Pharmacokinetics of Controlled Release and Immediate Release Morphine Sulphate Tablets after a Single Dose and Multiple Doses in Chinese Volunteers

健康志愿者１０名，随机交叉口服硫酸吗啡控释片（ＣＲＭＳ）３０ｍｇ（３０ｍｇ×１）和硫酸吗啡普通片（ＩＲＭＳ）２０ｍｇ（１０ｍｇ×２），分别于服药前后各时点取静脉血，用ＧＣＭＳ测定血浆中吗啡含量。以药代软件程序处理，分别求得ＣＲＭＳ和ＩＲＭＳ的Ｃｍａｘ为１９．３８±３．８０和２１．２７±６．２１ｎｇ／ｍｌ；ｔｍａｘ为２．３６±０．３７ｈ和０．５５±０．１６ｈ；ｔ１／２β为３．５３±０．８７ｈ和３．０３±０．７４ｈ，曲线下面积ＡＵＣ为１４５．１５±１７．６５和９３．０８±１６．６５ｎｇ·ｈ／ｍｌ。癌症病人多次口服硫酸吗啡至稳态，ＣＲＭＳ和ＩＲＭＳ的峰浓度分别为２７．４３±０．３３ｎｇ／ｍｌ，２２．６８±０．１６ｎｇ／ｍｌ；谷浓度分别为１９．４５±１．４４ｎｇ／ｍｌ；１８．１４±０．４９ｎｇ／ｍｌ。

Preparation and <i>in Vitro</i>Drug Release Evaluation of Once-Daily Metformin Hydrochloride Sustained-Release Tablets

The objective of this study was to develop once-daily metformin hydrochloride sustained-release tablets (MHSRT) and evaluate their in vitro release behavior. MHSRT were prepared by the film coating method. The in vitro drug release rate of MHSRT and the commercial tablets Fortamet? made in the United States of America in water was fitted with zero order kinetic equation, and Ritger-Peppas kinetic equation in 0.1 M HCl and pH 6.8-phosphate buffer, respectively. The similarity factor f2 values of MHSRT in three different dissolution medium were 82, 80 and 74, respectively in comparison with imported Fortamet?, which were all greater than 50. The results of storage-stability showed that MHSRT were stable for at least 6 months under stress condition (40℃ ± 2℃, RH 75% ± 5%). Therefore, in this study, MHSRT were successfully prepared using optimized formulation technologies that meet mass produce. The in vitro release behavior of MHSRT was almost similar to that of imported Fortamet?.

Preparation and evaluation of sustained-release azithromycin tablets in vitro and in vivo

The objective of this study was to prepare azithromycin(AZI)sustained-release products in order to allow for a high dose to be administered,reduce gastrointestinal side-effects and increase the compliance of patients.AZI sustained-release tablets with different release performance(F-I:T_(100%)=3 h and F-II:T_(100%)=8 h in pH 6.0 phosphate buffer)were successfully prepared by wet granulation.The in vitro release rate and drug release mechanism were studied.The release rate of F-Iwas affected by dissolutionmedia with different pH,but not for F-II.HixsoneCrowellmodel was the best regression fitting model for F-I and F-II.Additionally,F-I and F-II both belonged to non-Fick diffusion.Oral pharmacokinetics of the two tablets and one AZI dispersible tablet as reference were studied in six healthy beagle dogs after oral administration.Compared with the reference,the C_(max) of F-I and F-II were decreased,and the T_(max) were prolonged,in that case which meet the requirement of sustained-release tablets.The relative bioavailability of F-I and F-II were 79.12%and 64.09%.T-test ofAUC_(0-144),and AUC_(0-∞) for F-I and F-II indicated there was no significant difference between F-I and F-II.These mean that the extended release rate did not induce different pharmacokinetics in vivo.

