E-cadherin: A determinant molecule associated with ovarian cancer progression, dissemination and aggressiveness.

Ovarian cancer (OC) is the fifth cancer death cause in women worldwide. The malignant nature of this disease stems from its unique dissemination pattern. Epithelial-to-mesenchymal transition (EMT) has been reported in OC and downregulation of Epithelial cadherin (E-cadherin) is a hallmark of this process. However, findings on the relationship between E-cadherin levels and OC progression, dissemination and aggressiveness are controversial. In this study, the evaluation of E-cadherin expression in an OC tissue microarray revealed its prognostic value to discriminate between advanced- and early-stage tumors, as well as serous tumors from other histologies. Moreover, E-cadherin, Neural cadherin (N-cadherin), cytokeratins and vimentin expression was assessed in TOV-112, SKOV-3, OAW-42 and OV-90 OC cell lines grown in monolayers and under anchorage-independent conditions to mimic ovarian tumor cell dissemination, and results were associated with cell aggressiveness. According to these EMT-related markers, cell lines were classified as mesenchymal (M; TOV-112), intermediate mesenchymal (IM; SKOV-3), intermediate epithelial (IE; OAW-42) and epithelial (E; OV-90). M- and IM-cells depicted the highest migration capacity when grown in monolayers, and aggregates derived from M- and IM-cell lines showed lower cell death, higher adhesion to extracellular matrices and higher invasion capacity than E- and IE-aggregates. The analysis of E-cadherin, N-cadherin, cytokeratin 19 and vimentin mRNA levels in 20 advanced-stage high-grade serous human OC ascites showed an IM phenotype in all cases, characterized by higher proportions of N- to E-cadherin and vimentin to cytokeratin 19. In particular, higher E-cadherin mRNA levels were associated with cancer antigen 125 levels more than 500 U/mL and platinum-free intervals less than 6 months. Altogether, E-cadherin expression levels were found relevant for the assessment of OC progression and aggressiveness.

Efecto antimitogénico de extractos de Pygeum africanum sobre líneas celulares de cáncer de próstata humana y explantes de hiperplasia benigna de próstata / Antimytogenic effect of Pygeum africanum extracts on human prostate cancer cell lines and benign prostatic hyperplasia explants

OBJETIVOS: Analizar el efecto de extractos de Pygeum africanum sobre la proliferación de células de próstata humana, in vitro. MÉTODOS: Líneas celulares tumorales prostáticas, así como células epiteliales derivadas de hiperplasia benigna de próstata fueron puestas en cultivo y tratadas con extractos de P. africanum. El efecto sobre la proliferación celular fue monitorizado mediante incorporación de (3H)-timidina o bromodesoxiuridina y ensayos de citometría de flujo. RESULTADOS: La incubación con extractos de P. africanum, con o sin adición de aminoácidos, inhibe significativamente y de forma dosis-dependiente la proliferación de las líneas celulares derivadas de cáncer de próstata LNCaP, PZ-HPV-7, y CA-HPV-10. En las células PZ-HPV-7, los extractos de P. africanum contrarrestan la acción mitogénica de EGF y bloquean la transición G1 a S del ciclo celular. Los extractos de P. africanum ejercen también una potente acción antimitogénica sobre células epiteliales que derivan de explantes de hiperplasia benigna de próstata. CONCLUSIONES: Los extractos etanólicos de P. africanum tienen un efecto antimitogénico sobre células tumorales prostáticas y sobre células epiteliales derivadas de hiperplasia benigna de próstata. Dicho efecto está asociado a la inhibición de la acción mitogénica de EGF y se acompaña de una disminución de la entrada de las células en la fase S del ciclo celular (AU)