Increased COX-1 expression in benign prostate epithelial cells is triggered by mitochondrial dysfunction.

IF 1.5 Q3 UROLOGY & NEPHROLOGY American journal of clinical and experimental urology Pub Date : 2022-08-15 eCollection Date: 2022-01-01
Chandler N Hudson, Kai He, Laura E Pascal, Teresa Liu, Livianna K Myklebust, Rajiv Dhir, Pooja Srivastava, Naoki Yoshimura, Zhou Wang, William A Ricke, Donald B DeFranco
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Abstract

Background: Prostatic inflammation is closely linked to the development and progression of benign prostatic hyperplasia (BPH). Clinical studies of non-steroidal anti-inflammatory drugs, which inhibit cyclooxygenase-2 (COX-2), targeting prostate inflammation patients with symptomatic BPH have demonstrated conflicting results, with some studies demonstrating symptom improvement and others showing no impact. Thus, understanding the role of the cyclooxygenases in BPH and prostatic inflammation is important.

Methods: The expression of COX-1 was analyzed in a cohort of donors and BPH patients by immunohistochemistry and compared to previously determined characteristics for this same cohort. The impact of mitochondrial dysfunction on COX-1 and COX-2 was determined in experiments treating human benign prostate epithelial cell lines BPH-1 and RWPE-1 with rotenone and MitoQ. RWPE-1 cells were transfected with small interfering RNA specific to complex 1 gene NDUFS3.

Results: COX-1 expression was increased in the epithelial cells of BPH specimens compared to young healthy organ donor and normal prostate adjacent to BPH and frequently co-occurred with COX-2 alteration in BPH patients. COX-1 immunostaining was associated with the presence of CD8+ cytotoxic T-cells, but was not associated with age, prostate size, COX-2 or the presence of CD4+, CD20+ or CD68+ inflammatory cells. In cell line studies, COX protein levels were elevated following treatment with inhibitors of mitochondrial function. MitoQ significantly decreased mitochondrial membrane potential in RWPE-1 cells. Knockdown of NDUFS3 stimulated COX-1 expression.

Conclusion: Our findings suggest COX-1 is elevated in BPH epithelial cells and is associated with increased presence of CD8+ cytotoxic T-cells. COX-1 can be induced in benign prostate epithelial cells in response to mitochondrial complex I inhibition, and knockdown of the complex 1 protein NDUFS3. COX-1 and mitochondrial dysfunction may play more of a role than previously recognized in the development of age-related benign prostatic disease.

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良性前列腺上皮细胞中 COX-1 表达的增加是由线粒体功能障碍引发的。
背景:前列腺炎症与良性前列腺增生症(BPH)的发生和发展密切相关。针对有症状的良性前列腺增生症患者的前列腺炎症,非甾体抗炎药物(可抑制环氧化酶 2 (COX-2))的临床研究显示了相互矛盾的结果,一些研究显示症状有所改善,而另一些研究则显示没有影响。因此,了解环氧化酶在良性前列腺增生症和前列腺炎症中的作用非常重要:方法:通过免疫组化方法分析了一组供体和良性前列腺增生症患者体内 COX-1 的表达情况,并与之前确定的同一组群的特征进行了比较。在用鱼藤酮和 MitoQ 处理人类良性前列腺上皮细胞系 BPH-1 和 RWPE-1 的实验中,确定了线粒体功能障碍对 COX-1 和 COX-2 的影响。用特异性复合体 1 基因 NDUFS3 的小干扰 RNA 转染 RWPE-1 细胞:结果:与年轻的健康器官捐献者和与良性前列腺增生相邻的正常前列腺相比,COX-1 在良性前列腺增生症标本上皮细胞中的表达增加,而且在良性前列腺增生症患者中经常与 COX-2 改变同时存在。COX-1 免疫染色与 CD8+ 细胞毒性 T 细胞的存在有关,但与年龄、前列腺大小、COX-2 或 CD4+、CD20+ 或 CD68+ 炎症细胞的存在无关。在细胞系研究中,线粒体功能抑制剂治疗后 COX 蛋白水平升高。MitoQ 能明显降低 RWPE-1 细胞的线粒体膜电位。敲除 NDUFS3 可刺激 COX-1 的表达:我们的研究结果表明,COX-1在良性前列腺增生上皮细胞中升高,并与CD8+细胞毒性T细胞的增加有关。线粒体复合体 I 抑制和复合体 1 蛋白 NDUFS3 的敲除可诱导良性前列腺上皮细胞中的 COX-1。COX-1和线粒体功能障碍在与年龄相关的良性前列腺疾病的发生中可能扮演着比以前认识到的更重要的角色。
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