Department of Gynecologic Oncology and Reproductive Medicine, The University of Texas MD Anderson Cancer Center, Houston, TX, USA.
Br J Cancer. 2024 May;130(11):1875-1884. doi: 10.1038/s41416-024-02668-w. Epub 2024 Apr 6.
Other than for breast cancer, endocrine therapy has not been highly effective for gynecologic cancers. Endocrine therapy resistance in estrogen receptor positive gynecologic cancers is still poorly understood. In this retrospective study, we examined the estrogen receptor (ER) signaling pathway activities of breast, ovarian, endometrial, and cervical cancers to identify those that may predict endocrine therapy responsiveness.
Clinical and genomic data of women with breast and gynecological cancers were downloaded from cBioPortal for Cancer Genomics. Estrogen receptor alpha (ESR1) expression level and sample-level pathway enrichment scores (EERES) were calculated to classify patients into four groups (low/high ESR1 and low/high EERES). Correlation between ESR1/EERES score and survival was further validated with RNAseq data from low-grade serous ovarian cancer. Pathway analyses were performed among different ESR1/EERES groups to identify genes that correlate with endocrine resistance, which are validated using Cancer Cell Line Encyclopedia gene expression and Genomics of Drug Sensitivity in Cancer data.
We identified a novel combined prognostic value of ESR1 expression and the corresponding estrogen response signaling (EERES score) for breast cancer. The combined prognostic value (ESR1/EERES) may be applicable to other gynecologic cancers. More importantly, we discovered that ER signaling can cross-regulate MEK pathway activation. We identified downstream genes in the MEK pathway (EPHA2, INAVA, MALL, MPZL2, PCDH1, and TNFRSF21) that are potential endocrine therapy response biomarkers.
This study demonstrated that targeting both the ER and the ER signaling activity related MEK pathway may aid the development of endocrine therapy strategies for personalized medicine.
除乳腺癌外,内分泌治疗对妇科癌症的疗效并不高。雌激素受体阳性妇科癌症的内分泌治疗耐药性仍知之甚少。在这项回顾性研究中,我们检测了乳腺癌、卵巢癌、子宫内膜癌和宫颈癌的雌激素受体(ER)信号通路活性,以确定那些可能预测内分泌治疗反应性的通路。
从癌症基因组学 cBioPortal 下载了患有乳腺癌和妇科癌症的女性的临床和基因组数据。计算了雌激素受体α(ESR1)表达水平和样本水平途径富集评分(EERES),将患者分为 4 组(ESR1 低/高和 EERES 低/高)。使用低级别浆液性卵巢癌的 RNAseq 数据进一步验证了 ESR1/EERES 评分与生存之间的相关性。在不同的 ESR1/EERES 组之间进行了途径分析,以确定与内分泌耐药性相关的基因,这些基因使用癌症细胞系百科全书基因表达和癌症药物敏感性基因组学数据进行了验证。
我们确定了一种新的 ESR1 表达和相应的雌激素反应信号(EERES 评分)联合预后价值,可用于乳腺癌。这种联合预后价值(ESR1/EERES)可能适用于其他妇科癌症。更重要的是,我们发现 ER 信号可以交叉调节 MEK 途径的激活。我们鉴定了 MEK 途径下游基因(EPHA2、INAVA、MALL、MPZL2、PCDH1 和 TNFRSF21),这些基因可能是潜在的内分泌治疗反应生物标志物。
本研究表明,靶向 ER 和与 ER 信号活性相关的 MEK 途径可能有助于开发针对个体化医学的内分泌治疗策略。
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