Myers Jennifer S, Vallega Karin A, White Jason, Yu Kaixian, Yates Clayton C, Sang Qing-Xiang Amy
Department of Chemistry and Biochemistry and Institute of Molecular Biophysics, Florida State University, 95 Chieftan Way, Tallahassee, FL, 32306-4390, USA.
Department of Biology and Center for Cancer Research, Tuskegee University, Tuskegee, AL, 36088, USA.
BMC Cancer. 2017 Jul 11;17(1):480. doi: 10.1186/s12885-017-3462-7.
While many factors may contribute to the higher prostate cancer incidence and mortality experienced by African-American men compared to their counterparts, the contribution of tumor biology is underexplored due to inadequate availability of African-American patient-derived cell lines and specimens. Here, we characterize the proteomes of non-malignant RC-77 N/E and malignant RC-77 T/E prostate epithelial cell lines previously established from prostate specimens from the same African-American patient with early stage primary prostate cancer.
In this comparative proteomic analysis of RC-77 N/E and RC-77 T/E cells, differentially expressed proteins were identified and analyzed for overrepresentation of PANTHER protein classes, Gene Ontology annotations, and pathways. The enrichment of gene sets and pathway significance were assessed using Gene Set Enrichment Analysis and Signaling Pathway Impact Analysis, respectively. The gene and protein expression data of age- and stage-matched prostate cancer specimens from The Cancer Genome Atlas were analyzed.
Structural and cytoskeletal proteins were differentially expressed and statistically overrepresented between RC-77 N/E and RC-77 T/E cells. Beta-catenin, alpha-actinin-1, and filamin-A were upregulated in the tumorigenic RC-77 T/E cells, while integrin beta-1, integrin alpha-6, caveolin-1, laminin subunit gamma-2, and CD44 antigen were downregulated. The increased protein level of beta-catenin and the reduction of caveolin-1 protein level in the tumorigenic RC-77 T/E cells mirrored the upregulation of beta-catenin mRNA and downregulation of caveolin-1 mRNA in African-American prostate cancer specimens compared to non-malignant controls. After subtracting race-specific non-malignant RNA expression, beta-catenin and caveolin-1 mRNA expression levels were higher in African-American prostate cancer specimens than in Caucasian-American specimens. The "ECM-Receptor Interaction" and "Cell Adhesion Molecules", and the "Tight Junction" and "Adherens Junction" pathways contained proteins are associated with RC-77 N/E and RC-77 T/E cells, respectively.
Our results suggest RC-77 T/E and RC-77 N/E cell lines can be distinguished by differentially expressed structural and cytoskeletal proteins, which appeared in several pathways across multiple analyses. Our results indicate that the expression of beta-catenin and caveolin-1 may be prostate cancer- and race-specific. Although the RC-77 cell model may not be representative of all African-American prostate cancer due to tumor heterogeneity, it is a unique resource for studying prostate cancer initiation and progression.
与其他男性相比,许多因素可能导致非裔美国男性前列腺癌的发病率和死亡率更高,然而由于非裔美国患者来源的细胞系和标本数量不足,肿瘤生物学的作用尚未得到充分研究。在此,我们对先前从一名患有早期原发性前列腺癌的非裔美国患者的前列腺标本中建立的非恶性RC-77 N/E和恶性RC-77 T/E前列腺上皮细胞系的蛋白质组进行了表征。
在对RC-77 N/E和RC-77 T/E细胞进行的这项比较蛋白质组学分析中,鉴定了差异表达的蛋白质,并分析了其在PANTHER蛋白质类别、基因本体注释和通路中的过度表达情况。分别使用基因集富集分析和信号通路影响分析评估基因集的富集情况和通路显著性。分析了来自癌症基因组图谱的年龄和分期匹配的前列腺癌标本的基因和蛋白质表达数据。
RC-77 N/E和RC-77 T/E细胞之间结构蛋白和细胞骨架蛋白存在差异表达且在统计学上过度表达。β-连环蛋白、α-辅肌动蛋白-1和细丝蛋白-A在致瘤性RC-77 T/E细胞中上调,而整合素β-1、整合素α-6、小窝蛋白-1、层粘连蛋白γ-2亚基和CD44抗原下调。与非恶性对照相比,致瘤性RC-77 T/E细胞中β-连环蛋白水平升高和小窝蛋白-1蛋白水平降低反映了非裔美国前列腺癌标本中β-连环蛋白mRNA上调和小窝蛋白-1 mRNA下调。在减去种族特异性非恶性RNA表达后,非裔美国前列腺癌标本中β-连环蛋白和小窝蛋白-1 mRNA表达水平高于白种美国前列腺癌标本。“细胞外基质-受体相互作用”和“细胞粘附分子”以及“紧密连接”和“粘着连接”通路中的蛋白质分别与RC-77 N/E和RC-77 T/E细胞相关。
我们的结果表明,RC-77 T/E和RC-77 N/E细胞系可通过差异表达的结构蛋白和细胞骨架蛋白来区分,这些蛋白在多项分析的多个通路中出现。我们的结果表明,β-连环蛋白和小窝蛋白-1的表达可能具有前列腺癌和种族特异性。尽管由于肿瘤异质性,RC-77细胞模型可能不代表所有非裔美国前列腺癌,但它是研究前列腺癌发生和发展的独特资源。