Clinical observation of Baitou Weng Decoction combined with mesalazine sustained-release tablets in treating heat-toxic and smoldering ulcerative colitis

Objective:To observe the clinical efficacy of Baitou Weng Decoction combined with mesalazine sustained-release tablets in the treatment of ulcerative colitis with febrile heat and its effect on immune function and serum inflammatory factors.Methods: A total of 84 patients with ulcerative colitis were randomly divided into control group and treatment group, with 42 cases in each group. The control group was given mesalazine sustained-release tablets orally, while the treatment group was given Baitou Weng Decoction and mesalazine sustained-release tablets orally. The treatment period was 30 days and the patients were followed up for 3 months. After treatment, the clinical efficacy, quality of life, immune function and serum inflammatory factors of the two groups were observed.Results: The effective rate of treatment group (90.47%) was higher than that of control group (73.81%) (P<0.05);compared with before treatment, the scores of inflammatory bowel disease quality of life questionnaire scale in both groups were significantly improved (P<0.05), and the difference between the two groups was significant (P<0.05);after treatment, the plasma CD4+/CD8+ ratio and NK+ levels in both groups were significantly higher than those before treatment (P<0.05), and the treatment group was changed. The serum levels of tumor necrosis factor-α, interleukin-17 and interleukin-23 were significantly decreased in both groups after treatment (P<0.05), and the improvement was more significant in the treatment group (P<0.05). No significant adverse reactions were observed in the treatment group.Conclusions: Modified Baitou Weng Decoction combined with mesalazine in the treatment of heat-toxic and incandescent ulcerative colitis can significantly improve the clinical efficacy, improve the quality of life of patients, effectively regulate the expression level of serum inflammatory factors in ulcerative colitis patients, promote the recovery of patients' immune function, and have high drug safety.

Pharmacokinetic Study on Lovastatin Sustained-release Tablet and Sustained-release Capsule in Begal Dogs

This study pharmacokinetically examined the lovastatin sustained-release tablet and sustained-release capsule in Beagle dogs. An reversed-phase HPLC method was established for the determination of lovastatin in Beagle dog plasma. Pharmacokinetic findings were compared among three preparation(lovastatin sustained-release tablet,T p; sustained-release capsule,T J and conventional capsule). Our results showed that the pharmacokinetic parameters in 6 dogs after single-dose oral administration of three perparations were calculated. T max, C max and MRT revealed significant difference (P<0.05). Relative bioavailability was 111.5±16.9 % (T P) and 110.4%±9.6 % (T J). The pharmacokinetic parameters in the 6 dogs after multiple-dose oral administration of three perparations, T max, C max MRT and DF had significant difference (P<0.05); C av , C min and AUC 0-24 h displayed no significant difference (P>0.05). It is concluded that the lovastatin sustained-release tablet and sustained-release capsule are able to maintain a sustained-release for 24 h.

Simultaneous Analysis of Indapamide and Related Impurities in Sustained-Release Tablets by a Single-Run HPLC-PDA Method

The contents of indapamide and related impurities in generic indapamide sustained-release tablets were simultaneously detected by a single-run high performance liquid chromatography equipped with photodiode array detector(HPLC-PDA)method for the quality control in this paper.The results showed the method had a good selectivity and was validated through linearity,limits of detection and quantification,recovery,and precision.The linear ranges of indapamide,2-methyl-1-nitroso-2,3-dihydro-1H-indole(impurity A,ImA),4-chloro-N-(2-methyl-1H-indol-1-yl)-3-sulphamoyl-benzamide(impurity B,ImB)and 4-chloro-3-sulfamoylbenzoic acid(impurity 1,Im1)were 0.028-1.80μg/mL(R=0.99995),0.060-1.20μg/mL(R=0.9996),0.0324-1.20μg/mL(R=0.99985)and 0.060-1.20μg/mL(R=0.9997)with detection limits of 0.0093,0.012,0.012 and 0.006μg/mL,respectively.ImA and Im1 were not detectable in the generic drug.The content of indapamide was 96.7%of the labeled amount with a relative standard deviation(RSD)of 1.30%,and the percentage of ImB relative to the labeled amounts of indapamide was 0.106%with an RSD of 1.82%.The content of other unspecified impurities all met the reference quality standards.The results provided references for the quality control and the quality standard study of generic indapamide sustained-release tablets.

