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Diss Factsheets

Administrative data

Key value for chemical safety assessment

Toxic effect type:
dose-dependent

Effects on fertility

Description of key information

The study does not need to be conducted because a developmental toxicity study is available.

Link to relevant study records
Reference
Endpoint:
screening for reproductive / developmental toxicity
Data waiving:
study scientifically not necessary / other information available
Justification for data waiving:
the study does not need to be conducted because a pre-natal developmental toxicity study is available
Effect on fertility: via oral route
Endpoint conclusion:
no study available

Effects on developmental toxicity

Description of key information

The NOAEL of CJ303 in rat’s maternal toxicity, or teratogenic and embyo-/fetotoxicity performance was 1000 mg/kg/day (OECD TG414).

Link to relevant study records
Reference
Endpoint:
developmental toxicity
Type of information:
experimental study
Adequacy of study:
key study
Study period:
From June 20, 2018 to March 26, 2019
Reliability:
1 (reliable without restriction)
Rationale for reliability incl. deficiencies:
guideline study
Qualifier:
according to guideline
Guideline:
OECD Guideline 414 (Prenatal Developmental Toxicity Study)
GLP compliance:
yes
Species:
rat
Strain:
Sprague-Dawley
Details on test animals or test system and environmental conditions:
Supplier: Beijing Vital River Laboratory Animal Technology Co., Ltd.
Number of animals: 140 females, and the remaining male rats were used for mating.
Animal age on arrival: 84~90 days old
Body weight: 348-600g for males and 256-377g for females.

Animal Husbandry
Husbandry:
All animals were housed in plastic cages (L46.0xW31.5xH20.0cm) on cage racks (L170.0xW50.0xH160.0cm). There were 5 cages per layer, and 4 layers per rack. There were two rats at most per cage, and mated females were housed individually in cages. During the gestation period, the cage location of females was determined by the mating date.
Environmental conditions: Temperature and humidity in animal room were controlled automatically and daily recorded. The temperature was controlled within 21.1-24.4℃ and the relative humidity was controlled within 44-74% in the animal room. Lighting was controlled with the sequence of 12 hours light and 12 hours dark.

Food, Water and Bedding:
The sterilized SPF rodent growth and breeding feed supplied by Beijing Keao Xieli Feed Co., Ltd were used in this test; the lot number of the feed was 18613123. All the nutrition components and contaminants were within the permitted limits described in the national standard. An analysis report of diet was supplied by the supplier.
Drinking water was purified with HT-R01000 purity system and routinely analyzed (at least annually), and all parameters were within the permitted limits described in the national standard.
The corn cob bedding supplied by Beijing Keao Xieli Feed Co., Ltd was used in this test, and the lot number was 18039813, 18069813. The contaminants of the bedding were within the permitted limits described in the national standard for animal feed. An analysis report of bedding was supplied by the supplier.
Diet and water were available to the animals ad libitum during test. The diet, water and bedding were considered not to contain any contaminants that could reasonably be expected to affect the purpose or integrity of the study.

Animal Welfare:
Animal use in the whole study complied with national animal welfare laws and regulations (instructive notions with respect to caring for laboratory animals, PRC Ministry of Science, 2006). The animal care and use activities required for conduct of this study were supervised and approved by the testing facility Animal Care and Use Committee (IACUC).
Route of administration:
oral: gavage
Vehicle:
water
Details on exposure:
Route of administration: Gavage method (by oral).
Volume of administration: 5 ml/kg.bw. Animals in vehicle control group were given the same volume of drinking water.
Analytical verification of doses or concentrations:
yes
Details on analytical verification of doses or concentrations:
Based on the related requirements in OECD414 and according to the results of the preliminary test, three dose levels were used in this study including 100, 300 and 1000mg/kg.d. A concurrent vehicle control group was included at the same time.

The analytical check of test item concentrations was conducted on the first and final preparation. Formulations of different test-item concentrations and the vehicle control were sampled and analyzed. To be considered acceptable, the actual analysis results for at least 3/5 samples of each concentration are to be within ±10% of the nominal concentration and the relative standard deviation is not more than 10%.
The details about the methods used and the results obtained were shown in the analysis report attached in this final report. The results indicate that the concentrations of the prepared test item were within acceptable limits.
Details on mating procedure:
For each mating, two (or one) female rats and one male rat were put together at afternoon and separated in the next morning. The females were examined for presence of the sperms through vaginal smear method. The day of finding the sperms was defined as the day 0 of pregnancy (GD0). The female rats which failed to mate were put together with male rats and examined again until the number of pregnant rats met the requirements of the test. In the test, there were twenty-nine mated females in each group.
All treated animals survived until the end of the study were euthanized by CO2 inhalation. The spare animals were used for other studies.
Duration of treatment / exposure:
Experimental start date: July 11, 2018
(the beginning of animal mating)
Animal mating period: July 11~19, 2018
Animal dosage: July 17~August 07, 2018
Animal dissection: August 01~08, 2018
Soft tissue examination of fetus: Novembr 01~07, 2018
Skeleton examination of fetus: Octobor 31~Novembr 08, 2018
Preparation of test item: July 16~August 03, 2018
Frequency of treatment:
Schedule of administration: All animals were dosed daily in the morning during the day5~19 of pregnancy (GD5~GD19). The dosing volume for each animal was adjusted, based on the latest body weight.
Duration of test:
Experimental start date: July 11, 2018
(the beginning of animal mating)
Experimental completion date: November 08, 2018
Dose / conc.:
0 mg/kg bw/day
Remarks:
Solvent control
Dose / conc.:
100 mg/kg bw/day
Remarks:
Low dose level
Dose / conc.:
300 mg/kg bw/day
Remarks:
Middle dose level
Dose / conc.:
1 000 mg/kg bw/day
Remarks:
High dose level
No. of animals per sex per dose:
For each mating day, positive females were allocated to four groups based on body weight. All animals were identifiable by the individual cage card and be marked on fur at the same time. Details are shown as following:
Group Dose level (mg/kg.d) Sex Number of animals Animal Code

