Jaleel Ibrahim Asaad, Khalid S A Alazzawi, Sara S Rasheed, Rebah N Algafari, Rehab S Ramadhan, Marwah Amer Qamandar, Sura S Talib, Rawnaq Z Fadhil
{"title":"孕酮受体在伊拉克人前列腺癌发病率中的可能作用。","authors":"Jaleel Ibrahim Asaad, Khalid S A Alazzawi, Sara S Rasheed, Rebah N Algafari, Rehab S Ramadhan, Marwah Amer Qamandar, Sura S Talib, Rawnaq Z Fadhil","doi":"10.31083/j.fbs1603016","DOIUrl":null,"url":null,"abstract":"<p><strong>Background: </strong>Prostate cancer (PCa) is one of the leading diseases causing mortality. It comes in the third rank of common cancer types. It is considered extremely a complicated cancer type since it occurs in highly steroid-responsive and dependent tissues. Many factors are considered to play an important role in the disease progression of PCa, with some functioning at the molecular level.</p><p><strong>Methodology: </strong>After applying the exclusion criteria, 200 patients who underwent proctectomy were included in this study. Following receiving patient consent, blood samples were withdrawn from patients, DNA was extracted, and precise polymerase chain reaction (PCR) amplification was conducted using specifically designed primers. The resulting amplicons were sequenced and analyzed.</p><p><strong>Results: </strong>The progesterone receptor B (<i>PGRB</i>) DNA from patients showed four distinctive single-nucleotide polymorphisms (SNPs) at sites 11:101128812, 11:101128924, 11:101128949, and 11:101128986, which altered the amino acid sequences to Y>N, A>D, T>I, and C>R, respectively, compared to control. These SNPs resided in sensitive sites that either affected the control elements or promoted alterations in the protein configuration. This DNA change diminished the <i>PGR</i> gene function and promoted an imbalance in the encoded PGR protein structure and expression.</p><p><strong>Conclusions: </strong>Many factors may play a role in PCa manifestation, with steroids and progesterone initially noted as factors. Many studies have dealt with the hormonal effect on PCa; however, few have ultimately determined the molecular impact on disease progression. The presence of pathogenic SNPs in the enhancing region of the gene may impact the expression level of <i>PGR</i>. High or low expression levels may negatively affect gene function, which can be considered a reliable factor in prostate tumorigenesis.</p>","PeriodicalId":73070,"journal":{"name":"Frontiers in bioscience (Scholar edition)","volume":"16 3","pages":"16"},"PeriodicalIF":0.0000,"publicationDate":"2024-09-24","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"The Possible Role of Progesterone Receptors in Prostate Cancer Incidences in the Iraqi Population.\",\"authors\":\"Jaleel Ibrahim Asaad, Khalid S A Alazzawi, Sara S Rasheed, Rebah N Algafari, Rehab S Ramadhan, Marwah Amer Qamandar, Sura S Talib, Rawnaq Z Fadhil\",\"doi\":\"10.31083/j.fbs1603016\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p><strong>Background: </strong>Prostate cancer (PCa) is one of the leading diseases causing mortality. It comes in the third rank of common cancer types. It is considered extremely a complicated cancer type since it occurs in highly steroid-responsive and dependent tissues. Many factors are considered to play an important role in the disease progression of PCa, with some functioning at the molecular level.</p><p><strong>Methodology: </strong>After applying the exclusion criteria, 200 patients who underwent proctectomy were included in this study. Following receiving patient consent, blood samples were withdrawn from patients, DNA was extracted, and precise polymerase chain reaction (PCR) amplification was conducted using specifically designed primers. The resulting amplicons were sequenced and analyzed.