EFFECTS OF SECRETORY PRODUCTS OF BREAST CANCER CELLS ON OSTEOBLAST-LIKE CELLS.SECRETORY PRODUCTS OF BREAST CANCER CELLS SPECIFICALLY AFFECT HUMAN OSTEOBLASTIC CELLS: PARTIAL CHARACTERIZATION OF ACTIVE FACTORS.
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REGULATION OF C-FOS AND C-JUN EXPRESSION BY CALCITONIN IN HUMAN BREAST CANCER CELLS.


Marc Lacroix, Jean Jacques Body
Calcified Tissue International (1997) 60, 513-519

   Breast cancer cells (BCC) possess calcitonin (CT) receptors, yet the action of the hormone on these cells is largely unknown. We found that CT produced a strong and transient time- and dose-dependent increase in c-fos mRNA in BCC lines. This event was prevented by a protein kinase A (PKA) inhibitor, H89. CT alone did not influence the expression of c-jun and of the tissue inhibitors of metalloproteases (timp) -1 and -2 mRNAs; however, it reduced the induction of these mRNAs by the protein kinase C (PKC) activator phorbol 12-myristate 13-acetate (PMA), without apparent changes in the half-life of the mRNA (measured for c-jun). Along the same line, CT reduced the c-jun induction and T-47D growth stimulation by epidermal growth factor (EGF) and insulin. These effects were mimicked by forskolin and/or prevented by H89, suggesting that PKA activation was involved. These results indicate that CT modulates in BCC the mRNA levels of two important growth-related early response genes (c-fos and c-jun) and of two other genes (timp-1 and -2) involved in the control of metastatic events.



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Made in BELGIUM / WALLONIA / EUREGIO MAAS-RHINE - Fait en BELGIQUE / WALLONIE / EUREGIO MEUSE-RHIN - (Molecular breast cancer - Cancer du sein, aspects moléculaires) - Marc Lacroix & SciMedWeb® 1997-2009