Solvent control 0 female 29 2000-2028
Low-dose level 100 female 29 2100-2128
Mid-dose level 300 female 29 2200-2228
High-dose level 1000 female 29 2300-2328
Control animals:
yes, concurrent vehicle
Details on study design:
Prior to the start of this study, a preliminary test was performed in this lab. In the test, one dose group of 1000mg/kg.d and solvent control group were included. There were five female rats in each group. All animals were treated by gavage for two weeks. The animals were observed daily and weighed once per three days.
No dead and any toxic symptom were observed in the all dosed animals. At the same time, the body weights of the animals in the dosed group had no significant decrease compared to the control.

In this test, animal drinking water was used as solvent. As the preparation, calculated the theoretical weight and range of the test item according to the prepared volume and concentration shown below, weighed the test item and placed into a calibrated grinding-mouth jar, poured some vehicle into the jar and stirred with a glass rod to dissolve test item completely. After that, washed the glass rod with vehicle and poured the washing water into the jar. Finally, added vehicle to the calibrated scale line on the jar, shook well and labeled it for use.
Group Dose (mg/kg.d) Volume of administration (ml/kg.bw) Theoretical concentration (mg/ml)
Solvent control 0 5 0
Low dose level 100 5 20.0
Middle dose level 300 5 60.0
High dose level 1000 5 200.0
Note: Theoretical Concentration = dose/volume of administration
Theoretical weight of test item = prepared volume (ml) x concentration (mg/ml)
Weight range (the lowest value) = theoretical weight (g) x 98%
Weight range (the highest value) = theoretical weight (g) x 102%
Based on the stability analysis result in the validation test, the test item formulations were prepared and stored at RT no longer than four days based on the stability analysis result in the validation test, and were subpackaged as use. After administration, the remainder will be kept temporarily in special cabinet in building A and was transported to external professional environmental protection company for disposal.
Maternal examinations:
Maternal Data:
-Number of animals at test start, number of animals surviving, number of pregnant animals, number of animals with total intrauterine mortality
-Clinical signs (by gestation day)
-Mortality (by gestation day), if any
-Body weight and body weight gain: mean ± SD.
-Corrected body weight on GD20 (body weight - gravid uterine weight) and corrected body weight gain: mean ± SD.
-Net body weight change (body weight on GD20 – body weight on GD5 – gravid uterine weight): mean ± SD.
-Food consumption: mean ± SD.
-Gravid uterine weight
Fetal examinations:
Caesarean Section and Necropsy Data:
-Number of corpora lutea: mean ± SD.
-Number of implantations: mean ± SD.
-Number of viable fetuses: mean ± SD.
-Percent of viable fetuses
-Number and percent of intrauterine mortality: Sub-divided into pre-implantation loss, post-implantation loss, early and late embryonic as well as fetal death.
-Fetal body weight (accuracy 0.001g): mean ± SD.
Statistics:
Calculate the average and standard deviation of the data for each group including body weight, food consumption, body weight change corrected for gravid uterine weight, number of corpora lutea and implantations, number of viable fetuses and body weight of fetuses, etc. All of these data were statistic analyzed by decision tree. The data about abnormal clinical sign, ratio of absorptive fetus, dead fetus and viable fetus, and incidence of individual anomalies were evaluated by the chi-square test. All statistical analysis was done in SPSS 17.0.

Calculatioins:
Pre-implantation loss: %, group mean
(Number of corpora lutea - Number of implantation)x100/Number of corpora lutea

Post-implantation loss: %, group mean
(Number of implantations - Number of viable fetuses)x100/Number of implantations

Sex distribution: %, group mean
Number of male (female) fetuses x 100/Number of fetuses

External abnormalities/litter: %, group mean
Number of fetuses with abnormality x 100/Number of fetuses

Visceral abnormalities/litter: %, group mean
Number of fetuses with abnormality x 100/Number of fetuses