近红外光谱技术无损检测克咳片中麻黄类生物碱和吗啡含量研究

麻黄类生物碱以及吗啡含量对评价克咳片质量具有重要意义,该文基于近红外光谱(NIRS)技术建立了快速、无损、高效的克咳片质量评价方法,采用NIRS和偏最小二乘回归(PLSR)法建立了麻黄类生物碱以及吗啡的定量分析模型,并采用不同预处理方法和不同变量选择方法优化了模型性能。将校正集决定系数(R_(c)^(2))、验证集决定系数(R_(p)^(2))和相对分析误差(RPD)作为模型的评价指标。结果表明,标准正态变量变换(SNV)预处理方法结合竞争自适应重加权采样(CARS)变量选择方法所建立的模型性能最优。克咳片中麻黄类生物碱及吗啡近红外光谱模型的R_(c)^(2)、R_(p)^(2)及RPD分别为0.91、0.93、4.00和0.92、0.94、4.24,说明模型性能较好。该研究基于NIRS和CARS实现了克咳片指标成分的快速、无损分析,为克咳片的质量快检提供了参考。

超高效液相色谱法测定硫酸吗啡及硫酸吗啡缓释片的有关物质

目的:建立硫酸吗啡及其制剂杂质谱分析的超高效液相色谱法(UHPLC法)。方法:使用ACQUITY UPLC HSS C_(18)(100 mm×2.1 mm,1.8μm)色谱柱,以0.101%庚烷磺酸钠溶液(用50%磷酸溶液调节pH至2.6)和甲醇为流动相,梯度洗脱,柱温35℃,流速0.3 mL·min^(-1),检测波长230 nm。结果:本方法可实现磷酸可待因(杂质A)、伪吗啡(杂质B)、东罂粟碱(杂质C)、10-羟基吗啡(杂质D)、吗啡酮(杂质E)、吗啡氮氧化物(杂质F)和14-羟基吗啡酮(杂质G,基因毒性杂质)之间及其他相邻杂质之间的良好分离,UHPLC的使用,大大减少了分析时间和有机溶剂甲醇的消耗量,更为绿色环保。结论:该方法首次将硫酸吗啡各已知杂质和14-羟基吗啡酮在UHPLC条件下同时分离,专属性良好,并用校正因子法对原料药和制剂中的7个已知杂质进行准确定量,且可同时测定硫酸吗啡原料药及其制剂硫酸吗啡缓释片中的有关物质,为原料药的选择和制剂工艺的控制提供技术依据。

盐酸吗啡渗透泵片片芯促渗剂研究

目的探讨盐酸吗啡渗透泵片片芯促渗剂的选择。方法以体外释药行为为指标‚采用单因素考察法对渗透压活性物质、崩解剂、高分子聚合物的种类与用量进行考察,并根据优化结果进行验证试验。结果盐酸吗啡渗透泵片片芯处方中渗透压活性物质为60%乳糖,不加崩解剂,不加高分子聚合物,符合该品缓释规律。按处方工艺制备3批半透膜包衣片,其释放曲线良好,加速稳定性试验条件下体外累积释放度未发生显著变化。结论盐酸吗啡渗透泵片片芯促渗剂选择60%乳糖‚20 h时体外累积释放度达85%以上,产品质量稳定。

