Analysis of the Therapeutic Effect of Clopidogrel Bisulfate Tablets + Aspirin Enteric-Coated Tablets on Acute Myocardial Infarction

Objective:To investigate and analyze the clinical effect of clopidogrel bisulfate tablets combined with aspirin enteric-coated tablets on acute myocardial infarction(AMI)patients.Methods:The study period was from January 2020 to December 2023,the sample source was 82 AMI patients admitted to our hospital,grouped into an observation group(n=41)and a control group(n=41)by the numerical table method.The patients in the control group were treated with aspirin enteric-coated tablets,and the patients in the observation group were treated with aspirin enteric-coated tablets combined with clopidogrel bisulfate.The clinical efficacy,coagulation indexes,and the incidence of cardiovascular adverse events between the two groups were compared.Results:The clinical efficacy of the observation group was higher than that of the control group(P<0.05);the platelet aggregation rate(PAR)of the observation group was lower than that of the con-trol group after treatment(P<0.05),and there was no significant difference in the prothrombin time(PT)and activated partial thromboplastin time(APTT)between the two groups(P>0.05).The incidence of cardiovascular adverse events in the observation group was lower than that of the control group(P<0.05).Conclusion:The treatment effect of clopidogrel bisulfate tablets combined with aspirin enteric-coated tablets on AMI patients is remarkable.It reduces the PAR and the incidence of cardiovascular adverse events,so this treatment method should be popularized.

Classification and Quantitative Analysis of Azithromycin Tablets by Raman Spectroscopy and Chemometrics

Raman spectroscopy has been proven a noninvasive technique with high potential in pharmaceutical industry. In this study, micro Raman technique and chemometric tools were used for identification of azithromycin (AZM) tablets by different manufacturers and quantitative analysis of the active pharmaceutical ingredient (API) in the samples. Support vector machine (SVM), Bayes classifier and K-nearest neighbour (KNN) were employed for identification, partial least squares (PLS) regression was used for quantitative determination, and interval partial least squares (iPLS) and Monte Carlo based uninformative variable elimination (MC-UVE) methods were used to select informative variables for improving the models. The results show that all the samples can be classified into groups by manufacturers with high accuracy, and the correlation coefficient between the predicted API concentrations and reference values is as high as 0.96. Therefore, micro Raman spectroscopy coupled with chemometrics may be a fast and powerful tool for identification and quantitative determination of pharmaceutical tablets.

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.

双歧杆菌四联活菌片联合阿奇霉素治疗小儿重症肺炎的效果及对肺部超声评分、肠道菌群的影响

目的探讨双歧杆菌四联活菌片联合阿奇霉素治疗小儿重症肺炎的效果及对肺部超声评分、肠道菌群的影响。方法选取2021年2月至2023年2月信阳市中心医院收治的98例重症肺炎患儿作为研究对象,按随机数字表法分为观察组、对照组,各49例。对照组接受阿奇霉素治疗,观察组接受双歧杆菌四联活菌片联合阿奇霉素治疗。比较两组临床疗效、临床症状恢复情况、肺部超声评分、炎症反应指标[白细胞介素-17(IL-17)、可溶性髓系细胞触发受体-1(sTREM-1)、超敏C反应蛋白(hs-CRP)]、肠道菌群指标[肠杆菌、双歧杆菌、拟杆菌]。结果观察组总有效率(95.92%)高于对照组(71.43%)(P<0.05);治疗8 d后观察组心率恢复、肺部啰音消失、呼吸困难缓解、体温恢复、肺部阴影消失、咳嗽缓解时间均短于对照组(P<0.05);治疗1、3、8 d后观察组肺部超声评分低于对照组(P<0.05);治疗8 d后观察组IL-17、sTREM-1、hs-CRP水平均低于对照组(P<0.05);治疗8 d后观察组肠杆菌菌落数少于对照组,双歧杆菌、拟杆菌菌落数多于对照组(P<0.05)。结论双歧杆菌四联活菌片、阿奇霉素联合应用于小儿重症肺炎的治疗中效果显著,能有效改善机体炎症状态,维持肠道菌群平衡,降低肺部超声评分,利于促进预后恢复。