Skeletal abnormalities/litter: %, group mean
Number of fetuses with abnormality x 100/Number of fetuses
Clinical signs:
effects observed, non-treatment-related
Description (incidence and severity):
All of rats in the dose groups had blue faeces after being administrated, but which was considered to be caused with the color of the test item and without adverse effect. All rats in the vehicle control group exhibited no symptoms.
Mortality:
no mortality observed
Description (incidence):
No animal in all groups was dead in the test.
Body weight and weight changes:
effects observed, non-treatment-related
Description (incidence and severity):
During the administration period, the body weight of pregnant rats in all dose groups had no significant difference compared with the control group (P>0.05). The body-weight gain of pregnant rats in the low- and high- dose groups had a significantly increased from GD8 to GD11 (P≤0.05 or P≥0.01), but that was considered without toxicological significance. At the same time, the mean corrected body-weight gain during the gestation period and the mean maternal net body-weight gain from the day of treatment (GD5) to the termination (GD20) in the pregnant rats in all dose groups had no significant difference compared with the control group (P≥0.05).
Food consumption and compound intake (if feeding study):
no effects observed
Description (incidence and severity):
No statistically significant difference in food consumption of the pregnant rat during the treated period was observed in all dose groups as compared with the vehicle control group (P>0.05).
Organ weight findings including organ / body weight ratios:
no effects observed
Description (incidence and severity):
No statistically significant difference in the gravid-uterine weight and total placenta weight was observed in all dosed groups, compared with the vehicle control group (P>0.05).
Number of abortions:
no effects observed
Description (incidence and severity):
Within all dose-groups, no statistically significant difference was observed in the percent of absorbed fetuses compared with the vehicle control group (P>0.05).
Pre- and post-implantation loss:
no effects observed
Description (incidence and severity):
no statistically significant increase was observed in the pre-implantation loss and the post-implantation loss compared with the control group (P>0.05).
Dead fetuses:
no effects observed
Description (incidence and severity):
Within all dose-groups, no statistically significant difference was observed in the percent of dead fetuses compared with the vehicle control group (P>0.05).
Dose descriptor:
NOAEL
Effect level:
1 000 mg/kg bw/day (nominal)
Based on:
test mat.
Basis for effect level:
body weight and weight gain
clinical signs
dead fetuses
food consumption and compound intake
mortality
number of abortions
organ weights and organ / body weight ratios
pre and post implantation loss
Fetal body weight changes:
no effects observed
Description (incidence and severity):
No statistically significant difference in body weight of live fetuses was observed in all dosed groups, compared with the control group (P>0.05).
Changes in sex ratio:
no effects observed
Description (incidence and severity):
No statistically significant difference in sex distribution of live fetuses was observed in all dosed groups, compared with the control group (P>0.05).
External malformations:
no effects observed
Skeletal malformations:
no effects observed
Other effects:
effects observed, non-treatment-related
Description (incidence and severity):
One fetus respectively in the low- and high-dose groups showed signs of anury, 2, 4, 2 and 3 fetuses in the control group, low-, mid- and high- dose groups showed signs of hydronephrosis in one or double kidneys, but the frequency of these abnormalities in the dose groups had no significant difference compared with the control group (P>0.05) and which were considered as incidental findings.
Dose descriptor:
NOAEL
Effect level:
1 000 mg/kg bw/day
Based on:
test mat.
Sex:
male/female
Basis for effect level:
changes in sex ratio
fetal/pup body weight changes
external malformations
skeletal malformations
visceral malformations
Abnormalities:
effects observed, non-treatment-related
Description (incidence and severity):
One fetus respectively in the low- and high- dose groups showed signs of anury, 2, 4, 2, and 3 fetuses in the control group, low-, mid- and high- dose groups showed signs of hydronephrosis in one or double kidneys, but the frequency of these abnormalities in the dose groups had no significant difference compared with the control group (P>0.05) and which were considered as incidental findings. No adverse effect attributable to treatment was observed across all groups with respect to external, soft-tissue and skeletal malformations or variations except that some examined fetuses had less than six sternal ossification points, but there was no difference in the mean number of sternal ossification points in all dosed groups (P>0.05).
Developmental effects observed:
no
Lowest effective dose / conc.:
100 mg/kg bw/day
Treatment related:
no

Table 1-1. Observation results of animal symptoms (symptoms/animal number)

Gestation day Vehicle control Low-dose Mid-dose Hgih-dose
0 mg/kg.d. 100 mg/kg.d. 300 mg/kg.d. 1000 mg/kg.d.
Number# 29 29 29 29
GD0-4 - - - -
GD5 - - - -
GD6 - B/29** B/29** B/29**
GD7 - B/29** B/29** B/29**
GD8 - B/29** B/29** B/29**
GD9 - B/29** B/29** B/29**
GD10 - B/29** B/29** B/29**
GD11 - B/29** B/29** B/29**
GD12 - B/29** B/29** B/29**
GD13 - B/29** B/29** B/29**
GD14 - B/29** B/29** B/29**
GD15 - B/29** B/29** B/29**
GD16 - B/29** B/29** B/29**
GD17 - B/29** B/29** B/29**
GD18 - B/29** B/29** B/29**
GD19 - B/29** B/29** B/29**
GD20 - B/29** B/29** B/29**

Note: #Number of all tested rats including non-pregnant females

GD5~19 are dosing period; GD20 is the day of scheduled kill;

---: No symptom; B: Blue faeces

Statistic analysis by Chi-square test in SPSS17.0;

Compared with the control group, **-p≤0.01.

