| First Author | Cho KH | Year | 2008 |
| Journal | Toxicol Res | Volume | 24 |
| Issue | 1 | Pages | 59-68 |
| PubMed ID | 32038778 | Mgi Jnum | J:341261 |
| Mgi Id | MGI:7536947 | Doi | 10.5487/TR.2008.24.1.059 |
| Citation | Cho KH, et al. (2008) Studies on N-Ethyl-N-nitrosourea Mutagenesis in BALB/c Mice. Toxicol Res |
| abstractText | N-ethyl-N-nitrosoures (ENU) is effective in inducing hypermorphic mutation as well as hypomorphic and antimorphic mutations. Therefore, this mutagen is used to the production of mutant in the mice. In order to perform an effective ENU mutagenesis using BALB/cAnN mice, determination of optimal dosage and dosage regimen of ENU is necessary. And this study tried to develop a suitable screening method and searched for novel and various mutants as model animals in phenotypedriven ENU mutagenesis. We have carried out dosage regimen for mutagenizing dose of 200 mg/kg ENU in the BALB/c mice. Total screened mice were 30,133. As the results of Esaki and Choâs Phenotype Screening, we got 2,516 phenotypic and behavior abnormalities in G1, G2 and G3 mice. One hundred thirty five G1 phenodeviants were tested for inheritance and 16 dominant mutants were discovered. Forty two recessive mutants were also found in tested 201 micropedigrees. Early-onset mutant mice included the dysmorphology of face, eye, tail, limb, skin, and foot and abnormal behavior like circling, swimming, head tossing, stiff-walking, high cholesterol level, and tremor etc. In this study we could effectively screen G3 recessive mutants. The frequent and concise early-onset screening before weaning will be available for ENU mutagenesis. |
