EphB4-ephrin-B2是去势抵抗性前列腺癌的靶点。
EphB4-ephrin-B2 are targets in castration resistant prostate cancer.
作者信息
Li Grace Xiuqing, Ma Binyun, Zhang Shaobing, Liu Ren, Siddiqi Imran N, Sali Akash, El-Khoueiry Anthony, Gross Mitchell, Salhia Bodour, Sadeghi Sarmad, Gill Parkash S
机构信息
Department of Medicine, USC Norris Comprehensive Cancer Center, Keck School of Medicine, University of Southern California, Los Angeles, CA, USA.
Merck Pharmaceutical Inc. Previous: Department of Medicine, USC Norris Comprehensive Cancer Center, Keck School of Medicine, University of Southern California, Los Angeles, CA, USA.
出版信息
Br J Cancer. 2025 May;132(8):679-689. doi: 10.1038/s41416-025-02942-5. Epub 2025 Mar 5.
BACKGROUND
PI3K pathway activation is a common and early event in prostate cancer, from loss of function mutations in PTEN, or activating mutations in PIK3Ca or AKT leading to constitutive activation, induction of growth factor-receptors kinase EphB4 and its ligand ephrin-B2. We hypothesized that induction of EphB4 is an early event required for tumor initiation. Secondly, we hypothesized that EphB4 remains relevant when prostate cancer becomes androgen independent.
METHODS
Genetic mouse model of conditional PTEN deletion in prostate epithelium induces tumor in all mice. We tested this model against EPHB4 wild type and deleted in prostate epithelium. This allowed us to test its role in tumor initiation. We also tested an orthogonal approach by using decoy soluble EphB4 to block bidirectional signaling resulting from EphB4-ephrin-B2 interaction. Role of EphB4-ephrin-B2 in androgen deprived mice was tested for role in refractory cancer model.
RESULTS
PTEN deletion induces EphB4 and ephrin-B2 in prostate cancer which was substantially reduced when EPHB4 is deleted in the same prostate epithelial cells. sEphB4-alb fusion protein with improved pharmacokinetics similarly inhibited tumor formation, thus establishing the role in tumor initiation. sEphB4-alb retained the efficacy in castration resistant androgen independent prostate cancer. We have thus observed that induction of EphB4 is required for the initiation of prostate cancer in PTEN null mouse and that signaling downstream from EphB4 is required in androgen deprivation and thus castration resistant prostate cancer. Pharmacological inhibition of EphB4 pathway reproduced the results. Targeting EphB4 should be tested in prostate cancer especially those resistant to androgen deprivation therapy.
CONCLUSIONS
EphB4 and ephrin-B2 receptor ligand pair is induced in PTEN null prostate cancer, which significantly contributes to the tumor initiation. Secondly, EphB4-ephrin-B2 pathway continue to promote tumor progression even in androgen deprivation and thus hormone refractory tumor. EphB4-ephrin-B2 may be candidates for precision medicine with biomarker-based patient selection with and without concurrent standard of care.
背景
PI3K 通路激活是前列腺癌中常见的早期事件,其源于 PTEN 的功能丧失性突变,或 PIK3Ca 或 AKT 的激活突变,导致组成性激活,诱导生长因子受体激酶 EphB4 及其配体 ephrin-B2。我们假设 EphB4 的诱导是肿瘤起始所必需的早期事件。其次,我们假设当前列腺癌变为雄激素非依赖性时,EphB4 仍然具有相关性。
方法
前列腺上皮中条件性 PTEN 缺失的基因小鼠模型在所有小鼠中均诱导肿瘤形成。我们将该模型与前列腺上皮中 EPHB4 野生型和缺失型进行对照测试。这使我们能够测试其在肿瘤起始中的作用。我们还通过使用诱饵可溶性 EphB4 来阻断由 EphB4-ephrin-B2 相互作用产生的双向信号传导,测试了一种正交方法。在雄激素剥夺小鼠中测试 EphB4-ephrin-B2 在难治性癌症模型中的作用。
结果
PTEN 缺失在前列腺癌中诱导 EphB4 和 ephrin-B2,当在相同前列腺上皮细胞中缺失 EPHB4 时,其表达大幅降低。具有改善药代动力学的 sEphB4-alb 融合蛋白同样抑制肿瘤形成,从而确定了其在肿瘤起始中的作用。sEphB4-alb 在去势抵抗性雄激素非依赖性前列腺癌中仍保持疗效。因此,我们观察到在 PTEN 基因敲除小鼠中,EphB4 的诱导是前列腺癌起始所必需的,并且在雄激素剥夺及因此产生的去势抵抗性前列腺癌中,EphB4 下游的信号传导是必需的。EphB4 通路的药理学抑制重现了这些结果。针对 EphB4 的靶向治疗应在前列腺癌中进行测试,尤其是那些对雄激素剥夺疗法耐药的患者。
结论
EphB4 和 ephrin-B2 受体配体对在 PTEN 基因敲除的前列腺癌中被诱导,这对肿瘤起始有显著贡献。其次,EphB4-ephrin-B2 通路即使在雄激素剥夺及因此产生的激素难治性肿瘤中也继续促进肿瘤进展。EphB4-ephrin-B2 可能是基于生物标志物选择患者并同时结合或不结合标准治疗的精准医学候选靶点。
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