KRAS mutations in endometrial cancers: Possible prognostic and treatment implications

被引:0
|
作者
Kilowski, Karolina A. [1 ]
Ahmad, Sarfraz [1 ]
Dietrich, Martin F. [2 ]
Herzog, Thomas J. [4 ]
Xi, Joanne [3 ]
Thaker, Premal [5 ,6 ]
Baca, Yasmine [3 ]
Hinton, Andrew [3 ]
Holloway, Robert W. [1 ]
机构
[1] AdventHealth Canc Inst, Gynecol Oncol Program, 2501 N Orange Ave,Suite 786, Orlando, FL 32804 USA
[2] US Oncol Network, Canc Care Ctr Brevard, Rockledge, FL USA
[3] Med Affairs, Caris Life Sci, Phoenix, AZ USA
[4] Univ Cincinnati, Canc Ctr, Cincinnati, OH USA
[5] Washington Univ, Sch Med, St Louis, MO USA
[6] Siteman Canc Ctr, St Louis, MO USA
关键词
Endometrial cancer; KRAS mutations; Microsatellite instability; Tumor mutational burden; Immunotherapy; Targeted therapy; CELL LUNG-CANCER; MUTANT KRAS; IMMUNOTHERAPY; INHIBITOR; BLOCKADE; G12C; PD-1;
D O I
10.1016/j.ygyno.2024.10.026
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Background/Objectives. Patients with recurrent or metastatic endometrial cancer (EC) have poor prognoses with limited therapeutic options following immunotherapy or immunochemotherapy treatments. Inhibitors of KRAS mutations (KRAS-mut) have shown efficacy in early solid tumor studies, but data in EC are lacking. This study describes the frequency of KRAS-mut relative to other oncogenic alterations in EC to identify genomic characteristics of KRAS-mut tumors that could lead to novel therapeutic options. Methods. A molecular database of 7870 ECs was queried for presence of oncogenic mutations and immunotherapy biomarkers. Comparisons were performed using Fisher-Exact/ChiSquare (p-values) and adjusted for multiple tests by Benjamini-Hochberg (q) and pairwise nonparametric analysis using Wilcoxon Method. Results. KRAS-mut is a relatively frequent genotype in EC, detected in 16% of cases. Codon 12 was most frequently mutated, with G12D (31%) and G12V (27%) the most common subtypes. Biomarkers of immunotherapy response co-occur with KRAS-mut. Microsatellite instability-high and tumor mutational burden-high status were observed in 34.1% and 36.5% in KRAS-mut compared to 19.8% and 16.9% in KRAS-WT, respectively (p < 0.05). PD-L1 >1% was detected in 8.4% vs 6.4% of KRAS-mut vs KRAS-WT (p < 0.05). BRCA1/2 mutations were detected with similar low frequency (5.9% vs 4.9%) among KRAS-mut and KRAS-WT ECs (p > 0.05). KRAS-mut was inversely associated with Her-2 overexpression (1.8% KRAS-mut vs 13% KRAS-WT. (p < 0.0 01). Conclusions. KRAS-mut represents a genotypically distinct group of ECs. Overlap exists with genomic predictors (TMB-high, MSI-high) of immunotherapy response, suggesting a possible biomarker-driven combination option with immunotherapy. Clinical trials to evaluate these strategies should be developed.
引用
收藏
页码:299 / 306
页数:8
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