Safir Ullah Khan, Zahid Ullah, Hadia Shaukat, Sheeza Unab, Saba Jannat, Waqar Ali, Amir Ali, Muhammad Irfan, Muhammad Fiaz Khan, Rodolfo Daniel Cervantes-Villagrana
{"title":"TP53及其调控基因与皮肤黑色素瘤预后的关系。","authors":"Safir Ullah Khan, Zahid Ullah, Hadia Shaukat, Sheeza Unab, Saba Jannat, Waqar Ali, Amir Ali, Muhammad Irfan, Muhammad Fiaz Khan, Rodolfo Daniel Cervantes-Villagrana","doi":"10.1177/11769351231177267","DOIUrl":null,"url":null,"abstract":"<p><p>The present study was the first comprehensive investigation of genetic mutation and expression levels of the p53 signaling genes in cutaneous melanoma through various genetic databases providing large datasets. The mutational landscape of p53 and its signaling genes was higher than expected, with <i>TP53</i> followed by <i>CDKN2A</i> being the most mutated gene in cutaneous melanoma. Furthermore, the expression analysis showed <i>that TP53</i>, <i>MDM2</i>, <i>CDKN2A</i>, and <i>TP53BP1</i> were overexpressed, while <i>MDM4</i> and <i>CDKN2B</i> were under-expressed in cutaneous melanoma. Overall, TCGA data revealed that among all the other p53 signaling proteins, CDKN2A was significantly higher in both sun and non-sun-exposed healthy tissues than in melanoma. Likewise, MDM4 and TP53BP1 expressions were markedly greater in non-sun-exposed healthy tissues compared to other groups. However, CDKN2B expression was higher in the sun-exposed healthy tissues than in other tissues. In addition, various genes were expressed significantly differently among males and females. In addition, <i>CDKN2A</i> was highly expressed in the SK-MEL-30 skin cancer cell line, whereas, Immune cell type expression analysis revealed that the <i>MDM4</i> was highly expressed in naïve B-cells. Furthermore, all six genes were significantly overexpressed in extraordinarily overweight or obese tumor tissues compared to healthy tissues. <i>MDM2</i> expression and tumor stage were closely related. There were differences in gene expression across patient age groups and positive nodal status. <i>TP53</i> showed a positive correlation with B cells, <i>MDM2</i> with CD8+<i>T</i> cells, macrophages and neutrophils, and <i>MDM4</i> with neutrophils. <i>CDKN2A/B</i> had a non-significant correlation with all six types of immune cells. However, <i>TP53BP1</i> was positively correlated with all five types of immune cells except B cells. Only <i>TP53, MDM2</i>, and <i>CDKN2A</i> had a role in cutaneous melanoma-specific tumor immunity. All TP53 and its regulating genes may be predictive for prognosis. The results of the present study need to be validated through future screening, in vivo, and in vitro studies.</p>","PeriodicalId":35418,"journal":{"name":"Cancer Informatics","volume":"22 ","pages":"11769351231177267"},"PeriodicalIF":2.4000,"publicationDate":"2023-01-01","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://ftp.ncbi.nlm.nih.gov/pub/pmc/oa_pdf/c1/e4/10.1177_11769351231177267.PMC10475268.pdf","citationCount":"0","resultStr":"{\"title\":\"TP53 and its Regulatory Genes as Prognosis of Cutaneous Melanoma.\",\"authors\":\"Safir Ullah Khan, Zahid Ullah, Hadia Shaukat, Sheeza Unab, Saba Jannat, Waqar Ali, Amir Ali, Muhammad Irfan, Muhammad Fiaz Khan, Rodolfo Daniel Cervantes-Villagrana\",\"doi\":\"10.1177/11769351231177267\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p><p>The present study was the first comprehensive investigation of genetic mutation and expression levels of the p53 signaling genes in cutaneous melanoma through various genetic databases providing large datasets. The mutational landscape of p53 and its signaling genes was higher than expected, with <i>TP53</i> followed by <i>CDKN2A</i> being the most mutated gene in cutaneous melanoma. Furthermore, the expression analysis showed <i>that TP53</i>, <i>MDM2</i>, <i>CDKN2A</i>, and <i>TP53BP1</i> were overexpressed, while <i>MDM4</i> and <i>CDKN2B</i> were under-expressed in cutaneous melanoma. Overall, TCGA data revealed that among all the other p53 signaling proteins, CDKN2A was significantly higher in both sun and non-sun-exposed healthy tissues than in melanoma. Likewise, MDM4 and TP53BP1 expressions were markedly greater in non-sun-exposed healthy tissues compared to other groups. However, CDKN2B expression was higher in the sun-exposed