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Expression of TGF-β signaling factors in invasive breast cancers: relationships with age at diagnosis and tumor characteristics

机译:TGF-β信号传导因子在浸润性乳腺癌中的表达:与诊断年龄和肿瘤特征的关系

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The transforming growth factor beta (TGF-β) pathway can play either a tumor-suppressing or a tumor-promoting role in human breast carcinogenesis. In order to determine whether expression of TGF-β signaling factors varies by age at onset and breast tumor characteristics that have prognostic significance, we undertook a study of 623 women with invasive breast carcinoma enrolled in a population-based case–control study conducted in Poland from 2000 to 2003. TGF-β signaling factors were analyzed by immunohistochemistry in tumor tissue microarrays. We found that most tumors expressed extracellular-TGF-β1 (78%), TGF-β2 (91%), TGF-β3 (93%), TGF-βR2 (72%), and phospho-SMAD2 (61%), whereas intracellular-TGF-β1 was expressed in 32% of tumors. Expression of TGF-β ligands (β1, β2, and β3) was associated with prognostically favorable pathological features including small size, and low grade, and these associations were similar for ER-positive and negative tumors. On the contrary, expression of the receptor TGF-βR2 was primarily associated with small tumor size among ER-negative tumors, while expression of the transcription factor phospho-SMAD2 was associated with positive nodal status among ER-negative tumors. The greater frequency of expression of phospho-SMAD2 in cancers associated with lymph node metastases is consistent with a pro-progression role for TGF-β. In addition, expression of extracellular-TGF-β1 (P = 0.005), TGF-βR2 (P = 8.2E-11), and phospho-SMAD2 (P = 1.3E-8) was strongly associated with earlier age at onset, independent of ER status. Our data provide evidence that TGF-β signaling patterns vary by age and pathologic features of prognostic significance including ER expression. These results warrant analysis in studies of clinical outcomes accounting for age, ER status and treatment.
机译:转化生长因子β(TGF-β)途径可以在人类乳腺癌的癌变过程中起到抑瘤或促肿瘤的作用。为了确定TGF-β信号转导因子的表达是否随年龄的增长和具有预后意义的乳腺肿瘤特征而变化,我们在波兰进行了一项基于人群的病例对照研究,纳入了623名浸润性乳腺癌妇女从2000年至2003年。通过免疫组织化学分析肿瘤组织微阵列中的TGF-β信号转导因子。我们发现大多数肿瘤表达细胞外-TGF-β1(78%),TGF-β2(91%),TGF-β3(93%),TGF-βR2(72%)和磷酸-SMAD2(61%),而细胞内TGF-β1在32%的肿瘤中表达。 TGF-β配体(β1,β2和β3)的表达与预后良好的病理特征相关,包括体积小,分级低,并且这些关联在ER阳性和阴性肿瘤中相似。相反,在ER阴性肿瘤中,受体TGF-βR2的表达主要与小肿瘤有关,而在ER阴性肿瘤中,转录因子phospho-SMAD2的表达与淋巴结阳性有关。在与淋巴结转移相关的癌症中,磷酸化SMAD2的更高表达频率与TGF-β的促进作用相一致。另外,细胞外TGF-β1(P = 0.005),TGF-βR2(P = 8.2E-11)和磷酸化SMAD2(P = 1.3E-8)的表达与发病的早龄密切相关,独立ER状态。我们的数据提供了证据,表明TGF-β信号传导模式随年龄和包括ER表达在内的预后意义的病理特征而变化。这些结果值得在对年龄,ER状态和治疗的临床结局研究中进行分析。

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