Bortolini Maria A T, Feitosa Suellen M, Bilhar Andreisa P M, Salerno Gisela G R, Zanoteli Edmar, Simões Manuel J, Castro Rodrigo A
Sector of Urogynecology and Vaginal Surgery, Department of Gynecology, Federal University of São Paulo, Rua Barão do Triunfo, 427 cj 1206, São Paulo, SP, 04602-001, Brazil.
Department of Neurology, Faculty of Medicine, University of São Paulo, São Paulo, Brazil.
Int Urogynecol J. 2019 Mar;30(3):465-476. doi: 10.1007/s00192-018-3634-2. Epub 2018 Mar 21.
An animal model of vaginal distention (VD) was developed to reproduce the acute urethral injury and deficiency underlying stress urinary incontinence (SUI). Data on the chronic effects of urethral trauma and the recovery process are still scarce. We investigated acute, short- and long-term histomorphological and molecular changes in the urethra of rats post 12-h intermittent VD.
We evaluated the urethra of four groups of female rats (n = 72): control without trauma, 1 h, 7 days and 30 days post VD. We compared the gene and protein expression of the VEGF and NGF growth factors, collagens (COL1a1 and COL3a1), desmin, smooth muscle myosin (MYH11), skeletal muscle myosins (MYH1, MYH2 and MYH3) and cell proliferation marker MKi67. We used real-time RT-qPCR, and immunohistochemistry.
Histology showed urethral damage after VD mainly involving the muscular layers. VEGF, NGF, desmin and MKi67 mRNA were significantly upregulated in the urethras of rats 1-h post VD compared with controls (P < 0.05 for all). By 7 days post trauma, COL1a1, MYH11 and MYH3 genes were overexpressed compared with controls (p < 0.05 for all). The COL3a1 protein level was increased by 2.6 times by day 7, while MYH2 protein was significantly decreased (around two times) from 7 to 30 days post VD compared with controls (p < 0.05 for both).
The 12-h intermittent VD causes chronic alterations in the urethra represented by increased COL3a1 and decreased MYH2 protein levels in the long term. The model can potentially be used to study the mechanisms of urethral injury and recovery as well as the physiopathology of SUI.
构建了阴道扩张(VD)动物模型,以再现应激性尿失禁(SUI)潜在的急性尿道损伤和功能缺陷。关于尿道创伤的慢性影响及恢复过程的数据仍然匮乏。我们研究了大鼠在12小时间歇性VD后尿道的急性、短期和长期组织形态学及分子变化。
我们评估了四组雌性大鼠(n = 72)的尿道:未受创伤的对照组、VD后1小时、7天和30天组。我们比较了血管内皮生长因子(VEGF)和神经生长因子(NGF)、胶原蛋白(COL1a1和COL3a1)、结蛋白、平滑肌肌球蛋白(MYH11)、骨骼肌肌球蛋白(MYH1、MYH2和MYH3)以及细胞增殖标志物MKi67的基因和蛋白表达。我们使用了实时逆转录定量聚合酶链反应(RT-qPCR)和免疫组织化学方法。
组织学显示VD后尿道损伤主要累及肌层。与对照组相比,VD后1小时大鼠尿道中VEGF、NGF、结蛋白和MKi67 mRNA显著上调(均P < 0.05)。创伤后7天,与对照组相比,COL1a1、MYH11和MYH3基因过度表达(均p < 0.05)。到第7天,COL3a1蛋白水平增加了2.6倍,而与对照组相比,VD后7至30天MYH2蛋白显著降低(约两倍)(两者均p < 0.05)。
12小时间歇性VD导致尿道长期慢性改变,表现为COL3a1增加和MYH2蛋白水平降低。该模型可潜在地用于研究尿道损伤和恢复机制以及SUI的病理生理学。
