vehicle

Examinations

Maternal examinations:

Body weight: Yes (daily)
Food consumption: Yes (daily)
Clinical signs: Yes (daily)
Gross pathology and histopathology: Yes, gross external and visceral examination was performed for all animals.
Post-exposure period: Sacrifice on day 29 of gestation.

Ovaries and uterine content:

Examination of uterine content: Gravid uterine weight, number of corpora lutea, number of implantations, number of resorptions.

Fetal examinations:

General: Litter Size, number of live and dead foetuses, foetal weight, sex ratio, external alterations, retarded renal development.
Skeleton: Yes
Soft tissue: Yes

Statistics:

Linear contrast of means (Maternal weight, weight change, food consumption);
Jonckheere’s test (Live and dead foetuses, resorptions, implantations, incidence of foetal alterations);
Cochran-Armitage test (Incidence of pregnancy, clinical observations, maternal mortality, females with total resorptions, abortions/early deliveries);
Linear contrast of least square means (foetal weight, sex ratio).

Results and discussion

Results: maternal animals

Maternal developmental toxicity

Details on maternal toxic effects:

Maternal toxic effects:yes

Details on maternal toxic effects:
Three females of the high dose group were found dead during the study. One of them showed diarrhoea, red cageboard-staining, weakness, and irregular respiration prior to death. Gross necropsy of the three animals included stomach haemorrhage and/or ulceration, dark discolouration or mottling of lung tissue, pale liver, gelatinous tan rectal discharge, and brown liquid in chest cavity. In addition, two females of this dose group aborted. Diarrhoea was observed for one of them and the other animal showed red discoloured stomach lining upon necropsy. No mortality occurred at the low and mid dose levels. All animals of the test substance groups showed diarrhoea. Statistically significant adverse effects on maternal body weights, body weight changes and food consumption were observed at 9 and 18 mg Cu/kg bw/day. Marked reduction in food consumption and body weight losses were observed during the 1st week of dosing. The results are presented in Table 1.

Effect levels (maternal animals)

Maternal abnormalities

Results (fetuses)

Details on embryotoxic / teratogenic effects:

Embryotoxic / teratogenic effects:yes

Details on embryotoxic / teratogenic effects:
The number of foetuses, and numbers of early and late embryonic deaths were not adversely affected by maternal treatment. Mean foetal weight was slightly lower at 18 mg/kg bw/day (9 % lower than controls). The difference from control was considered treatment-related, but it was not statistically significant. The results are presented in Table 2.

There was a total of four foetuses with malformations: one control foetus showed fused ribs, one foetus at 6 mg/kg bw/day showed ectopic kidney, and two foetuses (from separate litters) at 18 mg/kg bw/day showed hemivertebra. These malformations were considered spontaneous and unrelated to treatment. There was a slight increase in incidence of foetuses at 18 mg/kg bw/day with retarded ossification of skull and pelvic bones. However, there was no correlation with foetal weight, and the biological significance of such a slight increase is uncertain, as there was no increase in the incidence of retarded sternebral ossification. Retarded sternebral ossification is a more common indicator of foetal immaturity. Rib alterations occurred at a very high incidence across all groups in this study; almost all litters were affected. The biological significance of an increase in incidence of a very common finding is uncertain. The results are presented in Table 3.

Effect levels (fetuses)

Fetal abnormalities

Overall developmental toxicity

Any other information on results incl. tables

Table 1. Maternal effects.

Parameter	Control	low dose	mid dose	high dose	dose response
Number of dams examined	22	22	22	21
Clinical findings during application of test substance Alopecia Diarrhea Irregular respiration Sore Stain cageboard Stain tail Weak	2 0 0 1 0 0 0	5 5* 0 0 0 3 0	2 5* 0 0 0 2 0	1 9* 1 0 3* 5* 1	- + - - - + -
Mortality of dams (%)	0	0	0	14 %*	-
Abortions	0	1	0	2	-
Body weight gain (day 7-29 of gestation) [g]	261.5±130.42	208.5±158.50	179.5±160.97	72.6±211.64*	+
Food consumption (day 7-29 of gestation) [g/day]	144.1 ± 10.61	134.8 ± 21.36	120.3 ± 32.62*	100.6±32.02*	+
Pregnancies (No. of dams pregnant)	21	21	21	21	-
* statistically significant trend ( p < 0.05)

Table 2. Litter response (Caesarean section data).