盐酸羟考酮缓释片与硫酸吗啡缓释片治疗中重度癌症疼痛患者的效果比较

目的探究盐酸羟考酮缓释片与硫酸吗啡缓释片治疗中重度癌症疼痛患者的临床效果。方法102例中重度癌症疼痛患者为研究对象,随机分为研究组和对照组,每组51例。对照组应用硫酸吗啡缓释片进行镇痛治疗,研究组患者则使用盐酸羟考酮缓释片进行镇痛治疗。对比两组患者的镇痛效果、治疗过程中不良反应发生情况以及镇痛前后生活质量评分。结果研究组患者镇痛总有效率为98.04%(50/51),显著高于对照组患者的82.35%(42/51)(P<0.05)。研究组患者不良反应发生率9.80%(5/51)显著低于对照组患者的45.10%(23/51)(P<0.05)。镇痛前两组患者生活质量评分组间差异无显著性(P>0.05);镇痛后两组患者生活质量评分较镇痛前明显降低,且研究组患者生活质量评分(12.23±5.13)分低于对照组的(16.59±4.81)分(P<0.05)。结论对中重度癌症疼痛患者使用盐酸羟考酮缓释片镇痛价值肯定,相较于硫酸吗啡缓释片镇痛效果更好,安全性更高,有助于提高患者的生活质量。

24 h盐酸吗啡缓释片与市售品在比格犬体内的药代动力学对比研究

目的建立测定比格犬血浆中盐酸吗啡浓度的液相色谱串联质谱(LC-MS/MS)法,比较自制24 h盐酸码啡缓释片与市售品的药代动力学行为和缓释特征。方法以磷酸可待因为内标,用乙腈沉淀分离蛋白;色谱柱为ACE Phenyl柱(100 mm×2.1 mm,5μm),流动相为0.1%甲酸水溶液-0.1%甲酸乙腈溶液(梯度洗脱),流速为500μL/min;采用电喷雾离子源、多反应监测模式,监测离子对分别为质荷比(m/z)286.1~165.3(吗啡)和m/z 300.2~165.1(可待因)。比格犬单剂量、三周期交叉口服方式给予24 h盐酸吗啡缓释片和2种盐酸吗啡市售品,采用LC-MS/MS法测定血药浓度,由Phoenix WinNonlin 7.0软件计算药代动力学参数。结果吗啡质量浓度在5~2000 ng/mL范围内与待测物和内标峰面积比值的线性关系良好(r=0.9984,n=8);准确度、精密度、稳定性试验结果的RSD和RE均低于20%。自制品与2种市售品的血药浓度时间曲线下面积(AUC_(0-t))、最大血药浓度(C_(max))无显著差异(P>0.05),达峰时间(t_(max))分别为市售品1的13.9倍、市售品2的7.1倍。结论自制24 h盐酸吗啡缓释片较2种市售品有明显的缓释特性。

盐酸吗啡缓释片联合复方苦参注射液治疗中重度癌痛患者临床观察

目的 研究盐酸吗啡缓释片联合复方苦参注射液治疗中重度癌痛患者的临床表现,为后续临床治疗提供思路。方法 选取医院2017年6月—2023年1月收治的121例中重度癌痛患者,将其按照电脑抽样随机分为治疗组(60例,口服盐酸吗啡缓释片+静滴复方苦参注射液)和对照组(61例,仅口服盐酸吗啡缓释片)。比较两组的临床疗效、疼痛程度数字评估量表(NRS)、Karnofsky评分(KPS)、匹兹堡睡眠质量指数(PSQI)和不良事件发生情况。结果 经治疗,对照组完全缓解(CR)30例,部分缓解(PR)17例,轻微缓解(PR)7例,无效(NR)7例,有效缓解率为77.05%(47/61),治疗组CR 42例,PR 15例,MR 3例,NR 0例,有效缓解率95.00%(57/60),差异具有统计学意义(χ^(2)=10.954,P=0.010);两组NRS评分均显著提高(P<0.01),两组差异无统计学意义(U=1516.000,Z=1.708,P=0.880),治疗后KPS评分均较治疗前差异有显著统计学意义(P<0.01),两组间治疗后差异具有显著统计学意义(U=489.00,Z=6.962,P=0.000);两组患者治疗前后PSQI评分比较,均差异有统计学意义(P<0.01),两组治疗后对比,差异有显著统计学意义(U=378.000,Z=7.675,P=0.000);治疗组不良反应发生率为18.33%(11/60),对照组不良反应发生率为39.34%(24/61),差异具有统计学意义(χ^(2)=6.495,P=0.011)。结论 中重度癌痛患者应用盐酸吗啡缓释片联合复方苦参注射液可以提高临床疗效,改善患者的生活质量,改善患者睡眠质量,减少药物不良事件的发生。

