Co-occurring Genomic Alterations Define Major Subsets of KRAS-Mutant Lung Adenocarcinoma with Distinct Biology, Immune Profiles, and Therapeutic Vulnerabilities

Skoulidis Ferdinandos; Byers Lauren A.; Diao Lixia; Papadimitrakopoulou Vassiliki A.; Tong Pan; Izzo Julie; Behrens Carmen; Kadara Humam; Parra Edwin R.; Canales Jaime Rodriguez; Zhang Jianjun; Giri Uma; Gudikote Jayanthi; Cortez Maria A.; Yang Chao; Fan Youhong; Peyton Michael; Girard Luc; Coombes Kevin R.; Toniatti Carlo; Heffernan Timothy P.; Choi Murim; Frampton Garrett M.; Miller Vincent; Weinstein John N.; Herbst Roy S.; Wong Kwok-Kin; Zhang Jianhua; Sharma Padmanee; Mills Gordon B.; Hong Waun K.; Minna John D.; Allison James P.; Futreal Andrew; Wang Jing; Wistuba Ignacio I.; Heymach John V.

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Co-occurring Genomic Alterations Define Major Subsets of KRAS-Mutant Lung Adenocarcinoma with Distinct Biology, Immune Profiles, and Therapeutic Vulnerabilities

机译：共同发生的基因组改变定义了KRAS突变型肺腺癌的主要亚集，具有不同的生物学，免疫学特征和治疗脆弱性

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The molecular underpinnings that drive the heterogeneity of KRAS-mutant lung adenocarcinoma are poorly characterized. We performed an integrative analysis of genomic, transcriptomic, and proteomic data from early-stage and chemorefractory lung adenocarcinoma and identified three robust subsets of KRAS-mutant lung adenocarcinoma dominated, respectively, by co-occurring genetic events in STK11/LKB1 (the KL subgroup), TP53 (KP), and CDKN2A/B inactivation coupled with low expression of the NKX2-1 (TTF1) transcription factor (KC). We further revealed biologically and therapeutically relevant differences between the subgroups. KC tumors frequently exhibited mucinous histology and suppressed mTORC1 signaling. KL tumors had high rates of KEAP1 mutational inactivation and expressed lower levels of immune markers, including PD-L1. KP tumors demonstrated higher levels of somatic mutations, inflammatory markers, immune checkpoint effector molecules, and improved relapse-free survival. Differences in drug sensitivity patterns were also observed; notably, KL cells showed increased vulnerability to HSP90-inhibitor therapy. This work provides evidence that co-occurring genomic alterations identify subgroups of KRAS-mutant lung adenocarcinoma with distinct biology and therapeutic vulnerabilities.

机译：驱动KRAS突变型肺腺癌异质性的分子基础很差。我们对来自早期和化学难治性肺腺癌的基因组，转录组和蛋白质组学数据进行了综合分析，并确定了STK11 / LKB1（KL亚组）中同时发生的遗传事件，分别确定了KRAS突变型肺腺癌的三个主要亚群。），TP53（KP）和CDKN2A / B失活，以及NKX2-1（TTF1）转录因子（KC）的低表达。我们进一步揭示了亚组之间的生物学和治疗学相关差异。 KC肿瘤经常表现出粘液组织学和抑制mTORC1信号。 KL肿瘤具有较高的KEAP1突变失活率，并表达较低水平的免疫标志物，包括PD-L1。 KP肿瘤表现出更高水平的体细胞突变，炎性标志物，免疫检查点效应分子，并改善了无复发生存率。还观察到药物敏感性模式的差异。值得注意的是，KL细胞显示出对HSP90抑制剂治疗的增加的脆弱性。这项工作提供的证据表明，共同发生的基因组改变可识别出具有明显生物学和治疗脆弱性的KRAS突变型肺腺癌亚组。

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《Cancer discovery.》 |2015年第8期|共18页
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Skoulidis Ferdinandos; Byers Lauren A.; Diao Lixia; Papadimitrakopoulou Vassiliki A.; Tong Pan; Izzo Julie; Behrens Carmen; Kadara Humam; Parra Edwin R.; Canales Jaime Rodriguez; Zhang Jianjun; Giri Uma; Gudikote Jayanthi; Cortez Maria A.; Yang Chao; Fan Youhong; Peyton Michael; Girard Luc; Coombes Kevin R.; Toniatti Carlo; Heffernan Timothy P.; Choi Murim; Frampton Garrett M.; Miller Vincent; Weinstein John N.; Herbst Roy S.; Wong Kwok-Kin; Zhang Jianhua; Sharma Padmanee; Mills Gordon B.; Hong Waun K.; Minna John D.; Allison James P.; Futreal Andrew; Wang Jing; Wistuba Ignacio I.; Heymach John V.;
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1. Co-occurring Genomic Alterations Define Major Subsets of KRAS-Mutant Lung Adenocarcinoma with Distinct Biology, Immune Profiles, and Therapeutic Vulnerabilities [J] . Skoulidis Ferdinandos, Byers Lauren A., Diao Lixia, Cancer discovery. . 2015,第8期

机译：共同发生的基因组改变定义了KRAS突变型肺腺癌的主要亚集，具有不同的生物学，免疫学特征和治疗脆弱性
2. Integrative analysis reveals distinct subtypes with therapeutic implications in KRAS-mutant lung adenocarcinoma [J] . Ke Liu, Jintao Guo, Kuai Liu, EBioMedicine . 2018,第184期

机译：综合分析揭示了在KRAS突变型肺腺癌中具有治疗意义的不同亚型
3. Distinct initiating events underpin the immune and metabolic heterogeneity of KRAS-mutant lung adenocarcinoma [J] . Sarah A. Best, Sheryl Ding, Ariena Kersbergen, Nature Communications . 2019,第1期

机译：不同的启动事件基于Kras-突变体肺腺癌的免疫和代谢异质性
4. Kinase Activity Profiling of Lung Adenocarcinoma to Understand Cancer Signaling and Select Targeted Therapeutics [C] . Melissa A. Hoffman, Bin Fang, Stephen Brantley, ASMS Conference on Mass Spectrometry and Allied Topics . 2016

机译：肺腺癌的激酶活性分析，了解癌症信号，选择有针对性的治疗方法
5. Single Cell Proteomics Microchip to Profile Immune Function, with Applications in Stem Cell Biology, Translational Disease Mechanism Study and Clinical Therapeutics Monitoring. [D] . Ma, Chao. 2013

机译：单细胞蛋白质组学Microchip可描述免疫功能，并应用于干细胞生物学，转化疾病机制研究和临床治疗学监测。
6. Co-occurring genomic alterations define major subsets of KRAS - mutant lung adenocarcinoma with distinct biology immune profiles and therapeutic vulnerabilities [O] . Ferdinandos Skoulidis, Lauren A. Byers, Lixia Diao, -1

机译：共同出现的基因组改变定义了KRAS的主要子集-突变的肺腺癌具有独特的生物学免疫谱和治疗脆弱性
7. Distinct initiating events underpin the immune and metabolic heterogeneity of KRAS-mutant lung adenocarcinoma [O] . Sarah A. Best, Sheryl Ding, Ariena Kersbergen, 2019

机译：不同的启动事件基于Kras-突变体肺腺癌的免疫和代谢异质性

Co-occurring Genomic Alterations Define Major Subsets of KRAS-Mutant Lung Adenocarcinoma with Distinct Biology, Immune Profiles, and Therapeutic Vulnerabilities

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