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首页> 外文期刊>Neurourology and urodynamics. >TGF‐β1 and connexin‐43 expression in neurogenic bladder from rats with sacral spinal cord injury
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TGF‐β1 and connexin‐43 expression in neurogenic bladder from rats with sacral spinal cord injury

机译:来自骶骨脊髓损伤大鼠神经源性膀胱的TGF-β1和Connexin-43表达

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Aims Sacral spinal cord injury (SCI) could induce underactive bladder (UAB). Malfunction of connexin 43 (CX43) regulated by TGF‐β1 might involve in urinary bladder dysfunction. We studied the changes of CX43 and TGF‐β1/Smad3 signaling in detrusor of neurogenic bladder (NB) in sacral SCI rats. Methods Sacral SCI was produced by hemisection (SSCH) or transection (SSCT) of spinal cord between L4 and L5 in female Wistar rats. BBB scores, residual urine volume and bladder weight as well as characteristic cystometric parameters at 6th week were used to confirm the successful establishment of NB. Western blotting and qRT‐PCR were used to exam the protein and mRNA expression levels of CX43, CX45, TGF‐β1, and Smad3 in detrusor. Results BBB scores were significantly decreased, with the lowest in SSCT rats ( P? ?0.01). The residual urine volume, mean bladder weight, and cystometric parameters were increased, with the highest in SSCT rats. CX43 and phospho‐CX43 protein levels were significantly decreased, but those of TGF‐β1, Smad3, and phospho‐Smad3 were significantly increased. It was the protein and mRNA levels of CX43 but not those of CX45 which were decreased in negative accordance with those of TGF‐β1 and Smad3. Those changes were more significant in SSCT than in SSCH rats. Conclusions This study indicates that voiding dysfunction is related to the decreased CX43 function in detrusor from NB. TGF‐β1/Smad3 signaling might be involved in the down‐regulation of CX43 in SCI rats. Early regulation of CX43 might be beneficial to patients with voiding dysfunction.
机译:目标骶骨脊髓损伤(SCI)可以诱导不良膀胱(UAB)。 TGF-β1调节的Connexin 43(CX43)的故障可能涉及膀胱功能障碍。我们研究了骶骨菌大鼠神经源性膀胱(NB)排尿中CX43和TGF-β1/ Smad3信号传导的变化。方法在雌性Wistar大鼠的L4和L5之间的脊髓的半联(SSCH)或横截面(SSCT)产生SachraLSCI。使用BBB分数,残留的尿量和膀胱重量以及第6周的特征囊曲线参数来证实Nb的成功建立。 Western Blotting和QRT-PCR用于检查逼尿肌中CX43,CX45,TGF-β1和Smad3的蛋白质和mRNA表达水平。结果BBB评分显着降低,SSCT大鼠中最低(P≤≤0.01)。剩余尿量,平均膀胱重量和胱术参数增加,SSCT大鼠中最高。 CX43和磷酸-CX43蛋白质水平显着降低,但TGF-β1,Smad3和磷酸 - Smad3的蛋白质水平显着增加。它是CX43的蛋白质和mRNA水平,但不是CX45的CX45,这根据TGF-β1和SMAD3的负数降低。这些变化在SSCT比SSCH大鼠中更重要。结论本研究表明,排尿功能障碍与来自NB的逼尿器中的CX43功能下降有关。 TGF-β1/ SMAD3信号可能涉及SCI大鼠CX43的下调。 CX43的早期调节可能对患有功能障碍的患者有益。

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