NOAEL Studies Colorant

CI 19140 (Tartrazine) NOAEL Studies

INCI: CI 19140

CAS: 1934-21-0

Raw No Observed Adverse Effect Level endpoint records grouped by source. This page does not render calculated Margin of Safety values.

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COSMOS_DB 21 endpoints
Source Endpoint Type Value Unit Species Route Duration Study Type Reference
COSMOS_DB LOAEL 792 mg/kg bw/day mouse oral 2 year Chronic PAFA; CAP
COSMOS_DB LOAEL 8919 mg/kg bw/day mouse oral 2 year Chronic PAFA; FOOD CHEM TOXICOL 26:189-194
COSMOS_DB LOAEL 53 mg/kg bw/day rat oral 2 year Chronic PAFA; FOOD CHEM TOXICOL 26:179-187
COSMOS_DB NOAEL 750 mg/kg bw/day rat oral 448 day Chronic US FDA CFSAN PAFA; US FDA CFSAN PAFA Study
COSMOS_DB NOAEL 1000 mg/kg bw/day rabbit oral 29 day Developmental US FDA CFSAN PAFA; US FDA CFSAN PAFA Study
COSMOS_DB NOAEL 2500 mg/kg bw/day rat oral 730 day Chronic US FDA CFSAN PAFA; US FDA CFSAN PAFA Study
COSMOS_DB NOAEL 1500 mg/kg bw/day dog oral 730 day Chronic US FDA CFSAN PAFA; US FDA CFSAN PAFA Study
COSMOS_DB NOAEL 2641 mg/kg bw/day rat oral 875 day Carcinogenicity US FDA CFSAN PAFA; US FDA CFSAN PAFA Study
COSMOS_DB NOAEL 984 mg/kg bw/day rat oral 798 day Carcinogenicity US FDA CFSAN PAFA; US FDA CFSAN PAFA Study
COSMOS_DB NOAEL 7500 mg/kg bw/day mouse oral 730 day Chronic US FDA CFSAN PAFA; US FDA CFSAN PAFA Study
COSMOS_DB NOAEL 5000 mg/kg bw/day rat oral 91 day Subchronic US FDA CFSAN PAFA; US FDA CFSAN PAFA Study
COSMOS_DB NOAEL 2190 mg/kg bw/day rat oral 728 day Carcinogenicity US FDA CFSAN PAFA; US FDA CFSAN PAFA Study
COSMOS_DB NOAEL 1105 mg/kg bw/day rat oral 798 day Chronic US FDA CFSAN PAFA; US FDA CFSAN PAFA Study
COSMOS_DB NOAEL 2995 mg/kg bw/day rat oral 875 day Chronic US FDA CFSAN PAFA; US FDA CFSAN PAFA Study
COSMOS_DB NOAEL 8919 mg/kg bw/day mouse oral 728 day Chronic US FDA CFSAN PAFA; US FDA CFSAN PAFA Study
COSMOS_DB NOAEL 500 mg/kg bw/day rat oral 125 day Neurotoxicity US FDA CFSAN PAFA; US FDA CFSAN PAFA Study
COSMOS_DB NOAEL 1064 mg/kg bw/day rat oral 20 day Developmental US FDA CFSAN PAFA; US FDA CFSAN PAFA Study
COSMOS_DB NOAEL 773 mg/kg bw/day mouse oral 117 day Reproductive US FDA CFSAN PAFA; US FDA CFSAN PAFA Study
COSMOS_DB NOAEL 2418 mg/kg bw/day mouse oral 2 year Chronic PAFA; FOOD CHEM TOXICOL 26:189-194
COSMOS_DB NOAEL 15 mg/kg bw/day rat oral 30 day Short Term Toxicity US FDA CFSAN PAFA; US FDA CFSAN PAFA Study
COSMOS_DB NOAEL 7.5 mg/kg bw/day rat oral 322 day Chronic US FDA CFSAN PAFA; US FDA CFSAN PAFA Study
EFSA_OpenFoodTox_EFSA_ReferencePoints.xlsx 1 endpoint
Source Endpoint Type Value Unit Species Route Duration Study Type Reference
EFSA_OpenFoodTox_EFSA_ReferencePoints.xlsx NOAEL =984 mg/kg bw/day Rat - - chronic/long term toxicity EFSA FEEDAP - 2016 - OutputID 2877 - body weight - systemic - Safety and efficacy of tartrazine (E 102) for cats and dogs, ornamental fish, grain-eating ornamental birds and small rodents - doi:10.2903/j.efsa.2016.4613
EFSA_OpenFoodTox_EFSA_ReferenceValues.xlsx 4 endpoints
Source Endpoint Type Value Unit Species Route Duration Study Type Reference
EFSA_OpenFoodTox_EFSA_ReferenceValues.xlsx ADI <=7.5 mg/kg bw/day Consumers - - ADI EFSA ANS - 2009 - OutputID 395 - Consumers - Scientific Opinion on the re-evaluation Tartrazine (E 102) - doi:10.2903/j.efsa.2009.1331
EFSA_OpenFoodTox_EFSA_ReferenceValues.xlsx ADI <=10 mg/kg bw/day Consumers - - ADI EFSA FEEDAP - 2016 - OutputID 2877 - Consumers - Safety and efficacy of tartrazine (E 102) for cats and dogs, ornamental fish, grain-eating ornamental birds and small rodents - doi:10.2903/j.efsa.2016.4613
EFSA_OpenFoodTox_EFSA_ReferenceValues.xlsx ADI <=7.5 mg/kg bw/day Consumers - - ADI EFSA ANS - 2009 - OutputID 395 - Consumers - Scientific Opinion on the re-evaluation Tartrazine (E 102) - doi:10.2903/j.efsa.2009.1331
EFSA_OpenFoodTox_EFSA_ReferenceValues.xlsx ADI <=10 mg/kg bw/day Consumers - - ADI EFSA FEEDAP - 2016 - OutputID 2877 - Consumers - Safety and efficacy of tartrazine (E 102) for cats and dogs, ornamental fish, grain-eating ornamental birds and small rodents - doi:10.2903/j.efsa.2016.4613
NTP_ICE_acute_oral 1 endpoint
Source Endpoint Type Value Unit Species Route Duration Study Type Reference
NTP_ICE_acute_oral LD50 >2000 mg/kg bw Rat oral acute Rat Acute Oral Toxicity record_id=acute_oral_3747; row=2223; data_type=In Vivo; mixture=Chemical; chemical_name=FD&C Yellow 5; preferred_name=C.I. Acid Yellow 23; dtxsid=DTXSID1021455; url_comptox=https://comptox.epa.gov/dashboard/chemical/details/DTXSID1021455; source_file=acute_oral.xlsx
NTP_ICE_endocrine 1 endpoint
Source Endpoint Type Value Unit Species Route Duration Study Type Reference
NTP_ICE_endocrine Model Score 0 unitless - - - ARPathway2016; AR Pathway Model, Antagonist sheet=Integrated_approaches; excel_row=6066; RecordID=ARPathway2016_966; DatasetName=ARPathway2016; DTXSID=DTXSID1021455; Assay=AR Pathway Model, Antagonist; Endpoint=Model Score; Response=0; Response_Unit=Unitless; URL_CompTox=https://comptox.epa.gov/dashboard/chemical/details/DTXSID1021455
SCCNFP_vision_codex 16 endpoints
Source Endpoint Type Value Unit Species Route Duration Study Type Reference
SCCNFP_vision_codex NOAEL =5 % - dermal Sub-chronic repeated dose toxicity {"citation":"Ref.: 2 2","dose":"No NOAEL in mg/kg/day could be derived due to the missing data on water consumption.","effect":"SCCNFP/0786/04 Evaluation and opinion on Acid Yellow 23 _____________________________________________________________________________________________ 7 of the 5 % group animals that died during the experiment. No information was given on histology of animals at the end of treatment. No NOAEL in mg/kg/day could be derived due to the missing data on water consumption. Ref.: 2 2.3.8. Sub-chronic dermal toxicity No data 2.3.9. Sub-chronic inhalation toxicity No data 2.3.10. Chronic toxicity No chronic study was provided. Several carcinogenicity studies were provided but there were many data gaps. It would seem from these studies that other than coloured fur and faeces there were no dose-related effects from Acid Yellow 23. A NOAEL was derived of 5% in food, equivalent to 2640 and 3348 mg/kg/day in m","page":7,"pdf":"out260_en.pdf","row_type":"noael_study","study_id":"out260_en_noael_001"}
SCCNFP_vision_codex NOAEL >1000 mg/kg/day rat oral - NOAEL study {"citation":"Ref.: 7 Mated, sperm-positive female rats were dosed with 0","dose":"The mean daily food consumption was significantly higher in the 1000 mg/kg dose group, indicating an effect on food utilization.","effect":"e-related differences between treatment groups and control group were noted in behaviour, external maternal findings, and body weight. The mean daily food consumption was significantly higher in the 1000 mg/kg dose group, indicating an effect on food utilization. No dose- related changes were observed in pregnancy rate, implantation efficiency, maternal findings, foetal viability or foetal development. Examination of offspring for external and skeletal variations revealed no dose-related increase of incidence. The NOAEL for teratogenicity of Acid Yellow 23 was > 1000 mg/kg/day in this study. The study is regarded as valid and relevant for risk assessment, as a sufficient number of animals and relevant endpoints were examined. Ref.: 7 Mated, sperm-positive female rats were dosed with 0.05, 0.1, 0.2, 0.4, or 0.7 % in drinking water (equivalent to 67 –1064 mg/kg/ day) with Acid Yellow 23, from GD 0 to 19. No unusual behaviour or remarkable external maternal findings were noted. Mean daily food consumption and body weight gain wer","page":13,"pdf":"out260_en.pdf","row_type":"noael_study","study_id":"out260_en_noael_003"}
SCCNFP_vision_codex NOAEL >0.7 % rat oral chronic reproductive toxicity {"citation":"Ref.: 8 A 2-generation chronic toxicity/carcinogenicity study was conducted with different concentrations of Acid Yellow 23","dose":"A significant increase in fluid consumption was observed in the 0.2, 0.4, and 0.7 % dose groups.","effect":"able external maternal findings were noted. Mean daily food consumption and body weight gain were similar in all groups. A significant increase in fluid consumption was observed in the 0.2, 0.4, and 0.7 % dose groups. No dose-related changes were observed in pregnancy rate, implantation efficiency, foetal viability or foetal development. Reproductive findings at necropsy were unremarkable. Examination of offspring for external, skeletal and soft tissue variations revealed no dose-related increase of incidence. The NOAEL for teratogenic toxicity of Acid Yellow 23 was > 0.7% corresponding to 1064 mg/kg/day based on the mean fluid consumption in this study. A sufficient number of animals was regarded and relevant endpoints were examined. The study is judged as valid and relevant for risk assessment. Ref.: 8 A 2-generation chronic toxicity/carcinogenicity study was conducted with different concentrations of Acid Yellow 23. Male and female rats were fed a basal diet (control group) or basal diet blended with commercial Acid Yellow 2","page":13,"pdf":"out260_en.pdf","row_type":"noael_study","study_id":"out260_en_noael_004"}
SCCNFP_vision_codex NOAEL =2640 mg/kg rat oral - carcinogenicity {"citation":"Ref.: 29 Human studies No data","dose":"Safety evaluation CALCULATION OF THE MARGIN OF SAFETY (Acid Yellow 23) (Semi-permanent) Maximum absorption through the skin A (µg/cm2) = 13.2 µg/cm2 Typical body weight of human = 60 kg Skin Area surface SAS (cm2) = 700 cm2 Dermal absorption per treatment SAS x A x 0.001 = 9.24 mg Systemic exposure dose (SED) SAS x A x 0.001/60 = 0.154 mg/kg No...","effect":"d not demonstrate carcinogenic effects. Ref.: 29 Human studies No data. 2.10. Special investigations No data 2.11. Safety evaluation CALCULATION OF THE MARGIN OF SAFETY (Acid Yellow 23) (Semi-permanent) Maximum absorption through the skin A (µg/cm2) = 13.2 µg/cm2 Typical body weight of human = 60 kg Skin Area surface SAS (cm2) = 700 cm2 Dermal absorption per treatment SAS x A x 0.001 = 9.24 mg Systemic exposure dose (SED) SAS x A x 0.001/60 = 0.154 mg/kg No observed effect level (mg/kg) NOEL = 2640 mg/kg (rat, carcinogenicity, oral) Margin of Safety NOAEL / SED = 17143 2.12. Conclusions Physical and chemical characterisation The information provided on the compound is largely incomplete and confusing regarding purity and physical constants. The stability data are not acceptable. The basic toxicity data for Acid Yellow 23 is poor. A NOAEL for Acid Yellow 23 was derived of 5% in food, equivalent to 2640 and 3348 mg/kg/day in male and female rats respectively. Acid Yellow 23 was not consider","page":20,"pdf":"out260_en.pdf","row_type":"noael_study","study_id":"out260_en_noael_006"}
