首页> 外文期刊>Oncology Research >Serum levels of soluble E-selectin are associated with the clinical course of metastatic disease in patients with liver metastases from breast cancer.
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Serum levels of soluble E-selectin are associated with the clinical course of metastatic disease in patients with liver metastases from breast cancer.

机译:患有乳腺癌的肝转移患者的血清可溶性E-选择素水平与转移性疾病的临床病程有关。

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Increasing evidence indicates that the expression of the endothelial adhesion molecule E-selectin is associated with progression and metastasis of breast cancer. Patients with liver metastases also show increased serum levels of the soluble form of E-selectin. It was our aim to compare serum levels of soluble E-selectin (sES) in such patients with the biology of the primary tumor and the course of the metastatic disease under therapy. We examined 69 patients with liver metastases from breast cancer who were selected to receive systemic tumor therapy because of progressive disease (n = 44) or newly detected liver metastases (n = 25). Serum concentrations of sES were measured before each therapy cycle using a specific ELISA. Serum concentrations of sES before the start of therapy were compared to clinical parameters and histopathological findings referring to the primary tumor. Secondly, serum levels of sES were compared to serum concentrations of the corresponding tumor markers. We observed a possible trend for certain unfavorable prognostic parameters (e.g., young women, low-graded tumors, human epidermal growth factor receptor 2 overexpression) to be related to higher serum levels of sES. Serum levels of sES were correlated with tumor marker levels in a logarithmical relation (r = 0.44, P < 0.0005). In some cases it could be demonstrated that serum levels of sES changed similarly to the course of tumor marker levels. We conclude that serum levels of sES are associated with the clinical course of liver metastases from breast cancer. Further investigations are needed to clarify if serum levels of sES may serve as tumor marker in certain clinical situations. E-selectin should be evaluated as a possible target for antimetastatic therapy studies.
机译:越来越多的证据表明,内皮粘附分子E-选择素的表达与乳腺癌的进展和转移有关。患有肝转移的患者还显示血清可溶性E-选择素的水平升高。我们的目的是比较这类患者的血清可溶性E-选择素(sES)的水平与原发肿瘤的生物学性质以及接受治疗的转移性疾病的病程。我们检查了69位患有乳腺癌的肝转移患者,这些患者因进行性疾病(n = 44)或新发现的肝转移(n = 25)而被选择接受系统性肿瘤治疗。在每个治疗周期之前,使用特异性ELISA测量sES的血清浓度。将治疗开始前的sES血清浓度与涉及原发性肿瘤的临床参数和组织病理学结果进行比较。其次,将sES的血清水平与相应的肿瘤标志物的血清浓度进行比较。我们观察到某些不利的预后参数(例如年轻女性,低分级肿瘤,人表皮生长因子受体2过表达)的可能趋势与较高的sES血清水平有关。 sES的血清水平与肿瘤标志物水平呈对数关系(r = 0.44,P <0.0005)。在某些情况下,可以证明血清sES的水平与肿瘤标志物水平的变化过程相似。我们得出结论,血清esES水平与乳腺癌的肝转移临床过程有关。需要进一步的研究来阐明血清sES水平在某些临床情况下是否可以作为肿瘤标志物。 E-选择素应作为抗转移疗法研究的可能靶点进行评估。

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