首页 | 本学科首页   官方微博 | 高级检索  
相似文献
 共查询到19条相似文献,搜索用时 500 毫秒
1.
《中国兽医学报》2014,(10):1657-1662
研究并比较了头孢噻呋注射液和速解灵注射液在猪体内药物代谢动力学特征和相对生物利用度。20头健康猪,随机均分为2组,进行单次给药剂量(5mg/kg)肌注头孢噻呋注射液(洛阳惠中)和速解灵注射液(美国辉瑞),前腔静脉采血,高效液相色谱法检测猪血浆中头孢噻呋的浓度。采用药动学软件WinNonlin 5.2.1的非房室模型分析方法,计算出药物的动力学参数。猪肌注头孢噻呋注射液和速解灵注射液后的药动学参数分别为:达峰时间(Tmax):(2.63±0.74)、(3.38±1.92)h;峰质量浓度(Cmax):(14.06±2.21)、(9.48±1.84)mg/L;消除半衰期(t1/2β):(17.65±2.07)、(17.70±2.43)h;平均滞留时间(MRT):(23.21±2.68)、(22.11±2.50)h;药时曲线下面积(AUClast):(240.81±47.73)、(182.51±36.12)μg·h·mL-1。参数Cmax、AUClast统计差异极显著(P<0.01),头孢噻呋注射液较速解灵注射液吸收迅速、完全,达峰时间短,峰浓度显著升高;参数Tmax、t1/2β、MRT统计差异不显著(P>0.05),头孢噻呋注射液的相对生物利用度为132%,高于速解灵注射液。结果表明头孢噻呋注射液肌注后吸收迅速、完全,达峰时间短,峰浓度高,生物利用度高。  相似文献   

2.
本研究采用肺部支气管灌流技术对盐酸头孢噻呋注射液在健康猪和患巴氏杆菌病的感染猪体内的药动学特征进行了比较,为指导盐酸头孢噻呋注射液治疗猪巴氏杆菌病提供临床数据支持。选取12头健康仔猪,随机均分为健康组和感染组。感染组通过人工感染多杀性巴氏杆菌建立疾病模型。2组动物分别按交叉试验设计,肌内注射盐酸头孢噻呋注射液,在不同时间点采集血液和支气管肺泡灌洗液,用高效液相色谱法(HPLC)检测头孢噻呋含量。健康猪血浆及支气管肺泡灌洗液中的药峰浓度(Cmax)分别为22.33和2.49 μg/mL,相差近9倍;消除半衰期(T1/2)分别为19.51和70.19 h,在肺部的消除非常缓慢,时长是血浆的3.6倍;药-时曲线下面积(AUC0-∞)分别为372.05和94.59 μg·h/mL;表观分布容积(Vd/F)分别为0.41和5.24 L/kg,头孢噻呋与肺脏呈现高度结合。感染组血浆及支气管肺泡液Cmax分别为11.81和5.05 μg/mL,T1/2分别为11.79和24.65 h,AUC0-∞分别为162.65和29.73 μg·h/mL,Vd/F分别为0.53和4.65 L/kg,与健康组表现出相同的特点。结果表明,盐酸头孢噻呋注射液在猪体内具有吸收迅速,消除缓慢,生物利用度高的药代动力学特点,且其在血浆和支气管肺泡灌洗液中的药动学参数存在显著差异。  相似文献   

3.
摘要:目的 为了比较美国盐酸头孢噻呋、大中农盐酸头孢噻呋与山东某生物科技公司新研制的头孢噻呋三种头孢噻呋注射液在白羽鸡血浆中的药物代谢动力学特征,以检测新研制盐酸头孢噻呋注射液在白羽鸡体内的药物动力学参数是否符合要求。方法 在给白羽鸡肌肉注射药物后,在0至48小时内于不同时间点采集血样,用碘乙酰胺衍生,把二硫赤鲜醇作为提取液,以水-三氟乙酸-乙腈(700:1:300)作为流动相,266nm紫外检测。结果 标准曲线线性相关很好,相关系数都在0.995以上。最低检测限为0.05μg/mL;最低定量限为0.1μg/mL,回收率都在90%以上。日间变异系数小于0.1,日内变异系数小于0.05。结果表明,新研制盐酸头孢噻呋的药物动力学参数符合产品要求。结论 三种剂型达峰时间相同;美国盐酸头孢噻呋和新研制盐酸头孢噻呋的半衰期相似,大中农盐酸头孢噻呋半衰期相对要短,但总体三种剂型的半衰期差异不显著;美国盐酸头孢噻呋和大中农盐酸头孢噻呋最高血药浓度相当,而新研制盐酸头孢噻呋相对高些,但总体三种剂型的血药浓度差异不显著。  相似文献   