SCCNFP_vision_codex NOAEL =5 % - dermal Sub-chronic repeated dose toxicity {"citation":"Ref.: 2 2","dose":"No NOAEL in mg/kg/day could be derived due to the missing data on water consumption.","effect":"SCCNFP/0786/04 Evaluation and opinion on Acid Yellow 23 _____________________________________________________________________________________________ 7 of the 5 % group animals that died during the experiment. No information was given on histology of animals at the end of treatment. No NOAEL in mg/kg/day could be derived due to the missing data on water consumption. Ref.: 2 2.3.8. Sub-chronic dermal toxicity No data 2.3.9. Sub-chronic inhalation toxicity No data 2.3.10. Chronic toxicity No chronic study was provided. Several carcinogenicity studies were provided but there were many data gaps. It would seem from these studies that other than coloured fur and faeces there were no dose-related effects from Acid Yellow 23. A NOAEL was derived of 5% in food, equivalent to 2640 and 3348 mg/kg/day in m","page":7,"pdf":"out260_en.pdf","row_type":"noael_study","study_id":"out260_en_noael_001"}
SCCNFP_vision_codex NOAEL >1000 mg/kg/day rat oral - NOAEL study {"citation":"Ref.: 7 Mated, sperm-positive female rats were dosed with 0","dose":"The mean daily food consumption was significantly higher in the 1000 mg/kg dose group, indicating an effect on food utilization.","effect":"e-related differences between treatment groups and control group were noted in behaviour, external maternal findings, and body weight. The mean daily food consumption was significantly higher in the 1000 mg/kg dose group, indicating an effect on food utilization. No dose- related changes were observed in pregnancy rate, implantation efficiency, maternal findings, foetal viability or foetal development. Examination of offspring for external and skeletal variations revealed no dose-related increase of incidence. The NOAEL for teratogenicity of Acid Yellow 23 was > 1000 mg/kg/day in this study. The study is regarded as valid and relevant for risk assessment, as a sufficient number of animals and relevant endpoints were examined. Ref.: 7 Mated, sperm-positive female rats were dosed with 0.05, 0.1, 0.2, 0.4, or 0.7 % in drinking water (equivalent to 67 –1064 mg/kg/ day) with Acid Yellow 23, from GD 0 to 19. No unusual behaviour or remarkable external maternal findings were noted. Mean daily food consumption and body weight gain wer","page":13,"pdf":"out260_en.pdf","row_type":"noael_study","study_id":"out260_en_noael_003"}
SCCNFP_vision_codex NOAEL >0.7 % rat oral chronic reproductive toxicity {"citation":"Ref.: 8 A 2-generation chronic toxicity/carcinogenicity study was conducted with different concentrations of Acid Yellow 23","dose":"A significant increase in fluid consumption was observed in the 0.2, 0.4, and 0.7 % dose groups.","effect":"able external maternal findings were noted. Mean daily food consumption and body weight gain were similar in all groups. A significant increase in fluid consumption was observed in the 0.2, 0.4, and 0.7 % dose groups. No dose-related changes were observed in pregnancy rate, implantation efficiency, foetal viability or foetal development. Reproductive findings at necropsy were unremarkable. Examination of offspring for external, skeletal and soft tissue variations revealed no dose-related increase of incidence. The NOAEL for teratogenic toxicity of Acid Yellow 23 was > 0.7% corresponding to 1064 mg/kg/day based on the mean fluid consumption in this study. A sufficient number of animals was regarded and relevant endpoints were examined. The study is judged as valid and relevant for risk assessment. Ref.: 8 A 2-generation chronic toxicity/carcinogenicity study was conducted with different concentrations of Acid Yellow 23. Male and female rats were fed a basal diet (control group) or basal diet blended with commercial Acid Yellow 2","page":13,"pdf":"out260_en.pdf","row_type":"noael_study","study_id":"out260_en_noael_004"}
SCCNFP_vision_codex NOAEL =2640 mg/kg rat oral - carcinogenicity {"citation":"Ref.: 29 Human studies No data","dose":"Safety evaluation CALCULATION OF THE MARGIN OF SAFETY (Acid Yellow 23) (Semi-permanent) Maximum absorption through the skin A (µg/cm2) = 13.2 µg/cm2 Typical body weight of human = 60 kg Skin Area surface SAS (cm2) = 700 cm2 Dermal absorption per treatment SAS x A x 0.001 = 9.24 mg Systemic exposure dose (SED) SAS x A x 0.001/60 = 0.154 mg/kg No...","effect":"d not demonstrate carcinogenic effects. Ref.: 29 Human studies No data. 2.10. Special investigations No data 2.11. Safety evaluation CALCULATION OF THE MARGIN OF SAFETY (Acid Yellow 23) (Semi-permanent) Maximum absorption through the skin A (µg/cm2) = 13.2 µg/cm2 Typical body weight of human = 60 kg Skin Area surface SAS (cm2) = 700 cm2 Dermal absorption per treatment SAS x A x 0.001 = 9.24 mg Systemic exposure dose (SED) SAS x A x 0.001/60 = 0.154 mg/kg No observed effect level (mg/kg) NOEL = 2640 mg/kg (rat, carcinogenicity, oral) Margin of Safety NOAEL / SED = 17143 2.12. Conclusions Physical and chemical characterisation The information provided on the compound is largely incomplete and confusing regarding purity and physical constants. The stability data are not acceptable. The basic toxicity data for Acid Yellow 23 is poor. A NOAEL for Acid Yellow 23 was derived of 5% in food, equivalent to 2640 and 3348 mg/kg/day in male and female rats respectively. Acid Yellow 23 was not consider","page":20,"pdf":"out260_en.pdf","row_type":"noael_study","study_id":"out260_en_noael_006"}
SCCNFP_vision_codex NOAEL =5 % - dermal Sub-chronic repeated dose toxicity {"citation":"Ref.: 2 2","dose":"No NOAEL in mg/kg/day could be derived due to the missing data on water consumption.","effect":"SCCNFP/0786/04 Evaluation and opinion on Acid Yellow 23 _____________________________________________________________________________________________ 7 of the 5 % group animals that died during the experiment. No information was given on histology of animals at the end of treatment. No NOAEL in mg/kg/day could be derived due to the missing data on water consumption. Ref.: 2 2.3.8. Sub-chronic dermal toxicity No data 2.3.9. Sub-chronic inhalation toxicity No data 2.3.10. Chronic toxicity No chronic study was provided. Several carcinogenicity studies were provided but there were many data gaps. It would seem from these studies that other than coloured fur and faeces there were no dose-related effects from Acid Yellow 23. A NOAEL was derived of 5% in food, equivalent to 2640 and 3348 mg/kg/day in m","page":7,"pdf":"out260_en.pdf","row_type":"noael_study","study_id":"out260_en_noael_001"}
SCCNFP_vision_codex NOAEL >1000 mg/kg/day rat oral - NOAEL study {"citation":"Ref.: 7 Mated, sperm-positive female rats were dosed with 0","dose":"The mean daily food consumption was significantly higher in the 1000 mg/kg dose group, indicating an effect on food utilization.","effect":"e-related differences between treatment groups and control group were noted in behaviour, external maternal findings, and body weight. The mean daily food consumption was significantly higher in the 1000 mg/kg dose group, indicating an effect on food utilization. No dose- related changes were observed in pregnancy rate, implantation efficiency, maternal findings, foetal viability or foetal development. Examination of offspring for external and skeletal variations revealed no dose-related increase of incidence. The NOAEL for teratogenicity of Acid Yellow 23 was > 1000 mg/kg/day in this study. The study is regarded as valid and relevant for risk assessment, as a sufficient number of animals and relevant endpoints were examined. Ref.: 7 Mated, sperm-positive female rats were dosed with 0.05, 0.1, 0.2, 0.4, or 0.7 % in drinking water (equivalent to 67 –1064 mg/kg/ day) with Acid Yellow 23, from GD 0 to 19. No unusual behaviour or remarkable external maternal findings were noted. Mean daily food consumption and body weight gain wer","page":13,"pdf":"out260_en.pdf","row_type":"noael_study","study_id":"out260_en_noael_003"}
SCCNFP_vision_codex NOAEL >0.7 % rat oral chronic reproductive toxicity {"citation":"Ref.: 8 A 2-generation chronic toxicity/carcinogenicity study was conducted with different concentrations of Acid Yellow 23","dose":"A significant increase in fluid consumption was observed in the 0.2, 0.4, and 0.7 % dose groups.","effect":"able external maternal findings were noted. Mean daily food consumption and body weight gain were similar in all groups. A significant increase in fluid consumption was observed in the 0.2, 0.4, and 0.7 % dose groups. No dose-related changes were observed in pregnancy rate, implantation efficiency, foetal viability or foetal development. Reproductive findings at necropsy were unremarkable. Examination of offspring for external, skeletal and soft tissue variations revealed no dose-related increase of incidence. The NOAEL for teratogenic toxicity of Acid Yellow 23 was > 0.7% corresponding to 1064 mg/kg/day based on the mean fluid consumption in this study. A sufficient number of animals was regarded and relevant endpoints were examined. The study is judged as valid and relevant for risk assessment. Ref.: 8 A 2-generation chronic toxicity/carcinogenicity study was conducted with different concentrations of Acid Yellow 23. Male and female rats were fed a basal diet (control group) or basal diet blended with commercial Acid Yellow 2","page":13,"pdf":"out260_en.pdf","row_type":"noael_study","study_id":"out260_en_noael_004"}
SCCNFP_vision_codex NOAEL =2640 mg/kg rat oral - carcinogenicity {"citation":"Ref.: 29 Human studies No data","dose":"Safety evaluation CALCULATION OF THE MARGIN OF SAFETY (Acid Yellow 23) (Semi-permanent) Maximum absorption through the skin A (µg/cm2) = 13.2 µg/cm2 Typical body weight of human = 60 kg Skin Area surface SAS (cm2) = 700 cm2 Dermal absorption per treatment SAS x A x 0.001 = 9.24 mg Systemic exposure dose (SED) SAS x A x 0.001/60 = 0.154 mg/kg No...","effect":"d not demonstrate carcinogenic effects. Ref.: 29 Human studies No data. 2.10. Special investigations No data 2.11. Safety evaluation CALCULATION OF THE MARGIN OF SAFETY (Acid Yellow 23) (Semi-permanent) Maximum absorption through the skin A (µg/cm2) = 13.2 µg/cm2 Typical body weight of human = 60 kg Skin Area surface SAS (cm2) = 700 cm2 Dermal absorption per treatment SAS x A x 0.001 = 9.24 mg Systemic exposure dose (SED) SAS x A x 0.001/60 = 0.154 mg/kg No observed effect level (mg/kg) NOEL = 2640 mg/kg (rat, carcinogenicity, oral) Margin of Safety NOAEL / SED = 17143 2.12. Conclusions Physical and chemical characterisation The information provided on the compound is largely incomplete and confusing regarding purity and physical constants. The stability data are not acceptable. The basic toxicity data for Acid Yellow 23 is poor. A NOAEL for Acid Yellow 23 was derived of 5% in food, equivalent to 2640 and 3348 mg/kg/day in male and female rats respectively. Acid Yellow 23 was not consider","page":20,"pdf":"out260_en.pdf","row_type":"noael_study","study_id":"out260_en_noael_006"}
