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首页> 外文期刊>World Journal of Surgery: Official Journal of the Societe Internationale de Chirurgie, Collegium Internationale Chirurgiae Digestivae, and of the International Association of Endocrine Surgeons >Reduced neuronal innervation in the distal end of the proximal esophageal atretic segment in cases of esophageal atresia with distal tracheoesophageal fistula.
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Reduced neuronal innervation in the distal end of the proximal esophageal atretic segment in cases of esophageal atresia with distal tracheoesophageal fistula.

机译:食管闭锁伴远端气管食管瘘的情况下,近端食管闭锁段远端的神经支配减少。

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摘要

BACKGROUND: Esophageal dysmotility is a common occurence after surgical repair of proximal esophageal atresia (EA) and distal tracheoesophageal fistula (TEF). The etiology of this motility disorder, however, remains controversial. Esophageal dysmotility also is present in isolated TEF or EA before surgery, suggesting a congenital cause. However, there is no information available in the literature with regard to the intramural nervous system of the human esophagus in EA-TEF. PATIENTS AND METHODS: We examined the distal end of proximal esophageal atretic segment of neonates undergoing EA-TEF repair for intrinsic neuronal innervation. Using specific antibodies, we studied neuronal markers of specimens from nine cases of EA-TEF and 9 cases of normal esophagus by immunohistochemistry using neurofilament (NF), synaptophysin (SY), S100, and glial cell line-derived neurotrophic factor (GDNF). RESULTS: In the atretic segment, specimens staining with hematoxylin and eosin showed that there were marked hypoganglionosis and immature ganglion cells in the myenteric plexus. GDNF immunoreactivity in the atretic esophagus were markedly reduced in both the muscular layer and myenteric plexus. SY and NF-immunorective nerve fibers were distributed throughout the myenteric plexus of the normal esophagus, but the scarcity of these immunoreactive nerve fibers in the atretic esophagus was apparent. In contrast, the density of immunorective nerve fibers for S100 in the myenteric plexus and muscular layer was increased in the distal end of the atretic esophagus. CONCLUSION: We concluded that the distribution of ganglion cells and some nerve fibers in the distal end of the atretic esophageal segment is deficient. Inadequate and abnormal neuronal innervation of the esophagus could be related to the esophageal dysmotility seen in EA. Because GDNF is a survival factor for central and peripheral neurons, defective expression of GDNF could have an important role in the defective and/or abnormal neuronal innervation of atretic esophageal segment.
机译:背景:食管动力障碍是外科手术修复近端食管闭锁(EA)和远端气管食管瘘(TEF)后发生的常见现象。然而,这种运动障碍的病因仍存在争议。术前孤立的TEF或EA中也存在食管动力障碍,提示是先天性病因。然而,在文献中没有关于EA-TEF中人食道的壁内神经系统的信息。患者和方法:我们检查了接受EA-TEF修复的内在神经元神经支配的新生儿近端食管闭锁段的远端。我们使用特异性抗体通过免疫组织化学使用神经丝(NF),突触素(SY),S100和神经胶质细胞源性神经营养因子(GDNF)进行免疫组织化学研究了9例EA-TEF和9例正常食道标本的神经元标记。结果:在心房区,用苏木精和曙红染色标本显示,在肌丛神经中有明显的神经节低下和神经节细胞未成熟。闭锁食管中的GDNF免疫反应性在肌肉层和肌间神经丛中均显着降低。 SY和NF免疫反应性神经纤维分布在正常食道的整个肌间神经丛中,但这些免疫反应性神经纤维在闭锁食道中却很稀缺。相比之下,在肌间神经丛和肌层中S100的免疫整流神经纤维的密度在闭孔食管的远端增加。结论:我们得出结论,闭锁食管段远端神经节细胞和一些神经纤维的分布不足。食管的神经元神经支配不足和异常可能与EA中发现的食管运动障碍有关。因为GDNF是中枢神经和周围神经元的生存因子,所以GDNF的缺陷表达可能在闭锁食管段的神经元神经功能缺损和/或异常中起重要作用。

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