Mitotane Effects in a H295R Xenograft Model of Adjuvant Treatment of Adrenocortical Cancer

Ö. Lindhe; B. Skogseid

doi:10.1055/s-0030-1261923

Hormone and Metabolic Research, Inhaltsverzeichnis

Horm Metab Res 2010; 42(10): 725-730
DOI: 10.1055/s-0030-1261923

Animals, Clinical

Mitotane Effects in a H295R Xenograft Model of Adjuvant Treatment of Adrenocortical Cancer

Ö. Lindhe¹ ^, ² , B. Skogseid¹

¹Department of Medical Sciences, Uppsala University, Uppsala, Sweden
²Uppsala Imanet AB, GE Healthcare, Uppsala, Sweden

Abstract

Adrenocortical cancer is one of the most aggressive endocrine malignancies. Growth through the capsule or accidental release of cancer cells during surgery frequently results in metastatic disease. We investigated the antitumoral effect of 2 adrenocorticolytic compounds, o,p′-DDD and MeSO2-DDE, in the adrenocortical cell line H295R both in vitro and as a xenograft model in vivo. H295R cells were injected s. c. in nude mice. o,p′-DDD, MeSO2-DDE, or oil (control) was administered i. p., either simultaneously with cell injection at day 0 (mimicking adjuvant treatment), or at day 48 (established tumors). Accumulation of PET tracers [¹¹C]methionine (MET), [¹¹C] metomidate (MTO), 2-deoxy-2-[¹⁸F]fluoro-d-glucose (FDG), and [¹⁸F]-l-tyrosine (FLT) in the aggregates were assessed ± drug treatment in vitro. Tumor growth was significantly inhibited when o,p′-DDD was given at the same time as injection of tumor cells. No significant growth inhibition was observed after treatment with o,p′-DDD at day 48. A significant reduction in FLT uptake and an increased FDG uptake, compared to control, were observed following treatment with 15 μM o,p′-DDD (p<0.01) in vitro. MeSO2-DDE (15 μM) treatment gave rise to a reduced MET and an increased FLT uptake (p<0.01). Both compounds reduced the uptake of MTO compared to control (p<0.01). Treatment with o,p′-DDD simultaneously to inoculation of H295R cells in mice, imitating release of cells during surgery, gave a markedly better effect than treatment of established H295R tumors. We suggest that FLT may be a potential PET biomarker when assessing adrenocortical cancer treatment with o,p′-DDD. Further studies in humans are needed to investigate this.

Key words

mitotane - adjuvant - adrenocortical - H295R - xenograft

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References

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Correspondence

Ö. LindhePhD

Dept of Medical Sciences

Uppsala University

51 85 Uppsala

Sweden

Telefon: +46 18 611 37 68

Fax: +46 18 55 36 01

eMail: orjan.lindhe@medsci.uu.se