Parameter	Control	low dose	medium dose	high dose	dose response + / -
No. mated	22	22	22	21
No. pregnant	21	21	21	21	-
No. aborted/delivered early	0	1	0	2	-
No. found dead	0	0	0	3*	-
No. accidentally killed	0	0	0	1	-
No. with total resorptions	0	1	0	0	-
Total number of litters	21	19	21	15	-
Means per litter:
Mean corpora lutea	10.0±2.06	10.2±1.51	9.1±1.96	10.1±2.26	-
Implantation/Nidations	8.8±2.04	9.0±1.33	7.8±2.04	9.0±2.36	-
Resorptions Total Early Late	1.0±1.47 0.8±1.47 0.1±0.48	1.0±1.45 0.7±1.41 0.3±0.56	0.2±0.54 0.2±0.51 0.0±0.22	0.6±0.91 0.4±0.63 0.2±0.56	- - -
No. of dead fetuses	0	0	0	0	-
No. of Live fetuses Total Males Females	7.9±2.63 3.9±1.77 4.0±1.73	8.0±1.73 4.7±2.10 3.3±1.45	7.6±2.04 3.9±1.59 3.7±1.74	8.4±2.03 4.3±2.12 4.1±1.88	- - -
Mean fetal weight Total Males Females	42.95±2.98 43.25±3.14 42.67±3.77	41.71±4.51 42.63±4.46 40.85±4.86	43.93±5.88 43.32±5.47 43.69±6.06	38.91±4.82 38.84±4.95 39.16±5.54	- - -
Fetal sex ratio	0.48±0.16	0.58±0.18	0.50±0.22	0.48 ±0.23	-
* significant trend (p£ 0.05)

 

Table 3. Examination of the fetuses.

Parameter	Control	low dose	medium dose	high dose	dose response
No. examined (no. of litters)	165 (21)	152 (19)	159 (21)	126 (15)
No. of fetuses (litters) with:
External malformations	0	0	0	0	-
External developmental variations	0	0	0	0	-
External variations due to retarded development	0	0	0	0	-
Skeletal malformations Rib- fused Vertebra - hemi	1 (1) 0	0 0	0 0	0 2* (2)	- -
Skeletal developmental variations Rib- supernumerary Sternebra - fused	105 (21) 1 (1)	102 (19) 2 (2)	127 (20) 0	110 (15)* 0	- -
Skeletal variations due to retarded development Mandible- retarded ossification Pelvis- retarded ossification Skull- bent Skull- retarded ossification Sternebra- retarded ossification Vertebra- retarded ossification	0 0 0 0 65 (16) 1 (1)	0 1 (1) 2 (2) 0 60 (12) 0	0 1 (1) 0 1 (1) 76 (18) 0	1 (1) 2 (1) 0 5 (2)* 51 (12) 0	- - - + - -
Visceral malformations Kidney- ectopic	0	1 (1)	0	0	-
Visceral developmental variations	0	0	0	0	-
Visceral variations due to retarded development Kidney: Small papilla- size 2 Kidney: Papilla- size 3	0 2 (2)	1 (1) 5 (5)	5 (3) 1 (1)	1 (1) 1 (1)	- -
Total (%) with retardation	68 (41%)	67 (44%)	80 (50%)	57 (45%)	-
Total (%) with variations	125 (76%)	124 (82%)	143 (90%)	118 (94%)	-
* statistically significant trend (p < 0.05)

Applicant's summary and conclusion

Conclusions:

Under the conditions of the current study, there was no evidence of test substance-related teratogenicity.

LO(A)EL maternal toxic effects: 9 mg Cu/kg bw/day
NO(A)EL maternal toxic effects: 6 mg Cu/kg bw/day
LO(A)EL developmental effects: 9 mg Cu/kg bw/day 
NO(A)EL developmental effects: 6 mg Cu/kg bw/day

Executive summary:

Materials and Methods

Copper hydroxide was administered at concentrations of 0, 6, 9, or 18 mg Cu/kg bw to pregnant rabbits by gavage from day 7 to day 28 of gestation. Potential effects on maternal and developmental parameters were assessed. The study was conducted according to OECD 414 (1981); method B.31 (87/302/EEC), and USEPA OPPTS 870.3700 (1998).

Results and Discussion

Administration of copper to pregnant rabbits at 18 mg/kg bw/day was associated with marked initial bodyweight loss, inappetance, abortion and death.  Pups in litters from surviving dams showed slightly lower mean foetal weight, and slightly increased incidence of a common skeletal variant.  Maternal treatment at 9 mg/kg bw/day was associated with initial bodyweight loss and inappetance; pups also showed slightly increased incidence of a common skeletal variant, but mean foetal weights were not adversely affected.  Maternal administration of copper hydroxide was not associated with increased incidence of foetal malformations, pre-implantation losses, or foetal (embryonic) deaths.  The maternal and foetal no observed effect level was 6 mg/kg bw/day, based on maternal weight loss, inappetance, and an increased incidence of a common skeletal variant in foetuses at 9 mg/kg bw/day.