Li Yiyang, Zhou Wei, Li Long, Li John W, Li Tianyue, Huang Cheng, Lazaro-Camp Vanessa J, Kavlashvili Tamar, Zhang Yuping, Reyes Henry, Li Yujun, Dai Donghai, Zhu William, Meng Xiangbing, Leslie Kimberly K, Yang Shujie
Department of Obstetrics and Gynecology, The University of Iowa Iowa City, IA 52242, USA.
Department of Gynecology, First Hospital of Jilin University Changchun 130021, Jilin, China.
Am J Cancer Res. 2022 Nov 15;12(11):5029-5048. eCollection 2022.
Uterine endometrial cancer (EC) incidence and deaths are on the rise. Hormone therapy, a traditional treatment regimen for this disease, uses progesterone and its synthetic analogue, progestin, to induce cell differentiation, apoptosis, and inhibition of invasion. This therapy is highly effective for progesterone receptor (PR) positive tumors in the short term. However, responsiveness decreases over time due to loss of PR expression; acquired resistance leads to treatment failure and poor prognosis. Primary resistance occurs in advanced, PR-negative tumors. Regardless, progestin therapy can be effective if the PR downregulation mechanism is reversed and if functional PR expression is restored. Using histone deacetylase inhibitors (HDACi), we inhibited cell proliferation in three EC cell lines and restored functional PR expression at the mRNA and protein levels. Two HDACi were tested using an endometrial xenograft tumor model: entinostat, an oral drug, and romidepsin, an IV drug. and studies support that entinostat decreased EC tumor growth, induced differentiation, and increased expression of the PR-targeted gene, PAEP. These findings supported the approval of a new NIH NCTN clinical trial, NRG-GY011, which concluded that dual treatment of MPA and entinostat, decreased expression of the proliferation marker, Ki67, but did not increase PR expression relative to single treatment with MPA in this short-term study. Therefore, a more potent HDACi, romidepsin, was investigated. Romidepsin treatment inhibited tumor growth and enhanced progestin treatment efficacy. More importantly, PR, PAEP, and KIAA1324 expressions were upregulated. Using a chromatin immunoprecipitation assay, we verified that HDACi can reverse PR downregulation mechanisms in mice models. Other potential drug efficacy markers, such as CD52, DLK1, GALNT9, and GNG2, were identified by transcriptome analysis and verified by q-PCR. Many of the upregulated drug efficacy markers predict favorable patient outcomes, while downregulated genes predict worse survival. Here, our current data suggests that romidepsin is a more potent HDACi that has the potential to achieve more robust upregulation of PR expression and may be a more promising candidate for future clinical trials.
子宫内膜癌(EC)的发病率和死亡率正在上升。激素疗法是这种疾病的传统治疗方案,使用孕酮及其合成类似物孕激素来诱导细胞分化、凋亡并抑制侵袭。这种疗法在短期内对孕激素受体(PR)阳性肿瘤非常有效。然而,由于PR表达丧失,随着时间的推移反应性会降低;获得性耐药导致治疗失败和预后不良。原发性耐药发生在晚期PR阴性肿瘤中。无论如何,如果PR下调机制得以逆转且功能性PR表达得以恢复,孕激素疗法可能会有效。我们使用组蛋白去乙酰化酶抑制剂(HDACi)抑制了三种EC细胞系中的细胞增殖,并在mRNA和蛋白质水平上恢复了功能性PR表达。使用子宫内膜异种移植肿瘤模型测试了两种HDACi:口服药物恩替诺特和静脉注射药物罗米地辛。研究支持恩替诺特可降低EC肿瘤生长、诱导分化并增加PR靶向基因PAEP的表达。这些发现支持了一项新的美国国立卫生研究院(NIH)国家临床试验网络(NCTN)临床试验NRG-GY011的批准,该试验得出结论,在这项短期研究中,与单用甲羟孕酮(MPA)治疗相比,MPA与恩替诺特联合治疗可降低增殖标志物Ki67的表达,但并未增加PR表达。因此,对一种更有效的HDACi罗米地辛进行了研究。罗米地辛治疗可抑制肿瘤生长并增强孕激素治疗效果。更重要的是,PR、PAEP和KIAA1324的表达上调。使用染色质免疫沉淀试验,我们在小鼠模型中验证了HDACi可逆转PR下调机制。通过转录组分析鉴定了其他潜在的药物疗效标志物,如CD52、DLK1、GALNT9和GNG2,并通过q-PCR进行了验证。许多上调的药物疗效标志物预示着患者预后良好而下调的基因预示着生存情况较差。在此,我们目前的数据表明罗米地辛是一种更有效的HDACi,有可能实现PR表达更强劲的上调,可能是未来临床试验中更有前景的候选药物。