4.
健康四川白鹅20只,随机分为A、B两组,A组单剂量静注头孢噻呋钠无菌粉针,B组单剂量肌注头孢噻呋钠混悬注射液,均按2.2mg·kg-1。用高效液相色谱法测定血浆中的药物浓度,3p97药代动力学程序软件处理药时数据。结果显示,A组药-时数据符合二室开放模型(W-1/C^2);主要药代动力学参数:t1/2。0.112h,tmB2.711h,CL0.234L·kg-1·h-1,V0.064L·kg,AUC9.400mg·h·L-1,B组药-时数据也符合二室开放模型(W-1/c2);主要药代动力学参数:t1/2结果表明,头孢噻呋钠混悬注射液在鹅体内分布广泛,生物利用度高,且具有长效缓释作用.。  相似文献   

5.
作者研究了头孢噻呋混悬液和头孢噻呋钠对人工诱发猪大肠杆菌病的疗效.对人工诱导发病的35日龄仔猪分别肌注头孢噻呋混悬液和头孢噻呋钠冻干粉(每种药设3和5 mg/kg2个剂量组),分别在第0、12、48、72 h给药,3 d共给药4次.同时设氨苄西林混悬注射液、Tinknium注射液以及健康和感染对照组.用药14 d后结果表明,头孢噻呋组有效率、治愈率及增重相对比显著高于氨苄西林和Tinknium组,头孢噻呋混悬液和头孢噻呋钠各剂量组之间死亡率、有效率、治愈率和增重相对比差异不显著.头孢噻呋混悬液和头孢噻呋钠冻干粉以3 mg/kg 3 d给药4次的治疗方案是可行的.  相似文献   

6.
为研究分析由本课题组研发的长效盐酸头孢噻呋注射液治疗猪呼吸道疾病的临床效果,同时与市售的同类产品进行疗效比较。本试验在上海市3个规模化猪场同时段进行,以患呼吸道疾病的猪为试验对象,将病猪随机分为两组,记为A组和B组,分别给予本课题组研发的长效盐酸头孢噻呋注射液和市售普通制剂治疗,观察两组动物在治疗1个疗程后的治疗效果。结果显示:长效盐酸头孢噻呋注射液对于治疗猪呼吸道疾病具有显著的疗效,与普通制剂相比,长效制剂的治愈率和有效率更高,适合在临床中推广应用。  相似文献   

7.
本文通过分析长效盐酸头孢噻呋注射液的质量影响因素,优化处方中助悬剂、湿润剂的组成,进行稳定性试验考察,完善了长效盐酸头孢噻呋注射液的处方与规模化生产工艺。优化后的长效盐酸头孢噻呋注射液处方合理,生产工艺可行,质量可控,适用于工业化大生产。  相似文献   

8.
盐酸头孢噻呋注射液在国外已广泛用于治疗奶牛急性产后子宫炎,本文结合国内外研究进展,阐述了盐酸头孢噻呋注射液的作用机制、抗菌活性、药代动力学、临床应用以及残留消除等内容,为盐酸头孢噻呋注射液在治疗奶牛急性产后子宫炎上的研究及应用提供相关参考。  相似文献   

9.
在奶牛乳房内灌注头孢噻呋钠后,采用超高效液相色谱一串联质谱法测定牛乳中头孢噻呋的浓度,对其消除动力学进行了研究。3头实验奶牛按每个乳房0.3g头孢噻呋灌注,牛乳中药物达到的最高浓度Cmax=107.89μg/mL,达峰时间Tmax=8h,药物半衰期T1/2=13.97h。在乳房内用药后的最初56h内,头孢噻呋浓度快速下降;最后一次给药88h后,所有乳腺中头孢噻呋的浓度都低于允许限量(0.1μg/mL)。故建议头孢噻呋在牛奶中的休药期为4d。  相似文献   

