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Expression of reactive oxygen species-related proteins in metastatic breast cancer is dependent on the metastatic site

机译:转移性乳腺癌中活性氧相关蛋白的表达取决于转移部位

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This study was performed to investigate the expression of reactive oxygen species (ROS)-related proteins and to analyze the implications for primary and metastatic breast cancer. We constructed a tissue microarray containing 143 metastatic breast cancers (52 lung metastases, 38 bone metastases, 37 brain metastases, and 16 liver metastases) and performed immunohistochemical staining for ROS-related proteins (catalase, GSTπ, TxNIP, and MnSOD). Analysis of ROS-related protein expression in metastatic breast cancers according to the metastatic sites revealed site-specific expression patterns. The expression of tumoral catalase was lower in bone metastases (emP/em = 0.012), and stromal GSTπ expression was higher in bone and liver metastases (emP/em < 0.001). The highest ROS activation status was observed for lung metastases, while non-activated ROS was observed for bone metastases (emP/em = 0.001). Primary cancers were positive for stromal GSTπ, but a subset of lung metastases were negative (emP/em = 0.021). Univariate analysis revealed that shorter overall survival (OS) was associated with negative catalase expression of the tumor (emP/em = 0.026). Furthermore, univariate analyses according to the metastatic sites revealed that shorter OS was associated with TxNIP-positive tumors (emP/em = 0.032) and the expression of stromal catalase (emP/em = 0.032) in brain metastases. Tumors that were negative for MnSOD expression (emP/em < 0.001) but positive for stromal catalase expression (emP/em = 0.022) were associated with shorter OS in patients with liver metastases. In conclusion, cancer cells and stromal tissues showed different ROS-related protein expression patterns according to the metastatic site. In addition, the expression of ROS-related proteins is associated with patient prognosis.
机译:进行这项研究以调查活性氧(ROS)相关蛋白的表达,并分析其对原发性和转移性乳腺癌的影响。我们构建了一个包含143个转移性乳腺癌(52个肺转移,38个骨转移,37个脑转移和16个肝转移)的组织微阵列,并对ROS相关蛋白(过氧化氢酶,GSTπ,TxNIP和MnSOD)进行了免疫组织化学染色。 。根据转移部位分析ROS相关蛋白在转移性乳腺癌中的表达,揭示了部位特异性表达模式。骨转移中肿瘤过氧化氢酶的表达较低( P = 0.012),间质GSTπ骨和肝转移中的表达较高( P < 0.001)。对于肺转移,观察到最高的ROS激活状态,而对于骨转移观察到未激活的ROS( P = 0.001)。原发性癌的间质性GST阳性,但是一部分肺转移癌阴性( P = 0.021)。单因素分析表明,较短的总生存期与肿瘤中过氧化氢酶阴性表达有关( P = 0.026)。此外,根据转移部位的单变量分析显示,较短的OS与TxNIP阳性肿瘤( P = 0.032)和基质过氧化氢酶的表达( P = 0.032)有关。在脑转移中。 MnSOD表达阴性( P < 0.001)但基质间过氧化氢酶表达阳性( P = 0.022)的肿瘤与肝转移患者的OS短相关。总之,癌细胞和基质组织根据转移部位显示出不同的ROS相关蛋白表达模式。另外,ROS相关蛋白的表达与患者的预后相关。

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