盐酸氢吗啡酮皮下滴定用于癌痛镇痛的临床分析

目的评价盐酸氢吗啡酮皮下滴定给药用于中重度癌痛镇痛的使用剂量、缓解疼痛结果及不良反应的发生情况。方法选取2021年9月—2022年8月莆田学院附属医院疼痛科的中重度癌痛患者60例,随机分为A、B两组,A组30例通过盐酸氢吗啡酮皮下给药滴定,B组30例口服盐酸吗啡片滴定,比较两组3天之内的药物剂量、治疗前后NRS评分、爆发性疼痛发作次数及不良反应发生率。结果A组Day3用量低于B组,差异有统计学意义(t=5.905,P<0.001)。A组Day3的NRS评分为(0.76±0.19)分,低于B组的(1.78±0.14)分,差异有统计学意义(t=-23.951,P<0.001)。A组Day3无发生爆发性疼痛患者占90.0%,高于B组的46.7%,差异有统计学意义(P<0.001)。治疗后,A组便秘发生率(13.3%)低于B组(36.7%),差异有统计学意义(χ^(2)=4.356,P<0.05),两组均未发生呼吸抑制。结论盐酸氢吗啡酮皮下给药滴定用于癌痛患者的药物使用剂量低、疼痛缓解率高,可显著减少爆发性疼痛发作次数,值得临床推广。

观察盐酸羟考酮缓释片联合盐酸吗啡片滴定治疗中重度癌痛的效果及对睡眠质量的影响

目的:观察盐酸羟考酮缓释片联合盐酸吗啡片滴定治疗中重度癌痛的效果及对睡眠质量的影响。方法:选取2019年10月至2020年10月内蒙古科技大学包头医学院第二附属医院收治的中重度癌痛患者150例作为研究对象,按照随机数字表法分为观察组和对照组,每组75例。对照组给予盐酸吗啡片治疗,观察组给予盐酸羟考酮缓释片联合盐酸吗啡片治疗。比较2组患者睡眠时间的差异,同时比较2组患者的疼痛缓解情况及不良反应发生率。结果:治疗后,观察组的疼痛缓解情况显著优于对照组,观察组患者睡眠时间显著长于对照组,2组比较差异均有统计学意义(均P<0.05);观察组不良反应发生率与对照组比较,差异无统计学意义(P>0.05)。结论:盐酸羟考酮缓释片联合盐酸吗啡片滴定有助于缓解中重度癌痛患者的疼痛,可显著延长患者的睡眠时间,不增加不良反应发生率。

盐酸吗啡缓释片治疗晚期癌痛的疗效、安全性及对睡眠影响观察

目的:探究盐酸吗啡缓释片治疗晚期癌痛的疗效、安全性及对睡眠影响。方法:选取2022年1月至2022年12月江西省信丰县人民医院肿瘤内科收治的晚期癌症患者120例作为研究对象,随机分为对照组和观察组,每组60例。分别给予氨酚羟考酮片和盐酸吗啡缓释片治疗,比较分析2组患者治疗效果、安全性及对睡眠影响。结果:观察组癌痛评价(4.11±0.92)分明显低于对照组的(5.13±1.01)分(P<0.05);观察组癌痛缓解率为80.00%,明显高于对照组的63.34%(P<0.05);观察组患者治疗睡眠评价为(6.02±1.01)分,明显低于对照组的(9.28±1.47)分,差异有统计学意义(P<0.05);2组患者不良反应比较,差异无统计学意义(P>0.05)。结论:在晚期癌症患者癌痛治疗中,服用盐酸吗啡缓释片,可以有效缓解疼痛程度,改善患者的睡眠质量,且用药安全,对于提高患者的生命质量具有显著意义。