10.
盐酸头孢噻呋(Ceftiofur Hydrochloride)是头孢噻呋的盐酸盐,是全球第一个专门用于动物的第3代头孢类抗生素,其抗菌活性强、药代动力学特征优良、毒副作用小、残留低,可用于牛、猪、羊等细菌性疾病防治。  相似文献   

11.
This study determined the impact of porcine reproductive and respiratory syndrome virus (PRRSV) and Streptococcus suis coinfection on the pharmacokinetic (PK) profile of ceftiofur hydrochloride in pigs after intramuscular (i.m.) injection. Eighteen clinically normal crossbred gilts were assigned by weight into a challenge group (10 pigs) and control group (eight pigs). Pigs in both groups received a single i.m. injection of ceftiofur hydrochloride (Excenel RTU Sterile Suspension; Zoetis) at a 5 mg/kg BW dose. Serial blood samples were collected to characterize the plasma concentration curve. After a 10 days drug washout period, the challenge group was inoculated with 2 mL of PRRSV isolate VR‐2385 (105.75 50% tissue culture infective doses per mL) intranasally and 8 days later inoculated S. suis. When clinical disease was evident, the second PK assessment began in both challenge and control groups. Coinfected pigs demonstrated lower values of AUC and CMAX, but higher values of Cl/F and Vz/F indicating drug kinetics were altered by infection. The data from this study have implications on ceftiofur treatment regimens in diseased pigs.  相似文献   

12.
Bioavailability of amoxycillin in pigs   总被引:4,自引:0,他引:4  
Amoxycillin was administered to pigs intravenously (i.v.), intramuscularly (i.m.) and orally (p.o.), in a cross-over design to examine the bioavailability ( F ) of various drug formulations. These included: a sodium salt for reconstitution in water and administration i.v.; trihydrate salt in an oil base for intramuscular administration producing 'conventional' duration of plasma concentrations; a trihydrate salt in oil base giving prolonged (LA) duration, and a trihydrate powder for oral administration in solution. The concentration of amoxycillin in plasma was measured by high-performance liquid chromatography, and its pharmacokinetic variables were assessed for the individual pigs by use of non-compartmental methods.
  Following i.v. administration (8.6 mg/kg), amoxycillin was eliminated rapidly with a mean residence time ( MRT ) of 1.4 h. After i.m. administration of the conventional formulation (14.7 mg/kg), the plasma amoxycillin concentration peaked at 2 h at 5.1 μg/mL. The bioavailability was 0.83. Intramuscular administration (14.1 mg/kg) of the long acting formulation (i.m. LA), lead to two peaks in plasma at 1.3 and 6.6 h. The bioavailability was calculated to be 1.11. After p.o. administration to fasted pigs, peak concentration was reached after 1.9 h, and the bioavailability was 0.33. In fed pigs, the corresponding values were 3.6 h and 0.28. Data showed that treatment of respiratory tract diseases in pigs by p.o. dosing alone, may not be optimal, because of the relatively low bioavailability and the fact that infections often result in reduced feed and water consumption. A rational treatment regime for susceptible respiratory pathogens includes an initial i.m. injection, followed by p.o. dosing every 12 h. Alternatively, the long acting formulation may be administered i.m. in a dose of 15 mg/kg, which would lead to active plasma concentrations for approximately 48 h.  相似文献   

13.
Pharmacokinetic studies of antibiotics in South American camelids are uncommon, therefore drugs are often administered to llamas and alpacas based on dosages established in other domestic species. The disposition of ceftiofur sodium was studied in llamas following intramuscular administration and in alpacas following intravenous and intramuscular administration. Eleven adult llamas were given ceftiofur sodium by intramuscular injection. Each animal received either a standard dose of 2.2 mg/kg or an allometrically scaled dose ranging from 2.62 to 2.99 mg/kg in a crossover design. Ten adult alpacas were given ceftiofur sodium by intravenous and intramuscular injections. Each animal received a standard dosage of 1 mg/kg or an allometrically scaled dose ranging from 1.27 to 1.44 mg/kg i.v., and 1.31-1.51 mg/kg i.m. Blood samples were collected at 0, 0.25, 0.5, 1, 2, 4, 8, 12, 24, 36, 48, and 72 h after administration of the ceftiofur. Pharmacokinetic parameters of ceftiofur in llamas and alpacas were similar following i.m. dosing at both dose levels. The only differences noted were in the total AUC between dose levels, but the AUC/dose values were not different. A sequence effect was noted in the alpaca data, which resulted in lower AUCs for the second dose when the i.v. dose was given first, and with higher AUCs for the second dose when the i.m. dose was given first. Overall, ceftiofur pharmacokinetics in llamas and alpacas are similar, and also very similar to reported parameters for sheep and goats.  相似文献   

