Small-molecule MAPK inhibitors restore radioiodine incorporation in mouse thyroid cancers with conditional BRAF activation
Debyani Chakravarty, … , Ronald Ghossein, James A. Fagin
Debyani Chakravarty, … , Ronald Ghossein, James A. Fagin
Published November 21, 2011
Citation Information: J Clin Invest. 2011;121(12):4700-4711. https://doi.org/10.1172/JCI46382.
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Research Article Oncology

Small-molecule MAPK inhibitors restore radioiodine incorporation in mouse thyroid cancers with conditional BRAF activation

Abstract

Advanced human thyroid cancers, particularly those that are refractory to treatment with radioiodine (RAI), have a high prevalence of BRAF (v-raf murine sarcoma viral oncogene homolog B1) mutations. However, the degree to which these cancers are dependent on BRAF expression is still unclear. To address this question, we generated mice expressing one of the most commonly detected BRAF mutations in human papillary thyroid carcinomas (BRAFV600E) in thyroid follicular cells in a doxycycline-inducible (dox-inducible) manner. Upon dox induction of BRAFV600E, the mice developed highly penetrant and poorly differentiated thyroid tumors. Discontinuation of dox extinguished BRAFV600E expression and reestablished thyroid follicular architecture and normal thyroid histology. Switching on BRAFV600E rapidly induced hypothyroidism and virtually abolished thyroid-specific gene expression and RAI incorporation, all of which were restored to near basal levels upon discontinuation of dox. Treatment of mice with these cancers with small molecule inhibitors of either MEK or mutant BRAF reduced their proliferative index and partially restored thyroid-specific gene expression. Strikingly, treatment with the MAPK pathway inhibitors rendered the tumor cells susceptible to a therapeutic dose of RAI. Our data show that thyroid tumors carrying BRAFV600E mutations are exquisitely dependent on the oncoprotein for viability and that genetic or pharmacological inhibition of its expression or activity is associated with tumor regression and restoration of RAI uptake in vivo in mice. These findings have potentially significant clinical ramifications.

Authors

Debyani Chakravarty, Elmer Santos, Mabel Ryder, Jeffrey A. Knauf, Xiao-Hui Liao, Brian L. West, Gideon Bollag, Richard Kolesnick, Tin Htwe Thin, Neal Rosen, Pat Zanzonico, Steven M. Larson, Samuel Refetoff, Ronald Ghossein, James A. Fagin

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Figure 4

Withdrawal of BRAFV600E expression leads to thyroid cancer cell apoptosis.

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Withdrawal of BRAFV600E expression leads to thyroid cancer cell apoptosi...
(A) Representative FFPE sections of thyroid tissues from Tg-rtTA/tetO-BRAFV600E fed dox for 1 week (on) and then regular chow (off) for the indicated times, assayed by TUNEL (top) and cleaved caspase-3 (bottom). There was a modest increase in apoptotic cells at 1 week on dox, which were scattered throughout the thyroid tumor specimen. In contrast, the brown-red staining cells were localized within the center of the cancer cell clusters 72 hours after dox withdrawal. Original magnification, ×400 (top panels); ×400 (bottom panels). (B and C) Quantification of TUNEL and cleaved caspase-3 (+) cells at the indicated times. Data are shown as mean ± SEM and correspond to manual counting of 3 high-power fields/mouse (n = 6).