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Differential effects of anticoagulants on tumor development of mouse cancer cell lines B16, K1735 and CT26 in lung

机译:抗凝剂对小鼠肺癌B16,K1735和CT26细胞株在肺癌中的分化作用

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摘要

Cancer progression is facilitated by blood coagulation. Anticoagulants, such as Hirudin and low molecular weight heparins (LMWHs), reduce metastasis mainly by inhibition of thrombin formation and L- and P-selectin-mediated cell-cell adhesion. It is unknown whether the effects are dependent on cancer cell type. The effects of anticoagulants on tumor development of K1735 and B16 melanoma cells and CT26 colon cancer cells were investigated in mouse lung. Tumor load was determined noninvasively each week up to day 21 in all experiments using bioluminescence imaging. Effects of anticoagulants on tumor development of the three cell lines were correlated with the fibrin/fibrinogen content in the tumors, expression of tissue factor (TF), protease activated receptor (PAR)-1 and -4 and CD24, a ligand of L- and P-selectins. Hirudin inhibited tumor development of B16 cells in lungs completely but did not affect tumor growth of K1735 and CT26 cells. Low molecular weight heparin did not have an effect on K1735 melanoma tumor growth either. TF and PAR-4 expression was similar in the three cell lines. PAR-1 and CD24 were hardly expressed by K1735, whereas CT26 cells expressed low levels and B16 high levels of PAR-1 and CD24. Fibrin content of the tumors was not affected by LMWH. It is concluded that effects of anticoagulants are dependent on cancer cell type and are correlated with their CD24 and PAR-1 expression.
机译:血液凝固促进了癌症的发展。抗凝剂,例如水rud素和低分子量肝素(LMWHs),主要是通过抑制凝血酶的形成以及L和P选择素介导的细胞粘附来减少转移。效果是否取决于癌细胞类型尚不清楚。在小鼠肺中研究了抗凝剂对K1735和B16黑色素瘤细胞以及CT26结肠癌细胞的肿瘤发展的影响。使用生物发光成像,在所有实验中直至第21天,每周无创地确定肿瘤负荷。抗凝剂对三种细胞系肿瘤发展的影响与肿瘤中纤维蛋白/纤维蛋白原含量,组织因子(TF),蛋白酶激活受体(PAR)-1和-4的表达以及CD24(L-的配体)相关和P-选择素。水rud素完全抑制肺中B16细胞的肿瘤发展,但不影响K1735和CT26细胞的肿瘤生长。低分子量肝素也对K1735黑色素瘤肿瘤生长没有影响。在这三种细胞系中,TF和PAR-4的表达相似。 K1735几乎不表达PAR-1和CD24,而CT26细胞表达的PAR-1和CD24的水平低而B16高。 LMWH不影响肿瘤的纤维蛋白含量。结论是抗凝剂的作用取决于癌细胞类型,并与其CD24和PAR-1表达相关。

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