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Expression of the TPα and TPβ isoforms of the thromboxane prostanoid receptor (TP) in prostate cancer: clinical significance and diagnostic potential

机译:血栓烷前列腺素受体(TP)的TPα和TPβ同工型在前列腺癌中的表达:临床意义和诊断潜力

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摘要

The prostanoid thromboxane (TX) A2 plays a central role in haemostasis and is increasingly implicated in cancer progression. TXA2 signals through two T Prostanoid receptor (TP) isoforms termed TPα and TPβ, with both encoded by the TBXA2R gene. Despite exhibiting several functional and regulatory differences, the role of the individual TP isoforms in neoplastic diseases is largely unknown.This study evaluated expression of the TPα and TPβ isoforms in tumour microarrays of the benign prostate and different pathological (Gleason) grades of prostate cancer (PCa). Expression of TPβ was significantly increased in PCa relative to benign tissue and strongly correlated with increasing Gleason grade. Furthermore, higher TPβ expression was associated with increased risk of biochemical recurrence (BCR) and significantly shorter disease-free survival time in patients post-surgery. While TPα was more variably expressed than TPβ in PCa, increased/high TPα expression within the tumour also trended toward increased BCR and shorter disease-free survival time. Comparative genomic CpG DNA methylation analysis revealed substantial differences in the extent of methylation of the promoter regions of the TBXA2R that specifically regulate expression of TPα and TPβ, respectively, both in benign prostate and in clinically-derived tissue representative of precursor lesions and progressive stages of PCa. Collectively, TPα and TPβ expression is differentially regulated both in the benign and tumourigenic prostate, and coincides with clinical pathology and altered CpG methylation of the TBXA2R gene. Analysis of TPβ, or a combination of TPα/TPβ, expression levels may have significant clinical potential as a diagnostic biomarker and predictor of PCa disease recurrence.
机译:前列腺素血栓烷(TX)A2在止血中起着核心作用,并越来越多地参与癌症的发展。 TXA2通过两个称为TPα和TPβ的T前列腺素受体(TP)异构体发出信号,两者均由TBXA2R基因编码。尽管表现出几种功能和调节差异,但个体TP亚型在赘生性疾病中的作用仍是未知的。 PCa)。相对于良性组织,TPa在PCa中的表达显着增加,并且与Gleason评分的升高密切相关。此外,更高的TPβ表达与术后生化复发(BCR)的风险增加以及无病生存时间明显缩短有关。尽管在PCa中TPα的表达比TPβ的变异更大,但肿瘤内TPα的增加/高表达也倾向于增加BCR和缩短无病生存时间。比较基因组CpG DNA甲基化分析显示,分别在良性前列腺和代表前体病变及进展阶段的临床来源组织中,分别特异性调节TPα和TPβ表达的TBXA2R启动子区域的甲基化程度存在实质性差异。 PCa。 TPα和TPβ的表达在良性和致瘤性前列腺中均受到差异调节,与TBXA2R基因的临床病理和CpG甲基化改变相吻合。分析TPβ或TPα/TPβ的组合表达水平可能具有重要的临床潜力,可作为PCa疾病复发的诊断生物标志物和预测因子。

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