Mechanism of the protective effect of ABT-263 on upper urinary tract damage by alleviating neurogenic bladder fibrosis

Wen Y1, He X1, Song Y1, Lu W2, Wen J1

Research Type

Pure and Applied Science / Translational

Abstract Category

Neurourology

Abstract 145
Research Methods, Models and Techniques in Applied and Pure Science
Scientific Podium Short Oral Session 18
Thursday 28th September 2023
11:30 - 11:37
Room 104CD
Animal Study Cell Culture Pharmacology Urodynamics Techniques
1. Department of Urology, Pediatric Urodynamic Center and the International Key Pediatric Urodynamic Laboratory of Henan Province, The First Affiliated Hospital of Zhengzhou University, 2. Xinyang Central Hospital of Zhengzhou University
Presenter
Links

Abstract

Hypothesis / aims of study
This study investigated the mechanism of ABT-263 in the treatment of neurogenic bladder fibrosis (NBF) and its protective effects against upper urinary tract damage (UUTD).
Study design, materials and methods
Neurogenic bladder (NB) refers to the dysfunction of lower urinary tract storage and urination due to damage to the central or peripheral nervous system, resulting in a series of lower urinary tract symptoms (LUTS) and complications [1]. So far, there are no good treatments to solve this disease. ABT-263 is a known BH3 mimetic drug which can prevent and reverse the progression of fibrotic diseases and myofibroblast apoptosis. Studies have shown that ABT-263 can alleviate the progression of skin fibrosis, pulmonary fibrosis, biliary fibrosis, and myocardial fibrosis by promoting myofibroblast apoptosis [2]. However, there are no reports on the therapeutic effect of ABT-263 in NBF, especially in severe NBF with UUTD. Therefore, this study explores the function and mechanism of ABT-263 in the treatment of NBF. Sixty 12-week-old SD rats were randomly divided into sham, sham + ABT-263 (50 mg/kg), NBF, NBF + ABT-263 (25 mg/kg, oral gavage), and NBF + ABT-263 (50 mg/kg, oral gavage) groups. After cystometry, bladder and kidney tissue samples were collected for hematoxylin and eosin (HE), Masson, and Sirius red staining, and WB and qPCR detection. Primary rat bladder fibroblasts were isolated, extracted, and cultured. After co-stimulation with TGF-β1 (10 ng/mL) and ABT-263 (concentrations of 0, 0.1, 1, 10, and 100 µmol/L) for 24 h, cells were collected. Cell apoptosis was detected using CCK8, WB, immunofluorescence, and annexin/PI assays.
Results
ABT-263 treatment can alleviate neurogenic hydronephrosis, improved the kidney morphology, reduce bladder fibrosis and improve the bladder function of NBF rats. Compared with the sham group, there was no significant difference in any physical parameters in the sham + ABT-263 (50 mg/kg) group. Compared with the NBF group, most of the markers involved in fibrosis were improved in the NBF + ABT-263 (25 mg/kg) and NBF + ABT-263 (50 mg/kg) groups, while the NBF + ABT-263 (50 mg/kg) group showed a significant improvement. Compared with the TGFβ1 group, when the concentration of ABT-263 increased to 10 umol/L, the cell viability of primary bladder fibroblasts began to decrease, the apoptosis rate increased, the fluorescence intensity of red fluorescent α-SMA decreased, and the protein expression of Cytoc and cleaved caspase-3 began to increase in cell culture.
Meanwhile, when the concentration of ABT-263 was increased to 10 µmol/L, the apoptosis rate of primary bladder fibroblasts increased, and the expression of the anti-apoptotic protein BCL-xL began to decrease.
Interpretation of results
ABT-263 may promote the apoptosis of bladder fibroblasts through apoptosis pathway and relieve related NBF symptoms.
Concluding message
ABT-263 may plays an important role in relieving alleviating neurogenic bladder fibrosis and protecting bladder and kidney function.
Figure 1
References
  1. Stein R, Bogaert G, Dogan HS, et al. EAU/ESPU guidelines on the management of neurogenic bladder in children and adolescent part I diagnostics and conservative treatment. Neurourol Urodyn. 2020;39(1):45–57.
Disclosures
Funding National Natural Science Foundation of China (U1904208) Clinical Trial No Subjects Animal Species rats Ethics Committee the Zhengzhou University Ethics Committee for Care and Use of Laboratory Animals
Citation

Continence 7S1 (2023) 100863
DOI: 10.1016/j.cont.2023.100863

25/11/2024 00:54:14