Sara Yaser Barham, Dorcas Omotade, Seda Yılmaz, Fatma Tuba Akdeniz, Betül Çapar Goralı, Rukset Attar, Turgay İsbir
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This study focuses on exploring the role of two NER-related genes, Xeroderma Pigmentosum Complementation Group C (XPC) and DNA Damage Binding Protein 2 (DDB2), in OC susceptibility.</p><p><strong>Objectives: </strong>This study aims to investigate the association between variations in two NER-related genes, XPC rs2228001 and DDB2 rs830083, among a cohort of Turkish individuals with OC and control subjects.</p><p><strong>Methods: </strong>Genotyping of XPC rs2228001 and DDB2 rs830083 was performed on 103 OC patients and 104 control subjects from the Turkish population using the Fast Real-Time 7500 PCR platform from Applied Biosystems.</p><p><strong>Results: </strong>Individuals with the homozygous AA genotype of XPC rs2228001 exhibited a reduced likelihood of developing OC (OR 0.511; 95% CI 0.261 - 1.003; <i>P-value</i> 0.049), whereas those with the CC variant faced an elevated risk (OR = 2.32, 95% CI = 1.75-3.08; <i>P-value</i> 0.035). The presence of the A allele was associated with decreased OC occurrence (<i>P-value</i> = 0.035). Similarly, for DDB2 rs830083, individuals with the homozygous CG genotype had a diminished risk of OC (<i>P-value</i> 0.036), compared to those with the GG polymorphism (OR 1.895; 95% CI 1.033 - 3.476; <i>P-value</i> 0.038). Furthermore, the presence of the C allele was associated with a 1.89-fold decrease in the likelihood of OC.</p><p><strong>Conclusion: </strong>These findings shed light on the genetic factors influencing OC susceptibility, emphasizing the importance of DNA repair systems in disease. Further research in larger and more diverse populations is warranted to validate these findings, facilitating precise risk assessment, and potentially guiding tailored treatment strategies for OC patients.</p>","PeriodicalId":49093,"journal":{"name":"Cancer Control","volume":null,"pages":null},"PeriodicalIF":2.5000,"publicationDate":"2024-01-01","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://www.ncbi.nlm.nih.gov/pmc/articles/PMC11378165/pdf/","citationCount":"0","resultStr":"{\"title\":\"Investigation of Polymorphisms in Global Genome Repair Genes in Patients With Ovarian Cancer in the Turkish Population.\",\"authors\":\"Sara Yaser Barham, Dorcas Omotade, Seda Yılmaz, Fatma Tuba Akdeniz, Betül Çapar Goralı, Rukset Attar, Turgay İsbir\",\"doi\":\"10.1177/10732748241270597\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p><strong>Introduction: </strong>Ovarian cancer (OC) poses significant challenges due to its high mortality rate, particularly in advanced stages where symptoms may not be evident. DNA repair mechanisms, including nucleotide excision repair (NER), are crucial in maintaining genomic stability and preventing cancer. This study focuses on exploring the role of two NER-related genes, Xeroderma Pigmentosum Complementation Group C (XPC) and DNA Damage Binding Protein 2 (DDB2), in OC susceptibility.</p><p><strong>Objectives: </strong>This study aims to investigate the association between variations in two NER-related genes, XPC rs2228001 and DDB2 rs830083, among a cohort of Turkish individuals with OC and control subjects.</p><p><strong>Methods: </strong>Genotyping of XPC rs2228001 and DDB2 rs830083 was performed on 103 OC patients and 104 control subjects from the Turkish population using the Fast Real-Time 7500 PCR platform from Applied Biosystems.