Rajendra Prasad, Sonia Panchal, Isha Rani, Jai Kishan, Gaurav Parashar
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Further, these identified h-TERT promoter mutations were analysed for the prediction of pathophysiological consequences using bioinformatics tools such as Tfsitescan and CIIDER. The average age of patients was 45 ± 8 years which was categorized in early onset of lung cancer with predominance of male patients by 5.6 fold. Interestingly, h-TERT promoter mutations were observed highly frequent in lung cancer. Identified mutations include c. G272A, c. T122A, c. C150A, c. 123 del C, c. C123T, c. G105A, c. 107 Ins A, c. 276 del C corresponding to -168 G>A, -18 T>A, -46 C>A, -19 del C, -19 C>T, -1 G>A, -3 Ins A, -172 del C respectively from the translation start site in the promoter of the telomerase reverse transcriptase gene which are the first time reported in germline genome from lung cancer. Strikingly, c. -18 T>A [C.T122A] was found the most prevalent variant with 75% frequency. Notwithstanding, other mutations viz c. -G168A [c. G272A] and c. -1 G>A [c. G105A] were found to be at 35% and 15% frequency respectively whilst the rest of the mutations were present at 10% and 5% frequency. Additionally, bioinformatics analysis revealed that these mutations can lead to either loss or gain of various transcription factor binding sites in the h-TERT promoter region. Henceforth, these mutations may play a pivotal role in h-TERT gene expression. Taken together, these identified novel promoter mutations may alter the epigenetics and subsequently various transcription factor binding sites which are of great functional significance. 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The recurrent h-TERT promoter mutations have been implicated in various cancer types. Thus, the present study is extended to analyze h-TERT promoter mutations from the North Indian lung carcinoma patients. Total 20 histopathologically and clinically confirmed cases of lung cancer were enrolled in this study. The genomic DNA was extracted from venous blood and subjected to amplification using appropriate h-TERT promoter primers. Amplified PCR products were subjected for DNA Sanger sequencing for the identification of novel h-TERT mutations. Further, these identified h-TERT promoter mutations were analysed for the prediction of pathophysiological consequences using bioinformatics tools such as Tfsitescan and CIIDER. The average age of patients was 45 ± 8 years which was categorized in early onset of lung cancer with predominance of male patients by 5.6 fold. Interestingly, h-TERT promoter mutations were observed highly frequent in lung cancer. Identified mutations include c. G272A, c. 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引用次数: 0
摘要
肺癌是一种严重的癌症,也是全球癌症相关死亡的主要原因。反复出现的 h-TERT 启动子突变与多种癌症类型都有关联。因此,本研究扩展分析了北印度肺癌患者的 h-TERT 启动子突变。共有 20 例经组织病理学和临床确诊的肺癌患者参与了本研究。从静脉血中提取基因组 DNA,并使用适当的 h-TERT 启动子引物进行扩增。扩增的 PCR 产物经 DNA Sanger 测序,以鉴定新型 h-TERT 基因突变。此外,还使用 Tfsitescan 和 CIIDER 等生物信息学工具对这些已确定的 h-TERT 启动子突变进行分析,以预测其病理生理后果。患者的平均年龄为 45 ± 8 岁,属于早发性肺癌,男性患者占多数,比例为 5.6 倍。有趣的是,h-TERT 启动子突变在肺癌中非常常见。已发现的突变包括 c. G272A、c. T122A、c. C150A、c. 123 del C、c. C123T、c. G105A、c. 107 Ins A、c.276 del C,分别对应于端粒酶反转录酶基因启动子翻译起始位点的-168 G>A、-18 T>A、-46 C>A、-19 del C、-19 C>T、-1 G>A、-3 Ins A、-172 del C,这在肺癌种系基因组中是首次报道。引人注目的是,c. -18 T>A [C.T122A]是最常见的变异,频率为75%。G168A [c. G272A]和 c. -1 G>A [c. G105A]的频率分别为35%和15%,而其他变异的频率分别为10%和5%。此外,生物信息学分析表明,这些突变可导致 h-TERT 启动子区域中各种转录因子结合位点的缺失或增益。因此,这些突变可能在h-TERT基因表达中起着关键作用。综上所述,这些已发现的新型启动子突变可能会改变表观遗传学,进而改变具有重要功能意义的各种转录因子结合位点。因此,这些种系突变可能是肺癌的易感因素,也可能通过纠缠不清的分子机制直接参与肺癌的病理生理学。
Identification of h-TERT Promoter Mutations in Germline DNA from North Indian Lung Carcinoma Patients.
Lung cancer is a severe and the leading cause of cancer related deaths worldwide. The recurrent h-TERT promoter mutations have been implicated in various cancer types. Thus, the present study is extended to analyze h-TERT promoter mutations from the North Indian lung carcinoma patients. Total 20 histopathologically and clinically confirmed cases of lung cancer were enrolled in this study. The genomic DNA was extracted from venous blood and subjected to amplification using appropriate h-TERT promoter primers. Amplified PCR products were subjected for DNA Sanger sequencing for the identification of novel h-TERT mutations. Further, these identified h-TERT promoter mutations were analysed for the prediction of pathophysiological consequences using bioinformatics tools such as Tfsitescan and CIIDER. The average age of patients was 45 ± 8 years which was categorized in early onset of lung cancer with predominance of male patients by 5.6 fold. Interestingly, h-TERT promoter mutations were observed highly frequent in lung cancer. Identified mutations include c. G272A, c. T122A, c. C150A, c. 123 del C, c. C123T, c. G105A, c. 107 Ins A, c. 276 del C corresponding to -168 G>A, -18 T>A, -46 C>A, -19 del C, -19 C>T, -1 G>A, -3 Ins A, -172 del C respectively from the translation start site in the promoter of the telomerase reverse transcriptase gene which are the first time reported in germline genome from lung cancer. Strikingly, c. -18 T>A [C.T122A] was found the most prevalent variant with 75% frequency. Notwithstanding, other mutations viz c. -G168A [c. G272A] and c. -1 G>A [c. G105A] were found to be at 35% and 15% frequency respectively whilst the rest of the mutations were present at 10% and 5% frequency. Additionally, bioinformatics analysis revealed that these mutations can lead to either loss or gain of various transcription factor binding sites in the h-TERT promoter region. Henceforth, these mutations may play a pivotal role in h-TERT gene expression. Taken together, these identified novel promoter mutations may alter the epigenetics and subsequently various transcription factor binding sites which are of great functional significance. Thereby, it is plausible that these germline mutations may involve either as predisposing factor or direct participation in the pathophysiology of lung cancer through entangled molecular mechanisms.
期刊介绍:
The primary mission of the journal is to promote improvement in the health and well-being of community through the development and practice of clinical biochemistry and dissemination of knowledge and recent advances in this discipline among professionals, diagnostics industry, government and non-government organizations. Indian Journal of Clinical Biochemistry (IJCB) publishes peer reviewed articles that contribute to the existing knowledge in all fields of Clinical biochemistry, either experimental or theoretical, particularly deal with the applications of biochemistry, molecular biology, genetics, biotechnology, and immunology to the diagnosis, treatment, monitoring and prevention of human diseases. The articles published also include those covering the analytical and molecular diagnostic techniques, instrumentation, data processing, quality assurance and accreditation aspects of the clinical investigations in which chemistry has played a major role, or laboratory animal studies with biochemical and clinical relevance.
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