Molecular markers of metastatic disease in KRAS-mutant lung adenocarcinoma

被引:5
作者
Boiarsky, D. [1 ]
Lydon, C. A. [2 ]
Chambers, E. S. [3 ]
Sholl, L. M. [4 ,5 ]
Nishino, M. [6 ]
Skoulidis, F. [7 ]
Heymach, J., V [7 ]
Luo, J. [8 ]
Awad, M. A. [2 ]
Janne, P. A. [3 ]
Van Allen, E. M. [2 ,9 ,10 ]
Barbie, D. A. [3 ,7 ]
Vokes, N. I. [11 ,12 ]
机构
[1] Tufts Med Ctr, Dept Med, Boston, MA USA
[2] Dana Farber Canc Inst, Dept Med Oncol, Boston, MA USA
[3] Dana Farber Canc Inst, Lowe Ctr Thorac Oncol, Boston, MA USA
[4] Brigham & Womens Hosp, Ctr Adv Mol Diagnost, Boston, MA USA
[5] Harvard Med Sch, Boston, MA USA
[6] Brigham & Womens Hosp, Dept Radiol, Boston, MA USA
[7] Univ Texas MD Anderson Canc Ctr, Dept Thorac Head & Neck Med Oncol, Houston, TX USA
[8] Dana Farber Canc Inst, Dept Med, Boston, MA USA
[9] Broad Inst Harvard & MIT, Cambridge, England
[10] Dana Farber Canc Inst, Ctr Canc Precis Med, Boston, MA USA
[11] Univ Texas MD Anderson Canc Ctr, Dept Genom Med, Houston, TX USA
[12] MD Anderson Canc Ctr, Dept Thorac Head & Neck Med Oncol, 1515 Holcombe Blvd, Houston, TX 77030 USA
来源
ANNALS OF ONCOLOGY | 2023年 / 34卷 / 07期
关键词
KRAS; KEAP1; STK11; lung adenocarcinoma; metastatic; COOCCURRING GENOMIC ALTERATIONS; CANCER GENOMICS; NRF2; ACTIVATION; RAS ONCOGENE; MUTATION; PATTERNS; EXPRESSION; PROFILES; BIOLOGY; ASSAY;
D O I
10.1016/j.annonc.2023.04.514
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Background: Prior studies characterized the association of molecular alterations with treatment-specific outcomes in KRAS-mutant (KRASMUT) lung adenocarcinoma (LUAD). Less is known about the prognostic role of molecular alterations and their associations with metastatic disease.Patients and methods: We analyzed clinicogenomic data from 1817 patients with KRASMUT LUAD sequenced at the Dana-Farber Cancer Institute (DFCI) and Memorial Sloan Kettering Cancer Center (MSKCC). Patients with metastatic (M1) and nonmetastatic (M0) disease were compared. Transcriptomic data from The Cancer Genome Atlas (TCGA) were investigated to characterize the biology of differential associations with clinical outcomes. Organ-specific metastasis was associated with overall survival (OS).Results: KEAP1 (DFCI: OR = 2.3, q = 0.04; MSKCC: OR = 2.2, q = 0.00027) and SMARCA4 mutations (DFCI: OR = 2.5, q = 0.06; MSKCC: OR = 2.6, q = 0.0021) were enriched in M1 versus M0 tumors. On integrative modeling, NRF2 activation was the genomic feature most associated with OS. KEAP1 mutations were enriched in M1 versus M0 tumors independent of STK11 status (KEAP1MUT/STK11WT: DFCI OR = 3.0, P = 0.0064; MSKCC OR = 2.0, P = 0.041; KEAP1MUT/STK11MUT: DFCI OR = 2.3, P = 0.0063; MSKCC OR = 2.5, P = 3.6 x 10-05); STK11 mutations without KEAP1 loss were not associated with stage (KEAP1WT/STK11MUT: DFCI OR = 0.97, P = 1.0; MSKCC OR = 1.2, P = 0.33) or outcome. KEAP1/KRAS-mutated tumors with and without STK11 mutations exhibited high functional STK11 loss. The negative effects of KEAP1 were compounded in the presence of bone (HR = 2.3, P = 4.4 x 10-14) and negated in the presence of lymph node metastasis (HR = 1.0, P = 0.91).Conclusions: Mutations in KEAP1 and SMARCA4, but not STK11, were associated with metastatic disease and poor OS. Functional STK11 loss, however, may contribute to poor outcomes in KEAP1MUT tumors. Integrating molecular data with clinical and metastatic-site annotations can more accurately risk stratify patients.
引用
收藏
页码:589 / 604
页数:16
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