Inhibition of calcineurin by cyclosporine A exerts multiple effects on human melanoma cell lines HT168 and WM35.

Tamás Juhász, Csaba Matta, Gábor Veress, Georgina Nagy, Zsolt Szíjgyártó, Zsanett Molnár, János Fodor, Róza Zákány, Pál Gergely

Department of Anatomy, Histology and Embryology, Medical and Health Science Centre, University of Debrecen, Hungary.

Journal Article: International Journal of Oncology (impact factor: 2.45). 05/2009; 34(4):995-1003.

Abstract

The immunosuppressant cyclosporine A (CsA) is a specific pharmacological inhibitor of calcineurin, the Ca2+-calmodulin activated phospho-Ser/Thr-specific protein phosphatase. Although calcineurin-inhibiting compounds are applied for local treatment of psoriasis or atopic dermatitis in dermatological practice, little is known about the functions of calcineurin in epidermis-derived malignancies. We investigated the effects of CsA on two human melanoma cell lines, the metastasis forming HT168 and WM35 established from an RGP primary lesion. CsA of 2 microM lowered the enzyme activity by 50% and caused elevation in both mRNA and protein expression of calcineurin. Cell proliferation was diminished, as well as the cellular morphology and the actin organization were altered in both cell lines. CsA increased cell death moderately in both cell lines and reduced the metabolic activity of HT168 cells, but not that of WM35 cells. CsA also elevated the expressions of both Bcl-2 and ERK1/2. Fibronectin guided migration of HT168 cells was stimulated under the effect of CsA, while that of WM35 cells was reduced, moreover, HT168 cells switched from the expression of beta3 to beta1 integrin, but WM35 cells continued to express beta3. Based on our results we propose a multiple, partly malignancy-dependent role of calcineurin in these melanoma cell lines.

Source: PubMed

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Keywords

actin organization
 
atopic dermatitis
 
beta1 integrin
 
Ca2+-calmodulin activated phospho-Ser/Thr-specific protein phosphatase
 
calcineurin-inhibiting compounds
 
cell death
 
cell lines
 
Cell proliferation
 
cellular morphology
 
dermatological practice
 
enzyme activity
 
epidermis-derived malignancies
 
human melanoma cell lines
 
immunosuppressant cyclosporine
 
local treatment
 
malignancy-dependent role
 
melanoma cell lines
 
RGP primary lesion
 
specific pharmacological inhibitor
 
WM35 cells