The interplay between FOXO3 and FOXM1 influences sensitivity to AKT inhibition in PIK3CA and PIK3CA/PTEN altered estrogen receptor positive breast cancer.

IF 7.6 2区医学 Q1 ONCOLOGY

NPJ Breast Cancer Pub Date : 2025-04-22 DOI:10.1038/s41523-025-00752-9

Valentina Cutano, Ming Li Chia, Eleanor M Wigmore, Lorna Hopcroft, Stuart C Williamson, Amanda L Christie, Brandon Willis, James Kerr, Jenny Ashforth, Rhys Fox, Sophie D'Arcy, Lauren Bradshaw, Catherine Blaker, Cath Eberlein, Lambert Montava-Garriga, Elza C de Bruin, Susan E Critchlow, Kevin M Brindle, Simon T Barry, Susana Ros

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引用次数: 0

Abstract

Loss of PTEN expression, via homozygous or hemizygous deletion, is common in PIK3CA mutant ER + BC tumors. We assessed reduction of PTEN protein expression on AKT inhibitor capivasertib efficacy in PIK3CA altered tumors. In PIK3CA altered, PTEN protein high models, PI3Kα and AKT inhibition was effective, however ablation and partial PTEN expression reduction attenuated PI3Kαi but not AKTi efficacy, alone or combined with fulvestrant. Efficacy was FOXO3 dependent and associated with FOXM1 downregulation. FOXO3A deletion reduced response to capivasertib, and increased FOXM1 expression. Long term capivasertib exposure of ER+ BC cells upregulated FOXM1 expression. Downregulating FOXM1 expression reversed resistance to capivasertib, while FOXM1 overexpression reduced capivasertib efficacy. Collectively this suggests the AKT-FOXO3-FOXM1 axis plays a pivotal role in response to AKTi in ER+ breast cancer with PIK3CA mutations with and without expression of PTEN, that FOXO3 expression loss can mediate resistance, and that FOXM1 downregulation is a potential biomarker of response.

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FOXO3和FOXM1之间的相互作用影响PIK3CA和PIK3CA/PTEN改变的雌激素受体阳性乳腺癌对AKT抑制的敏感性。

通过纯合子或半合子缺失，PTEN表达缺失在PIK3CA突变的ER + BC肿瘤中很常见。我们评估了降低AKT抑制剂capivasertib的PTEN蛋白表达对PIK3CA改变肿瘤的疗效。在PIK3CA改变、PTEN蛋白高的模型中，PI3Kα和AKT抑制有效，但消融和部分PTEN表达降低可减弱PI3Kαi，但不能减弱AKTi的效果，单独或联合氟维司汀。疗效依赖于FOXO3，并与FOXM1下调有关。FOXO3A的缺失降低了对capivasertib的反应，并增加了FOXM1的表达。长期暴露于ER+ BC细胞的capivasertib上调FOXM1的表达。下调FOXM1表达逆转了对capivasertib的耐药性，而FOXM1过表达则降低了capivasertib的疗效。总的来说，这表明AKT-FOXO3-FOXM1轴在具有或不具有PTEN表达的PIK3CA突变的ER+乳腺癌中对AKTi的应答中起关键作用，FOXO3表达缺失可以介导抗性，FOXM1下调是应答的潜在生物标志物。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

NPJ Breast Cancer Medicine-Pharmacology (medical)

CiteScore

10.10

自引率

1.70%

发文量

122

审稿时长

9 weeks

期刊介绍： npj Breast Cancer publishes original research articles, reviews, brief correspondence, meeting reports, editorial summaries and hypothesis generating observations which could be unexplained or preliminary findings from experiments, novel ideas, or the framing of new questions that need to be solved. Featured topics of the journal include imaging, immunotherapy, molecular classification of disease, mechanism-based therapies largely targeting signal transduction pathways, carcinogenesis including hereditary susceptibility and molecular epidemiology, survivorship issues including long-term toxicities of treatment and secondary neoplasm occurrence, the biophysics of cancer, mechanisms of metastasis and their perturbation, and studies of the tumor microenvironment.