- Carrot-Zhang, Jian;
- Yao, Xiaotong;
- Devarakonda, Siddhartha;
- Deshpande, Aditya;
- Damrauer, Jeffrey S;
- Silva, Tiago Chedraoui;
- Wong, Christopher K;
- Choi, Hyo Young;
- Felau, Ina;
- Robertson, A Gordon;
- Castro, Mauro AA;
- Bao, Lisui;
- Rheinbay, Esther;
- Liu, Eric Minwei;
- Trieu, Tuan;
- Haan, David;
- Yau, Christina;
- Hinoue, Toshinori;
- Liu, Yuexin;
- Shapira, Ofer;
- Kumar, Kiran;
- Mungall, Karen L;
- Zhang, Hailei;
- Lee, Jake June-Koo;
- Berger, Ashton;
- Gao, Galen F;
- Zhitomirsky, Binyamin;
- Liang, Wen-Wei;
- Zhou, Meng;
- Moorthi, Sitapriya;
- Berger, Alice H;
- Collisson, Eric A;
- Zody, Michael C;
- Ding, Li;
- Cherniack, Andrew D;
- Getz, Gad;
- Elemento, Olivier;
- Benz, Christopher C;
- Stuart, Josh;
- Zenklusen, JC;
- Beroukhim, Rameen;
- Chang, Jason C;
- Campbell, Joshua D;
- Hayes, D Neil;
- Yang, Lixing;
- Laird, Peter W;
- Weinstein, John N;
- Kwiatkowski, David J;
- Tsao, Ming S;
- Travis, William D;
- Khurana, Ekta;
- Berman, Benjamin P;
- Hoadley, Katherine A;
- Robine, Nicolas;
- Network, TCGA Research;
- Arora, Kanika;
- Shah, Minita;
- Shelton, Jennifer;
- Bowlby, Reanne;
- Friedl, Verena;
- Goldman, Mary;
- Craft, Brian;
- Heiman, David I;
- Hajirasouliha, Iman;
- Ricketts, Camir;
- Anur, Pavana;
- Chiotti, Kami E;
- Caesar-Johnson, Samantha J;
- Demchok, John A;
- Ferguson, Martin L;
- Kemal, Anab;
- Tarnuzzer, Roy;
- Wang, Zhining;
- Yang, Liming;
- Spellman, Paul T;
- Raphael, Benjamin;
- Akbani, Rehan;
- Zhu, Jingchun;
- Jones, Steven JM;
- Shen, Hui;
- Meyerson, Matthew;
- Govindan, Ramaswamy;
- Imielinski, Marcin
RTK/RAS/RAF pathway alterations (RPAs) are a hallmark of lung adenocarcinoma (LUAD). In this study, we use whole-genome sequencing (WGS) of 85 cases found to be RPA(-) by previous studies from The Cancer Genome Atlas (TCGA) to characterize the minority of LUADs lacking apparent alterations in this pathway. We show that WGS analysis uncovers RPA(+) in 28 (33%) of the 85 samples. Among the remaining 57 cases, we observe focal deletions targeting the promoter or transcription start site of STK11 (n = 7) or KEAP1 (n = 3), and promoter mutations associated with the increased expression of ILF2 (n = 6). We also identify complex structural variations associated with high-level copy number amplifications. Moreover, an enrichment of focal deletions is found in TP53 mutant cases. Our results indicate that RPA(-) cases demonstrate tumor suppressor deletions and genome instability, but lack unique or recurrent genetic lesions compensating for the lack of RPAs. Larger WGS studies of RPA(-) cases are required to understand this important LUAD subset.