SCCNFP_vision_codex NOAEL =5 % - dermal Sub-chronic repeated dose toxicity {"citation":"Ref.: 2 2","dose":"No NOAEL in mg/kg/day could be derived due to the missing data on water consumption.","effect":"SCCNFP/0786/04 Evaluation and opinion on Acid Yellow 23 _____________________________________________________________________________________________ 7 of the 5 % group animals that died during the experiment. No information was given on histology of animals at the end of treatment. No NOAEL in mg/kg/day could be derived due to the missing data on water consumption. Ref.: 2 2.3.8. Sub-chronic dermal toxicity No data 2.3.9. Sub-chronic inhalation toxicity No data 2.3.10. Chronic toxicity No chronic study was provided. Several carcinogenicity studies were provided but there were many data gaps. It would seem from these studies that other than coloured fur and faeces there were no dose-related effects from Acid Yellow 23. A NOAEL was derived of 5% in food, equivalent to 2640 and 3348 mg/kg/day in m","page":7,"pdf":"out260_en.pdf","row_type":"noael_study","study_id":"out260_en_noael_001"}
SCCNFP_vision_codex NOAEL >1000 mg/kg/day rat oral - NOAEL study {"citation":"Ref.: 7 Mated, sperm-positive female rats were dosed with 0","dose":"The mean daily food consumption was significantly higher in the 1000 mg/kg dose group, indicating an effect on food utilization.","effect":"e-related differences between treatment groups and control group were noted in behaviour, external maternal findings, and body weight. The mean daily food consumption was significantly higher in the 1000 mg/kg dose group, indicating an effect on food utilization. No dose- related changes were observed in pregnancy rate, implantation efficiency, maternal findings, foetal viability or foetal development. Examination of offspring for external and skeletal variations revealed no dose-related increase of incidence. The NOAEL for teratogenicity of Acid Yellow 23 was > 1000 mg/kg/day in this study. The study is regarded as valid and relevant for risk assessment, as a sufficient number of animals and relevant endpoints were examined. Ref.: 7 Mated, sperm-positive female rats were dosed with 0.05, 0.1, 0.2, 0.4, or 0.7 % in drinking water (equivalent to 67 –1064 mg/kg/ day) with Acid Yellow 23, from GD 0 to 19. No unusual behaviour or remarkable external maternal findings were noted. Mean daily food consumption and body weight gain wer","page":13,"pdf":"out260_en.pdf","row_type":"noael_study","study_id":"out260_en_noael_003"}
SCCNFP_vision_codex NOAEL >0.7 % rat oral chronic reproductive toxicity {"citation":"Ref.: 8 A 2-generation chronic toxicity/carcinogenicity study was conducted with different concentrations of Acid Yellow 23","dose":"A significant increase in fluid consumption was observed in the 0.2, 0.4, and 0.7 % dose groups.","effect":"able external maternal findings were noted. Mean daily food consumption and body weight gain were similar in all groups. A significant increase in fluid consumption was observed in the 0.2, 0.4, and 0.7 % dose groups. No dose-related changes were observed in pregnancy rate, implantation efficiency, foetal viability or foetal development. Reproductive findings at necropsy were unremarkable. Examination of offspring for external, skeletal and soft tissue variations revealed no dose-related increase of incidence. The NOAEL for teratogenic toxicity of Acid Yellow 23 was > 0.7% corresponding to 1064 mg/kg/day based on the mean fluid consumption in this study. A sufficient number of animals was regarded and relevant endpoints were examined. The study is judged as valid and relevant for risk assessment. Ref.: 8 A 2-generation chronic toxicity/carcinogenicity study was conducted with different concentrations of Acid Yellow 23. Male and female rats were fed a basal diet (control group) or basal diet blended with commercial Acid Yellow 2","page":13,"pdf":"out260_en.pdf","row_type":"noael_study","study_id":"out260_en_noael_004"}
SCCNFP_vision_codex NOAEL =2640 mg/kg rat oral - carcinogenicity {"citation":"Ref.: 29 Human studies No data","dose":"Safety evaluation CALCULATION OF THE MARGIN OF SAFETY (Acid Yellow 23) (Semi-permanent) Maximum absorption through the skin A (µg/cm2) = 13.2 µg/cm2 Typical body weight of human = 60 kg Skin Area surface SAS (cm2) = 700 cm2 Dermal absorption per treatment SAS x A x 0.001 = 9.24 mg Systemic exposure dose (SED) SAS x A x 0.001/60 = 0.154 mg/kg No...","effect":"d not demonstrate carcinogenic effects. Ref.: 29 Human studies No data. 2.10. Special investigations No data 2.11. Safety evaluation CALCULATION OF THE MARGIN OF SAFETY (Acid Yellow 23) (Semi-permanent) Maximum absorption through the skin A (µg/cm2) = 13.2 µg/cm2 Typical body weight of human = 60 kg Skin Area surface SAS (cm2) = 700 cm2 Dermal absorption per treatment SAS x A x 0.001 = 9.24 mg Systemic exposure dose (SED) SAS x A x 0.001/60 = 0.154 mg/kg No observed effect level (mg/kg) NOEL = 2640 mg/kg (rat, carcinogenicity, oral) Margin of Safety NOAEL / SED = 17143 2.12. Conclusions Physical and chemical characterisation The information provided on the compound is largely incomplete and confusing regarding purity and physical constants. The stability data are not acceptable. The basic toxicity data for Acid Yellow 23 is poor. A NOAEL for Acid Yellow 23 was derived of 5% in food, equivalent to 2640 and 3348 mg/kg/day in male and female rats respectively. Acid Yellow 23 was not consider","page":20,"pdf":"out260_en.pdf","row_type":"noael_study","study_id":"out260_en_noael_006"}
ToxValDB_ECHA_IUCLID 9 endpoints
Source Endpoint Type Value Unit Species Route Duration Study Type Reference
ToxValDB_ECHA_IUCLID NOAEL =2641 mg/kg bw/day Rat oral - chronic QUALITY=2 (reliable with restrictions); STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/669ea9f0e4b0a7c65d1b387d; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://echa.europa.eu/; SUBSOURCE_URL=https://echa.europa.eu/registration-dossier/-/registered-dossier/17292/7/8?documentUUID=34708cf7-8ebc-470f-9040-e36782cd74af; YEAR=1982; ORIGINAL_YEAR=1982; STUDY_GROUP=ECHA IUCLID:15820383:M:--; QC_CATEGORY=Programmatically extracted from structured data source; Source overall passed QC, and this record was expert reviewed; QC_STATUS=pass; SOURCE_HASH=ToxValhc_b0592eab777ba369fc6e978bc7961092
ToxValDB_ECHA_IUCLID NOAEL =3348 mg/kg bw/day Rat oral - chronic QUALITY=2 (reliable with restrictions); STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/669ea9f0e4b0a7c65d1b387d; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://echa.europa.eu/; SUBSOURCE_URL=https://echa.europa.eu/registration-dossier/-/registered-dossier/17292/7/8?documentUUID=34708cf7-8ebc-470f-9040-e36782cd74af; YEAR=1982; ORIGINAL_YEAR=1982; STUDY_GROUP=ECHA IUCLID:15820384:F:--; QC_CATEGORY=Programmatically extracted from structured data source; Source overall passed QC, and this record was expert reviewed; QC_STATUS=pass; SOURCE_HASH=ToxValhc_f2c3eb756df9b8c8bbeb294b2bfacf42
ToxValDB_ECHA_IUCLID NOAEL =1064.3 mg/kg bw/day Rat oral - reproduction developmental QUALITY=2 (reliable with restrictions); STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/669eabd2e4b0a7c65d1bbe90; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://echa.europa.eu/; SUBSOURCE_URL=https://echa.europa.eu/en/registration-dossier/-/registered-dossier/12236?documentUUID=99b7317c-4c1d-4b46-8d69-c269b8cd8271; YEAR=2019; ORIGINAL_YEAR=2019; TOXICOLOGICAL_EFFECT=maternal: body weight and weight gain|maternal: changes in number of pregnant|maternal: clinical signs|maternal: food consumption and compound intake|maternal: mortality|maternal: pre and post implantation loss|maternal: water consumption and compound intake; TOXICOLOGICAL_EFFECT_CATEGORY=body weight|clinical signs|food and/or water consumption|mortality/survival|reproduction; STUDY_GROUP=ECHA IUCLID_dup_Developmental Toxicity Teratogenicity_15823302_15823343:F:-maternal; QC_CATEGORY=Programmatically extracted from structured data source; Source overall passed QC, and this record was expert reviewed; QC_STATUS=pass; SOURCE_HASH=ToxValhc_1edf34afb222063908f415489ca46971
ToxValDB_ECHA_IUCLID NOAEL =1064 mg/kg bw/day Rat oral - reproduction developmental QUALITY=2 (reliable with restrictions); STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/669eac00e4b0a7c65d1bcdb8; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://echa.europa.eu/; SUBSOURCE_URL=https://echa.europa.eu/registration-dossier/-/registered-dossier/17292/7/9/3?documentUUID=34708cf7-8ebc-470f-9040-e36782cd74af; YEAR=1982; ORIGINAL_YEAR=1982; TOXICOLOGICAL_EFFECT=maternal: mortality; TOXICOLOGICAL_EFFECT_CATEGORY=mortality/survival; STUDY_GROUP=ECHA IUCLID_dup_Developmental Toxicity Teratogenicity_15823302_15823343:F:-maternal; QC_CATEGORY=Programmatically extracted from structured data source; Source overall passed QC, but this record was not manually checked; QC_STATUS=not determined; SOURCE_HASH=ToxValhc_31cdf1d175831e0e3bce3de833ef6a4b
ToxValDB_ECHA_IUCLID NOAEL =642.8 mg/kg bw/day Mouse oral - reproduction developmental QUALITY=2 (reliable with restrictions); STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/669eabd2e4b0a7c65d1bbe8e; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://echa.europa.eu/; SUBSOURCE_URL=https://echa.europa.eu/en/registration-dossier/-/registered-dossier/12236?documentUUID=99b7317c-4c1d-4b46-8d69-c269b8cd8271; YEAR=2019; ORIGINAL_YEAR=2019; STUDY_GROUP=ECHA IUCLID:15823761:F:-maternal; QC_CATEGORY=Programmatically extracted from structured data source; Source overall passed QC, and this record was expert reviewed; QC_STATUS=pass; SOURCE_HASH=ToxValhc_f990f0ddca26e31dd96603920220ed45
ToxValDB_ECHA_IUCLID NOAEL =1000 mg/kg bw/day Rat oral - developmental QUALITY=2 (reliable with restrictions); STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/669eac00e4b0a7c65d1bcdb6; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://echa.europa.eu/; SUBSOURCE_URL=https://echa.europa.eu/registration-dossier/-/registered-dossier/17292/7/9/3?documentUUID=34708cf7-8ebc-470f-9040-e36782cd74af; YEAR=1982; ORIGINAL_YEAR=1982; STUDY_GROUP=ECHA IUCLID:15824572:M/F:-fetal; QC_CATEGORY=Programmatically extracted from structured data source; Source overall passed QC, and this record was expert reviewed; QC_STATUS=pass; SOURCE_HASH=ToxValhc_b9437c9f52475c77b2675505c66d1b21
ToxValDB_ECHA_IUCLID NOAEL =1250 mg/kg bw/day Rat oral subchronic; 13 weeks subchronic QUALITY=2 (reliable with restrictions); STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/669eadc7e4b0a7c65d1c5f48; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://echa.europa.eu/; SUBSOURCE_URL=https://echa.europa.eu/registration-dossier/-/registered-dossier/21583/7/6/2?documentUUID=2f5ce440-67ff-4f67-a435-888350d4c19d; YEAR=2017; ORIGINAL_YEAR=2017; STUDY_GROUP=ECHA IUCLID_dup_Repeated Dose Toxicity Oral_15847799_15848283:M/F:--; QC_CATEGORY=Programmatically extracted from structured data source; Source overall passed QC, and this record was expert reviewed; QC_STATUS=pass; SOURCE_HASH=ToxValhc_fa18304b6f5bf0ef89424b9781fedd3d
