神经营养因子增强大鼠双侧海绵体神经挤压伤后勃起功能的恢复。
Neurturin enhances the recovery of erectile function following bilateral cavernous nerve crush injury in the rat.
作者信息
Bella Anthony J, Fandel Thomas M, Tantiwongse Kavirach, Brant William O, Klein Robert D, Garcia Carlos A, Lue Tom F
机构信息
Knuppe Molecular Urology Laboratory and Department of Urology, University of California, San Francisco, USA.
Rinat Neuroscience, South San Francisco, USA.
出版信息
J Brachial Plex Peripher Nerve Inj. 2007 Mar 6;2:5. doi: 10.1186/1749-7221-2-5.
BACKGROUND
The molecular mechanisms responsible for the survival and preservation of function for adult parasympathetic ganglion neurons following injury remain incompletely understood. However, advances in the neurobiology of growth factors, neural development, and prevention of cell death have led to a surge of clinical interest for protective and regenerative neuromodulatory strategies, as surgical therapies for prostate, bladder, and colorectal cancers often result in neuronal axotomy and debilitating loss of sexual function or continence. In vitro studies have identified neurturin, a glial cell line-derived neurotrophic factor, as a neuromodulator for pelvic cholinergic neurons. We present the first in vivo report of the effects of neurturin upon the recovery of erectile function following bilateral cavernous nerve crush injury in the rat.
METHODS
In these experiments, groups (n = 8 each) consisted of uninjured controls and animals treated with injection of albumin (blinded crush control group), extended release neurotrophin-4 or neurturin to the site of cavernous nerve crush injury (100 mug per animal). After 5 weeks, recovery of erectile function (treatment effect) was assessed by cavernous nerve electrostimulation and peak aortic pressures were measured. Investigators were unblinded to specific treatments after statistical analyses were completed.
RESULTS
Erectile dysfunction was not observed in the sham group (mean maximal intracavernous pressure [ICP] increase of 117.5 +/- 7.3 cmH2O), whereas nerve injury and albumin treatment (control) produced a significant reduction in ICP elevation of 40.0 +/- 6.3 cmH2O. Neurturin facilitated the preservation of erectile function, with an ICP increase of 55% at 62.0 +/- 9.2 cmH2O (p < 0.05 vs control). Extended release neurotrophin-4 did not significantly enhance recovery of erectile function with an ICP change of 46.9 +/- 9.6. Peak aortic blood pressures did not differ between groups. No significant pre- and post-treatment weight differences were observed between control, neurotrophin-4 and neurturin cohorts. All animals tolerated the five-week treatment course.
CONCLUSION
Treatment with neurturin at the site of cavernous nerve crush injury facilitates recovery of erectile function. Results support further investigation of neurturin as a neuroprotective and/or neuroregenerative agent facilitating functional recovery after cavernous or other pelvic autonomic nerve injuries.
背景
成人副交感神经节神经元损伤后存活及功能保留的分子机制仍未完全明确。然而,生长因子神经生物学、神经发育及细胞死亡预防方面的进展引发了临床对保护性和再生性神经调节策略的浓厚兴趣,因为前列腺癌、膀胱癌和结直肠癌的手术治疗常导致神经元轴突切断,并使性功能或控尿功能严重丧失。体外研究已确定胶质细胞系源性神经营养因子——神经营养素为盆腔胆碱能神经元的一种神经调节剂。我们首次在体内报告了神经营养素对大鼠双侧海绵体神经挤压伤后勃起功能恢复的影响。
方法
在这些实验中,分组(每组n = 8)包括未受伤的对照组以及接受白蛋白注射治疗的动物(盲法挤压对照组)、向海绵体神经挤压伤部位注射缓释神经营养因子-4或神经营养素的动物(每只动物100μg)。5周后,通过海绵体神经电刺激评估勃起功能的恢复情况(治疗效果),并测量主动脉峰值压力。在完成统计分析后,研究人员知晓具体治疗情况。
结果
假手术组未观察到勃起功能障碍(海绵体内平均最大压力[ICP]升高117.5±7.3 cmH₂O),而神经损伤和白蛋白治疗(对照组)使ICP升高显著降低至40.0±6.3 cmH₂O。神经营养素促进了勃起功能的保留,ICP升高至62.0±9.2 cmH₂O,增幅为55%(与对照组相比,p < 0.05)。缓释神经营养因子-4未显著增强勃起功能的恢复,ICP变化为46.9±9.6。各组间主动脉峰值血压无差异。对照组、神经营养因子-4组和神经营养素组在治疗前后体重无显著差异。所有动物均耐受为期5周的治疗过程。
结论
在海绵体神经挤压伤部位用神经营养素治疗可促进勃起功能的恢复。结果支持进一步研究神经营养素作为一种神经保护和/或神经再生剂,以促进海绵体或其他盆腔自主神经损伤后的功能恢复。
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