Table 1-2. Body weight and body-weight gain of pregnant rats (g)

Gestation day Vehicle control Low-dose Mid-dose Hgih-dose
0 mg/kg.d. 100 mg/kg.d. 300 mg/kg.d. 1000 mg/kg.d.
Number of pregnant rats 26 27 27 27
GD0 292.1±17.7 294.9±23.4 289.4±24.6 292.2±23.3
GD5 318.0±20.7 322.7±26.5 321.0±22.4 316.1±25.7
GD8 328.7±19.0 333.8±25.6 334.2±22.6 330.1±26.3
GD11 342.6±19.5 352.9±27.2 351.9±25.0 350.0±27.8
GD14 360.0±22.2 368.4±27.4 367.7±26.5 364.0±31.5
GD17 393.5±27.8 400.9±30.1 401.5±30.4 394.8±35.8
GD20 442.9±33.5 452.8±33.0 448.0±35.6 443.4±43.2
GD5-8 10.8±5.4 11.1±6.7 13.3±6.0 14.0±6.0
GD8-11 13.9±8.4 19.1±6.1 17.6±8.3 19.8±7.4**
GD11-14 17.3±8.3 15.5±5.5 15.9±5.7 14.1±8.2
GD14-17 33.5±8.6 32.5±8.0 33.7±7.5 30.7±8.6
GD17-20 49.5±10.3 51.9±8.0 46.5±9.8 48.6±12.3
GD5-20 125.0±20.5 130.1±15.8 127.0±22.8 127.3±30.0

Corrected

body-weight on GD20

 355.4±22.7 363.8±27.0 363.6±26.8 358.0±35.0

Corrected

body-weight gain

 63.3±13.0 68.9±11.8 74.2±25.0 65.8±23.3

Net body-weight change

 37.4±8.9 41.1±11.8 42.7±12.3 41.9±21.2

Note: Data expressed as mean ± SD

Statisctic analysis by ANOVA, followed by Duncan test as p<0.05 in SPSS17.0;

Compared woth the control group, *-p≤0.05, **-p≤0.01

Corrected body-weight on GD20 = Body weight on GD20 - Gravid uterine weight

Corrected body-weight gain = Correted Body weight on GD20 - Body weight on GD0

Net body-weight change = Body weight on GD20 - Body weight on GD5 - Gravid uterine weight

Table 1-3. Food consumption of animals (g/day)

Gestation day Vehicle control Low-dose Mid-dose Hgih-dose
0 mg/kg.d. 100 mg/kg.d. 300 mg/kg.d. 1000 mg/kg.d.

Number of

pregnant rats

 26 27 27 27
GD7-8 23.6±3.0 25.8±4.2 26.0±4.1 24.3±4.7
GD10-11 24.5±3.8 25.6±3.9 26.2±4.9 25.6±5.2
GD13-14 23.7±3.1 25.4±2.8 26.1±4.4 26.0±4.2
GD16-17 27.6±3.3 27.0±4.2 28.7±5.3 28.4±4.3
GD19-20 26.9±3.7 27.3±3.3 27.4±4.0 27.5±4.5

Note: Data expressed as mean ± SD

Statisctic analysis by ANOVA, followed by Duncan test as p<0.05 in SPSS17.0.

Table 1-4. The devlopmental endpoint results

Parameter Vehicle control Low-dose Mid-dose Hgih-dose
0 mg/kg.d. 100 mg/kg.d. 300 mg/kg.d. 1000 mg/kg.d.
Mated female (n) 29 29 29 29
Pregnant female (n) 26 27 27 27
Corpara lutea        
Total number 438 468 440 444
Mean±SD 16.8±3.3 17.3±2.8 16.3±3.6 16.4±3.1
Implantation        
Total number 405 431 406 410
Mean±SD 15.6±3.2 16.0±2.6 15.0±3.4 15.2±3.1
Gravid uterine weight (g)        
Mean±SD 87.5±18.3A 89.0±14.1 84.4±20.6 85.4±18.0
Total placental weight (g)        
Mean±SD 11.6±2.7A 11.5±2.4 10.7±2.8 11.1±2.5
Live fetus        
Number of litters 26 27 27 27
Total number 396 418 393 397
Mean ± SD 15.2±3.3 15.5±2.6 14.6±3.5 14.7±3.1
Percent (%) 97.8(396/405)C 97.0(418/431) 96.8(393/406) 96.8(397/410)
Absorbed fetus        
Total number1 7 9 10 12
Mean ± SD 8 13 13 13
Percent (%) 2.0(8/405)C 3.0(13/431) 3.2(13/406) 3.2(13/410)
Dead fetus        
Total number2 1 0 0 0
Mean ± SD 1 0 0 0
Percent (%) 0.2(1/405)C 0(0/431) 0(0/406) 0(0/410)
Pre-implantation loss (%) 0.2(1/405)C 7.9(37/468) 7.7.(34/440) 7.7.(34/444)
Post-implantation loss(%) 2.2(9/405)C 3.0(13/431) 3.2(13/406) 3.2(13/410)

Note: 1Including early absorbed fetuses and late absorbed fetuses

2Including early dead fetuses and late dead fetuses

CStatistic analysis by Chi-square test in SPSS17.0;

AStatisctic analysis by ANOVA, followed by Duncan test as p<0.05 in SPSS17.0.

