将抗心律失常药物重新定位用于前列腺癌治疗:一种向肿瘤抑制表型重编程癌相关成纤维细胞的新策略。
Repositioning of antiarrhythmics for prostate cancer treatment: a novel strategy to reprogram cancer-associated fibroblasts towards a tumor-suppressive phenotype.
机构信息
Molecular Pharmacology Unit, Department of Experimental Oncology, Fondazione IRCSS Istituto Nazionale Dei Tumori, Milan, 20133, Italy.
Vita-Salute San Raffaele University, IRCCS San Raffaele Hospital and Scientific Institute, Milan, 20132, Italy.
出版信息
J Exp Clin Cancer Res. 2024 Jun 11;43(1):161. doi: 10.1186/s13046-024-03081-0.
BACKGROUND
Cancer-associated fibroblasts (CAFs) play a significant role in fueling prostate cancer (PCa) progression by interacting with tumor cells. A previous gene expression analysis revealed that CAFs up-regulate genes coding for voltage-gated cation channels, as compared to normal prostate fibroblasts (NPFs). In this study, we explored the impact of antiarrhythmic drugs, known cation channel inhibitors, on the activated state of CAFs and their interaction with PCa cells.
METHODS
The effect of antiarrhythmic treatment on CAF activated phenotype was assessed in terms of cell morphology and fibroblast activation markers. CAF contractility and migration were evaluated by 3D gel collagen contraction and scratch assays, respectively. The ability of antiarrhythmics to impair CAF-PCa cell interplay was investigated in CAF-PCa cell co-cultures by assessing tumor cell growth and expression of epithelial-to-mesenchymal transition (EMT) markers. The effect on in vivo tumor growth was assessed by subcutaneously injecting PCa cells in SCID mice and intratumorally administering the medium of antiarrhythmic-treated CAFs or in co-injection experiments, where antiarrhythmic-treated CAFs were co-injected with PCa cells.
RESULTS
Activated fibroblasts show increased membrane conductance for potassium, sodium and calcium, consistently with the mRNA and protein content analysis. Antiarrhythmics modulate the expression of fibroblast activation markers. Although to a variable extent, these drugs also reduce CAF motility and hinder their ability to remodel the extracellular matrix, for example by reducing MMP-2 release. Furthermore, conditioned medium and co-culture experiments showed that antiarrhythmics can, at least in part, reverse the protumor effects exerted by CAFs on PCa cell growth and plasticity, both in androgen-sensitive and castration-resistant cell lines. Consistently, the transcriptome of antiarrhythmic-treated CAFs resembles that of tumor-suppressive NPFs. In vivo experiments confirmed that the conditioned medium or the direct coinjection of antiarrhythmic-treated CAFs reduced the tumor growth rate of PCa xenografts.
CONCLUSIONS
Collectively, such data suggest a new therapeutic strategy for PCa based on the repositioning of antiarrhythmic drugs with the aim of normalizing CAF phenotype and creating a less permissive tumor microenvironment.
背景
癌症相关成纤维细胞(CAFs)通过与肿瘤细胞相互作用,在推动前列腺癌(PCa)进展方面发挥着重要作用。之前的基因表达分析显示,与正常前列腺成纤维细胞(NPFs)相比,CAFs 上调了编码电压门控阳离子通道的基因。在这项研究中,我们探讨了抗心律失常药物(已知的阳离子通道抑制剂)对 CAF 激活状态及其与 PCa 细胞相互作用的影响。
方法
通过细胞形态和成纤维细胞激活标志物评估抗心律失常治疗对 CAF 激活表型的影响。通过 3D 凝胶胶原收缩和划痕实验分别评估 CAF 的收缩性和迁移能力。在 CAF-PCa 细胞共培养中,通过评估肿瘤细胞生长和上皮间质转化(EMT)标志物的表达,研究抗心律失常药物对 CAF-PCa 细胞相互作用的干扰能力。通过将 PCa 细胞皮下注射到 SCID 小鼠中和瘤内注射抗心律失常治疗的 CAF 培养基或共注射实验,评估其对体内肿瘤生长的影响,在共注射实验中,将抗心律失常治疗的 CAF 与 PCa 细胞共注射。
结果
激活的成纤维细胞表现出增加的钾、钠和钙通透性,与 mRNA 和蛋白质含量分析一致。抗心律失常药物调节成纤维细胞激活标志物的表达。尽管程度不同,但这些药物还降低了 CAF 的迁移能力,并阻碍了它们重塑细胞外基质的能力,例如通过减少 MMP-2 的释放。此外,条件培养基和共培养实验表明,抗心律失常药物至少部分逆转了 CAF 对 PCa 细胞生长和可塑性的促肿瘤作用,在雄激素敏感和去势抵抗细胞系中均如此。一致地,抗心律失常治疗的 CAF 的转录组类似于肿瘤抑制性 NPFs。体内实验证实,条件培养基或直接注射抗心律失常治疗的 CAF 降低了 PCa 异种移植物的肿瘤生长速度。
结论
总之,这些数据表明了一种基于重新定位抗心律失常药物的新的 PCa 治疗策略,旨在使 CAF 表型正常化并创造一个不太有利的肿瘤微环境。
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