ToxValDB_ECHA_IUCLID NOAEL ~8103 mg/kg bw/day Rat oral chronic; 104 weeks chronic QUALITY=2 (reliable with restrictions); STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/669eadc7e4b0a7c65d1c5dd6; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://echa.europa.eu/; SUBSOURCE_URL=https://echa.europa.eu/registration-dossier/-/registered-dossier/17292/7/6/2?documentUUID=34708cf7-8ebc-470f-9040-e36782cd74af; YEAR=1982; ORIGINAL_YEAR=1982; TOXICOLOGICAL_EFFECT=mortality; TOXICOLOGICAL_EFFECT_CATEGORY=mortality/survival; STUDY_GROUP=ECHA IUCLID:15849247:M:--; QC_CATEGORY=Programmatically extracted from structured data source; Source overall passed QC, and this record was expert reviewed; QC_STATUS=pass; SOURCE_HASH=ToxValhc_06ff5fa8b4da37951b65c9005c1c4445
ToxValDB_ECHA_IUCLID NOAEL ~9735 mg/kg bw/day Rat oral chronic; 104 weeks chronic QUALITY=2 (reliable with restrictions); STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/669eadc7e4b0a7c65d1c5dd6; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://echa.europa.eu/; SUBSOURCE_URL=https://echa.europa.eu/registration-dossier/-/registered-dossier/17292/7/6/2?documentUUID=34708cf7-8ebc-470f-9040-e36782cd74af; YEAR=1982; ORIGINAL_YEAR=1982; TOXICOLOGICAL_EFFECT=mortality; TOXICOLOGICAL_EFFECT_CATEGORY=mortality/survival; STUDY_GROUP=ECHA IUCLID:15849248:F:--; QC_CATEGORY=Programmatically extracted from structured data source; Source overall passed QC, and this record was expert reviewed; QC_STATUS=pass; SOURCE_HASH=ToxValhc_101a8342e47c02be8159bed1898de8d4
ToxValDB_ECOTOX 17 endpoints
Source Endpoint Type Value Unit Species Route Duration Study Type Reference
ToxValDB_ECOTOX LOEL =2 % Rat oral short-term; 14 days short-term LONG_REF=J. Toxicol. Environ. Health2(5): 1211-1220 Sobotka,T.J., R.E. Brodie, and S.L. Spaid Tartrazine and the Developing Nervous System of Rats 1977; TITLE=Tartrazine and the Developing Nervous System of Rats; AUTHOR=Sobotka,T.J., R.E. Brodie, and S.L. Spaid; DOI=10.1080/15287397709529519; QUALITY=Control type: Concurrent control; EXTERNAL_SOURCE_ID=76050; EXTERNAL_SOURCE_ID_DESC=ECOTOX Reference Number; STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/6759bce8e4b0a7c65d37bc5f; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://cfpub.epa.gov/ecotox/; YEAR=1977; ORIGINAL_YEAR=1977; TOXICOLOGICAL_EFFECT=Biochemistry: Hemoglobin|Cell(s): Red blood cell|Morphology: Weight; TOXICOLOGICAL_EFFECT_CATEGORY=hematology|other; STUDY_GROUP=ECOTOX_dup_EPA ORD_15599257_15599258:F:--; QC_CATEGORY=Data source QC'd by data provider prior to ECOTOX import; QC_STATUS=not determined; SOURCE_HASH=b7095d46c5bdae73100730cf9181839b
ToxValDB_ECOTOX LOEL =5 % Rat oral short-term; 14 days short-term LONG_REF=J. Nutr.107(5): 822-828 Ershoff,B.H. Effects of Diet on Growth and Survival of Rats Fed Toxic Levels of Tartrazine (FD & C Yellow No. 5) and Sunset Yellow FCF (FD & C Yellow No. 6) 1977; TITLE=Effects of Diet on Growth and Survival of Rats Fed Toxic Levels of Tartrazine (FD & C Yellow No. 5) and Sunset Yellow FCF (FD & C Yellow No. 6); AUTHOR=Ershoff,B.H.; DOI=10.1093/jn/107.5.822; QUALITY=Control type: Concurrent control; EXTERNAL_SOURCE_ID=76051; EXTERNAL_SOURCE_ID_DESC=ECOTOX Reference Number; STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/6759bce8e4b0a7c65d37bc5f; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://cfpub.epa.gov/ecotox/; YEAR=1977; ORIGINAL_YEAR=1977; TOXICOLOGICAL_EFFECT=Growth: Weight gain; TOXICOLOGICAL_EFFECT_CATEGORY=body weight; STUDY_GROUP=ECOTOX_dup_EPA ORD_15600716_15605647_15605648_15609604:M:--; QC_CATEGORY=Data source QC'd by data provider prior to ECOTOX import; QC_STATUS=not determined; SOURCE_HASH=914578f5440ebf73ad00347aea5ec93b
ToxValDB_ECOTOX LOEL =2.5 % w/v Rat oral chronic; 91 days chronic LONG_REF=Food Chem. Toxicol.25(12): 891-896 Maekawa,A., C. Matsuoka, H. Onodera, H. Tanigawa, K. Furuta, J. Kanno, J.J. Jang, Y. Hayashi, and T. Ogiu Lack of Carcinogenicity of Tartrazine (FD and C Yellow No. 5) in the F344 Rat 1987; TITLE=Lack of Carcinogenicity of Tartrazine (FD and C Yellow No. 5) in the F344 Rat; AUTHOR=Maekawa,A., C. Matsuoka, H. Onodera, H. Tanigawa, K. Furuta, J. Kanno, J.J. Jang, Y. Hayashi, and T. Ogiu; DOI=10.1016/0278-6915(87)90281-x; QUALITY=Control type: Concurrent control; EXTERNAL_SOURCE_ID=76017; EXTERNAL_SOURCE_ID_DESC=ECOTOX Reference Number; STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/6759bce8e4b0a7c65d37bc5f; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://cfpub.epa.gov/ecotox/; YEAR=1987; ORIGINAL_YEAR=1987; TOXICOLOGICAL_EFFECT=Morphology: Weight; TOXICOLOGICAL_EFFECT_CATEGORY=other; STUDY_GROUP=ECOTOX_dup_EPA ORD_15603926_15603927:M/F:--; QC_CATEGORY=Data source QC'd by data provider prior to ECOTOX import; QC_STATUS=not determined; SOURCE_HASH=2fe6e24d41f99ef73e369e158f6c34e4
ToxValDB_ECOTOX LOEL =10 mg/kg bw/day Mouse oral acute; 1 days acute LONG_REF=Mutat. Res.519(1/2): 103-119 Sasaki,Y.F., S. Kawaguchi, A. Kamaya, M. Ohshita, K. Kabasawa, K. Iwama, K. Taniguchi, and S. Tsuda The Comet Assay with 8 Mouse Organs: Results with 39 Currently Used Food Additives 2002; TITLE=The Comet Assay with 8 Mouse Organs: Results with 39 Currently Used Food Additives; AUTHOR=Sasaki,Y.F., S. Kawaguchi, A. Kamaya, M. Ohshita, K. Kabasawa, K. Iwama, K. Taniguchi, and S. Tsuda; DOI=10.1016/s1383-5718(02)00128-6; QUALITY=Control type: Concurrent control; EXTERNAL_SOURCE_ID=75840; EXTERNAL_SOURCE_ID_DESC=ECOTOX Reference Number; STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/6759bce8e4b0a7c65d37bc5f; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://cfpub.epa.gov/ecotox/; YEAR=2002; ORIGINAL_YEAR=2002; TOXICOLOGICAL_EFFECT=Genetics: Damage; TOXICOLOGICAL_EFFECT_CATEGORY=other; STUDY_GROUP=ECOTOX_dup_EPA ORD_15604354_15604355:M:--; QC_CATEGORY=Data source QC'd by data provider prior to ECOTOX import; QC_STATUS=not determined; SOURCE_HASH=b8f02a3881caf993744eb1f84e658299
ToxValDB_ECOTOX LOEL =7.5 % Rat oral short-term; 14 days short-term LONG_REF=J. Nutr.107(5): 822-828 Ershoff,B.H. Effects of Diet on Growth and Survival of Rats Fed Toxic Levels of Tartrazine (FD & C Yellow No. 5) and Sunset Yellow FCF (FD & C Yellow No. 6) 1977; TITLE=Effects of Diet on Growth and Survival of Rats Fed Toxic Levels of Tartrazine (FD & C Yellow No. 5) and Sunset Yellow FCF (FD & C Yellow No. 6); AUTHOR=Ershoff,B.H.; DOI=10.1093/jn/107.5.822; QUALITY=Control type: Concurrent control; EXTERNAL_SOURCE_ID=76051; EXTERNAL_SOURCE_ID_DESC=ECOTOX Reference Number; STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/6759bce8e4b0a7c65d37bc5f; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://cfpub.epa.gov/ecotox/; YEAR=1977; ORIGINAL_YEAR=1977; TOXICOLOGICAL_EFFECT=Growth: Weight gain; TOXICOLOGICAL_EFFECT_CATEGORY=body weight; STUDY_GROUP=ECOTOX_dup_EPA ORD_15600716_15605647_15605648_15609604:M:--; QC_CATEGORY=Data source QC'd by data provider prior to ECOTOX import; QC_STATUS=not determined; SOURCE_HASH=d8db789dab10e149e31320e34ae86bde
ToxValDB_ECOTOX LOEL =1 % Rat oral subchronic; 49 days subchronic LONG_REF=J. Toxicol. Environ. Health2(5): 1211-1220 Sobotka,T.J., R.E. Brodie, and S.L. Spaid Tartrazine and the Developing Nervous System of Rats 1977; TITLE=Tartrazine and the Developing Nervous System of Rats; AUTHOR=Sobotka,T.J., R.E. Brodie, and S.L. Spaid; DOI=10.1080/15287397709529519; QUALITY=Control type: Concurrent control; EXTERNAL_SOURCE_ID=76050; EXTERNAL_SOURCE_ID_DESC=ECOTOX Reference Number; STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/6759bce8e4b0a7c65d37bc5f; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://cfpub.epa.gov/ecotox/; YEAR=1977; ORIGINAL_YEAR=1977; TOXICOLOGICAL_EFFECT=Growth: Weight; TOXICOLOGICAL_EFFECT_CATEGORY=body weight; STUDY_GROUP=ECOTOX:15610471:F:--; QC_CATEGORY=Data source QC'd by data provider prior to ECOTOX import; QC_STATUS=not determined; SOURCE_HASH=b00bea42e7d9e86daa0bd0afc086ff24
ToxValDB_ECOTOX LOEL =589 mg/kg bw/day Rat oral chronic; 114 weeks chronic LONG_REF=- | Food Chem. Toxicol.26(3): 179-187 Borzelleca,J.F., and J.B. Hallagan Chronic Toxicity/Carcinogenicity Studies of FD & C Yellow No. 5 (Tartrazine) in Rats 1988; TITLE=Chronic Toxicity/Carcinogenicity Studies of FD & C Yellow No. 5 (Tartrazine) in Rats; AUTHOR=Borzelleca,J.F., and J.B. Hallagan; QUALITY=Control type: Concurrent control; EXTERNAL_SOURCE_ID=76020; EXTERNAL_SOURCE_ID_DESC=ECOTOX Reference Number; STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/6759bce8e4b0a7c65d37bc5f; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://cfpub.epa.gov/ecotox/; YEAR=1988; ORIGINAL_YEAR=1988; TOXICOLOGICAL_EFFECT=Growth: Weight; TOXICOLOGICAL_EFFECT_CATEGORY=body weight; STUDY_GROUP=ECOTOX:15613109:F:--; QC_CATEGORY=Data source QC'd by data provider prior to ECOTOX import; Source overall passed QC, and this record was expert reviewed and revised from ECOTOX source; QC_STATUS=pass; SOURCE_HASH=04969d91ae29fa0491f61e689329cd11
ToxValDB_ECOTOX LOEL =100 ppm Rat injection chronic; 273.96 days chronic LONG_REF=- | Cytobios62(249): 111-117 Giri,A.K., S.K. Das, G. Talukder, and A. Sharma Sister Chromatid Exchange and Chromosome Aberrations Induced by Curcumin and Tartrazine on Mammalian Cells In Vivo 1990; TITLE=Sister Chromatid Exchange and Chromosome Aberrations Induced by Curcumin and Tartrazine on Mammalian Cells In Vivo; AUTHOR=Giri,A.K., S.K. Das, G. Talukder, and A. Sharma; QUALITY=Control type: Concurrent control; EXTERNAL_SOURCE_ID=76048; EXTERNAL_SOURCE_ID_DESC=ECOTOX Reference Number; STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/6759bce8e4b0a7c65d37bc5f; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://cfpub.epa.gov/ecotox/; YEAR=1990; ORIGINAL_YEAR=1990; TOXICOLOGICAL_EFFECT=Genetics: Chromosomal aberrations, sister chromatid exchanges; STUDY_GROUP=ECOTOX:15613440:M:--; QC_CATEGORY=Data source QC'd by data provider prior to ECOTOX import; Source overall passed QC, and this record was expert reviewed and revised from ECOTOX source; QC_STATUS=pass; SOURCE_HASH=2a9c05c71a1b0af9d8a894e5c48e751b
ToxValDB_ECOTOX NOEL =1 % Rat oral short-term; 14 days short-term LONG_REF=J. Toxicol. Environ. Health2(5): 1211-1220 Sobotka,T.J., R.E. Brodie, and S.L. Spaid Tartrazine and the Developing Nervous System of Rats 1977; TITLE=Tartrazine and the Developing Nervous System of Rats; AUTHOR=Sobotka,T.J., R.E. Brodie, and S.L. Spaid; DOI=10.1080/15287397709529519; QUALITY=Control type: Concurrent control; EXTERNAL_SOURCE_ID=76050; EXTERNAL_SOURCE_ID_DESC=ECOTOX Reference Number; STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/6759bce8e4b0a7c65d37bc5f; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://cfpub.epa.gov/ecotox/; YEAR=1977; ORIGINAL_YEAR=1977; TOXICOLOGICAL_EFFECT=Biochemistry: Hemoglobin|Cell(s): Red blood cell|Morphology: Weight; TOXICOLOGICAL_EFFECT_CATEGORY=hematology|other; STUDY_GROUP=ECOTOX_dup_EPA ORD_15599257_15599258:F:--; QC_CATEGORY=Data source QC'd by data provider prior to ECOTOX import; QC_STATUS=not determined; SOURCE_HASH=0e797c201d47be218f7a805984c9d084