Compared with the control group, *-p≤0.05

Table 1-5. Fetal examination results

Parameter Vehicle control Low-dose Mid-dose Hgih-dose
0 mg/kg.d. 100 mg/kg.d. 300 mg/kg.d. 1000 mg/kg.d.
Body weight of fetus (g)        
Mean ± SD 3.59±0.27 3.68±0.26 3.65±0.25 3.68±0.27
Sex        
Number of male fetuses 199 195 198 212
Sex distribution(%) (males/total) 50.3(199/396)C 46.7(195/418) 50.4(198/393) 53.4(212/397)
Number of female fetuses 197 223 195 185
Sex distribution(%) (females/total) 49.7(197/3396) 53.3(223/418) 49.6(195/393) 46.6(185/397)
External exam        
Number of examined fetuses/litter 396/26 418/27 393/27 393/27
Number of external normal fetuses 396 417 393 396
Number of external abnormal fetuses/litter 2/1 4/2 2/1 3/2
Anury(%) 0(0/396)C 0.2(1/418) 0(0/393) 0.3(1/397)
External abnormalities (%) 0(0/396)C 0.2(1/418) 0(0/393) 0.3(1/397)
External abnormalities litter (%) 0(0/26)C 3.7(1/27) 0(0/27) 3.7(1/27)
Soft tissue exam        
Number of examined fetuses/litter 205/26 216/27 203/27 202/27
Number of visceral normal fetuses 203 212 201 199
Number of visceral abnormal fetuses/litter 2/1 4/2 2/1 3/2
left side pyelectasis (%) 1.0(2/205)C 0(0/216) 1.0(2/203) 0.5(1/202)
right side pyelectasis (%) 0(0/205)C 0.5(1/216) 0(0/203) 0.5(1/202)
bilateral pyelectasis (%) 0(0/205)C 1.4(3/216) 0(0/203) 0.5(1/202)
Visceral abnormalities (%) 1.0(2/205)C 1.9(4/216) 1.0(2/203) 1.5(3/202)
Visceral abnormalities litter(%) 3.8(1/26)C 7.4(2/27) 3.7(1/27) 7.4(2/27)
Skeleton exam        
Number of examined fetuses/litter 191/26 202/27 190/26 195/27
Number of skeletal normal fetuses 191 202 190 195
Skeletal abnormalities (%) 0 0 0 0
Sternal ossification points        
Mean ± SD 5.62±0.39A 5.57±0.42 5.62±0.32 5.63±0.49

Note: CStatistic analysis by Chi-square test in SPSS17.0;

AStatisctic analysis by ANOVA, followed by Duncan test as p<0.05 in SPSS17.0.

Table 2-1. Individual body weight (g)

Animal codes GD0 GD5 GD8 GD11 GD14 GD17 GD20
2000 256 283 303 323 336 360 407
2001 276 290 301 320 338 366 426
2002 277 292 310 323 331 361 419
2003 285 310 321 331 365 402 460
2004 286 305 310 323 344 369 419
2005 292 302 310 318 328 339 357
2006 294 308 328 340 360 390 439
2007 308 335 353 372 391 423 481
2008 323 349 360 376 384 420 468
2009 271 295 304 310 313 310 310
2010 272 296 315 324 340 375 420
2011 291 326 332 340 320 336 336
2012 291 317 324 331 349 378 422
2013 301 323 329 350 374 416 470
2014 306 351 353 380 400 432 488
2015 306 323 331 337 352 397 447
2016 338 373 381 372 416 464 527
2017 274 310 320 344 350 393 452
2018 278 313 320 342 360 396 446
2019 287 301 308 320 337 360 398
2020 288 332 342 362 380 422 456
2021 296 320 337 360 362 392 443
2022 299 325 330 352 371 420 466
2023 305 335 341 360 373 408 468
2024 310 340 347 357 364 361 362
2025 275 310 328 324 342 378 409
2026 276 310 318 328 345 373 432
2027 293 314 328 342 356 396 444
2028 313 340 346 354 375 400 452
2100 260 278 300 304 324 352 395
2101 276 307 328 338 353 386 442
2102 277 291 316 328 340 383 432
2103 283 305 316 338 358 391 450
2104 286 315 323 354 370 401 453
2105 291 305 324 345 367 396 457
2106 295 320 331 353 371 400 457
2107 306 340 350 380 391 430 480
2108 323 360 372 388 409 436 481
2109 267 297 309 330 341 381 435
2110 274 308 320 330 352 387 438
2111 289 320 331 348 378 387 454
2112 293 310 326 334 336 340 358
2113 299 313 327 351 363 403 455
2114 309 327 345 344 345 350 334
2115 295 318 330 350 371 400 446
2116 373 403 421 438 457 496 554
2117 270 300 305 320 330 360 406
2118 283 313 322 339 350 377 412
2119 286 315 320 342 358 382 440
2120 289 325 325 346 364 389 446
2121 296 316 320 334 350 376 424
2122 301 329 340 360 370 410 466
2123 305 336 340 362 376 406 442
2124 311 340 340 364 371 402 446
2125 339 378 378 400 410 452 506
2126 280 310 322 351 356 395 438
2127 293 320 333 350 367 396 456
2128 315 350 369 386 400 450 514
2200 264 289 298 315 326 365 410
2201 274 297 320 336 358 385 432
2202 278 296 321 338 354 390 431
2203 283 305 325 346 360 395 451
2204 286 300 310 334 344 382 428
2205 290 315 330 360 377 404 446
2206 296 328 350 368 356 383 381
2207 302 320 340 375 389 426 478
2208 328 356 378 399 416 446 500
2209 263 296 305 320 342 370 418
2210 277 305 310 322 350 390 444
2211 287 315 324 326 331 350 362
2212 296 310 326 342 356 383 413
2213 298 320 342 362 377 416 462
2214 332 370 388 387 416 455 503
2215 285 323 330 349 366 392 449
2216 208 327 345 356 383 417 468
2217 270 305 321 326 343 367 415
2218 284 337 347 370 384 413 466
2219 285 303 312 322 332 356 392
2220 291 320 329 347 362 401 456
2221 294 314 320 340 351 378 421
2222 301 346 360 382 400 446 492
2223 305 337 347 370 384 416 452
2224 320 360 366 396 412 463 518
2225 332 366 371 393 406 442 486
2226 290 316 328 335 350 390 439
2227 292 318 331 352 360 402 461
2228 326 363 370 399 400 387 391
2300 269 289 300 323 343 370 416
2301 270 300 323 334 341 376 420
2302 279 305 318 344 350 382 442
2303 282 304 316 328 346 370 423
2304 287 313 331 355 372 414 462
2305 288 305 320 345 376 408 470
2306 298 318 333 355 370 400 452
2307 300 334 358 378 406 442 500
2308 349 374 389 413 436 468 526
2309 260 280 300 325 330 360 409
2310 283 300 316 320 335 370 397
2311 285 321 341 356 375 407 452
2312 297 312 330 343 358 399 440
2313 298 313 323 336 353 384 432
2314 258 289 300 313 313 312 307
2315 281 310 312 337 350 372 428
2316 257 278 294 314 330 350 406
2317 262 290 303 311 320 350 380
2318 284 310 330 351 366 399 462
2319 285 307 315 322 310 308 315
2320 291 313 320 346 350 392 344
2321 294 300 320 352 367 396 450
2322 304 316 321 342 355 387 441
2323 304 334 338 360 364 386 416
2324 330 355 378 398 406 446 493
2325 330 363 375 397 417 452 508
2326 290 326 332 357 372 401 461
2327 291 319 324 358 371 406 363
2328 345 380 392 409 424 450 486

