前列腺癌中的剪接突变基因组变异。
Splice-disrupt genomic variants in prostate cancer.
机构信息
National Center for Biotechnology, Life Science and Environment Research Institute, King Abdulaziz City for Science and Technology (KACST), Riyadh, Saudi Arabia.
Department of Biochemistry, College of Science, King Saud University, Riyadh, Saudi Arabia.
出版信息
Mol Biol Rep. 2022 Jun;49(6):4237-4246. doi: 10.1007/s11033-022-07257-9. Epub 2022 Mar 14.
BACKGROUND
Splice-disrupt genomic variants are one of the causes of cancer-causing errors in gene expression. Little is known about splice-disrupt genomic variants.
METHODS AND RESULTS
Here, pattern of splice-disrupt variants was investigated using 21,842,764 genomic variants in different types of prostate cancer. A particular attention was paid to genomic locations of splice-disrupt variants on target genes. HLA-A in prostate cancer, MSR1 in familial prostate cancer, and EGFR in both castration-resistant prostate cancer and metastatic castration-resistant had the highest allele frequencies of splice-disrupt variations. Some splice-disrupt variants, located on coding sequences of NCOR2, PTPRC, and CRP, were solely present in the advanced metastatic castration-resistant prostate cancer. High-risk splice-disrupt variants were identified based on computationally calculated Polymorphism Phenotyping (PolyPhen), Sorting Intolerant From Tolerant (SIFT), and Genomic Evolutionary Rate Profiling (GERP) + + scores as well as the recorded clinical significance in dbSNP database of NCBI. Functional annotation of damaging splice-disrupt variants highlighted important cancer-associated functions, including endocrine resistance, lipid metabolic process, steroid metabolic process, regulation of mitotic cell cycle, and regulation of metabolic process. This is the first study that profiles the splice-disrupt genomic variants and their target genes in prostate cancer. Literature mining based variant analysis highlighted the importance of rs1800716 variant, located on the CYP2D6 gene, involved in a range of important functions, such as RNA spicing, drug interaction, death, and urotoxicity.
CONCLUSIONS
This is the first study that profiles the splice-disrupt genomic variants and their target genes in different types of prostate cancer. Unravelling alternative splicing opens a new avenue towards the establishment of new diagnostic and prognostic markers for prostate cancer progression and metastasis.
背景
剪接破坏基因组变异是导致基因表达致癌错误的原因之一。对于剪接破坏基因组变异,人们知之甚少。
方法和结果
在这里,使用不同类型前列腺癌中的 21842764 个基因组变异来研究剪接破坏变异的模式。特别关注了剪接破坏变异在靶基因上的基因组位置。在前列腺癌中,HLA-A、家族性前列腺癌中的 MSR1 以及去势抵抗性前列腺癌和转移性去势抵抗性前列腺癌中的 EGFR 具有最高的剪接破坏变异等位基因频率。一些剪接破坏变异位于 NCOR2、PTPRC 和 CRP 的编码序列中,仅存在于晚期转移性去势抵抗性前列腺癌中。根据计算得出的 Polymorphism Phenotyping(PolyPhen)、Sorting Intolerant From Tolerant(SIFT)和 Genomic Evolutionary Rate Profiling(GERP)+ +评分以及 NCBI 中 dbSNP 数据库记录的临床意义,确定了高危剪接破坏变异。对破坏性剪接破坏变异的功能注释突出了重要的癌症相关功能,包括内分泌抵抗、脂质代谢过程、类固醇代谢过程、有丝分裂细胞周期调节和代谢过程调节。这是首次在前列腺癌中对剪接破坏基因组变异及其靶基因进行分析的研究。基于变异分析的文献挖掘强调了位于 CYP2D6 基因上的 rs1800716 变异的重要性,该变异涉及一系列重要功能,如 RNA 剪接、药物相互作用、死亡和尿毒性。
结论
这是首次在不同类型的前列腺癌中分析剪接破坏基因组变异及其靶基因的研究。揭示选择性剪接为建立前列腺癌进展和转移的新诊断和预后标志物开辟了新途径。
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