复方甘草酸苷片联合阿奇霉素对小儿支原体肺炎患儿血清铁蛋白及乳酸脱氢酶水平的影响

目的探讨复方甘草酸苷片联合阿奇霉素对小儿支原体肺炎患儿血清铁蛋白(SF)及乳酸脱氢酶(LDH)水平的影响。方法选取2020年5月至2021年3月我院收治的88例小儿支原体肺炎患儿为研究对象,随机将其分为对照组(44例,阿奇霉素治疗)和观察组(44例,复方甘草酸苷片联合阿奇霉素治疗)。比较两组的治疗效果。结果观察组的治疗总有效率高于对照组(P<0.05)。治疗后,观察组的第1秒用力呼吸容积(FEV_(1))、用力肺活量(FVC)及呼气峰流速(PEF)高于对照组(P<0.05)。治疗后,观察组的肿瘤坏死因子-α(TNF-α)、白细胞介素-6(IL-6)、白细胞介素-10(IL-10)水平低于对照组(P<0.05)。治疗后,观察组的免疫球蛋白M(IgM)、免疫球蛋白G(IgG)及免疫球蛋白A(IgA)水平高于对照组(P<0.05)。治疗后,观察组的SF、LDH水平低于对照组(P<0.05)。结论复方甘草酸苷片联合阿奇霉素可提高小儿支原体肺炎的治疗效果,改善患儿的肺功能指标、炎症指标及免疫功能指标,降低SF、LDH水平,值得临床推广与应用。

阿奇霉素联合孟鲁司特钠片对小儿支原体肺炎症状、肺功能及免疫功能的影响

目的探讨阿奇霉素联合孟鲁司特钠片对小儿支原体肺炎症状、肺功能及免疫功能的影响。方法选择2021年1月~2023年8月某院接诊的98例支原体肺炎患儿,采用抽签法随机分为两组。对照组49例,给予阿奇霉素治疗,观察组49例,在对照组基础上给予孟鲁司特钠片治疗。比较两组的症状改善时间、肺功能及免疫功能。结果观察组的体温恢复正常时间、X线阴影消失时间、肺部啰音消失时间和咳嗽停止时间短于对照组(P<0.05);治疗前,两组的最大呼气中期流速(MMF)、最大肺活量(VC_(max))、呼气峰值流量(PEF)、最大自主通气量(MVV)和第1秒用力呼气容积占预计值百分比(FEV_(1)%)比较,差异无统计学意义(P>0.05),治疗后,两组的MMF、VC_(max)、PEF、MVV和FEV_(1)%均明显升高,且观察组更高(P<0.05);治疗前,两组的免疫球蛋白A(IgA)、免疫球蛋白G(IgG)及免疫球蛋白M(IgM)水平比较,差异无统计学意义(P>0.05),治疗后,两组的IgA、IgM和IgG水平均明显升高,且观察组更高(P<0.05);两组患儿的恶心、肝功能异常、皮疹及腹部不适发生率比较,差异无统计学意义(P>0.05)。结论阿奇霉素与孟鲁司特钠片联用能明显改善小儿支原体肺炎的症状、肺功能及免疫功能。

孟鲁司特钠片联合阿奇霉素注射液治疗小儿肺炎支原体肺炎的临床疗效

目的探究肺炎支原体肺炎患儿接受孟鲁司特钠片与阿奇霉素注射液联合治疗的效果。方法病例选取时间为2020年6月至2023年6月,选择封丘县妇幼保健院在此期间收治的86例肺炎支原体患儿作为本次研究对象,以随机数字表法将其分为两组,将43例接受单药阿奇霉素注射液治疗的患儿作为对照组,另43例接受孟鲁司特钠片联合阿奇霉素注射液治疗的患儿作为实验组,对比两组患儿临床治疗效果、炎性因子[C反应蛋白(CRP)、乳酸脱氢酶(LDH)和铁蛋白(SF)]与影像学检查结果、症状(发热、咳嗽与肺啰音)消失时间与安全性。结果与对照组相比,实验组患儿治疗有效率较高,症状消失时间缩短,差异有统计学意义(P<0.05)。治疗前,两组炎性因子水平差异无统计学意义(P>0.05),治疗后,两组炎性因子水平均降低,且实验组低于对照组,差异有统计学意义(P<0.05)。两组患儿不良反应发生率对比差异无统计学意义(P>0.05)。影像学检查结果显示,实验组胸腔积液、胸腔增厚、肺不张与肺实变发生率低于对照组,差异有统计学意义(P<0.05)。结论肺炎支原体肺炎患儿接受孟鲁司特钠片联合阿奇霉素注射液治疗后,其治疗效果提升,炎性因子水平降低,症状消失时间缩短,安全可靠,值得临床使用。