Table 2-2. Individual body weight gains (g)

Animal codes GD5-8 GD8-11 GD11-14 GD14-17 GD17-20 GD5-20 Corrected body weight on GD20 Corrected body weight gain Net body weight change
2000 20 20 13 24 47 124 317.154 61.154 34.154
2001 11 19 18 28 60 136 339.434 63.434 49.434
2002 18 13 8 30 58 127 330.362 53.362 38.362
2003 11 10 34 37 58 150 356.019 71.019 46.019
2004 5 13 21 25 50 114 325.344 39.344 20.344
2005 8 8 10 11 18 55 337.794 47.794 37.794
2006 20 12 20 30 49 131 358.555 64.555 50.555
2007 18 19 19 32 58 146 382.344 74.344 47.344
2008 11 16 8 36 48 119 385.620 62.620 36.620
2009 9 6 3 -3 0 15 - - -
2010 19 9 16 35 45 124 338.786 66.786 42.786
2011 6 8 -20 16 0 10 - - -
2012 7 7 18 29 44 105 350.332 59.332 33.332
2013 6 21 24 42 54 147 373.353 72.353 50.353
2014 2 27 20 32 56 137 381.222 75.222 30.222
2015 8 6 15 45 50 124 346.750 40.750 23.750
2016 8 -9 44 48 63 154 423.443 85.443 50.443
2017 10 24 6 43 59 142 356.779 82.779 46.779
2018 7 22 18 36 50 133 356.765 78.765 43.765
2019 7 12 17 23 38 97 330.952 43.952 29.952
2020 10 20 18 42 34 124 373.035 85.035 41.035
2021 17 23 2 30 51 123 342.738 46.738 22.738
2022 5 22 19 49 46 141 360.443 61.443 35.443
2023 6 19 13 35 60 133 366.134 61.134 31.134
2024 7 10 7 -3 1 22 - - -
2025 18 -4 18 36 31 99 343.857 68.857 33.857
2026 8 10 17 28 59 122 341.436 65.436 31.436
2027 14 14 14 40 48 130 351.351 58.351 37.351
2028 6 8 21 25 52 112 368.478 55.478 28.478
2100 22 4 20 28 43 117 328.945 68.945 50.945
2101 21 10 15 33 56 135 351.419 75.419 44.419
2102 25 12 12 43 49 141 329.855 52.855 38.855
2103 11 22 20 33 59 145 352.740 69.740 47.740
2104 8 31 16 31 52 138 355.453 69.453 40.453
2105 19 21 22 29 61 152 369.646 78.646 64.646
2106 11 22 18 29 57 137 371.350 76.350 51.350
2107 10 30 11 39 50 140 388.158 82.158 46.158
2108 12 16 21 27 45 121 408.609 85.609 48.609
2109 12 21 11 40 54 138 341.342 74.342 44.342
2110 12 10 22 35 51 130 346.575 72.575 38.575
2111 11 17 30 9 67 134 371.106 82.106 51.106
2112 16 8 2 4 18 48 - - -
2113 14 24 12 40 52 142 361.109 62.109 48.109
2114 18 -1 1 5 -16 7 - - -
2115 12 20 21 29 46 128 360.551 65.551 42.551
2116 18 17 19 39 58 151 445.890 72.890 42.890
2117 5 15 10 30 46 106 321.761 51.761 21.761
2118 9 17 11 27 35 99 359.109 76.109 46.109
2119 5 22 16 24 58 125 354.072 68.072 39.072
2120 0 21 18 25 57 121 347.447 58.447 22.447
2121 4 14 16 26 48 108 341.210 45.210 25.210
2122 11 20 10 40 56 137 347.571 46.571 18.571
2123 4 22 14 30 36 106 365.931 60.931 29.931
2124 0 24 7 31 44 106 370.260 59.260 30.260
2125 0 22 10 42 54 128 399.240 60.240 21.240
2126 12 29 5 39 43 128 362.240 82.240 52.240
2127 13 17 17 29 60 136 364.113 71.113 44.113
2128 19 17 14 50 64 164 405.830 90.830 55.830
2200 9 17 11 39 45 121 312.228 48.228 23.228
2201 23 16 22 27 50 138 350.727 76.727 53.727
2202 25 17 16 36 41 135 350.205 72.205 54.205
2203 20 21 14 35 56 146 356.365 73.362 51.362
2204 10 24 10 38 46 128 331.831 45.831 31.831
2205 15 30 17 27 42 131 369.951 79.951 54.951
2206 22 18 -12 27 -2 53 - - -
2207 20 35 14 37 52 158 380.645 78.645 60.645
2208 22 21 17 30 54 144 398.114 70.114 42.114
2209 9 15 22 28 48 122 324.661 61.661 28.661
2210 5 12 28 40 54 139 346.883 69.883 41.883
2211 9 2 5 19 12 47 354.496 67.496 39.496
2212 16 16 14 27 30 103 372.138 76.134 62.138
2213 22 20 15 39 46 142 375.962 77.962 55.962
2214 18 -1 29 39 48 133 404.845 72.845 34.845
