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首页> 外文期刊>Clinical proteomics. >Changes in glycoprotein expression between primary breast tumour and synchronous lymph node metastases or asynchronous distant metastases
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Changes in glycoprotein expression between primary breast tumour and synchronous lymph node metastases or asynchronous distant metastases

机译:原发性乳腺肿瘤与同步淋巴结转移或异步远处转移之间糖蛋白表达的变化

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Background Breast cancer is a very heterogeneous disease and some patients are cured by the surgical removal of the primary tumour whilst other patients suffer from metastasis and spreading of the disease, despite adjuvant therapy. A number of prognostic and treatment predictive factors have been identified such as tumour size, oestrogen (ER) and progesterone (PgR) receptor status, human epidermal growth factor receptor type 2 (HER2) status, histological grade, Ki67 and age. Lymph node involvement is also assessed during surgery to determine if the tumour has spread which requires dissection of the axilla and adjuvant treatment. The prognostic and treatment predictive factors assessing the nature of the tumour are all routinely based on the status of the primary tumour. Results We have analysed a unique tumour set of fourteen primary breast cancer tumours with matched synchronous axillary lymph node metastases and a set of nine primary tumours with, later developed, matched distant metastases from different sites in the body. We used a pairwise tumour analysis (from the same individual) since the difference between the same tumour-type in different patients was greater. Glycopeptide capture was used in this study to selectively isolate and quantify N-linked glycopeptides from tumours mixtures and the captured glycopeptides were subjected to label-free quantitative tandem mass spectrometry analysis. Differentially expressed proteins between primary tumours and matched lymph node metastasis and distant metastasis were identified. Two of the top hits, ATPIF1 and tubulin β-chain were validated by immunohistochemistry to be differentially regulated. Conclusions We show that the expression of a large number of glycosylated proteins change between primary tumours and matched lymph node metastases and distant metastases, confirming that cancer cells undergo a molecular transformation during the spread to a secondary site. The proteins are part of important pathways such as cell adhesion, migration pathways and immune response giving insight into molecular changes needed for the tumour to spread. The large difference between primary tumours and lymph node and distant metastases also suggest that treatment should be based on the phenotype of the lymph node and distant metastases.
机译:背景技术乳腺癌是一种非常不同的疾病,尽管有辅助治疗,但一些患者可通过手术切除原发肿瘤而治愈,而其他患者则患有该疾病的转移和扩散。已经确定了许多预后和治疗预测因素,例如肿瘤大小,雌激素(ER)和孕激素(PgR)受体状态,人类表皮生长因子受体2型(HER2)状态,组织学等级,Ki67和年龄。手术期间还评估了淋巴结受累情况,以确定肿瘤是否扩散,这需要解剖腋窝并进行辅助治疗。评估肿瘤性质的预后和治疗预测因素通常都是基于原发肿瘤的状态。结果我们分析了14个原发性乳腺癌肿瘤的独特肿瘤集,这些肿瘤具有相匹配的同步腋窝淋巴结转移,以及9个原发性肿瘤集,这些肿瘤后来从体内不同部位发生了远处转移。我们使用成对肿瘤分析(来自同一个体),因为不同患者中相同肿瘤类型之间的差异更大。在这项研究中使用糖肽捕获来从肿瘤混合物中选择性分离和定量N-连接的糖肽,并对捕获的糖肽进行无标记的定量串联质谱分析。确定了原发肿瘤与匹配的淋巴结转移和远处转移之间差异表达的蛋白。免疫组化方法验证了其中两个热门命中的ATPIF1和微管蛋白β链具有差异调节作用。结论我们表明,大量糖基化蛋白的表达在原发性肿瘤以及匹配的淋巴结转移和远处转移之间改变,这证实癌细胞在扩散至次要部位时经历了分子转化。这些蛋白质是重要途径的一部分,例如细胞粘附,迁移途径和免疫反应,从而洞悉了肿瘤扩散所需的分子变化。原发性肿瘤与淋巴结和远处转移之间的巨大差异也表明治疗应基于淋巴结和远处转移的表型。

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