</p><p><strong>Results: </strong>The progesterone receptor B (<i>PGRB</i>) DNA from patients showed four distinctive single-nucleotide polymorphisms (SNPs) at sites 11:101128812, 11:101128924, 11:101128949, and 11:101128986, which altered the amino acid sequences to Y>N, A>D, T>I, and C>R, respectively, compared to control. These SNPs resided in sensitive sites that either affected the control elements or promoted alterations in the protein configuration. This DNA change diminished the <i>PGR</i> gene function and promoted an imbalance in the encoded PGR protein structure and expression.</p><p><strong>Conclusions: </strong>Many factors may play a role in PCa manifestation, with steroids and progesterone initially noted as factors. Many studies have dealt with the hormonal effect on PCa; however, few have ultimately determined the molecular impact on disease progression. The presence of pathogenic SNPs in the enhancing region of the gene may impact the expression level of <i>PGR</i>. 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引用次数: 0
摘要
背景:前列腺癌(PCa)是导致死亡的主要疾病之一:前列腺癌(PCa)是导致死亡的主要疾病之一。它在常见癌症类型中排名第三。它被认为是一种极其复杂的癌症类型,因为它发生在对类固醇高度敏感和依赖的组织中。许多因素被认为在 PCa 的疾病进展中起着重要作用,其中一些因素在分子水平上起作用:在应用排除标准后,200 名接受直肠切除术的患者被纳入本研究。在征得患者同意后,抽取患者的血液样本,提取 DNA,并使用专门设计的引物进行精确的聚合酶链反应(PCR)扩增。对得到的扩增子进行测序和分析:结果:与对照组相比,患者的孕酮受体 B(PGRB)DNA 在 11:101128812、11:101128924、11:101128949 和 11:101128986 位点出现了四个明显的单核苷酸多态性(SNPs),其氨基酸序列分别变为 Y>N、A>D、T>I 和 C>R。这些 SNP 位于敏感位点,要么影响了控制元件,要么促进了蛋白质构型的改变。这种 DNA 变化削弱了 PGR 基因的功能,导致编码的 PGR 蛋白结构和表达失衡:结论:许多因素都可能在 PCa 的表现中发挥作用,其中类固醇和黄体酮是最初被注意到的因素。许多研究都涉及激素对 PCa 的影响,但很少有研究能最终确定激素对疾病进展的分子影响。基因增强区存在致病性 SNP 可能会影响 PGR 的表达水平。表达水平过高或过低都可能对基因功能产生负面影响,这可被视为前列腺肿瘤发生的一个可靠因素。
The Possible Role of Progesterone Receptors in Prostate Cancer Incidences in the Iraqi Population.
Background: Prostate cancer (PCa) is one of the leading diseases causing mortality. It comes in the third rank of common cancer types. It is considered extremely a complicated cancer type since it occurs in highly steroid-responsive and dependent tissues. Many factors are considered to play an important role in the disease progression of PCa, with some functioning at the molecular level.
Methodology: After applying the exclusion criteria, 200 patients who underwent proctectomy were included in this study. Following receiving patient consent, blood samples were withdrawn from patients, DNA was extracted, and precise polymerase chain reaction (PCR) amplification was conducted using specifically designed primers. The resulting amplicons were sequenced and analyzed.
Results: The progesterone receptor B (PGRB) DNA from patients showed four distinctive single-nucleotide polymorphisms (SNPs) at sites 11:101128812, 11:101128924, 11:101128949, and 11:101128986, which altered the amino acid sequences to Y>N, A>D, T>I, and C>R, respectively, compared to control. These SNPs resided in sensitive sites that either affected the control elements or promoted alterations in the protein configuration. This DNA change diminished the PGR gene function and promoted an imbalance in the encoded PGR protein structure and expression.
Conclusions: Many factors may play a role in PCa manifestation, with steroids and progesterone initially noted as factors. Many studies have dealt with the hormonal effect on PCa; however, few have ultimately determined the molecular impact on disease progression. The presence of pathogenic SNPs in the enhancing region of the gene may impact the expression level of PGR. High or low expression levels may negatively affect gene function, which can be considered a reliable factor in prostate tumorigenesis.