ToxValDB_ECOTOX NOEL =2 % w/v Rat oral chronic; 784 days chronic LONG_REF=Food Chem. Toxicol.25(12): 891-896 Maekawa,A., C. Matsuoka, H. Onodera, H. Tanigawa, K. Furuta, J. Kanno, J.J. Jang, Y. Hayashi, and T. Ogiu Lack of Carcinogenicity of Tartrazine (FD and C Yellow No. 5) in the F344 Rat 1987; TITLE=Lack of Carcinogenicity of Tartrazine (FD and C Yellow No. 5) in the F344 Rat; AUTHOR=Maekawa,A., C. Matsuoka, H. Onodera, H. Tanigawa, K. Furuta, J. Kanno, J.J. Jang, Y. Hayashi, and T. Ogiu; DOI=10.1016/0278-6915(87)90281-x; QUALITY=Control type: Concurrent control; EXTERNAL_SOURCE_ID=76017; EXTERNAL_SOURCE_ID_DESC=ECOTOX Reference Number; STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/6759bce8e4b0a7c65d37bc5f; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://cfpub.epa.gov/ecotox/; YEAR=1987; ORIGINAL_YEAR=1987; TOXICOLOGICAL_EFFECT=Injury: Malignant tumor; TOXICOLOGICAL_EFFECT_CATEGORY=cancer; STUDY_GROUP=ECOTOX:15599964:M:--; QC_CATEGORY=Data source QC'd by data provider prior to ECOTOX import; QC_STATUS=not determined; SOURCE_HASH=61a5c1019f05d253b644edf03cbb5e4d
ToxValDB_ECOTOX NOEL =2 % Rat oral short-term; 14 days developmental LONG_REF=J. Toxicol. Environ. Health2(5): 1211-1220 Sobotka,T.J., R.E. Brodie, and S.L. Spaid Tartrazine and the Developing Nervous System of Rats 1977; TITLE=Tartrazine and the Developing Nervous System of Rats; AUTHOR=Sobotka,T.J., R.E. Brodie, and S.L. Spaid; DOI=10.1080/15287397709529519; QUALITY=Control type: Concurrent control; EXTERNAL_SOURCE_ID=76050; EXTERNAL_SOURCE_ID_DESC=ECOTOX Reference Number; STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/6759bce8e4b0a7c65d37bc5f; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://cfpub.epa.gov/ecotox/; YEAR=1977; ORIGINAL_YEAR=1977; TOXICOLOGICAL_EFFECT=Development: Eye opening|Physiology: Neuroresponse|Reproduction: Progeny counts/numbers; TOXICOLOGICAL_EFFECT_CATEGORY=development|neurobehavior|reproduction; STUDY_GROUP=ECOTOX:15600386:F:--; QC_CATEGORY=Data source QC'd by data provider prior to ECOTOX import; QC_STATUS=not determined; SOURCE_HASH=db305996467c867493de981fb476a038
ToxValDB_ECOTOX NOEL =1064.32 mg/L Rat oral short-term; 20 days developmental LONG_REF=Food Chem. Toxicol.30(4): 263-268 Collins,T.F.X., T.N. Black, M.W.,Jr. O\'Donnell, and P. Bulhack Study of the Teratogenic Potential of FD & C Yellow No. 5 when Given in Drinking-Water 1992; TITLE=Study of the Teratogenic Potential of FD & C Yellow No. 5 when Given in Drinking-Water; AUTHOR=Collins,T.F.X., T.N. Black, M.W.,Jr. O\'Donnell, and P. Bulhack; DOI=10.1016/0278-6915(92)90002-3; QUALITY=Control type: Concurrent control; EXTERNAL_SOURCE_ID=76022; EXTERNAL_SOURCE_ID_DESC=ECOTOX Reference Number; STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/6759bce8e4b0a7c65d37bc5f; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://cfpub.epa.gov/ecotox/; YEAR=1992; ORIGINAL_YEAR=1992; TOXICOLOGICAL_EFFECT=Development: Abnormal|Feeding behavior: Water consumption; TOXICOLOGICAL_EFFECT_CATEGORY=development|food and/or water consumption; STUDY_GROUP=ECOTOX:15601661:F:--; QC_CATEGORY=Data source QC'd by data provider prior to ECOTOX import; QC_STATUS=not determined; SOURCE_HASH=20f098e5b2fcd31ab29225d3acc6e1a9
ToxValDB_ECOTOX NOEL =1.25 % w/v Rat oral chronic; 91 days chronic LONG_REF=Food Chem. Toxicol.25(12): 891-896 Maekawa,A., C. Matsuoka, H. Onodera, H. Tanigawa, K. Furuta, J. Kanno, J.J. Jang, Y. Hayashi, and T. Ogiu Lack of Carcinogenicity of Tartrazine (FD and C Yellow No. 5) in the F344 Rat 1987; TITLE=Lack of Carcinogenicity of Tartrazine (FD and C Yellow No. 5) in the F344 Rat; AUTHOR=Maekawa,A., C. Matsuoka, H. Onodera, H. Tanigawa, K. Furuta, J. Kanno, J.J. Jang, Y. Hayashi, and T. Ogiu; DOI=10.1016/0278-6915(87)90281-x; QUALITY=Control type: Concurrent control; EXTERNAL_SOURCE_ID=76017; EXTERNAL_SOURCE_ID_DESC=ECOTOX Reference Number; STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/6759bce8e4b0a7c65d37bc5f; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://cfpub.epa.gov/ecotox/; YEAR=1987; ORIGINAL_YEAR=1987; TOXICOLOGICAL_EFFECT=Morphology: Weight; TOXICOLOGICAL_EFFECT_CATEGORY=other; STUDY_GROUP=ECOTOX_dup_EPA ORD_15603926_15603927:M/F:--; QC_CATEGORY=Data source QC'd by data provider prior to ECOTOX import; QC_STATUS=not determined; SOURCE_HASH=8f505f81798a68a4b3dc8217732fe2b3
ToxValDB_ECOTOX NOEL =1 mg/kg bw/day Mouse oral acute; 1 days acute LONG_REF=Mutat. Res.519(1/2): 103-119 Sasaki,Y.F., S. Kawaguchi, A. Kamaya, M. Ohshita, K. Kabasawa, K. Iwama, K. Taniguchi, and S. Tsuda The Comet Assay with 8 Mouse Organs: Results with 39 Currently Used Food Additives 2002; TITLE=The Comet Assay with 8 Mouse Organs: Results with 39 Currently Used Food Additives; AUTHOR=Sasaki,Y.F., S. Kawaguchi, A. Kamaya, M. Ohshita, K. Kabasawa, K. Iwama, K. Taniguchi, and S. Tsuda; DOI=10.1016/s1383-5718(02)00128-6; QUALITY=Control type: Concurrent control; EXTERNAL_SOURCE_ID=75840; EXTERNAL_SOURCE_ID_DESC=ECOTOX Reference Number; STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/6759bce8e4b0a7c65d37bc5f; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://cfpub.epa.gov/ecotox/; YEAR=2002; ORIGINAL_YEAR=2002; TOXICOLOGICAL_EFFECT=Genetics: Damage; TOXICOLOGICAL_EFFECT_CATEGORY=other; STUDY_GROUP=ECOTOX_dup_EPA ORD_15604354_15604355:M:--; QC_CATEGORY=Data source QC'd by data provider prior to ECOTOX import; QC_STATUS=not determined; SOURCE_HASH=993f6a691d6ea110a7cfb077008c075b
ToxValDB_ECOTOX NOEL =2.5 % Rat oral short-term; 14 days short-term LONG_REF=J. Nutr.107(5): 822-828 Ershoff,B.H. Effects of Diet on Growth and Survival of Rats Fed Toxic Levels of Tartrazine (FD & C Yellow No. 5) and Sunset Yellow FCF (FD & C Yellow No. 6) 1977; TITLE=Effects of Diet on Growth and Survival of Rats Fed Toxic Levels of Tartrazine (FD & C Yellow No. 5) and Sunset Yellow FCF (FD & C Yellow No. 6); AUTHOR=Ershoff,B.H.; DOI=10.1093/jn/107.5.822; QUALITY=Control type: Concurrent control; EXTERNAL_SOURCE_ID=76051; EXTERNAL_SOURCE_ID_DESC=ECOTOX Reference Number; STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/6759bce8e4b0a7c65d37bc5f; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://cfpub.epa.gov/ecotox/; YEAR=1977; ORIGINAL_YEAR=1977; TOXICOLOGICAL_EFFECT=Growth: Weight gain; TOXICOLOGICAL_EFFECT_CATEGORY=body weight; STUDY_GROUP=ECOTOX_dup_EPA ORD_15600716_15605647_15605648_15609604:M:--; QC_CATEGORY=Data source QC'd by data provider prior to ECOTOX import; QC_STATUS=not determined; SOURCE_HASH=a996366425a33816110716bb8bef37d1
ToxValDB_ECOTOX NOEL =1800.97 mg/kg bw/day Mouse oral chronic; 730.56 days chronic LONG_REF=- | Food Chem. Toxicol.26(3): 189-194 Borzelleca,J.F., and J.B. Hallagan A Chronic Toxicity/Carcinogenicity Study of FD & C Yellow No. 5 (Tartrazine) in Mice 1988; TITLE=A Chronic Toxicity/Carcinogenicity Study of FD & C Yellow No. 5 (Tartrazine) in Mice; AUTHOR=Borzelleca,J.F., and J.B. Hallagan; QUALITY=Control type: Concurrent control; EXTERNAL_SOURCE_ID=76019; EXTERNAL_SOURCE_ID_DESC=ECOTOX Reference Number; STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/6759bce8e4b0a7c65d37bc5f; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://cfpub.epa.gov/ecotox/; YEAR=1988; ORIGINAL_YEAR=1988; TOXICOLOGICAL_EFFECT=Growth: Weight|Mortality: Survival| Haematological parameters: lesions; TOXICOLOGICAL_EFFECT_CATEGORY=body weight|mortality/survival|multiple; STUDY_GROUP=ECOTOX:15613130:F:--; QC_CATEGORY=Data source QC'd by data provider prior to ECOTOX import; Source overall passed QC, and this record was expert reviewed and revised from ECOTOX source; QC_STATUS=pass; SOURCE_HASH=fdf57dc05da3db642abe775dfbf6bab6
ToxValDB_ECOTOX NOEL =1499.06 mg/kg bw/day Mouse oral chronic; 730.56 days chronic LONG_REF=- | Food Chem. Toxicol.26(3): 189-194 Borzelleca,J.F., and J.B. Hallagan A Chronic Toxicity/Carcinogenicity Study of FD & C Yellow No. 5 (Tartrazine) in Mice 1988; TITLE=A Chronic Toxicity/Carcinogenicity Study of FD & C Yellow No. 5 (Tartrazine) in Mice; AUTHOR=Borzelleca,J.F., and J.B. Hallagan; QUALITY=Control type: Concurrent control; EXTERNAL_SOURCE_ID=76019; EXTERNAL_SOURCE_ID_DESC=ECOTOX Reference Number; STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/6759bce8e4b0a7c65d37bc5f; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://cfpub.epa.gov/ecotox/; YEAR=1988; ORIGINAL_YEAR=1988; TOXICOLOGICAL_EFFECT=Growth: Weight|Mortality: Survival| Haematological parameters: lesions; TOXICOLOGICAL_EFFECT_CATEGORY=body weight|mortality/survival|multiple; STUDY_GROUP=ECOTOX:15613428:M:--; QC_CATEGORY=Data source QC'd by data provider prior to ECOTOX import; Source overall passed QC, and this record was expert reviewed and revised from ECOTOX source; QC_STATUS=pass; SOURCE_HASH=43943059a553d4739211a498a379c323
ToxValDB_EFSA 1 endpoint
Source Endpoint Type Value Unit Species Route Duration Study Type Reference
ToxValDB_EFSA NOAEL =984 mg/kg bw/day Rat oral - chronic LONG_REF=EFSA FEEDAP (2016). Safety and efficacy of tartrazine (E 102) for cats and dogs, ornamental fish, grain-eating ornamental birds and small rodents. doi:10.2903/j.efsa.2016.4613.; TITLE=Safety and efficacy of tartrazine (E 102) for cats and dogs, ornamental fish, grain-eating ornamental birds and small rodents; AUTHOR=EFSA FEEDAP; DOI=doi:10.2903/j.efsa.2016.4613; STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/65201d30e4b0f0a60ddd1165; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://zenodo.org/record/5076033#.Y9fEoXbMI2z; YEAR=2016; ORIGINAL_YEAR=2016; TOXICOLOGICAL_EFFECT=body weight; TOXICOLOGICAL_EFFECT_CATEGORY=body weight; STUDY_GROUP=EFSA:15614315:M:--; QC_CATEGORY=Programmatically extracted from structured data source; Source overall passed QC, but this record was not manually checked; QC_STATUS=not determined; SOURCE_HASH=ToxValhc_fe32cf62c832f1e188a080db8809f56d
ToxValDB_GESTIS_DNEL 1 endpoint
Source Endpoint Type Value Unit Species Route Duration Study Type Reference
ToxValDB_GESTIS_DNEL DNEL systemic =372.52 mg/m3 Human inhalation - Toxicity Value STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/6543dd69e4b045b9ff7cd87e; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://www.dguv.de/ifa/gestis/gestis-dnel-liste/index-2.jsp; STUDY_GROUP=GESTIS DNEL:15635049:-:--; QC_CATEGORY=Programmatically extracted from structured data source; Source overall passed QC, but this record was not manually checked; QC_STATUS=not determined; SOURCE_HASH=ToxValhc_b3de98b8eb39513e5c6944260e30c878
