مرکز منطقه ای اطلاع رساني علوم و فناوري -

پديد آورندگان :

Khorramizadeh M R نويسنده , Saadat F نويسنده , Allahyary H نويسنده , Pezeshki M نويسنده , Sarrafnejad A نويسنده , Mirshafiey A نويسنده , Safavifar F نويسنده , Alimoghaddam K نويسنده , Ghavamzadeh A نويسنده , Sadeghian S نويسنده

چكيده لاتين :

Recent evidences suggest that multiple myeloma phenotypes (MMPs) are involved in the infiltration of multiple myelomaaffected marrow foci. In this study, the effects of arsenic trioxide on the invasive and angiogenic phenotypes of multiple myeloma (MM) cell line were assessed on a dose-response and time-course basis. Multiple myeloma cell line, Karpas 707, was treated with step-wise elevated concentrations of arsenic trioxide compound at 24, 48, and 72 h intervals. Cytotoxicity was assessed with a colorimetric assay. Potential antiinvasive phenotype was analyzed with MMP-2 zymography. To verify directly the anti angiogenic effect, F1 endothelial cell line was also treated with arsenic and the dose-dependent cytotoxicity was assessed with a colorimetric assay. Apoptotic properties of arsenic trioxide compound were investigated using TUNEL assay. The significant dose-dependent inhibitory effects of arsenic trioxide on MMP-2 were seen at given concentrations. Cytotoxicity analysis revealed much higher cell death than untreated cells (P< 0.01), both in Karpas 707 and F1 endothelial cell lines. Colectively, this study showed that arsenic trioxide might potentially elicit anti-invasive anti-angiogenesis properties in the treatment of myeloma dissemination process. In addition, the concurrent inhibition of MMPs activity and endothelial cell proliferation could compose the scenario of neoangiogenesis inhibition in the marrow-infiltrated foci.