成人盆底痉挛综合征型便秘的分型及其病理生理机制

目的:探讨成人盆底痉挛综合征型便秘的分型及其病理生理机制,以及生物反馈治疗该型便秘的原理.方法:使用基础电路电压为1.53μV的Medtronic公司生产的生物反馈训练仪对18例盆底痉挛综合征型便秘的成人患者首先进行约20min放松练习,肛门塞电极记录到外括约肌的静息电位值,然后患者完成模拟排便动作,获得模拟排便及放松两种状态下外括约肌电位的两组数值,并进行统计学比较.结果:根据肛门外括约肌的静息电位以及模拟排便外括约肌的电位变化,成人盆底痉挛综合征型便秘表现为三种病理分型,即Ⅰ型:高静息电位+矛盾运动(占44.44%),Ⅱ型:高静息电位(占33.33%),Ⅲ型:矛盾运动(占22.22%),其中外括约肌的高静息电位占本组便秘患者的77.77%.各病理分型外括约肌静息电位之间两两比较均具有显著性差异(P=0.001).结论:外括约肌的高静息电位以及在此基础上并发的外括约肌矛盾运动构成了盆底痉挛综合征型便秘的病理生理机制,生物反馈训练能够有效降低外括约肌的静息电位并消除可能出现的外括约肌矛盾运动.

国内外便秘诊治指南比较分析

对国内外'便秘诊治指南'的各自特点进行比较分析。阐述内容包括便秘的概念、发病率、分型及病因分类、诊断方法和治疗4个方面。便秘是一种发病率较高的疾病,老年人和患有其他各种疾病患者发病率更高;便秘分为结肠慢传输型、出口梗阻型和功能性排便障碍型等类型。病因分为功能性疾病、器质性疾病和药物3类。对便秘患者行全面检查有利于了解便秘的病因和分型,以指导精准的治疗;应重视便秘患者的结肠镜检查,易于发现其结直肠息肉和器质性病变。便秘的非手术治疗包括健康教育、饮食的调节、排便习惯的建立、药物的分级应用。结肠慢传输型便秘手术方法包括次全结肠切除盲肠直肠吻合术、全结肠切除回肠直肠吻合术、结肠旷置术、回肠造口术。对于出口梗阻型便秘中的直肠内脱垂,目前国外多采用腹腔镜腹侧补片直肠悬吊术;直肠前突手术方法包括经阴道和经肛手术。

胃肠道传输时间对便秘诊断的临床意义

目的探讨胃肠传输时间对便秘诊断的临床意义。方法 (1)对20名正常组人群和80名便秘组患者口服不透光X线标志物法进行观察,即标志物在胃肠中的传输时间及各段时间内残留标志物数目。(2)不透光标志物在消化道传输的过程中,根据标志物在某一肠段处长时间停滞不前或分散面广泛,结合病史分析将便秘分为4型:①全结肠慢传输型;②出口梗阻型;③左结肠缓慢型;④右结肠缓慢型。(3)80例便秘患者与20例对照者患者,标记物在肠道内通过各段时间比较。结果便秘组标志物通过结直肠时间较对照组明显延长,两组比较差异有统计学意义(P<0.05)。便秘组在12h、24h、48h、72h各时间段肠内残留标记物数目明显多于对照组,两组比较差异有统计学意义(P<0.01)。结论便秘病因分型为临床提供客观的诊疗依据。

Proteomic analysis of down-regulated proteins in colonic mucosa of chronic slow transit constipation rats

Objective： To investigate the alternations of proteins in the colonic mucosa of chronic slow transit constipation （STC） rats with a 2-DE-based proteomic method and analyze the function of these down-regulated proteins so as to provide theoretical basis for the pathogenesis of intestinal mucosa of chronic STC rats. Methods： STC model was established by feeding rats with 8 mg/（kg＇d） diphenoxylate for 120 d. An experimental model of chronic STC rat was used for separation of proteomics from colonic mucosa using two-dimensional electrophoresis （2-DE）. Proteins altered in expressional level were identified by Image Master 2DElite, mass spectrometry, and bibliometrics were applied to identify the differential protein expression and their clinical s observed in the pathogenesis lgn of ificance and function were analyzed. Results： Obvious differential protein expression was STC, including mast cell protease （A1）, non-specific dipeptidase （A2） and chondrosome succinate dehydrogenase precursor （A3）. The expressions of A1, A2 and A3 were down-regulated in the gel graph of STC rats Conclusion： The down-regulation of chondrosome succinate dehydrogenase, mast cell protease as well as non-specific dipeptidase in rat colon suggests the functional impairment of the oxidoreduction of mitochondrion is very important in the genesis and development of STC. The immunological reaction of STC rats is weakened, and the function of digesting and absorbing protein may be damaged to some extent.