</p><p><strong>Results: </strong>Individuals with the homozygous AA genotype of XPC rs2228001 exhibited a reduced likelihood of developing OC (OR 0.511; 95% CI 0.261 - 1.003; <i>P-value</i> 0.049), whereas those with the CC variant faced an elevated risk (OR = 2.32, 95% CI = 1.75-3.08; <i>P-value</i> 0.035). The presence of the A allele was associated with decreased OC occurrence (<i>P-value</i> = 0.035). Similarly, for DDB2 rs830083, individuals with the homozygous CG genotype had a diminished risk of OC (<i>P-value</i> 0.036), compared to those with the GG polymorphism (OR 1.895; 95% CI 1.033 - 3.476; <i>P-value</i> 0.038). Furthermore, the presence of the C allele was associated with a 1.89-fold decrease in the likelihood of OC.</p><p><strong>Conclusion: </strong>These findings shed light on the genetic factors influencing OC susceptibility, emphasizing the importance of DNA repair systems in disease. 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引用次数: 0
摘要
导言:卵巢癌(OC)的死亡率很高,尤其是在症状不明显的晚期,这给研究带来了巨大挑战。DNA 修复机制,包括核苷酸切除修复(NER),是维持基因组稳定性和预防癌症的关键。本研究主要探讨两个与 NER 相关的基因--色素沉着病补体 C 组(XPC)和 DNA 损伤结合蛋白 2(DDB2)在 OC 易感性中的作用:本研究旨在调查土耳其 OC 患者和对照组中两个 NER 相关基因(XPC rs2228001 和 DDB2 rs830083)变异之间的关联:使用应用生物系统公司的快速实时 7500 PCR 平台对土耳其人群中的 103 名 OC 患者和 104 名对照组受试者进行了 XPC rs2228001 和 DDB2 rs830083 的基因分型:结果:XPC rs2228001的同源AA基因型个体患OC的可能性降低(OR 0.511;95% CI 0.261 - 1.003;P值0.049),而CC变体个体的风险升高(OR = 2.32,95% CI = 1.75-3.08;P值0.035)。A 等位基因的存在与 OC 发生率的降低有关(P 值 = 0.035)。同样,就 DDB2 rs830083 而言,与 GG 多态性(OR 1.895;95% CI 1.033 - 3.476;P 值 0.038)的个体相比,同源 CG 基因型的个体发生 OC 的风险降低(P 值 0.036)。此外,C 等位基因的存在与发生 OC 的可能性降低 1.89 倍相关:这些发现揭示了影响 OC 易感性的遗传因素,强调了 DNA 修复系统在疾病中的重要性。为了验证这些发现,我们有必要在更大范围、更多样化的人群中开展进一步研究,以便进行精确的风险评估,并为 OC 患者量身定制治疗策略提供潜在指导。
Investigation of Polymorphisms in Global Genome Repair Genes in Patients With Ovarian Cancer in the Turkish Population.
Introduction: Ovarian cancer (OC) poses significant challenges due to its high mortality rate, particularly in advanced stages where symptoms may not be evident. DNA repair mechanisms, including nucleotide excision repair (NER), are crucial in maintaining genomic stability and preventing cancer. This study focuses on exploring the role of two NER-related genes, Xeroderma Pigmentosum Complementation Group C (XPC) and DNA Damage Binding Protein 2 (DDB2), in OC susceptibility.
Objectives: This study aims to investigate the association between variations in two NER-related genes, XPC rs2228001 and DDB2 rs830083, among a cohort of Turkish individuals with OC and control subjects.
Methods: Genotyping of XPC rs2228001 and DDB2 rs830083 was performed on 103 OC patients and 104 control subjects from the Turkish population using the Fast Real-Time 7500 PCR platform from Applied Biosystems.
Results: Individuals with the homozygous AA genotype of XPC rs2228001 exhibited a reduced likelihood of developing OC (OR 0.511; 95% CI 0.261 - 1.003; P-value 0.049), whereas those with the CC variant faced an elevated risk (OR = 2.32, 95% CI = 1.75-3.08; P-value 0.035). The presence of the A allele was associated with decreased OC occurrence (P-value = 0.035). Similarly, for DDB2 rs830083, individuals with the homozygous CG genotype had a diminished risk of OC (P-value 0.036), compared to those with the GG polymorphism (OR 1.895; 95% CI 1.033 - 3.476; P-value 0.038). Furthermore, the presence of the C allele was associated with a 1.89-fold decrease in the likelihood of OC.
Conclusion: These findings shed light on the genetic factors influencing OC susceptibility, emphasizing the importance of DNA repair systems in disease. Further research in larger and more diverse populations is warranted to validate these findings, facilitating precise risk assessment, and potentially guiding tailored treatment strategies for OC patients.
期刊介绍:
Cancer Control is a JCR-ranked, peer-reviewed open access journal whose mission is to advance the prevention, detection, diagnosis, treatment, and palliative care of cancer by enabling researchers, doctors, policymakers, and other healthcare professionals to freely share research along the cancer control continuum. Our vision is a world where gold-standard cancer care is the norm, not the exception.
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