食管静脉曲张套扎术和口服普萘洛尔治疗肝硬化食管静脉曲张的疗效对比

目的:观察食管静脉曲张套扎术(endoscopic variceal ligation,EVL)和口服普萘洛尔治疗肝硬化食管静脉曲张(esophagealvarices,EV)的临床疗效对比.方法:对140例临床诊断为肝硬化EV患者进行分组疗效观察,观察组治疗为EVL,对照组为口服普萘洛尔.观察两组患者的疗效及不良反应情况.结果:经过18-36 mo的临床随访,对照组共有22.86%的患者发生出血,观察组为20.0%,2组差异无统计学意义(P>0.05).总死亡率与出血相关死亡率,对照组为22.86%、11.43%,观察组为17.14%、8.57%,两组差异无统计学意义(P>0.05).观察组有20.0%的患者出现不良反应,明显低于对照组的51.43%,两组差异有统计学意义(P<0.05).结论:EVL与普萘洛尔在治疗肝硬化EV患者中均有良好的疗效,可以有效预防出血.但普萘洛尔不良反应较EVL少,且未进行侵入性操作,因此值得临床应用.

内镜干预及联合普萘洛尔预防食管静脉曲张破裂再出血的疗效

目的:对比评估内镜下套扎或硬化剂治疗与内镜治疗联合普萘洛尔对预防食管静脉曲张破裂再出血的疗效.方法:将69例肝硬化患者随机分为2组,即单纯内镜治疗组(套扎或硬化剂治疗)40例和联合治疗组(套扎或硬化剂治疗后服用普萘洛尔)29例.随访1年以上并评估治疗后再出血情况、死亡率及再出血相关死亡率,并根据日本门脉高压协会诊断标准评估两种治疗方法对内镜下食管曲张静脉外观特征的影响.结果:治疗前后2组患者肝功能、血常规、电解质无显著差异.单纯内镜治疗后食管曲张静脉的直径显著减小(治疗前vs治疗后,10.92±2.91vs8.45±2.26,P<0.05),联合治疗组曲张静脉直径虽减小但不具有统计学意义(治疗前vs治疗后,10.14±2.46vs8.95±2.21,P>0.05).治疗后联合治疗组曲张静脉近端距门齿距离明显下移(治疗前vs治疗后,22.79±2.83vs24.85±3.96,P<0.05),且曲张静脉表面红色征较治疗前明显减少(治疗前vs治疗后,100%vs76.19%,P<0.05).与单纯内镜治疗组相比,联合治疗组胃底静脉曲张(治疗前vs治疗后,10.34%vs28.10%,P<0.05)及门脉高压性胃病的发生率均高于治疗前(治疗前vs治疗后,10.34%vs42.86%,P<0.05).2组曲张静脉形态均主要由串珠状转变为蚯蚓状,且均具有统计学意义(P<0.05).2组间再出血率(单纯内镜治疗组vs联合治疗组,50.00%vs51.71%,P>0.05)无统计学差异,但联合治疗组患者死亡率显著低于单纯内镜治疗组(联合治疗组vs单纯内镜治疗组,7.41%vs27.50%,P<0.05),且2组患者主要的死因为上消化道再出血.结论:内镜治疗后联合普萘洛尔预防食管静脉曲张破裂再出血在一定程度上可以降低患者死亡风险、减少内镜下曲张静脉高危再出血因素.

Myocardial Protection with Beta Blocker Treatment in Infants with Heart Failure Due to Congenital Heart Defects and Duchenne Muscular Dystrophy

Our first intention to treat infants’ heart failure with beta blockers was to improve the clinical condition as shown in our prospective randomized trial. We only use non-selective beta blockers in these infants, carvedilol in those with left ventricular dysfunction and propranolol in those with congenital heart disease without ventricular dysfunction. Despite a significant improvement of Ross’s heart failure score, we could not convince most colleagues within the last 25 years if the concept of neurohumoral activation in heart failure is not well-established pediatric cardiology. Recently, Honghai Liu et al. published that cardiomyocyte cytokinesis failure was increased in congenital heart disease. Inactivation of the beta adreno receptors genes and administration of the beta-blocker propranolol increased cardiomyocyte division in neonatal mice, which increased the number of cardiomyocytes (endowment) and conferred benefit after myocardial infarction in adults. We currently realize that propranolol in infants with congenital heart disease not only decrease highly elevated NT-Pro-BNP values but also decrease cardiac troponin T values that may indicate myocardial injury due to neurohumoral activation. We reproduce this observation, primarily seen in infants with congenital heart disease, in an infant with Duchenne muscular dystrophy. These observations were in good accordance with current data from H. Liu et al., who showed that treatment with non-selective beta blockers early after birth might rescue cytokinesis defects and prevent heart dysfunction in adulthood in a mouse model.