Osorio Lucia, Grazioso Tatiana P, de Velasco Guillermo, Etxaniz Olatz, Pérez-Gracia Jose Luis, Pinto Álvaro, Durán Ignacio, Grande Enrique, Garcia Pablo Borrega, Lázaro Martín, Rodriguez Laura, Villalobos Maria Laura, García Lourdes, Cuellar Andrés, Solís-Hernández María Pilar, Pernaut Cristina, Rodríguez-Moreno Juan Francisco, Rodriguez-Antona Cristina, García-Donas Jesús
Servicio de Urología, Urología Hospitalaria, Hospital HM La Rosaleda, Santiago de Compostela, Spain.
Instituto de Investigación Sanitaria HM Hospitales (IISHM), Madrid, Spain.
Clin Transl Oncol. 2025 May;27(5):2241-2255. doi: 10.1007/s12094-024-03652-9. Epub 2024 Oct 4.
Despite that incorporating antiangiogenic in combination with immune-checkpoint inhibitors as the standard first-line treatment for advanced clear cell renal cell cancer (ccRCC) yields promising outcomes, these regimens often lead to significant toxicity. However, a subgroup of patients has shown responsiveness to VEGFR tyrosine-kinase inhibitors (TKIs) in monotherapy, leading to the question of whether employing combination therapies can significantly enhance overall survival in all patients over monotherapy. Thus, we aim to identify gene expression signatures that can predict TKI response within subpopulations that might benefit from single-agent therapies, to minimize unnecessary exposure to combination therapies and their associated toxicities, as well as to discover new potential therapeutic targets to improve ccRCC treatment. Based on prior data, the androgen receptor (AR) might meet both conditions.
We evaluated the association between AR expression, assessed through NanoString technology-derived mRNA counts, and the clinical outcomes of 98 ccRCC patients treated with first-line antiangiogenics and determined its association with other genes implicated in ccRCC tumorigenesis.
Higher AR-expression correlates significantly with better prognosis and survival based on the MSKCC risk score, and longer PFS. Furthermore, we have identified a gene set signature associated with AR-overexpression and several genes involved in angiogenesis and transcriptional targets of the hypoxia-inducible factor, a cornerstone of ccRCC.
AR-overexpression and its association with other genes could favor a transcriptomic signature set to aid in identifying patients suitable for TKI in monotherapy, rather than aggressive combinations, enhancing thus, precision and personalized therapeutic decisions.
尽管将抗血管生成药物与免疫检查点抑制剂联合作为晚期透明细胞肾细胞癌(ccRCC)的标准一线治疗方案取得了令人鼓舞的成果,但这些方案往往会导致显著的毒性。然而,有一小部分患者对VEGFR酪氨酸激酶抑制剂(TKIs)单药治疗表现出反应,这引发了一个问题,即联合治疗是否能在所有患者中显著提高总生存期,超过单药治疗。因此,我们旨在识别基因表达特征,以预测可能从单药治疗中获益的亚群内对TKI的反应,尽量减少不必要的联合治疗暴露及其相关毒性,并发现新的潜在治疗靶点以改善ccRCC治疗。基于先前的数据,雄激素受体(AR)可能符合这两个条件。
我们通过基于NanoString技术的mRNA计数评估AR表达与98例接受一线抗血管生成治疗的ccRCC患者临床结局之间的关联,并确定其与ccRCC肿瘤发生中涉及的其他基因的关联。
基于MSKCC风险评分,较高的AR表达与更好的预后、生存率以及更长的无进展生存期显著相关。此外,我们确定了一个与AR过表达相关的基因集特征以及几个参与血管生成和缺氧诱导因子转录靶点的基因,缺氧诱导因子是ccRCC的一个基石。
AR过表达及其与其他基因的关联可能有利于一种转录组特征集,以帮助识别适合TKI单药治疗而非激进联合治疗的患者,从而提高精准度和个性化治疗决策。
