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iTRAQ 鉴定与人类前列腺癌转移进展相关的候选血清生物标志物。

iTRAQ identification of candidate serum biomarkers associated with metastatic progression of human prostate cancer.

机构信息

Department of Human Metabolism, The Medical School, The Mellanby Centre for Bone Research, University of Sheffield, Sheffield, United Kingdom.

出版信息

PLoS One. 2012;7(2):e30885. doi: 10.1371/journal.pone.0030885. Epub 2012 Feb 15.

Abstract

A major challenge in the management of patients with prostate cancer is identifying those individuals at risk of developing metastatic disease, as in most cases the disease will remain indolent. We analyzed pooled serum samples from 4 groups of patients (n = 5 samples/group), collected prospectively and actively monitored for a minimum of 5 yrs. Patients groups were (i) histological diagnosis of benign prostatic hyperplasia with no evidence of cancer 'BPH', (ii) localised cancer with no evidence of progression, 'non-progressing' (iii) localised cancer with evidence of biochemical progression, 'progressing', and (iv) bone metastasis at presentation 'metastatic'. Pooled samples were immuno-depleted of the 14 most highly abundant proteins and analysed using a 4-plex iTRAQ approach. Overall 122 proteins were identified and relatively quantified. Comparisons of progressing versus non-progressing groups identified the significant differential expression of 25 proteins (p<0.001). Comparisons of metastatic versus progressing groups identified the significant differential expression of 23 proteins. Mapping the differentially expressed proteins onto the prostate cancer progression pathway revealed the dysregulated expression of individual proteins, pairs of proteins and 'panels' of proteins to be associated with particular stages of disease development and progression. The median immunostaining intensity of eukaryotic translation elongation factor 1 alpha 1 (eEF1A1), one of the candidates identified, was significantly higher in osteoblasts in close proximity to metastatic tumour cells compared with osteoblasts in control bone (p = 0.0353, Mann Whitney U). Our proteomic approach has identified leads for potentially useful serum biomarkers associated with the metastatic progression of prostate cancer. The panels identified, including eEF1A1 warrant further investigation and validation.

摘要

在管理前列腺癌患者方面,一个主要的挑战是识别那些有发生转移性疾病风险的个体,因为在大多数情况下,这种疾病仍处于惰性状态。我们分析了 4 组患者的混合血清样本(每组 n=5 个样本),这些样本是前瞻性收集并进行了至少 5 年的主动监测。患者组包括:(i)组织学诊断为良性前列腺增生且无癌症证据的“BPH”;(ii)无进展证据的局限性癌症“非进展”;(iii)有生化进展证据的局限性癌症“进展”;(iv)初诊时出现骨转移的“转移性”。混合样本通过免疫耗尽了 14 种最丰富的蛋白质,并使用 4 重 iTRAQ 方法进行分析。总共鉴定和相对定量了 122 种蛋白质。进展组与非进展组的比较鉴定出 25 种蛋白质的显著差异表达(p<0.001)。转移性组与进展性组的比较鉴定出 23 种蛋白质的显著差异表达。将差异表达的蛋白质映射到前列腺癌进展途径上,揭示了单个蛋白质、蛋白质对和“面板”的失调表达与疾病发展和进展的特定阶段相关。在与转移性肿瘤细胞相邻的成骨细胞中,真核翻译延伸因子 1 样蛋白 1(eEF1A1)的免疫染色强度中位数明显高于对照骨中的成骨细胞(p=0.0353,Mann Whitney U)。我们的蛋白质组学方法已经确定了与前列腺癌转移进展相关的潜在有用血清生物标志物的线索。鉴定出的包括 eEF1A1 的面板值得进一步研究和验证。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4ca1/3280251/8fca41b8f834/pone.0030885.g001.jpg

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