连花清瘟胶囊联合西药治疗社区获得性肺炎临床研究

目的:观察连花清瘟胶囊联合西药治疗社区获得性肺炎(CAP)痰热壅肺证的临床疗效。方法:选取98例CAP痰热壅肺证患者,以随机数字表法分为治疗组49例与对照组49例。剔除治疗组1例,对照组3例,最终纳入研究治疗组48例、对照组46例。对照组给予阿奇霉素片联合注射用头孢曲松钠治疗,治疗组在对照组基础上给予连花清瘟胶囊治疗。2组均治疗7 d。比较2组临床疗效、中医证候评分、炎症指标[超敏C-反应蛋白(hs-CRP)、白细胞介素-6(IL-6)、肿瘤坏死因子-α(TNF-α)]及免疫指标[免疫球蛋白(Ig)A、IgG、IgM]水平。结果:治疗后,治疗组总有效率95.83%,高于对照组82.61%(P<0.05)。2组咳嗽、痰多、痰白干黏或痰黄、胸痛、发热、口渴、尿黄、大便秘结、腹胀评分均较治疗前降低(P<0.05),治疗组上述9项中医证候评分均低于对照组(P<0.05)。2组血清hs-CRP、IL-6、TNF-α水平均较治疗前降低(P<0.05),治疗组上述3项指标水平均低于对照组(P<0.05)。2组血清IgA、IgG、IgM水平均较治疗前升高(P<0.05),治疗组上述3项指标水平均高于对照组(P<0.05)。结论:连花清瘟胶囊联合西药治疗CAP痰热壅肺证疗效显著,可减轻临床症状,抑制炎症反应,增强免疫功能。

Gradient high performance liquid chromatography method for simultaneous determination of ilaprazole and its related impurities in commercial tablets

A methodology(HPLC)proposed in this paper for simultaneously quantitative determination of ilaprazole and its related impurities in commercial tablets was developed and validated.The chromatographic separation was carried out by gradient elution using an Agilent C8 column(4.6 mm×250 mm,5 mm)which was maintained at 25℃.The mobile phase composed of solvent A(methanol)and solvent B(solution consisting 0.02 mmol/l monopotassium phosphate and 0.025 mmol/l sodium hydroxide)was at a flow rate of 1.0 ml/min.The samples were detected and quantified at 237 nm using an ultraviolet absorbance detector.Calibration curves of all analytes from 0.5 to 3.5 mg/ml were good linearity(r≥0.9990)and recovery was greater than 99.5% for each analyte.The lower limit of detection(LLOD)and quantification(LOQ)of this analytical method were 10 ng/ml and 25 ng/ml for all impurities,respectively.The stress studies indicated that the degradation products could not interfere with the detection of ilaprazole and its related impurities and the assay can thus be considered stability-indicating.The method precisions were in the range of 0.41-1.21 while the instrument precisions were in the range of 0.38-0.95 in terms of peak area RSD% for all impurities,respectively.This method is considered stabilityindicating and is applicable for accurate and simultaneous measuring of the ilaprazole and its related impurities in commercial enteric-coated tablets.

Delayed-release oral mesalamine tablet mimicking a small jejunal gastrointestinal stromal tumor:A case report

BACKGROUND Enteric-coated medications are supposed to pass intact through the gastric environment and to release the drug content into the small intestine or the colon.Before dissolution of the enteric coating,they may appear hyperdense on computed tomography(CT).Unfortunately,few reports have been published on this topic so far.In this case report,the hyperdense appearance on contrastenhanced CT of an enteric-coated mesalamine tablet was initially misinterpreted as a jejunal gastrointestinal stromal tumor(GIST).CASE SUMMARY An asymptomatic 81-year-old male patient,who had undergone laparoscopic right nephrectomy four years earlier for stage 1 renal carcinoma,was diagnosed with a jejunal GIST at the 4-year follow-up thoraco-abdominal CT scan.He was referred to our hub hospital for gastroenterological evaluation,and subsequently underwent 18-fluorodeoxyglucose positron emission tomography,abdominal magnetic resonance imaging,and video capsule endoscopy.None of these examinations detected any lesion of the small intestine.After reviewing all the CT images in a multidisciplinary setting,the panel estimated that the hyperdense jejunal image was consistent with a tablet rather than a GIST.The tablet was an 800 mg delayed-release enteric-coated oral mesalamine tablet(Asacol®),which had been prescribed for non-specific colitis,while not informing the hospital physicians.CONCLUSION Delayed-release oral mesalamine(Asacol®),like other enteric-coated medications,can appear as a hyperdense image on a CT scan,mimicking a small intestinal GIST.Therefore,adetailed knowledge of the patients’medications and a multidisciplinary review of the images areessential.

