Targeting IL-8 and Its Receptors in Prostate Cancer: Inflammation, Stress Response, and Treatment Resistance

Cancers Pub Date : 2024-08-08 DOI:10.3390/cancers16162797
Shauna McClelland, P. Maxwell, Cristina Branco, Simon T Barry, C. Eberlein, Melissa J. LaBonte
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Abstract

This review delves into the intricate roles of interleukin-8 (IL-8) and its receptors, CXCR1 and CXCR2, in prostate cancer (PCa), particularly in castration-resistant (CRPC) and metastatic CRPC (mCRPC). This review emphasizes the crucial role of the tumour microenvironment (TME) and inflammatory cytokines in promoting tumour progression and response to tumour cell targeting agents. IL-8, acting through C-X-C chemokine receptor type 1 (CXCR1) and type 2 (CXCR2), modulates multiple signalling pathways, enhancing the angiogenesis, proliferation, and migration of cancer cells. This review highlights the shift in PCa research focus from solely tumour cells to the non-cancer-cell components, including vascular endothelial cells, the extracellular matrix, immune cells, and the dynamic interactions within the TME. The immunosuppressive nature of the PCa TME significantly influences tumour progression and resistance to emerging therapies. Current treatment modalities, including androgen deprivation therapy and chemotherapeutics, encounter persistent resistance and are complicated by prostate cancer’s notably “immune-cold” nature, which limits immune system response to the tumour. These challenges underscore the critical need for novel approaches that both overcome resistance and enhance immune engagement within the TME. The therapeutic potential of inhibiting IL-8 signalling is explored, with studies showing enhanced sensitivity of PCa cells to treatments, including radiation and androgen receptor inhibitors. Clinical trials, such as the ACE trial, demonstrate the efficacy of combining CXCR2 inhibitors with existing treatments, offering significant benefits, especially for patients with resistant PCa. This review also addresses the challenges in targeting cytokines and chemokines, noting the complexity of the TME and the need for precision in therapeutic targeting to avoid side effects and optimize outcomes.
靶向 IL-8 及其受体治疗前列腺癌:炎症、应激反应和治疗耐受性
本综述深入探讨了白细胞介素-8(IL-8)及其受体CXCR1和CXCR2在前列腺癌(PCa)中的复杂作用,尤其是在耐阉割(CRPC)和转移性CRPC(mCRPC)中的作用。本综述强调了肿瘤微环境(TME)和炎性细胞因子在促进肿瘤进展和对肿瘤细胞靶向药物的反应中的关键作用。IL-8通过C-X-C趋化因子受体1型(CXCR1)和2型(CXCR2)发挥作用,调节多种信号通路,促进血管生成、增殖和癌细胞迁移。本综述强调了 PCa 研究重点已从单纯的肿瘤细胞转移到非癌细胞成分,包括血管内皮细胞、细胞外基质、免疫细胞以及 TME 内的动态相互作用。PCa TME 的免疫抑制特性极大地影响了肿瘤的进展和对新疗法的耐受性。目前的治疗方法,包括雄激素剥夺疗法和化疗,都会遇到持续的抗药性,而前列腺癌明显的 "免疫冷 "特性又限制了免疫系统对肿瘤的反应,使治疗变得更加复杂。这些挑战凸显了对既能克服抗药性又能增强肿瘤组织间质内免疫参与的新型方法的迫切需要。抑制 IL-8 信号的治疗潜力已得到探索,研究显示 PCa 细胞对放射和雄激素受体抑制剂等治疗的敏感性增强。临床试验(如 ACE 试验)表明,将 CXCR2 抑制剂与现有治疗方法结合使用具有显著疗效,尤其是对耐药 PCa 患者。本综述还讨论了靶向细胞因子和趋化因子所面临的挑战,指出了TME的复杂性以及精确靶向治疗的必要性,以避免副作用并优化疗效。
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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