Procoagulant properties of human MV3 melanoma cells

A correlation between cancer and prothrombotic states has long been described. More recently, a number of studies have focused on the procoagulant mechanisms exhibited by tumor cells. In the present study, we dissected the molecular mechanisms responsible for the procoagulant activity of MV3, a high...

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Main Authors: D.L.A. Geaquinto, R.S. Fernandes, L.G. Lima, C. Barja-Fidalgo, R.Q. Monteiro
Format: Article
Language:English
Published: Associação Brasileira de Divulgação Científica 2008-02-01
Series:Brazilian Journal of Medical and Biological Research
Subjects:
Online Access:http://www.scielo.br/scielo.php?script=sci_arttext&pid=S0100-879X2008000200004
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spelling doaj-9034ab8d0e40428eacc80a1f4b872f672020-11-24T22:29:39ZengAssociação Brasileira de Divulgação CientíficaBrazilian Journal of Medical and Biological Research0100-879X1414-431X2008-02-0141299105Procoagulant properties of human MV3 melanoma cellsD.L.A. GeaquintoR.S. FernandesL.G. LimaC. Barja-FidalgoR.Q. MonteiroA correlation between cancer and prothrombotic states has long been described. More recently, a number of studies have focused on the procoagulant mechanisms exhibited by tumor cells. In the present study, we dissected the molecular mechanisms responsible for the procoagulant activity of MV3, a highly aggressive human melanoma cell line. It was observed that tumor cells strongly accelerate plasma coagulation as a result of: i) expression of the blood clotting initiator protein, a tissue factor, as shown by flow cytometry and functional assays (factor Xa formation in the presence of cells and factor VIIa), and ii) direct activation of prothrombin to thrombin by cells, as evidenced by hydrolysis of the synthetic substrate, S-2238, and the natural substrate, fibrinogen. This ability was highly potentiated by the addition of exogenous factor Va, which functions as a co-factor for the enzyme factor Xa. In contrast, prothrombin activation was not observed when cells were previously incubated with DEGR-factor Xa, an inactive derivative of the enzyme. Moreover, a monoclonal antibody against bovine factor Xa reduced the prothrombin-converting activity of tumor cells. In conclusion, the data strongly suggest that MV3 cells recruit factor Xa from the culture medium, triggering an uncommon procoagulant mechanism.http://www.scielo.br/scielo.php?script=sci_arttext&pid=S0100-879X2008000200004MV3 melanomaBlood clottingTissue factor
collection DOAJ
language English
format Article
sources DOAJ
author D.L.A. Geaquinto
R.S. Fernandes
L.G. Lima
C. Barja-Fidalgo
R.Q. Monteiro
spellingShingle D.L.A. Geaquinto
R.S. Fernandes
L.G. Lima
C. Barja-Fidalgo
R.Q. Monteiro
Procoagulant properties of human MV3 melanoma cells
Brazilian Journal of Medical and Biological Research
MV3 melanoma
Blood clotting
Tissue factor
author_facet D.L.A. Geaquinto
R.S. Fernandes
L.G. Lima
C. Barja-Fidalgo
R.Q. Monteiro
author_sort D.L.A. Geaquinto
title Procoagulant properties of human MV3 melanoma cells
title_short Procoagulant properties of human MV3 melanoma cells
title_full Procoagulant properties of human MV3 melanoma cells
title_fullStr Procoagulant properties of human MV3 melanoma cells
title_full_unstemmed Procoagulant properties of human MV3 melanoma cells
title_sort procoagulant properties of human mv3 melanoma cells
publisher Associação Brasileira de Divulgação Científica
series Brazilian Journal of Medical and Biological Research
issn 0100-879X
1414-431X
publishDate 2008-02-01
description A correlation between cancer and prothrombotic states has long been described. More recently, a number of studies have focused on the procoagulant mechanisms exhibited by tumor cells. In the present study, we dissected the molecular mechanisms responsible for the procoagulant activity of MV3, a highly aggressive human melanoma cell line. It was observed that tumor cells strongly accelerate plasma coagulation as a result of: i) expression of the blood clotting initiator protein, a tissue factor, as shown by flow cytometry and functional assays (factor Xa formation in the presence of cells and factor VIIa), and ii) direct activation of prothrombin to thrombin by cells, as evidenced by hydrolysis of the synthetic substrate, S-2238, and the natural substrate, fibrinogen. This ability was highly potentiated by the addition of exogenous factor Va, which functions as a co-factor for the enzyme factor Xa. In contrast, prothrombin activation was not observed when cells were previously incubated with DEGR-factor Xa, an inactive derivative of the enzyme. Moreover, a monoclonal antibody against bovine factor Xa reduced the prothrombin-converting activity of tumor cells. In conclusion, the data strongly suggest that MV3 cells recruit factor Xa from the culture medium, triggering an uncommon procoagulant mechanism.
topic MV3 melanoma
Blood clotting
Tissue factor
url http://www.scielo.br/scielo.php?script=sci_arttext&pid=S0100-879X2008000200004
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