普瑞巴林联合盐酸吗啡缓释片治疗前列腺癌神经病理性癌痛的临床疗效研究

目的研究普瑞巴林联合盐酸吗啡缓释片治疗前列腺癌神经病理性癌痛的治疗效果以及治疗过程中的安全性。方法选取前列腺癌伴有神经病理性癌痛患者60例,并随机将60例病患分为盐酸吗啡缓释片联合普瑞巴林组(联合组)与单用盐酸吗啡缓释片组(对照组),比较联合组和对照组的患者用药前后疼痛数字评分(NRS)、盐酸吗啡缓释片每日用药剂量、爆发痛每日发作次数、所产生的不良反应和生活质量(QOL)评分等多个方面。结果在采取服用药物治疗后的第2、第4、第8周后,联合组NRS评分低于对照组,差异有统计学意义(P<0.05)。在用药治疗后的第1、第2、第4、第8周,联合组和对照组所表现出的生活质量评分都出现升高情况。同时,对照组生活质量明显逊于联合组,差异有统计学意义(P<0.05)。治疗后4周、8周,联合组盐酸吗啡缓释片人均日剂量低于对照组,差异有统计学意义(P<0.05);治疗后,联合组爆发痛人均日发作次数均少于对照组。联合组所产生的不良反应情况发生率为16.67%(5/30),优于对照组所产生的不良反应情况发生率60.00%(18/30),差异存在统计学意义(P<0.05)。结论联合使用普瑞巴林与盐酸吗啡缓释片可以有效使病患的疼痛评分有所降低,吗啡用量减少,并且抑制了爆发痛次数,患者的生活质量和情绪状态都得到改善,减少不良反应情况的发生。

阿片类药物治疗中晚期癌症患者癌痛的临床效果

目的观察盐酸羟考酮缓释片联合盐酸吗啡片治疗中晚期癌症患者癌痛的临床效果。方法选择210例中重度癌痛患者进行2周以上的阿片类药物治疗及随访,收集相关治疗数据。比较不同年龄、性别、肿瘤部位及体质量指数(BMI)患者的癌痛缓解率、数字评分量表(NRS)评分、吗啡日均用量,分析不良反应发生情况。结果不同年龄患者的癌痛缓解率、NRS评分、吗啡日均用量比较,差异无统计学意义(P>0.05)。男性和女性患者的癌痛缓解率、NRS评分、吗啡日均用量比较,差异无统计学意义(P>0.05)。不同肿瘤部位患者的癌痛缓解率、NRS评分比较,差异无统计学意义(P>0.05);不同肿瘤部位患者的吗啡日均用量比较,差异具有统计学意义(P<0.05)。不同BMI患者的癌痛缓解率、NRS评分比较,差异无统计学意义(P>0.05);不同BMI患者的吗啡日均用量比较,差异具有统计学意义(P<0.05)。患者应用阿片类药物期间出现的不良反应主要为便秘。结论在以阿片类药物为主的癌痛治疗过程中,肿瘤部位及BMI是影响药物用量的重要因素。

