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年轻和老年患者发生的胰腺导管腺癌表现出相似的分子特征。

Pancreatic Ductal Adenocarcinoma Arising in Young and Old Patients Displays Similar Molecular Features.

作者信息

Raffenne Jérôme, Martin Fernando A, Nicolle Rémy, Konta Marina, Blum Yuna, Torrisani Jérôme, Puleo Francesco, Bachet Jean Baptiste, Svrcek Magali, Bardier-Dupas Armel, Emile Jean Francois, Demetter Peter, Radman Miroslav, Van Laethem Jean Luc, Hammel Pascal, Rebours Vinciane, Paradis Valérie, Couvelard Anne, Cros Jérôme

机构信息

INSERM U1149, Inflammation Research Center, Beaujon Hospital, 92110 Clichy, France.

Proteomic Research Group, Mediterranean Institute for Life Science, 21000 Split, Croatia.

出版信息

Cancers (Basel). 2021 Mar 11;13(6):1234. doi: 10.3390/cancers13061234.

Abstract

Pancreatic ducal adenocarcinoma is classically diagnosed in the 7th decade, but approximately 10% of patients are diagnosed under 55 years (y.o.). While the genomic and transcriptomic landscapes of late-onset tumors (LOT) have been described, little is known about early-onset tumors (EOT). Ageing is known to impact DNA methylation and proteome integrity through carbonylation-related oxidative damages. We therefore aimed to assess the global molecular features of EOT. We compared 176 EOT (≤55 y.o.) and 316 LOT (≥70 y.o.) from three distinct surgical cohorts at the clinical/genomic/epigenomic/transcriptomic level. Furthermore, we assessed oxidative stress responses and oxidative proteome damages using 2D gel electrophoresis followed by mass spectrometry protein identification. There was no consistent clinical difference between EOT and LOT across the three cohorts. The mutational landscape of key driver genes and the global methylation profile were similar in the two groups. LOT did display age-related features such as enriched DNA repair gene signatures and upregulation of oxidative stress defenses together with increased proteome carbonylation. However, these age-related differences were more preeminent in non-tumor tissues while tumor proteome and proteome damages were fairly comparable. In conclusion, this multi-omics comparison showed that EOT harbor a comparable molecular profile to that of LOT.

摘要

胰腺导管腺癌通常在70岁左右被诊断出来,但约10%的患者在55岁以下被诊断。虽然已经描述了晚发性肿瘤(LOT)的基因组和转录组特征,但对于早发性肿瘤(EOT)却知之甚少。已知衰老会通过羰基化相关的氧化损伤影响DNA甲基化和蛋白质组完整性。因此,我们旨在评估EOT的整体分子特征。我们在临床/基因组/表观基因组/转录组水平上比较了来自三个不同手术队列的176例EOT(≤55岁)和316例LOT(≥70岁)。此外,我们使用二维凝胶电泳结合质谱蛋白质鉴定来评估氧化应激反应和氧化蛋白质组损伤。在三个队列中,EOT和LOT之间没有一致的临床差异。两组中关键驱动基因的突变情况和整体甲基化谱相似。LOT确实表现出与年龄相关的特征,如DNA修复基因特征富集、氧化应激防御上调以及蛋白质组羰基化增加。然而,这些与年龄相关的差异在非肿瘤组织中更为突出,而肿瘤蛋白质组和蛋白质组损伤相当。总之,这种多组学比较表明,EOT具有与LOT相当的分子特征。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0f19/7999057/300045096b9f/cancers-13-01234-g001.jpg

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