14.
Collard, W. T., Cox, S. R., Lesman, S. P., Grover, G. S., Boucher, J. F., Hallberg, J. W., Robinson, J. A., Brown, S. A. Pharmacokinetics of ceftiofur crystalline‐free acid sterile suspension in the equine. J. vet. Pharmacol. Therap. 34 , 476–481. Absolute bioavailability and dose proportionality studies were performed with ceftiofur in horses. In the absolute bioavailability study, thirty animals received either an intravenous dose of ceftiofur sodium at 1.0 mg/kg or an intramuscular (i.m.) dose of ceftiofur crystalline‐free acid (CCFA) at 6.6 mg/kg. In the dose proportionality study, 48 animals received daily i.m. ceftiofur sodium injections at 1.0 mg/kg for ten doses or two doses of CCFA separated by 96 h, with CCFA doses of 3.3, 6.6, or 13.2 mg/kg. Noncompartmental and mixed‐effect modeling procedures were used to assess pharmacokinetics (PK). CCFA was well absorbed with a bioavailability of 100%. AUC0–∞ and Cmax increased in a dose‐related manner following administration of the two doses of CCFA at 3.3, 6.6, and 13.2 mg/kg. The least‐squares mean terminal half‐life (t½) following the tenth daily i.m. injection of ceftiofur sodium at 2.2 mg/kg was 40.8 h, but the least‐squares mean t½ following the second i.m. injection of CCFA at 6.6 mg/kg was 100 h. The time that plasma ceftiofur equivalent concentrations remain above a threshold concentration of 0.2 μg/mL has been associated with efficacy, and following administration of two 6.6 mg/kg doses of CCFA, the mean time above 0.2 μg/mL was 262 h. Simulations with the nonlinear mixed‐effect PK model predicted that more than 97.5% of horses will have plasma ceftiofur equivalent concentrations >0.2 μg/mL for 96 h after the second 6.6 mg/kg dose of CCFA.  相似文献   

15.
Ceftiofur sodium, a broad-spectrum cephalosporin, is active against gram-positive and gram-negative pathogens of veterinary importance. Two studies were designed to compare the intramuscular bioavailability of the current sodium salt and the new hydrochloride salt in pigs at doses of either 3 mg or 5 mg ceftiofur equivalents (CE)/kg body weight. Twenty-six healthy young pigs were selected for these two-period, two-treatment crossover studies, 12 for the 3 mg/kg study and 14 for the 5 mg/kg study. Each animal received one intramuscular (i.m.) injection of ceftiofur sodium and one i.m. injection of ceftiofur hydrochloride with a 14-day washout period between the two treatments. Blood samples were collected serially for up to 96 h postinjection. Plasma samples were then analysed using a validated assay that measures ceftiofur and all desfuroylceftiofur-related metabolites by high-performance liquid chromatography. In the 3 mg/kg dosage study, average maximum plasma concentration (C(max)) after administration of ceftiofur sodium was 15.8+/-3.40 microg/mL at 0.4-4 h after injection. After administration of ceftiofur hydrochloride, the C(max) was 11.8+/-1.67 microg/mL at 1-4 h after injection. Concentrations of ceftiofur and metabolites 72 h after the injection were 0.392+/-0.162 microg/mL for ceftiofur hydrochloride and 0.270+/-0.118 microg/mL for ceftiofur sodium. The mean area under the curve (AUC), from time 0 to the limit of quantitation (AUC(O-LOQ)) after ceftiofur hydrochloride administration, was 216+/-28.0 microg x h/mL, compared to 169+/-45.4 microg x h/mL after ceftiofur sodium administration. The calculated time during which plasma concentrations remained above 0.02 microg/mL (t(>0.2)) was 85.3+/-10.6 h for ceftiofur sodium and 77.2+/-10.7 h for ceftiofur hydrochloride. In the 5 mg/kg dosage study, C(max) after administration of ceftiofur sodium was 28.3+/-4.45 microg/mL at 0.33-2 h after injection. After administration of ceftiofur hydrochloride, the C(max) was 29.7+/-6.72 microg/mL at 0.66-2 h after injection. Concentrations of ceftiofur and metabolites 96 h after the injection were 0.274+/-0.0550 microg/mL for ceftiofur hydrochloride and 0.224+/-0.0350 microg/mL for ceftiofur sodium. The mean AUC(O-LOQ) after ceftiofur hydrochloride administration was 382+/-89.8 microg x h/mL compared to 302+/-54.4 microg x h/mL after ceftiofur sodium administration. The t(>0.2) was 78.9+/-9.65 h for ceftiofur sodium and 94.2+/-8.64 h for ceftiofur hydrochloride. Based on the similarity of the pharmacokinetic parameters of the sodium and hydrochloride formulations of ceftiofur, similar therapeutic efficacy can be inferred for the two products.  相似文献   