ToxValDB_HPVIS 5 endpoints
Source Endpoint Type Value Unit Species Route Duration Study Type Reference
ToxValDB_HPVIS NOAEL =5 % diet Rat oral chronic; 113 weeks chronic LONG_REF=Borzelleca J. and Hallagan J. (1988a) A chronic toxicity/carcinogenicity study of FD & C Yellow No. 5 (Tartazine) in rats. Fd Chem Toxic 26, 179-187.; TITLE=A chronic toxicity/carcinogenicity study of FD & C Yellow No. 5 (Tartazine) in rats; AUTHOR=Borzelleca J. and Hallagan J; QUALITY=1; EXTERNAL_SOURCE_ID=62461; EXTERNAL_SOURCE_ID_DESC=HPVIS ID; STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/63861d6de4b04f6bb1480596; RECORD_SOURCE_LEVEL=Extraction document; YEAR=1988; ORIGINAL_YEAR=1988; STUDY_GROUP=HPVIS:15639301:-:--; QC_CATEGORY=Programmatically extracted from structured data source; Source overall passed QC, but this record was not manually checked; QC_STATUS=not determined; SOURCE_HASH=ToxValhc_2b62e7008da20ce55ffd8f6c4f608e15
ToxValDB_HPVIS NOAEL =8103 mg/kg bw/day Mouse oral subchronic; 3 months subchronic LONG_REF=Borzelleca J. and Hallagan J. (1988b) A chronic toxicity/carcinogenicity study of FD & C Yellow No. 5 (Tartazine) in mice. Fd Chem Toxic 26, 189-194.; TITLE=A chronic toxicity/carcinogenicity study of FD & C Yellow No. 5 (Tartazine) in mice; AUTHOR=Borzelleca J. and Hallagan J; QUALITY=1; EXTERNAL_SOURCE_ID=61453; EXTERNAL_SOURCE_ID_DESC=HPVIS ID; STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/63861d6de4b04f6bb1480596; RECORD_SOURCE_LEVEL=Extraction document; YEAR=1988; ORIGINAL_YEAR=1988; STUDY_GROUP=HPVIS:15640245:M:--; QC_CATEGORY=Programmatically extracted from structured data source; Source overall passed QC, and this record was expert reviewed; QC_STATUS=pass; SOURCE_HASH=ToxValhc_72df1355ad833ccc1e011e18fe24d8b6
ToxValDB_HPVIS NOAEL =9753 mg/kg bw/day Mouse oral subchronic; 3 months subchronic LONG_REF=Borzelleca J. and Hallagan J. (1988b) A chronic toxicity/carcinogenicity study of FD & C Yellow No. 5 (Tartazine) in mice. Fd Chem Toxic 26, 189-194.; TITLE=A chronic toxicity/carcinogenicity study of FD & C Yellow No. 5 (Tartazine) in mice; AUTHOR=Borzelleca J. and Hallagan J; QUALITY=1; EXTERNAL_SOURCE_ID=61454; EXTERNAL_SOURCE_ID_DESC=HPVIS ID; STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/63861d6de4b04f6bb1480596; RECORD_SOURCE_LEVEL=Extraction document; YEAR=1988; ORIGINAL_YEAR=1988; STUDY_GROUP=HPVIS:15640246:F:--; QC_CATEGORY=Programmatically extracted from structured data source; Source overall passed QC, and this record was expert reviewed; QC_STATUS=pass; SOURCE_HASH=ToxValhc_d1ae46de0df7e480f0098dd58969568c
ToxValDB_HPVIS NOAEL =2641 mg/kg bw/day Rat oral chronic; 114 weeks reproduction developmental LONG_REF=Borzelleca J. and Hallagan J. (1988a) A chronic toxicity/carcinogenicity study of FD & C Yellow No. 5 (Tartazine) in rats. Fd Chem Toxic 26, 179-187.; TITLE=A chronic toxicity/carcinogenicity study of FD & C Yellow No. 5 (Tartazine) in rats; AUTHOR=Borzelleca J. and Hallagan J; QUALITY=1; EXTERNAL_SOURCE_ID=65358; EXTERNAL_SOURCE_ID_DESC=HPVIS ID; STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/63861d6de4b04f6bb1480598; RECORD_SOURCE_LEVEL=Extraction document; YEAR=1988; ORIGINAL_YEAR=1988; STUDY_GROUP=HPVIS:15643187:M:--; QC_CATEGORY=Programmatically extracted from structured data source; Source overall passed QC, and this record was expert reviewed; QC_STATUS=pass; SOURCE_HASH=ToxValhc_c501a85c6c23e3a024ac82e354894851
ToxValDB_HPVIS NOAEL =3348 mg/kg bw/day Rat oral chronic; 114 weeks reproduction developmental LONG_REF=Borzelleca J. and Hallagan J. (1988a) A chronic toxicity/carcinogenicity study of FD & C Yellow No. 5 (Tartazine) in rats. Fd Chem Toxic 26, 179-187.; TITLE=A chronic toxicity/carcinogenicity study of FD & C Yellow No. 5 (Tartazine) in rats; AUTHOR=Borzelleca J. and Hallagan J; QUALITY=1; EXTERNAL_SOURCE_ID=65359; EXTERNAL_SOURCE_ID_DESC=HPVIS ID; STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/63861d6de4b04f6bb1480598; RECORD_SOURCE_LEVEL=Extraction document; YEAR=1988; ORIGINAL_YEAR=1988; STUDY_GROUP=HPVIS:15643188:M:-paternal; QC_CATEGORY=Programmatically extracted from structured data source; Source overall passed QC, and this record was expert reviewed; QC_STATUS=pass; SOURCE_HASH=ToxValhc_c3b355d90b659024fa3440a19a059cba
ToxValDB_WHO_JECFA_ADI 1 endpoint
Source Endpoint Type Value Unit Species Route Duration Study Type Reference
ToxValDB_WHO_JECFA_ADI ADI <=10 mg/kg Human oral - Toxicity Value STORED_SOURCE_RECORD=https://clowder.edap-cluster.com/files/650afc40e4b0d99f5a87c0aa; RECORD_SOURCE_LEVEL=Extraction document; SOURCE_URL=https://apps.who.int/food-additives-contaminants-jecfa-database/; SUBSOURCE_URL=https://apps.who.int/food-additives-contaminants-jecfa-database/Home/Chemical/477; YEAR=2016; ORIGINAL_YEAR=2016; STUDY_GROUP=WHO JECFA ADI:15715372:-:--; QC_CATEGORY=Programmatically extracted from structured data source; Source overall passed QC, but this record was not manually checked; QC_STATUS=not determined; SOURCE_HASH=ToxValhc_eb5e3cc371b5dc63568bd12ef5df6f10
UnifiedCodex:SCCNFP:beta.noael_studies 9 endpoints
Source Endpoint Type Value Unit Species Route Duration Study Type Reference
UnifiedCodex:SCCNFP:beta.noael_studies - >1000 mg/kg/day rat oral - - SOURCE_SUBDIR=out260_en; REPORT_TITLE=OPINION OF THE SCIENTIFIC COMMITTEE ON COSMETIC PRODUCTS AND NON-FOOD PRODUCTS INTENDED FOR CONSUMERS CONCERNING ACID YELLOW 23 COLIPA n° C29; OPINION_NUMBER=SCCNFP/0786/04; COMMITTEE=SCCNFP; REPORT_DATE=adopted by the SCCNFP on 23 April 2004; VALUE_TEXT=> 1000; DOSE=The mean daily food consumption was significantly higher in the 1000 mg/kg dose group, indicating an effect on food utilization.; EFFECT=e-related differences between treatment groups and control group were noted in behaviour, external maternal findings, and body weight. The mean daily food consumption was significantly higher in the 1000 mg/kg dose group, indicating an effect on food utilization. No dose- related changes were observed in pregnancy rate, implantation efficiency, maternal findings, foetal viability or foetal development. Examination of offspring for external and skeletal variations revealed no dose-related increase of incidence. The NOAEL for teratogenicity of Acid Yellow 23 was > 1000 mg/kg/day in this study. The study is regarded as valid and relevant for risk assessment, as a sufficient number of animals and relevant endpoints were examined. Ref.: 7 Mated, sperm-positive female rats were dosed with 0.05, 0.1, 0.2, 0.4, or 0.7 % in drinking water (equivalent to 67 –1064 mg/kg/ day) with Acid Yellow 23, from GD 0 to 19. No unusual behaviour or remarkable external maternal findings were noted. Mean daily food consumption and body weight gain wer; CITATION=Ref.: 7 Mated, sperm-positive female rats were dosed with 0; CITATION_NUMBERS=[7]; REFERENCE=Ref.: 7 Mated, sperm-positive female rats were dosed with 0; DETAILS_JSON={"cas_number":"1934-21-0","citation":"Ref.: 7 Mated, sperm-positive female rats were dosed with 0","dose":"The mean daily food consumption was significantly higher in the 1000 mg/kg dose group, indicating an effect on food utilization.","duration":"","effect":"e-related differences between treatment groups and control group were noted in behaviour, external maternal findings, and body weight. The mean daily food consumption was significantly higher in the 1000 mg/kg dose group, indicating an effect on food utilization. No dose- related changes were observed in pregnancy rate, implantation efficiency, maternal findings, foetal viability or foetal development. Examination of offspring for external and skeletal variations revealed no dose-related increase of incidence. The NOAEL for teratogenicity of Acid Yellow 23 was > 1000 mg/kg/day in this study. The study is regarded as valid and relevant for risk assessment, as a sufficient number of animals and relevant endpoints were examined. Ref.: 7 Mated, sperm-positive female rats were dosed with 0.05, 0.1, 0.2, 0.4, or 0.7 % in drinking water (equivalent to 67 –1064 mg/kg/ day) with Acid Yellow 23, from GD 0 to 19. No unusual behaviour or remarkable external maternal findings were noted. Mean daily food consumption and body weight gain wer","endpoint":"","ingredient":"codes","loael_value":"","noael_unit":"mg/kg/day","noael_value":"> 1000","page":13,"route":"oral","species":"rat","study_id":"out260_en_noael_003"}
UnifiedCodex:SCCNFP:beta.noael_studies carcinogenicity =2640 mg/kg rat oral - carcinogenicity SOURCE_SUBDIR=out260_en; REPORT_TITLE=OPINION OF THE SCIENTIFIC COMMITTEE ON COSMETIC PRODUCTS AND NON-FOOD PRODUCTS INTENDED FOR CONSUMERS CONCERNING ACID YELLOW 23 COLIPA n° C29; OPINION_NUMBER=SCCNFP/0786/04; COMMITTEE=SCCNFP; REPORT_DATE=adopted by the SCCNFP on 23 April 2004; VALUE_TEXT== 2640; DOSE=Safety evaluation CALCULATION OF THE MARGIN OF SAFETY (Acid Yellow 23) (Semi-permanent) Maximum absorption through the skin A (µg/cm2) = 13.2 µg/cm2 Typical body weight of human = 60 kg Skin Area surface SAS (cm2) = 700 cm2 Dermal absorption per treatment SAS x A x 0.001 = 9.24 mg Systemic exposure dose (SED) SAS x A x 0.001/60 = 0.154 mg/kg No...; EFFECT=d not demonstrate carcinogenic effects. Ref.: 29 Human studies No data. 2.10. Special investigations No data 2.11. Safety evaluation CALCULATION OF THE MARGIN OF SAFETY (Acid Yellow 23) (Semi-permanent) Maximum absorption through the skin A (µg/cm2) = 13.2 µg/cm2 Typical body weight of human = 60 kg Skin Area surface SAS (cm2) = 700 cm2 Dermal absorption per treatment SAS x A x 0.001 = 9.24 mg Systemic exposure dose (SED) SAS x A x 0.001/60 = 0.154 mg/kg No observed effect level (mg/kg) NOEL = 2640 mg/kg (rat, carcinogenicity, oral) Margin of Safety NOAEL / SED = 17143 2.12. Conclusions Physical and chemical characterisation The information provided on the compound is largely incomplete and confusing regarding purity and physical constants. The stability data are not acceptable. The basic toxicity data for Acid Yellow 23 is poor. A NOAEL for Acid Yellow 23 was derived of 5% in food, equivalent to 2640 and 3348 mg/kg/day in male and female rats respectively. Acid Yellow 23 was not consider; CITATION=Ref.: 29 Human studies No data; CITATION_NUMBERS=[29]; REFERENCE=Ref.: 29 Human studies No data; DETAILS_JSON={"cas_number":"1934-21-0","citation":"Ref.: 29 Human studies No data","dose":"Safety evaluation CALCULATION OF THE MARGIN OF SAFETY (Acid Yellow 23) (Semi-permanent) Maximum absorption through the skin A (µg/cm2) = 13.2 µg/cm2 Typical body weight of human = 60 kg Skin Area surface SAS (cm2) = 700 cm2 Dermal absorption per treatment SAS x A x 0.001 = 9.24 mg Systemic exposure dose (SED) SAS x A x 0.001/60 = 0.154 mg/kg No...","duration":"","effect":"d not demonstrate carcinogenic effects. Ref.: 29 Human studies No data. 2.10. Special investigations No data 2.11. Safety evaluation CALCULATION OF THE MARGIN OF SAFETY (Acid Yellow 23) (Semi-permanent) Maximum absorption through the skin A (µg/cm2) = 13.2 µg/cm2 Typical body weight of human = 60 kg Skin Area surface SAS (cm2) = 700 cm2 Dermal absorption per treatment SAS x A x 0.001 = 9.24 mg Systemic exposure dose (SED) SAS x A x 0.001/60 = 0.154 mg/kg No observed effect level (mg/kg) NOEL = 2640 mg/kg (rat, carcinogenicity, oral) Margin of Safety NOAEL / SED = 17143 2.12. Conclusions Physical and chemical characterisation The information provided on the compound is largely incomplete and confusing regarding purity and physical constants. The stability data are not acceptable. The basic toxicity data for Acid Yellow 23 is poor. A NOAEL for Acid Yellow 23 was derived of 5% in food, equivalent to 2640 and 3348 mg/kg/day in male and female rats respectively. Acid Yellow 23 was not consider","endpoint":"carcinogenicity","ingredient":"codes","loael_value":"","noael_unit":"mg/kg","noael_value":"= 2640","page":20,"route":"oral","species":"rat","study_id":"out260_en_noael_006"}
