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首页> 外文期刊>Scientific reports. >Downregulation of WNT11 is associated with bladder tissue fibrosis in patients with interstitial cystitis/bladder pain syndrome without Hunner lesion
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Downregulation of WNT11 is associated with bladder tissue fibrosis in patients with interstitial cystitis/bladder pain syndrome without Hunner lesion

机译:WNT11的下调与无亨纳病灶的间质性膀胱炎/膀胱疼痛综合征患者的膀胱组织纤维化有关

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This study assessed the functional role of WNT genes and the association between WNT signalling cascades and fibrosis in interstitial cystitis/bladder pain syndrome (IC/BPS) patients. Twenty-five patients (3 males, 22 females; mean age 59.7?±?10.9 years), included 7 non-Hunner-type IC (NHIC), 18 Hunner-type IC (HIC), and 5 non-IC (control) groups. The expression of sonic hedgehog, WNT gene family, and genes previously reported as biomarkers for IC/BPS were examined using RT-PCR in biopsy specimens from the mucosa and submucosa layer of the bladder. WNT2B, WNT5A, WNT10A, and WNT11 functions in the urothelium were evaluated by silencing in an HBlEpC cell line. Pelvic Pain and Urgency/Frequency Patient Symptom Scale scores, O’Leary-Sant Symptom and Problem Index scores, and Visual Analogue Scores did not differ between the NHIC and HIC groups. However, HIC patients had significantly shorter symptom duration (30.9 vs 70.8 months, p?=?0.046), higher daily urinary frequency (16.1 versus 8.5 times, p?=?0.006), and smaller bladder capacity (208.6 versus 361.4?ml, p?=?0.006) than NHIC patients. Overall WNT gene expression was lower in NHIC than HIC patients. Bladder epithelial tissues from HIC patients were characterised by the downregulation of WNT11. Silencing of WNT11, WNT2B, WNT5A, and WNT10A in HBlEpCs resulted in fibrotic changes, indicated by fibrotic morphology, increased fibrosis-related gene expression, and nuclear localisation of phosphorylated SMAD2, and increased vimentin and fibronectin levels. Downregulation of WNT11 results in fibrotic changes of bladder epithelial cells and is associated with the pathogenesis and differential diagnosis of NHIC. Decreased expression of WNT11 is a potential biomarker for predicting NHIC.
机译:这项研究评估了间质性膀胱炎/膀胱疼痛综合征(IC / BPS)患者中WNT基因的功能作用以及WNT信号级联和纤维化之间的关联。 25例患者(男3例,女22例;平均年龄59.7±10.9岁),包括7例非亨氏型IC(NHIC),18例亨氏型IC(HIC)和5例非IC(对照)组。使用RT-PCR在膀胱粘膜和粘膜下层的活检标本中检查了声波刺猬,WNT基因家族和先前报道为IC / BPS生物标志物的基因的表达。通过在HB1EpC细胞系中沉默来评估尿路上皮中的WNT2B,WNT5A,WNT10A和WNT11功能。 NHIC和HIC组之间的骨盆疼痛和紧急/频率患者症状量表评分,O'Leary-Sant症状和问题指数评分以及视觉类似物评分没有差异。然而,HIC患者的症状持续时间显着缩短(30.9 vs. 70.8个月,p?=?0.046),每日尿频较高(16.1 vs 8.5倍,p?=?0.006),膀胱容量较小(208.6 vs 361.4?ml, p?=?0.006)。 NHIC患者的整体WNT基因表达水平低于HIC患者。 HIC患者的膀胱上皮组织的特征在于WNT11的下调。 HBlEpCs中WNT11,WNT2B,WNT5A和WNT10A的沉默导致纤维化改变,表现为纤维化形态,纤维化相关基因表达增加,磷酸化SMAD2的核定位以及波形蛋白和纤连蛋白水平的升高。 WNT11的下调导致膀胱上皮细胞的纤维化变化,并与NHIC的发病机理和鉴别诊断有关。 WNT11表达降低是预测NHIC的潜在生物标志物。

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