16.
复方盐酸头孢噻呋混悬剂的药代动力学研究   总被引:2,自引:2,他引:0  
利用药物动力学的方法考察复方盐酸头孢噻呋混悬剂是否具备缓释长效的特点,同时研究鱼腥草油对头孢噻呋药代动力学的影响。36只SPF大鼠随机平均分成三组:A组单剂量注射复方盐酸头孢噻呋混悬剂,B组单剂量注射盐酸头孢噻呋混悬剂,C组单剂量注射头孢噻呋钠粉针;三组注射剂量均为50 mg/(kg.bw)。采用反相高效液相色谱内标法测定血浆药物浓度,并以DAS2.0药动学程序和SPSS(11.0)统计软件对所得数据进行分析。A、B、C组药时数据均符合一级吸收二室模型(权重=1/cc),主要动力学参数如下:A组:T1/2Ka=(1.253±0.100)h,Tpeak=(2.000±0.000)h,Cmax=(35.203±5.732)mg/L,AUC=(229.51±18.278)mg.h/L;B组:T1/2Ka=(0.341±0.090)h,Tpeak=(1.000±0.000)h,Cmax=(43.919±1.51)mg/L,AUC=(188.488±9.611)mg.h/L;C组:T1/2Ka=(0.044±0.012)h,Tpeak=(0.167±0.000)h,Cmax=(159.091±19.971)mg/L,AUC=(128.554±6.625)mg.h/L。实验数据表明,复方盐酸头孢噻呋混悬剂肌肉注射后,其药物动力学特征表现为吸收缓慢,血药浓度平稳,消除半衰期延长,生物利用度高等特点,在临床上注射1次,连用3 d,可以维持有效血液浓度。  相似文献   

17.
A study was conducted to measure concentrations of potentially active ceftiofur derivatives, in plasma, in uterine tissues (endometrium and caruncles) and in uterine secretions at different time points after a single subcutaneous administration of ceftiofur hydrochloride (Excenel RTU Sterile Suspension) at the dose of 1 mg/kg body weight in Holstein-Friesian dairy cows. The animals (n=4) were injected within 24 h of calving, after expulsion of the foetal membranes. Plasma, lochial fluid, caruncles and endometrium were collected before ceftiofur hydrochloride administration and at 1, 2, 4, 8, 12 and 24 h after treatment. For each cow the concentrations of ceftiofur in the biological matrices were quantified using an high-performance liquid chromatography (HPLC) assay. The limit of quantification of the method was 0.1 microg/mL for plasma and 0.1 microg/g for lochial fluid, caruncles and endometrium. The concentrations of potentially active ceftiofur derivatives detected in plasma reached a maximum of 2.85 +/- 1.11 microg/mL at 2 h and decreased to 0.64 +/- 0.14 microg/mL at 24 h after administration. In lochial fluid, these concentrations reached a maximum of 0.97 +/- 0.25 microg/g at 4 h and decreased to 0.22 +/- 0.21 microg/g at 24 h after administration. In endometrium, these concentrations reached a maximum of 2.23 +/- 0.82 microg/g at 4 h and decreased to 0.56 +/- 0.14 microg/g at 24 h following the injection, whereas these levels in caruncles were 0.96 +/- 0.45 and 0.60 +/- 0.39 microg/g obtained at 8 and 24 h, respectively. At the dose of 1 mg/kg body weight in healthy dairy cows, subcutaneous administration of ceftiofur (as ceftiofur hydrochloride) after parturition results in concentrations of ceftiofur derivatives in uterine tissues and in lochial fluid that exceed the reported minimal inhibitory concentrations (MICs) for the common pathogens (Escherichia coli, Fusobacterium necrophorum, Bacteroides spp., and Arcanobacterium pyogenes) associated with acute puerperal metritis.  相似文献   