UnifiedCodex:SCCNFP:beta.noael_studies carcinogenicity =2640 mg/kg rat oral - carcinogenicity SOURCE_SUBDIR=out260_en; REPORT_TITLE=OPINION OF THE SCIENTIFIC COMMITTEE ON COSMETIC PRODUCTS AND NON-FOOD PRODUCTS INTENDED FOR CONSUMERS CONCERNING ACID YELLOW 23 COLIPA n° C29; OPINION_NUMBER=SCCNFP/0786/04; COMMITTEE=SCCNFP; REPORT_DATE=adopted by the SCCNFP on 23 April 2004; VALUE_TEXT== 2640; DOSE=Safety evaluation CALCULATION OF THE MARGIN OF SAFETY (Acid Yellow 23) (Semi-permanent) Maximum absorption through the skin A (µg/cm2) = 13.2 µg/cm2 Typical body weight of human = 60 kg Skin Area surface SAS (cm2) = 700 cm2 Dermal absorption per treatment SAS x A x 0.001 = 9.24 mg Systemic exposure dose (SED) SAS x A x 0.001/60 = 0.154 mg/kg No...; EFFECT=. 2.10. Special investigations No data 2.11. Safety evaluation CALCULATION OF THE MARGIN OF SAFETY (Acid Yellow 23) (Semi-permanent) Maximum absorption through the skin A (µg/cm2) = 13.2 µg/cm2 Typical body weight of human = 60 kg Skin Area surface SAS (cm2) = 700 cm2 Dermal absorption per treatment SAS x A x 0.001 = 9.24 mg Systemic exposure dose (SED) SAS x A x 0.001/60 = 0.154 mg/kg No observed effect level (mg/kg) NOEL = 2640 mg/kg (rat, carcinogenicity, oral) Margin of Safety NOAEL / SED = 17143 2.12. Conclusions Physical and chemical characterisation The information provided on the compound is largely incomplete and confusing regarding purity and physical constants. The stability data are not acceptable. The basic toxicity data for Acid Yellow 23 is poor. A NOAEL for Acid Yellow 23 was derived of 5% in food, equivalent to 2640 and 3348 mg/kg/day in male and female rats respectively. Acid Yellow 23 was not considered maternotoxic or foetotoxic up to 5% in food. No data concerning skin; CITATION_NUMBERS=[]; DETAILS_JSON={"cas_number":"1934-21-0","citation":"","dose":"Safety evaluation CALCULATION OF THE MARGIN OF SAFETY (Acid Yellow 23) (Semi-permanent) Maximum absorption through the skin A (µg/cm2) = 13.2 µg/cm2 Typical body weight of human = 60 kg Skin Area surface SAS (cm2) = 700 cm2 Dermal absorption per treatment SAS x A x 0.001 = 9.24 mg Systemic exposure dose (SED) SAS x A x 0.001/60 = 0.154 mg/kg No...","duration":"","effect":". 2.10. Special investigations No data 2.11. Safety evaluation CALCULATION OF THE MARGIN OF SAFETY (Acid Yellow 23) (Semi-permanent) Maximum absorption through the skin A (µg/cm2) = 13.2 µg/cm2 Typical body weight of human = 60 kg Skin Area surface SAS (cm2) = 700 cm2 Dermal absorption per treatment SAS x A x 0.001 = 9.24 mg Systemic exposure dose (SED) SAS x A x 0.001/60 = 0.154 mg/kg No observed effect level (mg/kg) NOEL = 2640 mg/kg (rat, carcinogenicity, oral) Margin of Safety NOAEL / SED = 17143 2.12. Conclusions Physical and chemical characterisation The information provided on the compound is largely incomplete and confusing regarding purity and physical constants. The stability data are not acceptable. The basic toxicity data for Acid Yellow 23 is poor. A NOAEL for Acid Yellow 23 was derived of 5% in food, equivalent to 2640 and 3348 mg/kg/day in male and female rats respectively. Acid Yellow 23 was not considered maternotoxic or foetotoxic up to 5% in food. No data concerning skin","endpoint":"carcinogenicity","ingredient":"codes","loael_value":"","noael_unit":"mg/kg","noael_value":"= 2640","page":20,"route":"oral","species":"rat","study_id":"out260_en_noael_007"}
UnifiedCodex:SCCNFP:beta.noael_studies carcinogenicity 5 % rat oral - carcinogenicity SOURCE_SUBDIR=out260_en; REPORT_TITLE=OPINION OF THE SCIENTIFIC COMMITTEE ON COSMETIC PRODUCTS AND NON-FOOD PRODUCTS INTENDED FOR CONSUMERS CONCERNING ACID YELLOW 23 COLIPA n° C29; OPINION_NUMBER=SCCNFP/0786/04; COMMITTEE=SCCNFP; REPORT_DATE=adopted by the SCCNFP on 23 April 2004; VALUE_TEXT=5; DOSE=mal absorption per treatment SAS x A x 0.001 = 9.24 mg Systemic exposure dose (SED) SAS x A x 0.001/60 = 0.154 mg/kg No observed effect level (mg/kg) NOEL = 2640 mg/kg (rat, carcinogenicity, oral) Margin of Safety NOAEL / SED = 17143 2.12.; EFFECT=mal absorption per treatment SAS x A x 0.001 = 9.24 mg Systemic exposure dose (SED) SAS x A x 0.001/60 = 0.154 mg/kg No observed effect level (mg/kg) NOEL = 2640 mg/kg (rat, carcinogenicity, oral) Margin of Safety NOAEL / SED = 17143 2.12. Conclusions Physical and chemical characterisation The information provided on the compound is largely incomplete and confusing regarding purity and physical constants. The stability data are not acceptable. The basic toxicity data for Acid Yellow 23 is poor. A NOAEL for Acid Yellow 23 was derived of 5% in food, equivalent to 2640 and 3348 mg/kg/day in male and female rats respectively. Acid Yellow 23 was not considered maternotoxic or foetotoxic up to 5% in food. No data concerning skin irritation of Acid Yellow 23 are available. No conclusions from limited reported patch tests are possible. Acid Yellow 23 it is not expected to cause irritant effects following repeated treatment of eyes in a concentration of 3 % in aqueous solution. A guinea pig maximization test pointed to; CITATION_NUMBERS=[]; DETAILS_JSON={"cas_number":"1934-21-0","citation":"","dose":"mal absorption per treatment SAS x A x 0.001 = 9.24 mg Systemic exposure dose (SED) SAS x A x 0.001/60 = 0.154 mg/kg No observed effect level (mg/kg) NOEL = 2640 mg/kg (rat, carcinogenicity, oral) Margin of Safety NOAEL / SED = 17143 2.12.","duration":"","effect":"mal absorption per treatment SAS x A x 0.001 = 9.24 mg Systemic exposure dose (SED) SAS x A x 0.001/60 = 0.154 mg/kg No observed effect level (mg/kg) NOEL = 2640 mg/kg (rat, carcinogenicity, oral) Margin of Safety NOAEL / SED = 17143 2.12. Conclusions Physical and chemical characterisation The information provided on the compound is largely incomplete and confusing regarding purity and physical constants. The stability data are not acceptable. The basic toxicity data for Acid Yellow 23 is poor. A NOAEL for Acid Yellow 23 was derived of 5% in food, equivalent to 2640 and 3348 mg/kg/day in male and female rats respectively. Acid Yellow 23 was not considered maternotoxic or foetotoxic up to 5% in food. No data concerning skin irritation of Acid Yellow 23 are available. No conclusions from limited reported patch tests are possible. Acid Yellow 23 it is not expected to cause irritant effects following repeated treatment of eyes in a concentration of 3 % in aqueous solution. A guinea pig maximization test pointed to","endpoint":"carcinogenicity","ingredient":"codes","loael_value":"","noael_unit":"%","noael_value":"5","page":20,"route":"oral","species":"rat","study_id":"out260_en_noael_008"}
UnifiedCodex:SCCNFP:beta.noael_studies carcinogenicity 2640 mg/kg rat oral - carcinogenicity SOURCE_SUBDIR=out260_en; REPORT_TITLE=OPINION OF THE SCIENTIFIC COMMITTEE ON COSMETIC PRODUCTS AND NON-FOOD PRODUCTS INTENDED FOR CONSUMERS CONCERNING ACID YELLOW 23 COLIPA n° C29; OPINION_NUMBER=SCCNFP/0786/04; COMMITTEE=SCCNFP; REPORT_DATE=adopted by the SCCNFP on 23 April 2004; VALUE_TEXT=2640; DOSE=No observed effect level (mg/kg) (rat, carcinogenicity, oral) | NOEL | 2640 mg/kg; EFFECT=CALCULATION OF THE MARGIN OF SAFETY (Acid Yellow 23) (Semi-permanent): No observed effect level (mg/kg) (rat, carcinogenicity, oral) | NOEL | 2640 mg/kg; CITATION_NUMBERS=[]; DETAILS_JSON={"cas_number":"1934-21-0","citation":"","dose":"No observed effect level (mg/kg) (rat, carcinogenicity, oral) | NOEL | 2640 mg/kg","duration":"","effect":"CALCULATION OF THE MARGIN OF SAFETY (Acid Yellow 23) (Semi-permanent): No observed effect level (mg/kg) (rat, carcinogenicity, oral) | NOEL | 2640 mg/kg","endpoint":"carcinogenicity","ingredient":"codes","loael_value":"","noael_unit":"mg/kg","noael_value":"2640","page":20,"route":"oral","species":"rat","study_id":"out260_en_noael_009"}
UnifiedCodex:SCCNFP:beta.noael_studies repeated dose toxicity 5 % - dermal Sub-chronic repeated dose toxicity SOURCE_SUBDIR=out260_en; REPORT_TITLE=OPINION OF THE SCIENTIFIC COMMITTEE ON COSMETIC PRODUCTS AND NON-FOOD PRODUCTS INTENDED FOR CONSUMERS CONCERNING ACID YELLOW 23 COLIPA n° C29; OPINION_NUMBER=SCCNFP/0786/04; COMMITTEE=SCCNFP; REPORT_DATE=adopted by the SCCNFP on 23 April 2004; VALUE_TEXT=5; DOSE=No NOAEL in mg/kg/day could be derived due to the missing data on water consumption.; EFFECT=SCCNFP/0786/04 Evaluation and opinion on Acid Yellow 23 _____________________________________________________________________________________________ 7 of the 5 % group animals that died during the experiment. No information was given on histology of animals at the end of treatment. No NOAEL in mg/kg/day could be derived due to the missing data on water consumption. Ref.: 2 2.3.8. Sub-chronic dermal toxicity No data 2.3.9. Sub-chronic inhalation toxicity No data 2.3.10. Chronic toxicity No chronic study was provided. Several carcinogenicity studies were provided but there were many data gaps. It would seem from these studies that other than coloured fur and faeces there were no dose-related effects from Acid Yellow 23. A NOAEL was derived of 5% in food, equivalent to 2640 and 3348 mg/kg/day in m; CITATION=Ref.: 2 2; CITATION_NUMBERS=[2]; REFERENCE=Ref.: 2 2; DETAILS_JSON={"cas_number":"1934-21-0","citation":"Ref.: 2 2","dose":"No NOAEL in mg/kg/day could be derived due to the missing data on water consumption.","duration":"Sub-chronic","effect":"SCCNFP/0786/04 Evaluation and opinion on Acid Yellow 23 _____________________________________________________________________________________________ 7 of the 5 % group animals that died during the experiment. No information was given on histology of animals at the end of treatment. No NOAEL in mg/kg/day could be derived due to the missing data on water consumption. Ref.: 2 2.3.8. Sub-chronic dermal toxicity No data 2.3.9. Sub-chronic inhalation toxicity No data 2.3.10. Chronic toxicity No chronic study was provided. Several carcinogenicity studies were provided but there were many data gaps. It would seem from these studies that other than coloured fur and faeces there were no dose-related effects from Acid Yellow 23. A NOAEL was derived of 5% in food, equivalent to 2640 and 3348 mg/kg/day in m","endpoint":"repeated dose toxicity","ingredient":"codes","loael_value":"","noael_unit":"%","noael_value":"5","page":7,"route":"dermal","species":"","study_id":"out260_en_noael_001"}