血府逐瘀汤加减联合盐酸吗啡缓释片治疗肝癌疼痛瘀血内阻证疗效研究

目的:探讨血府逐瘀汤加减联合盐酸吗啡缓释片治疗肝癌疼痛瘀血内阻证临床疗效。方法:选取肝癌疼痛瘀血内阻证患者108例,按照随机信封法分为两组,对照组(n=54)给予盐酸吗啡缓释片治疗,观察组(n=54)给予血府逐瘀汤加减联合盐酸吗啡缓释片治疗。比较两组患者镇痛效果、疼痛评分、中医症状积分、镇痛因子以及生活质量。结果:治疗4周后观察组疼痛有效缓解率高于对照组(P<0.05)。治疗前、治疗2周后,两组患者数字疼痛分级量表(NRS)评分比较,差异无统计学意义(均P>0.05)。治疗3、4周后,观察组NRS评分低于对照组,差异有统计学意义(P<0.05)。治疗前两组患者肝区疼痛、腹内癥块、纳呆、情志抑郁中医症状积分比较,差异无统计学意义(均P>0.05)。治疗4周后观察组各项中医症状积分均低于对照组,差异有统计学意义(P<0.05)。治疗4周后观察组PGE2、NO低于对照组,差异有统计学意义(均P<0.05)。治疗4周后观察组QLQ-30量表各维度高于对照组,差异有统计学意义(均P<0.05)。结论:血府逐瘀汤加减联合盐酸吗啡缓释片治疗肝癌疼痛瘀血内阻证患者可降低镇痛因子水平,提升镇痛效果,缓解中医症状,改善生活质量。

盐酸羟考酮缓释片治疗中晚期恶性肿瘤疼痛患者的效果

目的:观察盐酸羟考酮缓释片治疗中晚期恶性肿瘤疼痛患者的效果。方法:选取2019年1月至2022年1月该院收治的80例中晚期恶性肿瘤患者进行前瞻性研究,采用掷硬币法将其分为对照组和观察组各40例。对照组予以盐酸吗啡缓释片治疗,观察组予以盐酸羟考酮缓释片治疗,比较两组疼痛缓解效果、治疗前后致痛因子[血清5-羟色胺(5-HT)、缓激肽(BK)和脑脊液神经肽-Y(NPY)]水平、睡眠质量[匹兹堡睡眠质量指数量表(PSQI)]评分、生命质量[欧洲癌症研究与治疗组织生命质量测定量表(EORTC QLQ-C30)]评分和不良反应发生情况。结果:观察组疼痛缓解率为95.00%(38/40),高于对照组的77.50%(31/40),差异有统计学意义(P<0.05);治疗后,两组5-HT、BK和NPY水平均低于治疗前,且观察组低于对照组,差异有统计学意义(P<0.05);治疗后,两组PSQI、EORTC QLQ-C30评分均低于治疗前,且观察组低于对照组,差异有统计学意义(P<0.05);观察组不良反应发生率为5.00%(2/40),低于对照组的20.00%(8/40),差异有统计学意义(P<0.05)。结论:盐酸羟考酮缓释片治疗中晚期恶性肿瘤疼痛患者可提高疼痛缓解效果,降低致痛因子水平和不良反应发生率,改善睡眠质量和生命质量,效果优于盐酸吗啡缓释片治疗。

高效液相色谱法测定尿通卡克乃其片中吗啡含量

目的建立测定尿通卡克乃其片中吗啡含量的高效液相色谱法。方法色谱柱为岛津Shim-pack GIST-C_(18)柱(250 mm×4.6 mm,5μm),流动相为乙腈-0.05 mol/L磷酸氢二钾溶液-0.025 mol/L庚烷磺酸钠溶液(15∶45∶40,V/V/V),流速为1.0 mL/min,检测波长为220 nm,柱温为35℃,进样量为10μL。结果吗啡的质量浓度在3.979~198.950μg/mL范围内与峰面积线性关系良好(r=0.9999,n=6);检测限为1μg/mL,定量限为3μg/mL;精密度、稳定性、重复性试验结果的RSD均小于2.5%(n=6);平均加样回收率为102.77%,RSD为3.84%(n=9)。10批样品中吗啡的平均含量为每片0.32 mg。结论该方法操作简便、结果准确,可用于尿通卡克乃其片中吗啡的含量测定。