疑似联合用药导致药物性肝损伤1例的诊治分析

药物性肝损伤(DILI)是指由各类处方或非处方的药物、保健品、膳食补充剂或其代谢产物乃至辅料引起的肝损伤,是常见且严重的药物不良反应,重者可导致急性肝衰竭甚至死亡。在我国,临床药物种类多,不规范用药较普遍,DILI形势更为严峻。本文通过分析1例疑似由于氨酚氯雷伪麻缓释片、氨酚咖敏片和阿奇霉素联合用药所致DILI患者,探讨发生肝损伤原因,以期引导临床减少不合理药物联用,增强安全用药意识。

国产阿奇霉素分散片的人体生物利用度及其药动学

目的 :研究阿奇霉素国产分散片与进口片剂人体相对生物利用度及药物动力学。方法 :12名健康受试者自身交叉单剂量口服阿奇霉素国产分散片和进口片剂各 5 0 0mg ,定时取血 ,用微生物法测定血药浓度。结果 :受试制剂国产阿奇霉素分散片与参比制剂进口片剂的血药浓度时间曲线基本一致 ,符合一级吸收二房室模型。国产分散片、进口片两种制剂的主要药动学参数分别为 :消除半衰期t1/ 2 β:(45 .2± 10 .3)h ,(45 .7± 9.2 )h ;Tmax:(1.3± 0 .6 )h ,(2 .0± 1.0 )h ;Cmax:(414.7± 12 3.8) μg·L-1,(35 2 .5± 92 .1) μg·L-1。药动学参数经配对t检验 ,P >0 .0 5 ,差异均无显著性。两种制剂的药时曲线下面积AUC0→tn平均值分别为 :国产分散片 (480 4.2± 95 7.6 ) μg·L-1·h-1,进口片剂 :(5 10 9.8± 10 10 .5 ) μg·L-1·h-1;国产分散片的相对生物利用度为 :F =(94.7± 13.4) %。结论 :统计学结果表明受试制剂国产阿奇霉素分散片与参比制剂生物等效。

阿奇霉素分散片的人体相对生物利用度

10名健康男性受试者 ,分别单次空腹口服两种国产阿奇霉素分散片 5 0 0mg后 ,测定不同时间血中阿奇霉素的浓度 ,绘制了血药浓度 时间曲线 .结果表明 :两种制剂中阿奇霉素的药物动力学过程均符合二室模型 ,阿奇霉素分散片 (被试制剂 )的Cmax=(0 6 5± 0 18) μg/mL ;tmax=(1 80±0 79)h ;t1/ 2 (ke) =(0 5 6± 0 39)h ;AUC0～∞ =(9 6 9± 1 6 6 ) μg/mL·h .阿奇霉素分散片 (参比制剂 )的Cmax=(0 6 4± 0 2 1) μg/mL ;tmax=(1 80± 0 6 3)h ;t1/ 2 (ke) =(0 48± 0 2 9)h ;AUC0～∞ =(9 5 2± 2 0 8)μg/mL·h .比较两种制剂动力学参数 ,两种制剂间阿奇霉素的Cmax、tmax和AUC0→∞ 均无显著差异 ,P>0 0 5 .阿奇霉素分散片的平均相对生物利用度为 (10 3 38± 12 94) % 。

茜素红荷移分光光度法测定阿奇霉素片的溶出度

目的建立茜素红荷移分光光度法测定阿奇霉素片溶出度的方法.方法采用中国药典附录XC第三法,以250mlpH5的磷酸盐缓冲液为溶剂,转速为100r/min,经45min取样,茜素红荷移分光光度法在538nm处测定阿奇霉素的溶出度,限度为标示量的75%.结果阿奇霉素在51～255μg/ml范围内线性关系良好(r=0.9996),平均回收率为99.2%.结论该方法准确、简便,可用于阿奇霉素片溶出度的测定.