healthy tissues than in other tissues. In addition, various genes were expressed significantly differently among males and females. In addition, <i>CDKN2A</i> was highly expressed in the SK-MEL-30 skin cancer cell line, whereas, Immune cell type expression analysis revealed that the <i>MDM4</i> was highly expressed in naïve B-cells. Furthermore, all six genes were significantly overexpressed in extraordinarily overweight or obese tumor tissues compared to healthy tissues. <i>MDM2</i> expression and tumor stage were closely related. There were differences in gene expression across patient age groups and positive nodal status. <i>TP53</i> showed a positive correlation with B cells, <i>MDM2</i> with CD8+<i>T</i> cells, macrophages and neutrophils, and <i>MDM4</i> with neutrophils. <i>CDKN2A/B</i> had a non-significant correlation with all six types of immune cells. However, <i>TP53BP1</i> was positively correlated with all five types of immune cells except B cells. Only <i>TP53, MDM2</i>, and <i>CDKN2A</i> had a role in cutaneous melanoma-specific tumor immunity. All TP53 and its regulating genes may be predictive for prognosis. 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TP53 and its Regulatory Genes as Prognosis of Cutaneous Melanoma.
The present study was the first comprehensive investigation of genetic mutation and expression levels of the p53 signaling genes in cutaneous melanoma through various genetic databases providing large datasets. The mutational landscape of p53 and its signaling genes was higher than expected, with TP53 followed by CDKN2A being the most mutated gene in cutaneous melanoma. Furthermore, the expression analysis showed that TP53, MDM2, CDKN2A, and TP53BP1 were overexpressed, while MDM4 and CDKN2B were under-expressed in cutaneous melanoma. Overall, TCGA data revealed that among all the other p53 signaling proteins, CDKN2A was significantly higher in both sun and non-sun-exposed healthy tissues than in melanoma. Likewise, MDM4 and TP53BP1 expressions were markedly greater in non-sun-exposed healthy tissues compared to other groups. However, CDKN2B expression was higher in the sun-exposed healthy tissues than in other tissues. In addition, various genes were expressed significantly differently among males and females. In addition, CDKN2A was highly expressed in the SK-MEL-30 skin cancer cell line, whereas, Immune cell type expression analysis revealed that the MDM4 was highly expressed in naïve B-cells. Furthermore, all six genes were significantly overexpressed in extraordinarily overweight or obese tumor tissues compared to healthy tissues. MDM2 expression and tumor stage were closely related. There were differences in gene expression across patient age groups and positive nodal status. TP53 showed a positive correlation with B cells, MDM2 with CD8+T cells, macrophages and neutrophils, and MDM4 with neutrophils. CDKN2A/B had a non-significant correlation with all six types of immune cells. However, TP53BP1 was positively correlated with all five types of immune cells except B cells. Only TP53, MDM2, and CDKN2A had a role in cutaneous melanoma-specific tumor immunity. All TP53 and its regulating genes may be predictive for prognosis. The results of the present study need to be validated through future screening, in vivo, and in vitro studies.
期刊介绍:
The field of cancer research relies on advances in many other disciplines, including omics technology, mass spectrometry, radio imaging, computer science, and biostatistics. Cancer Informatics provides open access to peer-reviewed high-quality manuscripts reporting bioinformatics analysis of molecular genetics and/or clinical data pertaining to cancer, emphasizing the use of machine learning, artificial intelligence, statistical algorithms, advanced imaging techniques, data visualization, and high-throughput technologies. As the leading journal dedicated exclusively to the report of the use of computational methods in cancer research and practice, Cancer Informatics leverages methodological improvements in systems biology, genomics, proteomics, metabolomics, and molecular biochemistry into the fields of cancer detection, treatment, classification, risk-prediction, prevention, outcome, and modeling.
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