2215 7 19 17 26 57 126 366.638 81.638 43.638
2216 18 11 27 34 51 141 384.618 176.618 57.618
2217 16 5 17 24 48 110 331.257 61.257 26.257
2218 10 23 14 29 53 129 382.504 98.504 45.504
2219 9 10 10 24 36 89 321.312 36.312 18.312
2220 9 18 15 39 55 136 357.101 66.101 337.101
2221 6 20 11 27 43 107 352.493 58.493 38.493
2222 14 22 18 46 46 146 399.534 98.534 53.534
2223 10 23 14 32 36 115 372.852 67.852 35.852
2224 6 30 16 51 55 158 406.180 86.180 46.180
2225 5 22 13 36 44 120 405.001 73.001 39.001
2226 12 7 15 40 49 123 339.320 49.320 23.320
2227 13 21 8 42 59 143 370.038 78.038 52.038
2228 7 29 1 -13 4 28 - - -
2300 11 23 20 27 46 127 335.075 66.075 46.075
2301 23 11 7 35 44 120 343.315 73.315 43.315
2302 13 26 6 32 60 137 345.224 66.224 40.224
2303 12 12 18 24 53 119 334.687 52.687 30.687
2304 18 24 17 42 48 149 364.354 77.354 51.354
2305 15 25 31 32 62 165 361.275 73.275 56.275
2306 15 22 15 30 52 134 379.124 81.124 61.124
2307 24 20 28 36 58 166 399.166 99.166 65.166
2308 15 24 23 32 58 152 413.790 64.790 39.790
2309 20 25 5 30 49 129 338.976 78.976 58.976
2310 16 4 15 35 27 97 327.142 44.142 27.142
2311 20 15 19 32 45 131 359.511 74.511 38.511
2312 18 13 15 41 41 128 346.103 49.103 34.103
2313 10 13 17 31 48 119 343.598 45.598 30.598
2314 11 13 0 -1 -5 18 - - -
2315 2 25 13 22 56 118 353.069 72.069 43.069
2316 16 20 16 20 56 128 328.755 71.755 50.755
2317 13 8 9 30 30 90 327.070 65.070 37.070
2318 20 21 15 33 63 152 365.190 81.190 55.190
2319 8 7 -12 -2 7 8 262.907 -22.093 -44.093
2320 7 26 4 42 -48 31 252.550 -38.450 -60.450
2321 20 32 15 29 54 150 368.430 74.430 68.430
2322 5 21 13 32 54 125 344.425 40.425 28.425
2323 4 22 4 22 30 82 - - -
2324 23 20 8 40 47 138 381.017 51.017 26.017
2325 12 22 20 35 56 145 413.683 83.683 50.683
2326 6 25 15 29 60 135 363.854 73.854 37.854
2327 5 34 13 35 -43 44 271.334 -19.666 -47.666
2328 12 17 15 26 36 106 447.454 102.454 67.454
Conclusions:
The exposure of gestating rats to different doses of CJ303 by gavage during GD5~GD19 did not result in any death or significant specific toxicity at the dose of 1000 mg/kg.d. At the same time, no treatment related effect on the body weight gain and food consumption of pregnant rats was observed. Based on these results, it is concluded that the test item had no maternal toxicity at this dose level.
In all dose groups, no adverse effect was observed in all prenatal reproductive parameters. The fetal examination showed that no adverse effect in the survival, body weight and sex distribution of live fetuses was observed in all dosed groups, additionally, no adverse effect attributable to treatment was observed across all groups with respect to external, soft-tissue and skeletal malformations or variations. Based on these results, it is concluded that the test item had no developmental toxicity and teratogenicity at the dose of 10000 mg/kg.d.
In conclusion, under the conditions of this investigation, CJ303 administered to pregnant SD rats by gavage in water, did not produce any dose-related maternal toxicity, teratogenic and embryo-/fetotoxicity at the dose of 1000 mg/kg.d.
Based on these findings, the following effect levels, No Observed Adverse Effect Level (NOAEL) were derived:
NOAEL(maternal toxicity): 1000 mg/kg bw.d
NOAEL(embryo-/fetotoxicity): 1000 mg/kg bw.d
NOAEL(teratogenicity): 1000 mg/kg bw.d
Executive summary:

