对“综合基因组分析揭示早发性前列腺癌中雄激素驱动的体细胞改变图谱”的评论。作者:魏申费尔德特J、西蒙R、费尔巴赫L、施兰根K、魏肯汉D、明纳S、武蒂希D、瓦尔纳茨HJ、施泰尔H、劳施T、耶格尔N、顾L、博加蒂罗娃O、施图茨AM、克劳斯R、艾尔斯J、艾尔斯R、格哈泽尔C、黄PH、胡特尔B、卡贝R、劳伦茨C、拉多姆斯基S、巴托洛梅CC、法尔特M、加德S、施密特M、阿姆施勒N、哈斯T、加拉尔R、乔尼J、库纳R、贝尔C、马瑟S、冯·卡勒C、齐chner T、贝内斯V、雷德尔B、马德M、阿姆蒂斯拉夫斯基V、阿夫奇M、莱赫拉赫H、帕尔霍姆丘克D、苏丹M、伯克哈特L、格雷芬M、胡兰德H、克卢特M、克罗恩A、西尔马H、施图姆L、施特勒S、格鲁普K、苏尔特曼H、绍特G、普拉斯C、布罗斯B、亚斯波ML、科尔贝尔JO、施洛姆T,欧洲分子生物学实验室(EMBL)基因组生物学组,德国海德堡。发表于《癌细胞》2013年;23(2):159 - 70。
Commentary on "integrative genomic analyses reveal an androgen-driven somatic alteration landscape in early-onset prostate cancer." Weischenfeldt J, Simon R, Feuerbach L, Schlangen K, Weichenhan D, Minner S, Wuttig D, Warnatz HJ, Stehr H, Rausch T, Jäger N, Gu L, Bogatyrova O, Stütz AM, Claus R, Eils J, Eils R, Gerhäuser C, Huang PH, Hutter B, Kabbe R, Lawerenz C, Radomski S, Bartholomae CC, Fälth M, Gade S, Schmidt M, Amschler N, Haß T, Galal R, Gjoni J, Kuner R, Baer C, Masser S, von Kalle C, Zichner T, Benes V, Raeder B, Mader M, Amstislavskiy V, Avci M, Lehrach H, Parkhomchuk D, Sultan M, Burkhardt L, Graefen M, Huland H, Kluth M, Krohn A, Sirma H, Stumm L, Steurer S, Grupp K, Sültmann H, Sauter G, Plass C, Brors B, Yaspo ML, Korbel JO, Schlomm T, Genome Biology Unit, European Molecular Biology Laboratory (EMBL), Heidelberg, Germany.: Cancer Cell 2013;23(2):159-70.
作者信息
Olumi Aria F
出版信息
Urol Oncol. 2014 Feb;32(2):212. doi: 10.1016/j.urolonc.2013.08.018.
Early-onset prostate cancer (EO-PCA) represents the earliest clinical manifestation of prostate cancer. To compare the genomic alteration landscapes of EO-PCA with "classical" (elderly-onset) PCA, we performed deep sequencing-based genomics analyses in 11 tumors diagnosed at young age, and pursued comparative assessments with seven elderly-onset PCA genomes. Remarkable age-related differences in structural rearrangement (SR) formation became evident, suggesting distinct disease pathomechanisms. Whereas EO-PCAs harbored a prevalence of balanced SRs, with a specific abundance of androgen-regulated ETS gene fusions including TMPRSS2:ERG, elderly-onset PCAs displayed primarily non-androgen-associated SRs. Data from a validation cohort of>10,000 patients showed age-dependent androgen receptor levels and a prevalence of SRs affecting androgen-regulated genes, further substantiating the activity of a characteristic "androgen-type" pathomechanism in EO-PCA.
早发性前列腺癌(EO-PCA)是前列腺癌最早的临床表现。为了比较EO-PCA与“经典”(老年发病)PCA的基因组改变图谱,我们对11例年轻患者诊断出的肿瘤进行了基于深度测序的基因组分析,并与7个老年发病PCA基因组进行了比较评估。结构重排(SR)形成方面显著的年龄相关差异变得明显,提示不同的疾病发病机制。EO-PCA中平衡SRs占优势,有特定数量的雄激素调节的ETS基因融合,包括TMPRSS2:ERG,而老年发病PCA主要表现为非雄激素相关的SRs。来自超过10000名患者的验证队列的数据显示雄激素受体水平与年龄相关,以及影响雄激素调节基因的SRs的发生率,进一步证实了EO-PCA中特征性“雄激素型”发病机制的活性。
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