18.
The objectives of this study were to determine pharmacokinetics of intravenous (i.v.) ceftiofur in foals, to compare ultra-high performance liquid chromatography tandem mass spectometry (UPLC-MS/MS) and microbiologic assay for the measurement of ceftiofur concentrations, and to determine the minimum inhibitory concentration ( MIC ) of ceftiofur against common equine bacterial pathogens. In a cross-over design, ceftiofur sodium was administered i.v. to six foals (1–2 days-of-age and 4–5 weeks-of-age) at dosages of 5 and 10 mg/kg. Subsequently, five doses of ceftiofur were administered i.v. to six additional foals between 1 and 5 days of age at a dose of 5 mg/kg q 12 h. Concentrations of desfuroylceftiofur acetamide (DCA), the acetamide derivative of ceftiofur and desfuroylceftiofur-related metabolites were measured in plasma, synovial fluid, urine, and CSF by use of UPLC-MS/MS. A microbiologic assay was used to measure ceftiofur activity for a subset of plasma samples. Following i.v. administration of ceftiofur at a dose of 5 mg/kg to 1–2 day-old foals, DCA had a t ½ of 7.8 ± 0.1 h, a body clearance of 74.4 ± 8.4 mL/h/kg, and an apparent volume of distribution of 0.83 ± 0.09 L/kg. After multiple i.v. doses at 5 mg/kg, DCA concentrations in CSF were significantly lower than concurrent plasma concentrations. Ceftiofur activity using a microbiologic assay significantly underestimated plasma concentrations of DCA. The MIC of ceftiofur required to inhibit growth of 90% of isolates of Escherichia coli , Pasteurella spp, Klebsiella spp, and β-hemolytic streptococci was <0.5 μg/mL. Intravenous administration of ceftiofur sodium at the rate of 5 mg/kg every 12 h would provide sufficient coverage for the treatment of susceptible bacterial isolates.  相似文献   

19.
Ceftiofur hydrochloride was tested for effectiveness against induced colibacillosis in neonatal swine. In this model, pigs less than 12 hours old were inoculated via stomach tube with a virulent, K99+, nalidixic acid-resistant strain of Escherichia coli. Six hours after challenge exposure, 1 dose of ceftiofur was administered either IM or orally in experiment 1 and orally only in experiment 2. Mortality, shedding of bacteria, fecal consistency scores, and body weight changes were monitored for 10 days. In experiment 1 (n = 383 pigs), all treatments at dosage that ranged between 0.5 and 64.0 mg of ceftiofur/kg of body weight significantly (P less than 0.001) reduced mortality, bacterial shedding, and diarrhea and increased weight gain, compared with findings in untreated controls. There were no detectable differences between oral and IM routes, except that there was greater reduction in bacteria shedding associated with the oral route of administration. In experiment 2 (n = 505 pigs), ceftiofur was administered orally either once at 6 hours after challenge exposure or twice at 6 and at 48 hours after the first dose. Dosage of ceftiofur was 0, 5, 10, 20, 30, or 60 mg/kg administered once, or half the same dose was administered at each of 2 times. At the optimal dosage (10 mg/kg), a single dose was as effective as 2 doses. The single administration at all dosages reduced mortality, bacterial shedding, and diarrhea scores and increased body weight gain, compared with findings in untreated pigs (P less than 0.01). In this induced infection model, the optimal treatment dosage was determined to be 10 mg/kg administered once.  相似文献   

设为首页 | 免责声明 | 关于勤云 | 加入收藏

Copyright©北京勤云科技发展有限公司  京ICP备09084417号