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Patient-derived tumor xenograft study with CDK4/6 inhibitor plus AKT inhibitor for the management of metastatic castration-resistant prostate cancer

前列腺癌 医学 阉割 癌症研究 癌症 前列腺 蛋白激酶B 内科学 肿瘤科 生物 细胞凋亡 激素 生物化学
作者
Adam M. Kase,Justyna Trynda,James L. Miller,Erin Miller,Joachim L. Petit,Michael T. Barrett,Yumei Zhou,Ephraim E. Parent,Hancheng Cai,Joshua A. Knight,Jacob J. Orme,Jordan Reynolds,William F. Durham,Thomas Metz,Nathalie Meurice,Brandy Edenfield,Aylin Alasonyalılar Demirer,Ahmet Bilgili,Peyton G. Hickman,Matthew L. Pawlush
出处
期刊:Molecular Cancer Therapeutics [American Association for Cancer Research]
卷期号:23 (6): 823-835 被引量:4
标识
DOI:10.1158/1535-7163.mct-23-0296
摘要

Metastatic castration-resistant prostate cancer (mCRPC) is an aggressive malignancy with poor outcomes. To investigate novel therapeutic strategies, we characterized three new metastatic prostate cancer patient derived-tumor xenograft (PDTX) models and developed 3D spheroids from each to investigate molecular targeted therapy combinations including CDK4/6 inhibitors (CDK4/6i) with AKT inhibitors (ATKi). Metastatic prostate cancer tissue was collected and three PDTX models were established and characterized using whole-exome sequencing. PDTX 3D spheroids were developed from these three PDTXs to show resistance patterns and test novel molecular-targeted therapies. CDK4/6i's were combined with AKTi's to assess synergistic antitumor response to prove our hypothesis that blockade of AKT overcomes drug resistance to CDK4/6i. This combination was evaluated in PDTX three-dimensional (3D) spheroids and in vivo experiments with responses measured by tumor volumes, PSA, and Ga-68 PSMA-11 PET-CT imaging. We demonstrated CDK4/6i's with AKTi's possess synergistic antitumor activity in three mCRPC PDTX models. These models have multiple unique pathogenic and deleterious genomic alterations with resistance to single-agent CDK4/6i's. Despite this, combination therapy with AKTi's was able to overcome resistance mechanisms. The IHC and Western blot analysis confirmed on target effects, whereas tumor volume, serum PSA ELISA, and radionuclide imaging demonstrated response to therapy with statistically significant SUV differences seen with Ga-68 PSMA-11 PET-CT. These preclinical data demonstrating antitumor synergy by overcoming single-agent CDK 4/6i as well as AKTi drug resistance provide the rational for a clinical trial combining a CDK4/6i with an AKTi in patients with mCRPC whose tumor expresses wild-type retinoblastoma 1.
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