可溶性鸟苷酸环化酶途径被抑制，以逃避雄激素剥夺诱导的衰老并促进向去势抵抗的进展。

The soluble guanylyl cyclase pathway is inhibited to evade androgen deprivation-induced senescence and enable progression to castration resistance.

作者信息

Zhang Ling, Troccoli Clara I, Mateo-Victoriano Beatriz, Lincheta Laura Misiara, Jackson Erin, Shu Ping, Plastini Trisha, Tao Wensi, Kwon Deukwoo, Chen Xi, Sharma Janaki, Jorda Merce, Gulley James L, Bilusic Marijo, Lockhart Albert Craig, Beuve Annie, Rai Priyamvada

出版信息

bioRxiv. 2023 May 3:2023.05.03.537252. doi: 10.1101/2023.05.03.537252.

DOI:10.1101/2023.05.03.537252

PMID:37205442

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10187243/

Abstract

UNLABELLED

Castration-resistant prostate cancer (CRPC) is fatal and therapeutically under-served. We describe a novel CRPC-restraining role for the vasodilatory soluble guanylyl cyclase (sGC) pathway. We discovered that sGC subunits are dysregulated during CRPC progression and its catalytic product, cyclic GMP (cGMP), is lowered in CRPC patients. Abrogating sGC heterodimer formation in castration-sensitive prostate cancer (CSPC) cells inhibited androgen deprivation (AD)-induced senescence, and promoted castration-resistant tumor growth. We found sGC is oxidatively inactivated in CRPC. Paradoxically, AD restored sGC activity in CRPC cells through redox-protective responses evoked to protect against AD-induced oxidative stress. sGC stimulation via its FDA-approved agonist, riociguat, inhibited castration-resistant growth, and the anti-tumor response correlated with elevated cGMP, indicating on-target sGC activity. Consistent with known sGC function, riociguat improved tumor oxygenation, decreasing the PC stem cell marker, CD44, and enhancing radiation-induced tumor suppression. Our studies thus provide the first evidence for therapeutically targeting sGC via riociguat to treat CRPC.

STATEMENT OF SIGNIFICANCE

Prostate cancer is the second highest cancer-related cause of death for American men. Once patients progress to castration-resistant prostate cancer, the incurable and fatal stage, there are few viable treatment options available. Here we identify and characterize a new and clinically actionable target, the soluble guanylyl cyclase complex, in castration-resistant prostate cancer. Notably we find that repurposing the FDA-approved and safely tolerated sGC agonist, riociguat, decreases castration-resistant tumor growth and re-sensitizes these tumors to radiation therapy. Thus our study provides both new biology regarding the origins of castration resistance as well as a new and viable treatment option.

摘要

未标记

去势抵抗性前列腺癌（CRPC）是致命的，且治疗手段不足。我们描述了血管舒张性可溶性鸟苷酸环化酶（sGC）途径在抑制CRPC方面的新作用。我们发现，在CRPC进展过程中，sGC亚基失调，且CRPC患者体内其催化产物环磷酸鸟苷（cGMP）水平降低。在去势敏感性前列腺癌（CSPC）细胞中消除sGC异二聚体的形成可抑制雄激素剥夺（AD）诱导的衰老，并促进去势抵抗性肿瘤生长。我们发现sGC在CRPC中发生氧化失活。矛盾的是，AD通过引发氧化还原保护反应来恢复CRPC细胞中的sGC活性，以抵御AD诱导的氧化应激。通过其获得美国食品药品监督管理局（FDA）批准的激动剂利奥西呱刺激sGC，可抑制去势抵抗性生长，且抗肿瘤反应与cGMP升高相关，表明sGC激动剂作用于靶点。与已知的sGC功能一致，利奥西呱改善了肿瘤氧合，降低了前列腺癌干细胞标志物CD44，并增强了辐射诱导的肿瘤抑制作用。因此，我们的研究首次提供了通过利奥西呱靶向sGC治疗CRPC的证据。

意义声明

前列腺癌是美国男性癌症相关死亡的第二大原因。一旦患者进展为去势抵抗性前列腺癌这一无法治愈的致命阶段，几乎没有可行的治疗选择。在这里，我们在去势抵抗性前列腺癌中鉴定并表征了一个新的且具有临床可操作性的靶点——可溶性鸟苷酸环化酶复合物。值得注意的是，我们发现重新利用已获得FDA批准且安全耐受的sGC激动剂利奥西呱，可减少去势抵抗性肿瘤生长，并使这些肿瘤对放射治疗重新敏感。因此，我们的研究既提供了关于去势抵抗起源的新生物学信息，也提供了一种新的可行治疗选择。