Development and initial characterization of several new inbred strains of SENCAR mice for studies of multistage skin carcinogenesis

doi:10.1093/carcin/21.4.641

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Carcinogenesis, Vol. 21, No. 4, 641-646, April 2000
© 2000 Oxford University Press

Carcinogenesis

Development and initial characterization of several new inbred strains of SENCAR mice for studies of multistage skin carcinogenesis

Lezlee G. Coghlan, I. Gimenez-Conti¹, Heather E. Kleiner¹, Susan M. Fischer¹, Joyce E. Rundhaug¹, Claudio J. Conti¹, Thomas J. Slaga and John DiGiovanni¹^,2

The University of Texas M.D. Anderson Cancer Center, Science Park–Department of Veterinary Sciences, Bastrop, TX 78602 and
¹ The University of Texas M.D. Anderson Cancer Center, Science Park–Research Division, Smithville, TX 78957, USA

The development and initial characterization of five new inbredstrains of SENCAR mice are described in this paper. Ten randomlyselected pairs of outbred SENCAR mice were mated and offspringfrom each separately maintained parental line were sib matedat each successive generation to result in inbred strains. Dueto poor reproductive performance only five of the original 10lines were bred to homogeneity. Initial characterization ofthe five remaining lines (referred to as SL2/sprd, SL5/sprd,SL7/sprd, SL8/sprd and SLl0/sprd) at F12 for their responsivenessto a two-stage carcinogenesis protocol (10 nmol 7,12-dimethylbenz[a]anthraceneand 0.25 µg 12-O-tetradecanoylphorbol-13 acetate) revealedthree groups of responders in terms of the number of papillomasper mouse: SL2/sprd and SL8/sprd > SL7/sprd and SL10/sprd>> SL5/sprd. The papilloma responses in SL2/sprd and SL8/sprdwere very similar to SENCAR B/Pt compared at the same doses.Papillomas induced on SL2/sprd had the highest propensity toprogress to squamous cell carcinomas, similar to that observedin outbred SENCAR and SENCAR B/Pt mice. More detailed comparisonof the responsiveness of SL2/sprd and SL5/sprd at Fl5 showedthat these two inbred strains differed in their sensitivityto TPA-induced epidermal hyperplasia and that the dose of TPArequired to produce a tumor response in SL5/sprd in comparisonwith that in SL2/sprd was 4–20 times higher. Overall,the availability of the different inbred SENCAR strains willgreatly aid mechanistic studies of multistage skin carcinogenesisas well as studies to understand the underlying genetic basisof resistance to tumor promotion and progression in this modelsystem.

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