#618 Carcinogenicity (two rodent species)
Objective of the study
The objective of carcinogenicity study is to determine the carcinogenic effects of a substance in a mammalian species following prolonged and repeated exposure. More specifically, the carcinogenicity study aims to:
- Identify the carcinogenic properties of a chemical, resulting in an increased incidence of neoplasms, increased proportion of malignant neoplasms or a reduction in the time to appearance of neoplasms, compared with concurrent control groups;
- Identify target organ(s) of carcinogenicity;
- Identify the time to appearance of neoplasms;
- Characterise the tumour dose-response relationship;
- Identify of a no-observed-adverse-effect level (NOAEL) or point of departure for establishment of a Benchmark Dose (BMD).
If possible, the carcinogenicity study should be combined with the long-term oral toxicity study
Circumstances under which the study is recommended to be required
The carcinogenicity study is recommended if:
- The use of the pesticide is likely to result in significant human exposure over a considerable portion of the human lifespan which is significant in terms of either frequency, duration or magnitude of exposure; or
- The use requires a maximum residue limit or an exemption from the requirement of a maximum residue limit; or
- The active ingredient, metabolite, degradate, or impurity (a) is structurally related to a recognized carcinogen, or (b) causes mutagenic effects as demonstrated by in vitro or in vivo testing, or (c) produces a morphologic effect in any organ (e.g. hyperplasia, metaplasia) in sub-chronic studies that may lead to a neoplastic change.
If it is claimed that such testing is unnecessary, that claim shall be fully justified.
Test organism
The carcinogenicity study is normally conducted in two rodent species; rat and mouse are preferred.
Studies designed to simultaneously fulfil the requirements of both the carcinogenicity and the chronic oral studies (i.e. a combined study) may be conducted. Minimum acceptable study durations are:
- Chronic rodent study (food use): 24 months.
- Chronic rodent study (non-food use): 12 months.
- Mouse carcinogenicity study: 18 months.
- Rat carcinogenicity study: 24 months.
If comparative metabolism data indicate that either rat or mouse is an inappropriate model for human cancer risk assessment, an alternative species should be considered.
Test substance
- Technical grade active ingredient
Typical endpoints of the study
The No Observed Adverse Effect Level (NOAEL) is reported whenever possible.
Other typical endpoints of the study include, but are not limited to: survival, body weight, toxic response, necropsy findings, histopathological findings.
Conventional histopathological terminology such as that published by the International Agency for Research on Cancer (IARC) should be used in the nomenclature and reporting of tumours.
Test guidelines
The following test guidelines may be used for the long-term oral toxicity study:
- OECD Guidelines for the Testing of Chemicals. Test No. 451: Carcinogenicity studies.
- OECD Guidelines for the Testing of Chemicals. Test No. 453: Combined chronic toxicity/carcinogenicity studies.
- US EPA Health Effects Test Guidelines. OPPTS 870.4200. Carcinogenicity.
- US EPA Health Effects Test Guidelines. OPPTS 870.4300. Combined chronic toxicity/carcinogenicity.
- EC Testing Method B.32. Carcinogenicity test. Council Regulation (EC) No 440/2008.
- EC Testing Method B.33. Combined chronic toxicity/carcinogenicity test. Council Regulation (EC) No 440/2008.