神经节苷脂相关吉兰巴雷综合征病例的回顾性分析

目的:了解单唾液酸四己糖神经节苷脂(GM1)相关吉兰巴雷综合征的发生与特点,为临床安全用药提供参考。方法:收集某院静注GM1注射液致吉兰巴雷综合征病例,同时检索中文期刊数据库中GM1相关吉兰巴雷综合征的个案报道,合并文献病例与院内病例,回顾性统计分析患者性别、年龄、原患疾病、基础疾病、前驱感染史、用药剂量及疗程、合并用药、不良反应起始症状、主要表现、双侧腱反射减弱或消失情况、发生时间、疾病平均达峰时间、实验室检查、严重程度、治疗和转归等项目。结果:收集院内病例5例,文献检索获得病例17例,合计入选病例22例,其中男21例,女1例,50~60岁患者占50.00%。GM1相关吉兰巴雷综合征多发生于脑出血、脑梗死及脑外伤患者;31.82%的患者有自身免疫相关性疾病。GM1的剂量、疗程与不良反应严重程度无明确相关性。GM1相关吉兰巴雷综合征多以肌力及肌张力下降起病,所有病例均以四肢无力为主要表现,且大多合并颅神经受累、意识障碍、自主神经功能障碍、感觉及呼吸功能异常。不良反应多在8~14 d出现,1~3 d达峰;所致肢体瘫痪程度较重,临床结局较差。结论:GM1可能导致吉兰巴雷综合征,临床应用时应严格把握用药指征,用药时加强用药监护,确诊吉兰巴雷综合征后应及时停药并应用静注人免疫球蛋白,避免不良反应的进一步加重。

缬沙坦氨氯地平片联合辛伐他汀治疗老年高血压合并血脂异常患者的疗效及血清学变化分析

目的探讨缬沙坦氨氯地平片联合辛伐他汀对老年高血压合并血脂异常患者疗效及血清学变化分析。方法选取2018年2月至2019年6月本院收治的老年高血压合并血脂异常患者142例,按照随机数字表法分为试验组和对照组,其中对照组采用缬沙坦氨氯地平片,试验组采用缬沙坦氨氯地平片联合辛伐他汀,每组各71例,比较两组患者的临床治疗效果、血脂指标、血压情况及并发症发生情况。结果试验组总有效率为95.77%,高于对照组的81.69%,差异有统计学意义(P<0.05)。两组患者治疗前TG、TC、LDL-C和HDL-C比较,差异无统计学意义(P>0.05);治疗后试验组明显优于对照组,差异有统计学意义(P<0.05)。治疗前两组舒张压及收缩压比较,差异无统计学意义(P>0.05);治疗后两组均有明显改善,且试验组优于对照组,差异有统计学意义(P<0.05);试验组患者血压恢复正常的时间短于对照组,差异有统计学意义(P<0.05)。试验组并发症总发生率为5.63%,对照组为8.45%,差异无统计学意义(P>0.05)。结论缬沙坦氨氯地平片联合辛伐他汀在治疗老年高血压合并血脂异常患者中具有较好的临床疗效,可以降低血压、改善血脂指标,且安全性较好,值得临床推广。

miR-210 over-expression enhances mesenchymal stem cell survival in an oxidative stress environment through antioxidation and c-Met pathway activation

microRNA-210(miR-210)has generally been reported to be associated with cell survival under hypoxia.However,there are few data regarding the role of miR-210 in the survival of mesenchymal stem cells(MSCs)under oxidative stress conditions.Thus,we sought to investigate whether miR-210 over-expression could protect MSCs against oxidative stress injury and what the primary mechanisms involved are.The results showed that over-expression of miR-210 significantly reduced the apoptosis of MSCs under oxidative stress,accompanied by obvious increases in cell viability and superoxide dismutase activity and remarkable decreases in malonaldehyde content and reactive oxygen species production,resulting in a noticeable reduction of apoptotic indices when compared with the control.Moreover,the above beneficial effects of miR-210 could be significantly reduced by c-Met pathway repression.Collectively,these results showed that miR-210 over-expression improved MSC survival under oxidative stress through antioxidation and c-Met pathway activation,indicating the potential development of a novel approach to enhance the efficacy of MSC-based therapy for injured myocardium.