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首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >Quantification of PKC family genes in sporadic breast cancer by qRT-PCR: Evidence that PKCi/λ overexpression is an independent prognostic factor
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Quantification of PKC family genes in sporadic breast cancer by qRT-PCR: Evidence that PKCi/λ overexpression is an independent prognostic factor

机译:通过qRT-PCR定量分析散发性乳腺癌中PKC家族基因:PKCi /λ过表达是独立的预后因素的证据

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Drugs targeting protein kinase C (PKC) show promising therapeutic activity. However, little is known about the expression patterns of the 11 PKC genes in human tumors, and the clinical significance of most PKC genes is unknown. We used qRT-PCR assays to quantify mRNA levels of the 11 PKC genes in 458 breast tumors from patients with known clinical/pathological status and long-term outcome. The proportion of tumors in which the expression of the different genes was altered varied widely, from 9.6% for PKN2 to 40.2% for PKCi/λ. In breast tumors, overexpression was the main alteration observed for PKCi/λ (33.4%), PKCδ (29.5%) and PKCζ (9.6%), whereas underexpression was the main alteration observed for PKCα (27.3%), PKCε (11.6%), PKCη (8.7%) and PKN2 (8.1%). Both overexpression and underexpression were observed for PKCβ (underexpression 15.5%, overexpression 13.8%), PKCθ (underexpression 14.8%, overexpression 10.0%) and PKN1 (underexpression 6.6%, overexpression 7.4%). Several links were found between different PKC genes; and also between the expression patterns of PKC genes and several classical pathological and clinical parameters. PKCi/λ alone was found to have prognostic significance (p = 0.043), whereas PKCα showed a trend towards an influence on relapse-free survival (p = 0.052). PKCi/λ retained its prognostic significance in Cox multivariate regression analysis (p = 0.031). These results reveal very complex expression patterns of PKC genes in breast tumors, and suggest that their expression should be considered together when evaluating anti-tumoral drugs. PKCi/λ seems to be the most promising therapeutic target in breast cancer.
机译:靶向蛋白激酶C(PKC)的药物显示出有希望的治疗活性。然而,关于11种PKC基因在人肿瘤中的表达模式知之甚少,并且大多数PKC基因的临床意义尚不清楚。我们使用qRT-PCR分析来量化来自已知临床/病理状态和长期结果的458名乳腺肿瘤中11个PKC基因的mRNA水平。改变不同基因表达的肿瘤比例差异很大,从PKN2的9.6%到PKCi /λ的40.2%。在乳腺肿瘤中,过表达是PKCi /λ(33.4%),PKCδ(29.5%)和PKCζ(9.6%)的主要改变,而过表达是PKCα(27.3%),PKCε(11.6%)的主要改变。 ,PKCη(8.7%)和PKN2(8.1%)。 PKCβ(表达不足15.5%,过表达13.8%),PKCθ(表达不足14.8%,过表达10.0%)和PKN1(表达不足6.6%,过表达7.4%)均观察到过表达和表达不足。在不同的PKC基因之间发现了几个联系。以及PKC基因的表达方式与一些经典的病理和临床参数之间。发现仅PKCi /λ具有预后意义(p = 0.043),而PKCα则显示出对无复发生存的影响趋势(p = 0.052)。 PKCi /λ在Cox多元回归分析中保留了其预后意义(p = 0.031)。这些结果揭示了PKC基因在乳腺肿瘤中非常复杂的表达模式,并建议在评估抗肿瘤药物时应一起考虑它们的表达。 PKCi /λ似乎是乳腺癌中最有希望的治疗靶标。

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