EZH2 and matrix co-regulate phenotype and KCNB2 expression in bladder smooth muscle cells.

IF 1.5 Q3 UROLOGY & NEPHROLOGY American journal of clinical and experimental urology Pub Date : 2023-01-01
Priyank Yadav, Tabina Ahmed, Suejean Park, Martin Sidler, Annette Schröder, Karen J Aitken, Darius Bägli
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Abstract

Background: Partial bladder outlet obstruction (PBO) is a widespread cause of urinary dysfunction and patient discomfort, resulting in immense health care costs. Previously, we found that obstruction is associated with altered regulation of epigenetic machinery and altered function. Here we examined if PBO and chronic bladder obstructive disease (COBD) affect epigenetic marks in a proof of principle gene and explored mechanisms of its epigenetic regulation using in vitro models.

Methods: Archival obstruction tissues from COBD had been created in 200-250 g female Sprague-Dawley rats by surgical ligation of the urethra for 6 weeks, followed by removal of the suture and following animals for 6 more weeks. Obstruction (PBO) is the 6-week ligation only. Sham ligations comprise passing the suture behind the urethra. Histone3 lysine27 trimethylation (H3K27me3) was studied by immunostaining and Chromatin immunoprecipitation (ChIP)/PCR. The interaction of matrix with KCNB2 regulation was studied in human bladder SMC plated on damaged matrix and native collagen and treated with vehicle or UNC1999. Cells were analyzed by immunostaining for cell phenotype, and western blotting for KCNB2, H3K27me3 and EZH2. Effects of conditioned media from these cells were also examined on cell phenotype. siRNA against KCNB2 was examined for effects on cell phenotype and gene expression by RT-qPCR.

Results: H3K27me3 increased by immunofluorescence during PBO, and by ChIP/PCR during COBD in the CpG Island (CGI) as well as 350 bp upstream. Obstruction vs. sham also showed an increase in H3K27me3 deposition. In SMC in vitro, EZH2 inhibition restored KCNB2 expression and partially restored SMC phenotype.

Conclusions: Regulation of KCNB2 at the promoter demonstrated dynamic changes in H3K27me3 during COBD and obstruction. In vitro models suggest that matrix plays a role in regulation of EZH2, H3K27me3 and KCNB2, which may play a role in the regulation of smooth muscle phenotype in vivo.

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EZH2和基质共同调控膀胱平滑肌细胞的表型和KCNB2表达。
背景:部分膀胱出口梗阻(PBO)是泌尿功能障碍和患者不适的普遍原因,导致巨大的医疗费用。先前,我们发现梗阻与表观遗传机制的调节改变和功能改变有关。在这里,我们研究了PBO和慢性膀胱阻塞性疾病(COBD)是否影响一个原理证明基因的表观遗传标记,并利用体外模型探讨了其表观遗传调控机制。方法:取200 ~ 250 g雌性Sprague-Dawley大鼠,结扎尿道6周,拆除缝线,再随访6周,形成COBD的闭塞组织。梗阻(PBO)仅为6周结扎。假结扎包括通过尿道后面的缝合线。通过免疫染色和染色质免疫沉淀(ChIP)/PCR研究组蛋白3赖氨酸27三甲基化(H3K27me3)。研究了基质与KCNB2调控在人膀胱SMC上的相互作用。通过免疫染色检测细胞表型,western blotting检测KCNB2、H3K27me3和EZH2。这些细胞的条件培养基对细胞表型的影响也进行了检测。RT-qPCR检测siRNA对KCNB2细胞表型和基因表达的影响。结果:PBO期间免疫荧光显示H3K27me3升高,COBD期间CpG岛(CGI)及上游350 bp的ChIP/PCR显示H3K27me3升高。梗阻组与假手术组也显示H3K27me3沉积增加。在体外SMC中,EZH2抑制恢复了KCNB2的表达,部分恢复了SMC的表型。结论:在COBD和梗阻期间,KCNB2启动子处的调控显示H3K27me3的动态变化。体外模型显示基质对EZH2、H3K27me3和KCNB2有调控作用,可能在体内对平滑肌表型有调控作用。
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