UnifiedCodex:SCCNFP:beta.noael_studies repeated dose toxicity 5 % rabbit dermal Sub-chronic repeated dose toxicity SOURCE_SUBDIR=out260_en; REPORT_TITLE=OPINION OF THE SCIENTIFIC COMMITTEE ON COSMETIC PRODUCTS AND NON-FOOD PRODUCTS INTENDED FOR CONSUMERS CONCERNING ACID YELLOW 23 COLIPA n° C29; OPINION_NUMBER=SCCNFP/0786/04; COMMITTEE=SCCNFP; REPORT_DATE=adopted by the SCCNFP on 23 April 2004; VALUE_TEXT=5; DOSE=No NOAEL in mg/kg/day could be derived due to the missing data on water consumption.; EFFECT=rmation was given on histology of animals at the end of treatment. No NOAEL in mg/kg/day could be derived due to the missing data on water consumption. Ref.: 2 2.3.8. Sub-chronic dermal toxicity No data 2.3.9. Sub-chronic inhalation toxicity No data 2.3.10. Chronic toxicity No chronic study was provided. Several carcinogenicity studies were provided but there were many data gaps. It would seem from these studies that other than coloured fur and faeces there were no dose-related effects from Acid Yellow 23. A NOAEL was derived of 5% in food, equivalent to 2640 and 3348 mg/kg/day in males and females respectively. Ref.: 9, 2, 3 2.4. Irritation & corrosivity 2.4.1. Irritation (skin) No data concerning skin irritation of Acid Yellow 23 are available. No conclusions from limited reported patch tests are possible. 2.4.2. Irritation (mucous membranes) Repeated eye irritation study in rabbits Guideline : / Species : New Zealand White rabbits Group size : 6 of each sex Test substance : Acid Yellow 23; commercial sample; no in; CITATION=Ref.: 2 2; CITATION_NUMBERS=[2]; REFERENCE=Ref.: 2 2; DETAILS_JSON={"cas_number":"1934-21-0","citation":"Ref.: 2 2","dose":"No NOAEL in mg/kg/day could be derived due to the missing data on water consumption.","duration":"Sub-chronic","effect":"rmation was given on histology of animals at the end of treatment. No NOAEL in mg/kg/day could be derived due to the missing data on water consumption. Ref.: 2 2.3.8. Sub-chronic dermal toxicity No data 2.3.9. Sub-chronic inhalation toxicity No data 2.3.10. Chronic toxicity No chronic study was provided. Several carcinogenicity studies were provided but there were many data gaps. It would seem from these studies that other than coloured fur and faeces there were no dose-related effects from Acid Yellow 23. A NOAEL was derived of 5% in food, equivalent to 2640 and 3348 mg/kg/day in males and females respectively. Ref.: 9, 2, 3 2.4. Irritation & corrosivity 2.4.1. Irritation (skin) No data concerning skin irritation of Acid Yellow 23 are available. No conclusions from limited reported patch tests are possible. 2.4.2. Irritation (mucous membranes) Repeated eye irritation study in rabbits Guideline : / Species : New Zealand White rabbits Group size : 6 of each sex Test substance : Acid Yellow 23; commercial sample; no in","endpoint":"repeated dose toxicity","ingredient":"codes","loael_value":"","noael_unit":"%","noael_value":"5","page":7,"route":"dermal","species":"rabbit","study_id":"out260_en_noael_002"}
UnifiedCodex:SCCNFP:beta.noael_studies reproductive toxicity >0.7 % rat oral chronic reproductive toxicity SOURCE_SUBDIR=out260_en; REPORT_TITLE=OPINION OF THE SCIENTIFIC COMMITTEE ON COSMETIC PRODUCTS AND NON-FOOD PRODUCTS INTENDED FOR CONSUMERS CONCERNING ACID YELLOW 23 COLIPA n° C29; OPINION_NUMBER=SCCNFP/0786/04; COMMITTEE=SCCNFP; REPORT_DATE=adopted by the SCCNFP on 23 April 2004; VALUE_TEXT=> 0.7; DOSE=A significant increase in fluid consumption was observed in the 0.2, 0.4, and 0.7 % dose groups.; EFFECT=able external maternal findings were noted. Mean daily food consumption and body weight gain were similar in all groups. A significant increase in fluid consumption was observed in the 0.2, 0.4, and 0.7 % dose groups. No dose-related changes were observed in pregnancy rate, implantation efficiency, foetal viability or foetal development. Reproductive findings at necropsy were unremarkable. Examination of offspring for external, skeletal and soft tissue variations revealed no dose-related increase of incidence. The NOAEL for teratogenic toxicity of Acid Yellow 23 was > 0.7% corresponding to 1064 mg/kg/day based on the mean fluid consumption in this study. A sufficient number of animals was regarded and relevant endpoints were examined. The study is judged as valid and relevant for risk assessment. Ref.: 8 A 2-generation chronic toxicity/carcinogenicity study was conducted with different concentrations of Acid Yellow 23. Male and female rats were fed a basal diet (control group) or basal diet blended with commercial Acid Yellow 2; CITATION=Ref.: 8 A 2-generation chronic toxicity/carcinogenicity study was conducted with different concentrations of Acid Yellow 23; CITATION_NUMBERS=[8,2,23]; REFERENCE=Ref.: 8 A 2-generation chronic toxicity/carcinogenicity study was conducted with different concentrations of Acid Yellow 23; DETAILS_JSON={"cas_number":"1934-21-0","citation":"Ref.: 8 A 2-generation chronic toxicity/carcinogenicity study was conducted with different concentrations of Acid Yellow 23","dose":"A significant increase in fluid consumption was observed in the 0.2, 0.4, and 0.7 % dose groups.","duration":"chronic","effect":"able external maternal findings were noted. Mean daily food consumption and body weight gain were similar in all groups. A significant increase in fluid consumption was observed in the 0.2, 0.4, and 0.7 % dose groups. No dose-related changes were observed in pregnancy rate, implantation efficiency, foetal viability or foetal development. Reproductive findings at necropsy were unremarkable. Examination of offspring for external, skeletal and soft tissue variations revealed no dose-related increase of incidence. The NOAEL for teratogenic toxicity of Acid Yellow 23 was > 0.7% corresponding to 1064 mg/kg/day based on the mean fluid consumption in this study. A sufficient number of animals was regarded and relevant endpoints were examined. The study is judged as valid and relevant for risk assessment. Ref.: 8 A 2-generation chronic toxicity/carcinogenicity study was conducted with different concentrations of Acid Yellow 23. Male and female rats were fed a basal diet (control group) or basal diet blended with commercial Acid Yellow 2","endpoint":"reproductive toxicity","ingredient":"codes","loael_value":"","noael_unit":"%","noael_value":"> 0.7","page":13,"route":"oral","species":"rat","study_id":"out260_en_noael_004"}
UnifiedCodex:SCCNFP:beta.noael_studies reproductive toxicity 5 % rat oral 2 months reproductive toxicity SOURCE_SUBDIR=out260_en; REPORT_TITLE=OPINION OF THE SCIENTIFIC COMMITTEE ON COSMETIC PRODUCTS AND NON-FOOD PRODUCTS INTENDED FOR CONSUMERS CONCERNING ACID YELLOW 23 COLIPA n° C29; OPINION_NUMBER=SCCNFP/0786/04; COMMITTEE=SCCNFP; REPORT_DATE=adopted by the SCCNFP on 23 April 2004; VALUE_TEXT=5; DOSE=Slight decreases in body weight (4-5 %), and slight increases in food consumption were noted at the 5.0 % dose group.; EFFECT=was conducted with different concentrations of Acid Yellow 23. Male and female rats were fed a basal diet (control group) or basal diet blended with commercial Acid Yellow 23 (0.1, 1.0, 2.0, 5.0 %) for approx. 2 months prior to mating. No treatment-related effects on fertility, gestation, parturition, lactation, pup survival through weaning or number of alive and still-born pups were observed. Slight decreases in body weight (4-5 %), and slight increases in food consumption were noted at the 5.0 % dose group. The NOAEL for reproductive and teratogenic toxicity of Acid Yellow 23 was 5 % in the diet. Ref.: 9 2.7. Toxicokinetics (incl. Percutaneous Absorption) Due to the effects of Acid Yellow 23 following ingestion as a food colorant, it is assumed that intestinal absorption of Acid Yellow 23 occurs. However, no metabolism studies are available. 2.7.1. Percutaneous Absorption in vitro Guideline : OECD Draft Guideline (1996) Species : Pig; CITATION=Ref.: 9 2; CITATION_NUMBERS=[9,2]; REFERENCE=Ref.: 9 2; DETAILS_JSON={"cas_number":"1934-21-0","citation":"Ref.: 9 2","dose":"Slight decreases in body weight (4-5 %), and slight increases in food consumption were noted at the 5.0 % dose group.","duration":"2 months","effect":"was conducted with different concentrations of Acid Yellow 23. Male and female rats were fed a basal diet (control group) or basal diet blended with commercial Acid Yellow 23 (0.1, 1.0, 2.0, 5.0 %) for approx. 2 months prior to mating. No treatment-related effects on fertility, gestation, parturition, lactation, pup survival through weaning or number of alive and still-born pups were observed. Slight decreases in body weight (4-5 %), and slight increases in food consumption were noted at the 5.0 % dose group. The NOAEL for reproductive and teratogenic toxicity of Acid Yellow 23 was 5 % in the diet. Ref.: 9 2.7. Toxicokinetics (incl. Percutaneous Absorption) Due to the effects of Acid Yellow 23 following ingestion as a food colorant, it is assumed that intestinal absorption of Acid Yellow 23 occurs. However, no metabolism studies are available. 2.7.1. Percutaneous Absorption in vitro Guideline : OECD Draft Guideline (1996) Species : Pig","endpoint":"reproductive toxicity","ingredient":"codes","loael_value":"","noael_unit":"%","noael_value":"5","page":13,"route":"oral","species":"rat","study_id":"out260_en_noael_005"}
openFDA substances 4 endpoints
Source Endpoint Type Value Unit Species Route Duration Study Type Reference
openFDA substances FDA UNII substance identifier I753WB2F1M UNII - - - chemical {"approval_status":null,"molecular_formula":"C16H9N4O9S2.3Na","source_table":"substance_identifiers_fda","substance_class":"chemical","unii_code":"I753WB2F1M"}
openFDA substances FDA UNII substance identifier I753WB2F1M UNII - - - chemical {"approval_status":null,"molecular_formula":"C16H9N4O9S2.3Na","source_table":"substance_identifiers_fda","substance_class":"chemical","unii_code":"I753WB2F1M"}
openFDA substances FDA UNII substance identifier I753WB2F1M UNII - - - chemical {"approval_status":null,"molecular_formula":"C16H9N4O9S2.3Na","source_table":"substance_identifiers_fda","substance_class":"chemical","unii_code":"I753WB2F1M"}
openFDA substances FDA UNII substance identifier I753WB2F1M UNII - - - chemical {"approval_status":null,"molecular_formula":"C16H9N4O9S2.3Na","source_table":"substance_identifiers_fda","substance_class":"chemical","unii_code":"I753WB2F1M"}