Apoptosis in Stages of Mouse Hepatocarcinogenesis: Failure to Counterbalance Cell Proliferation and to Account for Strain Differences in Tumor Susceptibility

doi:10.1093/toxsci/kfi129

ToxSci Advance Access originally published online on February 23, 2005
Toxicological Sciences 2005 85(1):515-529; doi:10.1093/toxsci/kfi129

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Toxicological Sciences vol. 85 no. 1 © The Author 2005. Published by Oxford University Press on behalf of the Society of Toxicology. All rights reserved. For Permissions, please email: journals.permissions@oupjournals.org

Apoptosis in Stages of Mouse Hepatocarcinogenesis: Failure to Counterbalance Cell Proliferation and to Account for Strain Differences in Tumor Susceptibility

Wilfried Bursch^*^,1, Monika Chabicovsky^*^,2, Ute Wastl^*, Bettina Grasl-Kraupp^*, Krystina Bukowska^*, Henryk Taper and Rolf Schulte-Hermann^*

^* Medizinische Universität Wien, Univ. Klinik für Innere MedizinI, Abtl. Institut für Krebsforschung, Borschkegasse 8a, A-1090 Wien, and Unité de Biochemie Toxicologique et Cancérologique, Université Catholique Louvain, UCL 7369, B-1200 Bruxelles

Received July 20, 2004; accepted February 14, 2005

C3H/He and B6C3F1 show much higher liver cancer susceptibilitythan C57BL/6J mice. We studied the hypothesis that this differencemight result from failure of apoptosis. Hepatocarcinogenesiswas induced by a single dose of N-nitrosodiethylamine (NDEA),followed by phenobarbital (PB) for up to 90 weeks. We observed(1) earlier appearance of putative preneoplastic foci (PPF),hepatocellular adenoma (HCA), and carcinoma (HCC) in C3H/Hethan in C57Bl/6J mice and (2) an increase of hepatocellularDNA synthesis in C3H/He and C57Bl/6J mice, compared to normalliver, via PPF and HCA to HCC. PB enhanced DNA synthesis andgrowth of PPF, in the C3H/He strain only, and of HCA and HCCof both strains. Apoptoses were rare in unaltered livers aswell as in preneoplastic lesions, but tended to increase inHCA and HCC of both strains. PB lowered apoptotic activity inPPF of C3H/He mice, but enhanced it in HCA and HCC of C57Bl/6Jmice at late stages. In conclusion, the strain difference ingrowth rates of PPF and tumors is largely determined by higherrates of cell proliferation in C3H/He mice, with and withoutpromotion by PB. Moreover, in C57Bl/6J mice the promoting effectof PB was restricted to HCA and HCC and was not seen in PPF.Apoptosis was generally low and was not a major cause of thestrain difference in tumor susceptibility. In contrast withrat liver, inhibition of apoptosis appears to be a minor determinantof tumor promotion in mice.

Key Words: B6C3F1; C3H/He; C57BL/6J; hepatocarcinogenesis; tumor susceptibility; apoptosis; cell proliferation; phenobarbital.

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