《中医治未病实践指南·鼻鼽》临床一致性评价研究

张家港市中医医院作为课题协作单位,参加了国家中医药管理局课题《中医治未病实践指南·鼻鼽》临床一致性评价工作,评价结果提示该指南基本符合临床实际。本文从"中、西医诊断明确,英文翻译可斟酌""鼻鼽缓解期定义难,辨体质干预创新意""充分发挥中医治未病特色优势,提高患者满意度"三方面总结了此次临床评价体会。

以临床用药一致性为依据的枳壳标准汤剂制备工艺及含量测定

依据临床用药一致性原则制备枳壳标准汤剂,研究枳壳标准汤剂的制备工艺及含量测定方法。选择同一批枳壳饮片,分别对煎煮的容器、饮片浸泡时间、溶剂用量、煎煮时间及次数等参数进行研究,同时制备3批标准汤剂,采用LC MS法测定枳壳标准汤剂中6种成分的含量。研究初步确定了枳壳标准汤剂制备的工艺参数:容器选择陶瓷药罐,饮片浸泡60 min;第一煎加10倍水,煎煮30 min;第二煎加8倍水,煎煮20 min。结果表明:柚皮苷、新橙皮苷、芸香柚皮苷、橙皮苷、水合橙皮内酯和川陈皮素的平均含量分别为165.98、86.03、29.64、10.74、3.73和10.67μg/g。本研究建立了枳壳标准汤剂的提取工艺,为以临床用药一致性为基础的标准汤剂研究提供了理论基础和科学依据。

《中医儿科临床诊疗指南·小儿口疮(修订)》的临床一致性评价

目的评价《中医儿科临床诊疗指南·小儿口疮(修订)》的临床一致性,为指南修订提供参考。方法按照国家中医药管理局中医诊疗指南临床应用评价实施方案要求,由全国13家三级甲等医院采用前瞻性和回顾性病例调查分析方法,完成小儿口疮病例信息采集,填写中医诊疗指南一致性测试表(病例调查表),评价临床病例在诊断、辨证分型、治则、汤药、中成药、其他疗法、预防调摄方面与指南的一致性。结果所收集的254例有效病例临床资料与指南比较,在中医诊断(总体一致率100%)、中医诊断依据(99.22%)、西医诊断(99.61%)、西医诊断依据(99.61%)、中医辨证分型(98.03%)、证候诊断依据(98.42%)、治则(98.01%)、预防调摄(98.02%)方面一致性较高,方药组成及用法(85.92%)、中成药(87.28%)用法一致性略低,其他疗法(62.5%)的一致性较低。结论该指南临床一致性较好,符合临床实践。

红外定位系统(OPS)辅助摆位新技术在肝癌放疗中的应用

目的:研究红外定位系统(optical positioning system,OPS)辅助摆位新技术在肝癌放射治疗中对摆位误差的影响及其在肝癌精确放疗中的应用价值。方法:本研究选取30例肝癌患者,均应用OPS技术辅助摆位。将CBCT扫描作为标准,比较OPS技术和室内激光系统(十字线)在X(左右)、Y(头脚)、Z(面背)三个方向的线性误差;并根据摆位误差折线图分别计算出OPS和十字线的临床摆位一致性百分比。结果:通过OPS摆位在X、Y、Z方向上的摆位误差分别为(2.74±1.27)mm、(3.45±1.17)mm、(2.85±1.11)mm;通过十字线摆位在X、Y、Z方向上的摆位误差分别为(4.37±1.45)mm、(5.79±1.52)mm、(4.27±1.55)mm,各方向对应的P均<0.001。以±5 mm为标准,OPS在三个方向上的临床一致性分别为96.7%、90.0%、98.7%;十字线在三个方向上的临床一致性分别为68.0%、32.7%、72.7%。结论:OPS在肝癌放射治疗定位摆位方面非常有效。作为一种无辐射、低成本、简便快捷的定摆位新技术,OPS比室内激光系统更能提高整体的摆位精度。

他克莫司胶囊在健康人体内药动学一致性的预评估

目的:建立人全血中他克莫司浓度的LC-MS/MS测定法,并用于他克莫司胶囊受试或参比药物在中国健康男性中单剂量空腹给药的一致性预评估。方法:采用单剂量给药,四周期、双序列、完全重复交叉、参比药物校正的平均生物等效性实验(RSABE)设计,12名健康受试者单剂量交叉口服1 mg他克莫司胶囊受试或参比药物后,0~120 h内间隔取血,对全血提取富集后测定他克莫司血药浓度,用WinNonlin7.0软件计算药动学参数并进行一致性预评估。结果:2次服用参比药物后主要药动学参数Cmax、AUC0-τ、AUC0-∞个体内标准差均>0.294,用RSABE的判断标准,参比药物与受试药物主要药代动力学参数Cmax、AUC0-τ、AUC0-∞的单侧95%置信区间上限(critbound)≤0,几何均数比值(GMR)点估计值(pointest)不超过0.80~1.25。故可以判定他克莫司胶囊受试与参比药物具有生物等效应。结论:建立的LC-MS/MS法准确灵敏度高,可用于他克莫司胶囊的药代动力学研究和临床一致性的评价。

Pharmacokinetic and pharmacodynamic comparison between Glucophage~? and a generic metformin in a rat model

In the present study, we aimed to compare the pharmacokinetics and pharmacodynamics between Glucophage~? and a generic metformin formulation in a diabetic rat model in order to assess the bioequivalence of the generic formulation. Adult male Zucker diabetes fatty rats received Glucophage~? or the generic metformin through gastric gavage at a dose of 180 mg/kg(n = 6 per condition). Both pharmacokinetic parameters(AUC0–t, AUC0–∞, Cmax) of metformin and plasma glucose levels were compared between the two groups. For pharmacodynamics, rats received Glucophage~? or the generic metformin at doses of 180 and 300 mg·kg–1·d–1 for 6 weeks. The measurements included body weight, fasting plasma glucose, glycosylated serum protein(GSP) and serum insulin. Data were analyzed with SPSS 22.0 and Prism 7. The level of statistical significance was set at P<0.05. In single dosing experiments, pharmacokinetic parameters(t1/2, AUC0–t and Cmax) did not differ between Glucophage~? and the generic metformin(P>0.05). However, plasma glucose was significantly higher in the generic metformin group at 2 h(P = 0.03) and 4 h(P = 0.04) after drug treatment. In repeated dosing experiments, fasting glucose, HOMA-IR and body weight in rats receiving high-dose Glucophage~? were significantly lower at the end of the 6-week treatment period than those in rats receiving high-dose generic metformin(P<0.05 for all). GSP and serum insulin did not differ significantly between the two groups. In rats receiving low-dose metformin, fasting glucose was lower in the Glucophage~? group. HOMA-IR and body weight did not differ between the two groups. Moreover, blood lipids did not differ significantly between the two groups. The generic metformin used in the current study did not differ significantly in pharmacokinetic characteristics with Glucophage~?. However, Glucophage~? was superior in terms of glucose control, body weight loss and insulin sensitivity in repeated administration.