Abstract LB136: Targeting GCN2 kinase-driven stress response inactivation by orally available small molecules to restore immune tumor microenvironment in prostate cancers

Kyle Medley, Zhaoliang Li, D. Yan, U. Swami, N. Agarwal, H. Vankayalapati
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Abstract

In patients with metastatic castration-resistant prostate cancers (mCRPC) who have previously been treated with abiraterone or enzalutamide, the median overall survival is only 14 months. Unlike many other cancers, immunotherapies have had limited successes, due to the fact that there are very few T cells in the tumor microenvironment of prostate cancer (PC) patients. Identifying ways to boost immunotherapy responses could change the paradigm of mCRPC, a disease still difficult to treat. The highly proliferative nature of tumor cells, along with infiltration of myeloid cells into the tumors, leads to depletion of nutrients such as functional/natural amino acids. This metabolically stressful milieu causes activation of nutrient stress pathways, autophagy, and repressed immune responses. A key meditator of this nutrient stress pathway is a cytoplasmic Ser/Thr protein kinase called General Control Nonderepressible 2 (GCN2), also called EIF2AK4. GCN2 switches on by a reduction of amino acids, and its activity results in T cell inactivation, T cell death, regulatory T cell expansion, and the potentiation of myeloid-derived suppressor cells (MDSCs). We have developed and synthesized a series of novel small molecule immunotherapeutic agents that reversibly bind to GCN2 kinase, competitively block the ATP site, and elicit pharmacological responses in immune cells. GCN2 cell-free kinase binding, kinome selectivity, pGCN2, pEIF2α, ATF-4 phosphorylation inhibition assays were performed and confirmed it9s on-target efficacy and potency of lead GCN2 inhibitor HCI-1046. In these studies, our lead GCN2 kinase inhibitor HCI-1046 demonstrated potent activity with an IC50 of 36 nM in inhibiting GCN2. GCN2 expression has been detected in PC-3, DU-145, and LNCap cell lines, and HCI-1046 exhibited cellular efficacy with an IC50 of 0.9 to 8 μM range, reduced phosphorylation of GCN2, ATF-4 significantly and its downstream target eIF2α. HCI-1046 inhibited pGCN2 and pEIF2α in human prostate cancer clinical patient samples derived MDSC cultured in amino-acid starved conditions. HCI-1046, in a dose-dependent fashion, restored CD8+ T cell proliferation and function in clinical samples of PC patients. Our preliminary results support the hypothesis that inhibition of GCN2 reinstates anti-tumor immunity and blocks tumor progression in PC cellular models. In vivo PK studies of HCI-1046 in rodent species showed excellent PK properties; 55% oral bioavailability, low clearance, and >5 hours half-life. HCI-1046 is nominated as a pre-clinical agent. Additional 3D cellular efficacy studies, FACS for cellular apoptosis, cell migration, live PC cells including immuno-ELISA, ELISpot experimental results for MDSCs suppressive function of T cells, and restoration by HCI-1046 will be presented at the conference. PC mouse model efficacy studies will also be discussed. Citation Format: Kyle Medley, Zhaoliang Li, Dongqing Yan, Umang Swami, Neeraj Agarwal, Hariprasad Vankayalapati. Targeting GCN2 kinase-driven stress response inactivation by orally available small molecules to restore immune tumor microenvironment in prostate cancers [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2021; 2021 Apr 10-15 and May 17-21. Philadelphia (PA): AACR; Cancer Res 2021;81(13_Suppl):Abstract nr LB136.
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LB136:口服小分子靶向GCN2激酶驱动的应激反应失活,恢复前列腺癌免疫肿瘤微环境
转移性去势抵抗性前列腺癌(mCRPC)患者先前接受过阿比特龙或恩杂鲁胺治疗,中位总生存期仅为14个月。与许多其他癌症不同,免疫疗法的成功有限,因为前列腺癌(PC)患者的肿瘤微环境中很少有T细胞。确定增强免疫治疗反应的方法可能会改变mCRPC的模式,这是一种仍然难以治疗的疾病。肿瘤细胞的高度增殖特性,以及骨髓细胞向肿瘤的浸润,导致功能性/天然氨基酸等营养物质的消耗。这种代谢应激环境导致营养应激途径的激活、自噬和免疫反应的抑制。这种营养胁迫途径的一个关键介导因子是一种称为GCN2 (General Control nonderexpression 2)的细胞质丝氨酸/苏氨酸蛋白激酶,也称为EIF2AK4。GCN2通过氨基酸的减少而开启,其活性导致T细胞失活、T细胞死亡、调节性T细胞扩增和髓源性抑制细胞(MDSCs)的增强。我们已经开发和合成了一系列新的小分子免疫治疗剂,它们可逆地结合GCN2激酶,竞争性地阻断ATP位点,并在免疫细胞中引起药理反应。通过GCN2无细胞激酶结合、激酶组选择性、pGCN2、pEIF2α、ATF-4磷酸化抑制实验,证实了其对GCN2铅抑制剂HCI-1046的靶向疗效和效力。在这些研究中,我们的主要GCN2激酶抑制剂HCI-1046显示出抑制GCN2的有效活性,IC50为36 nM。GCN2在PC-3、DU-145和LNCap细胞系中均有表达,HCI-1046的IC50值为0.9 ~ 8 μM,显著降低了GCN2、ATF-4及其下游靶点eIF2α的磷酸化水平。HCI-1046在氨基酸饥饿条件下培养的人前列腺癌临床患者MDSC样品中抑制pGCN2和pEIF2α。HCI-1046以剂量依赖性的方式恢复PC患者临床样本中的CD8+ T细胞增殖和功能。我们的初步结果支持了抑制GCN2恢复抗肿瘤免疫并阻断PC细胞模型中肿瘤进展的假设。HCI-1046在啮齿类动物体内的PK研究显示出优异的PK性能;55%口服生物利用度,低清除率,半衰期>5小时。HCI-1046被提名为临床前药物。其他3D细胞功效研究、细胞凋亡的FACS、细胞迁移、活PC细胞(包括免疫elisa、MDSCs抑制T细胞功能的ELISpot实验结果以及HCI-1046的修复)将在会议上发表。还将讨论PC小鼠模型的功效研究。引文格式:Kyle Medley, Zhaoliang Li, Dongqing Yan, Umang Swami, Neeraj Agarwal, Hariprasad Vankayalapati。口服小分子靶向GCN2激酶驱动的应激反应失活,恢复前列腺癌免疫肿瘤微环境[摘要]。见:美国癌症研究协会2021年年会论文集;2021年4月10日至15日和5月17日至21日。费城(PA): AACR;癌症杂志,2021;81(13 -增刊):摘要nr LB136。
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