Introduction

This study is conducted to detect maternal and developmental toxicity during the “critical” phase of organogenesis, in particular focused on structural abnormalities in and altered growth of the fetus caused by CJ303 after prenatal exposure. The method of this test was designed to be compatible with OECD414.

Method

This study was conducted in SD rats and all animals were SPF grade. Based on the results of a preliminary range finding test, the animals were treated in the main study with test item at doses of 100, 300 and 1000mg/kg.d. A concurrent vehicle control group was included in the study. There were 29 mated female rats in each group, which resulted in 26, 27, 27 and 27 pregnant rats in the vehicle control group and the low-, mid- and high-, respectively. In the test, all animals were administered the test item by gavage daily during the day 5~19 of pregnancy (GD5~GD19), and were euthanized with CO2 on GD20. After that, removed the uterus of each animal immediately ascertained the pregnancy status, weighed gravid uterine and total placenta, counted the number of corpora lutea, adsorptive fetuses, dead fetuses and viable fetuses for each pregnant animal. Each fetus was examined for external alterations, and the sex and body weight of each fetus were determined at the same time. The fetus was examined for soft tissue or skeleton after being prepared.

Results

No deaths or treatment-related clinical toxicity were observed during the course of this study. All of rats in dose groups had blue faeces after being administrated, but which was considered to be caused with the color of the test item and without adverse effect.

During the administration period, the mean body weight and body weight change of pregnant rats in all dose groups had no significant difference compared with the control group. At the same time, no significant effect in food consumption of the pregnant rat during the treated period was observed in all dose groups.

In all dose groups, no adverse effect was observed in all prenatal reproductive parameters.

The fetal examination showed that no adverse effect in body weight and sex distribution of live fetuses was observed in all dosed groups. No adverse effect attributable to treatment was observed across all groups with respect to external, soft-tissue and skeletal malformations or variations except that some examined fetuses had less than six sternal ossification points, but there was no difference in the men number of sternal ossification points, but there was no difference in the mean number of sternal ossification points in all dosed groups as compared with the control group.

Conclusion

In conclusion, under the conditions of this study, CJ303 administered to pregnant SD rats by gavage in water, had not produced any maternal toxicity, or teratogenic and embryo-/fetotoxicity at the dose of 1000 mg/kg.d.

Based on these findings, the following effect levels, No Observed Adverse Effect Level (NOAEL) were derived:

NOAEL(maternal toxicity): 1000 mg/kg bw.d

NOAEL(embryo-/fetotoxicity): 1000 mg/kg bw.d

NOAEL(teratogenicity): 1000 mg/kg bw.d

Effect on developmental toxicity: via oral route
Endpoint conclusion:
no adverse effect observed
Dose descriptor:
NOAEL
1 000 mg/kg bw/day
Study duration:
subacute
Species:
rat
Additional information

Effect on developmental toxicity: via oral route

The exposure of gestating rats to different doses of CJ303 by gavage during GD5~GD19 did not result in any death or significant specific toxicity at the dose of 1000 mg/kg.d. At the same time, no treatment related effect on the body weight gain and food consumption of pregnant rats was observed. Based on these results, it is concluded that the test item had no maternal toxicity at this dose level.

In all dose groups, no adverse effect was observed in all prenatal reproductive parameters. The fetal examination showed that no adverse effect in the survival, body weight and sex distribution of live fetuses was observed in all dosed groups, additionally, no adverse effect attributable to treatment was observed across all groups with respect to external, soft-tissue and skeletal malformations or variations. Based on these results, it is concluded that the test item had no developmental toxicity and teratogenicity at the dose of 10000 mg/kg.d.

In conclusion, under the conditions of this investigation, CJ303 administered to pregnant SD rats by gavage in water, did not produce any dose-related maternal toxicity, teratogenic and embryo-/fetotoxicity at the dose of 1000 mg/kg.d.

Justification for classification or non-classification

Additional information