Toscano-Guerra Emily, Maggio Valentina, García Javier, Semidey Maria Eugenia, Celma Ana, Morote Juan, de Torres Inés, Giralt Marina, Ferrer-Costa Roser, Paciucci Rosanna
Cell Signaling and Cancer Progression Laboratory, Vall d'Hebron Institute of Research (VHIR), Barcelona, Spain.
Department of Biochemistry and Molecular Biology, Autonomous University of Barcelona, Barcelona, Spain.
Front Oncol. 2024 Aug 13;14:1398411. doi: 10.3389/fonc.2024.1398411. eCollection 2024.
Prostate cancer (PCa) is a leading cause of cancer-related deaths in European men, emphasizing the urgent need for effective risk assessment strategies. The TP53 gene, a tumor suppressor gene frequently mutated in cancer, commonly harbors the rs1042522 single nucleotide polymorphism (SNP), known as the P72R SNP, which may influence PCa susceptibility. This study investigated the prevalence of the P72R SNP in European Caucasian PCa samples and its association with PCa risk.
Genotyping was conducted on 12 hormone-naïve aggressive PCa cultures (hnPCs) from untreated patients (Gleason ≥8), 11 radical prostatectomies (RP), and 94 serum samples using DNA Sanger sequencing and melting curve analysis. Comparative analysis utilized data from the GnomAD database's European Caucasian non-cancer population.
Our results demonstrate a significantly higher frequency of the P72R SNP in PCa samples and serums compared to the general European non-cancer population. A robust and statistically significant association (p < 0.0001) between the SNP and prostate cancer risk was identified, with an odds ratio of 7.937 (95% CI 5.37-11.00). Notably, the G allele (R72) showed a pronounced prevalence in high Gleason score (≥8) patients, although statistical significance was not reached. These results highlight a potential association with undifferentiated and malignant PCa lesions.
The compelling association between the P72R SNP and prostate cancer risk underscores the potential utility of this marker for the early identification of patients at risk of aggressive metastatic prostate cancer. This insight could empower further research to intervene at an early stage by offering enhanced opportunities for timely and targeted interventions.
前列腺癌(PCa)是欧洲男性癌症相关死亡的主要原因,这凸显了对有效风险评估策略的迫切需求。TP53基因是一种在癌症中经常发生突变的肿瘤抑制基因,通常存在rs1042522单核苷酸多态性(SNP),即P72R SNP,它可能影响PCa易感性。本研究调查了欧洲白种人PCa样本中P72R SNP的患病率及其与PCa风险的关联。
使用DNA桑格测序和熔解曲线分析,对12例未经治疗患者( Gleason评分≥8)的未接受激素治疗的侵袭性PCa培养物(hnPCs)、11例根治性前列腺切除术(RP)样本和94份血清样本进行基因分型。比较分析利用了GnomAD数据库中欧洲白种人非癌症人群的数据。
我们的结果表明,与一般欧洲非癌症人群相比,PCa样本和血清中P72R SNP的频率显著更高。该SNP与前列腺癌风险之间存在强烈且具有统计学意义的关联(p < 0.0001),优势比为7.937(95% CI 5.37 - 11.00)。值得注意的是,G等位基因(R72)在高Gleason评分(≥8)患者中显示出明显的患病率,尽管未达到统计学意义。这些结果突出了与未分化和恶性PCa病变的潜在关联。
P72R SNP与前列腺癌风险之间令人信服的关联强调了该标志物在早期识别侵袭性转移性前列腺癌风险患者方面的潜在效用。这一见解可为进一步研究提供支持,通过提供更多及时和有针对性干预的机会,在早期进行干预。
