c-MYC induces mammary tumorigenesis by means of a preferred pathway involving spontaneous Kras2 mutations

D’Cruz, Celina M.; Gunther, Edward J.; Boxer, Robert; Hartman, J; Sintasath, Louis; Moody, Susan E.; Cox, James D.; Ha, Seung I.; Belka, George K.; Golant, Alexander; Cardiff, Robert D.; Chodosh, Lewis A.

doi:10.1038/84691

Cited by 386 publications

(326 citation statements)

References 18 publications

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“…This finding suggests that as tumors increase in size, they acquire additional genetic alterations that allow them to become independent of the initiating oncogene, IGF-IR. Regression rates observed with the 500 mm 3 tumors in the MTB-IGF-IR transgenics were similar to those observed in mammary tumors induced by Wnt1 (Gunther et al, 2003) or constitutively active ErbB2 (Moody et al, 2002) but considerably higher than regression rates observed in c-Myc-induced mammary tumors (D'Cruz et al, 2001;Boxer et al, 2004). The effect of tumor size on regression rates was not explored in these other doxycycline inducible mammary tumor models.…”

Section: Discussionmentioning

confidence: 62%

Reversibility and recurrence of IGF-IR-induced mammary tumors

et al. 2009

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Section: Discussionmentioning

confidence: 62%

Reversibility and recurrence of IGF-IR-induced mammary tumors

et al. 2009

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“…The 1.02 kb constitutively active human Alk5 T204D cDNA fragment including the carboxy-terminal HA tag was subcloned into the pBS-MMTVpA-GSK vector (D'Cruz et al, 2001) (provided by Lewis Chodosh, University of Pennsylvania). The linearized Tg was injected into one-cell-stage FVB mouse embryos, which were transplanted into pseudo-pregnant females.…”

Section: Methodsmentioning

confidence: 99%

Activated type I TGFβ receptor kinase enhances the survival of mammary epithelial cells and accelerates tumor progression

et al. 2005

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We have examined the effects of transforming growth factor-beta (TGFb) signaling on mammary epithelial cell survival. Transgenic mice expressing an active mutant of Alk5 in the mammary gland (MMTV-Alk5 T204D ) exhibited reduced apoptosis in terminal endbuds and during postlactational involution. Transgene-expressing mammary cells contained lower Smad2/3 and higher c-myc levels than controls, high ligand-independent phosphatidylinositol-3 kinase (PI3K) and Akt activities, and were insensitive to TGFb-mediated growth arrest. Treatment with a proteasome inhibitor increased Smad2/3 levels and ligand-independent Smad transcriptional reporter activity, as well as reduced both c-myc protein and basal cell proliferation. Treatment with an Alk5 kinase small-molecule inhibitor upregulated Smad2/3 levels, reduced PI3K activity, P-Akt, and c-myc, and inhibited cell survival. Although Alk5 T204D -expressing mice did not develop mammary tumors, bigenic MMTV-Alk T204D Â Neu mice developed cancers that were more metastatic than those occurring in MMTV-Neu transgenics. These data suggest that (1) TGFb can signal to PI3K/Akt and enhance mammary epithelial cell survival in vivo before cytological or histological evidence of transformation, and (2) TGFb signaling can provide epithelial cells with a 'gain-of-function' effect that synergizes with oncogene-induced transformation.

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“…Overexpression of c-Myc in transgenic mice results in an increased tumor formation, which is greatly enhanced by co-expression of Ras (Sinn et al, 1987). It has recently been demonstrated that c-Myc-induced mammary tumorigenesis proceeds through a preferred secondary oncogenic pathway involving Kras2 (D'Cruz et al, 2001). The mechanisms by which c-Myc participates in tumorigenesis are not yet completely understood.…”

Section: Introductionmentioning

confidence: 99%