阿奇霉素纳米晶体片剂的制备及其质量评价

以纳米晶体技术为基础制备阿奇霉素纳米晶体片剂,以期提高阿奇霉素的溶出度。采用介质研磨法制备阿奇霉素纳米晶体,在此基础上制备阿奇霉素纳米晶体片剂。参考《中华人民共和国药典》对其质量进行评价,采用浆法测定溶出度,HPLC法测定含量和有关物质。通过影响因素试验、加速试验及留样试验,考察片剂的稳定性。自制阿奇霉素纳米晶体片剂符合《中华人民共和国药典》2010版二部附录片剂项下要求,溶出度较上市片剂显著提高。影响因素试验结果表明,自制片剂对高温和强光较稳定,但对环境湿度较为敏感。加速试验及留样试验结果表明,自制片剂6个月内较为稳定,贮存时应置于密闭、干燥阴凉处。

高效液相色谱法测定阿奇霉素普通片和分散片含量

目的:测定阿奇霉素含量。方法:采用高效液相色谱法对9个不同厂家产品进行测定。结果:各厂生产的产品含量均符合中国药典要求。结论:采用高效液相色谱法进行含量测定方便、有效、准确。

阿奇霉素分散片的人体药物动力学及相对生物利用度研究

８ 名健康男性志愿者交叉单剂量口服５００ ｍ ｇ 阿奇霉素分散片及片剂，采用微生物法测定不同时间的血药浓度，求得分散片和普通片的药物动力学参数分别如下：ｋａ 为１．２８±０．２３、１．２１±０．１８ ｈ－ １；ｔ１／２（（β）为４６．２７±８．１６、４９．８１±８．８２ ｈ；Ｃｍ ａｘ 为０．６２±０．１１、０．５８±０．１１ μｇ／ｍ ｌ；Ｔｍ ａｘ 为１．７３±０．１５、１．８２±０．１５ ｈ；ＡＵＣ为１０．１６±２．３５、１０．６５±３．４３ μｇ·ｈ／ｍ ｌ。经统计学处理，两制剂的ｋａ、Ｃｍ ａｘ、Ｔｍａｘ、ｔ１／２（β）均无显著性差异（Ｐ＞ ０．０５）。分散片相对生物利用度Ｆ为９５．０９±４．９８％ 。经方差分析、配对ｔ检验，均得出两制剂具有生物等效性的结论。

阿奇霉素分散片人体相对生物利用度及药动学

目的:研究受试制剂阿奇霉素分散片与参比制剂人体相对生物利用度及药动学。方法:20名健康受试者自身交叉单剂量口服阿奇霉素分散片受试制剂和参比制剂各500mg,定时取血,用微生物法测定血药浓度。结果:受试制剂阿奇霉素分散片与参比制剂的血药浓度-时间曲线基本一致,符合一级吸收二房室模型。受试制剂与参比制剂的主要药动学参数分别为:消除半衰期t1/2β:(36.1±7.8)h,(39.9±10.3)h;Tmax:(2.4±0.5)h,(2.4±0.5)h;Cmax:(413.0±72.5)μg.L-1,(404.0±69.5)μg.L-1。药动学参数经配对t检验,P>0.05,差异均无显著性。两种制剂的药时曲线下面积AUC0→t平均值分别为:受试制剂分散片(9 806±1 308)μg.L-1.h-1,参比制剂(9 949±1 395)μg.L-1.h-1;受试制剂分散片的相对生物利用度为:(99.0±9.0)%。结论:统计学结果表明,受试制剂阿奇霉素分散片与参比制剂生物等效。

阿奇霉素片在健康人体的相对生物利用度和药代动力学

目的研究阿奇霉素片(大环内酯类抗生素)在健康人体的相对生物利用度及药代动力学。方法19名健康受试者自身交叉单剂量口服阿奇霉素片受试制剂和参比药物各500mg后,用微生物法测定用药后不同时间血药浓度。结果2制剂的血药浓度-时间曲线基本一致,符合二房室模型,受试制剂和参比药物的药代动力学参数:t1/2β分别为(34.61±7.42),(31.16±5.28)h;tmax分别为(2.60±0.21),(2.55±0.16)h;Cmax分别为(557.15±129.57),(548.34±137.46)μg·L-1;AUC0-tn分别为(8.45±2.29),(8.66±2.34)h·mg·L-1;受试制剂的相对生物利用度为(99.35±19.77)%。结论受试制剂与参比药物生物等效。

阿齐霉素片的溶出度测定方法研究

阿齐霉素片经硫酸显色后采用分光光度法测定其溶出度，测定波长４８２ｎｍ；线性范围：１０～９０μｇ／ｍｌ（ｎ＝５，ｒ＝０．９９９２）；平均回收率９９．４％（ＲＳＤ＝２．３０％）。溶出度用转篮法测定，转速１００ｒ／ｍｉｎ；溶出介质ｐＨ６．０磷酸盐缓冲液，４５ｍｉｎ的累积溶出度大于９０％，不同批号阿齐霉素片溶出度测定结果重现性良好。