Formulation Optimization Utilizing D-Optimal Experimental Design of Oral Capsules Containing Enteric-Coated Pellets of Lansoprazole and<i>in vivo </i>Bioequivalence

An optimized formulation of capsules containing Lansoprazole enteric-coated pellets using D-Optimal design with a polynomial statistical model were prepared by using Eudragit?L100 as an enteric coated polymer to provide resistance to simulated gastric acid dissolution in buffer media. D-Optimal experimental design was used to determine the optimal level for three coating layers that were applied to formulate the enteric-coated pellets including a drug loading layer, a sub-coating, and an outer enteric coating. Dissolution studies were performed on the prepared Lansoprazole capsules. Less than 5 percent of Lansoprazole was released in 60 minutes in an acidic dissolution medium (pH 1.2) and greater than 90 percent of active ingredient was released in the next 60 minutes in a buffer dissolution medium (pH 6.8). The Lansoprazole capsules were stable with no observable change in physico-chemical properties in accelerated and normal storage conditions for 6 and 18 months, respectively. The pharmacokinetic parameters Cmax, Tmax, AUC0-t, and AUC0-∞ were determined after administration of the D-Optimal design optimized capsules of LPZ to healthy beagle dogs and were statistically compared to Gastevin? capsules as a reference (KRKA, Slovenia) using the non-compartmental method with the aid of WinNonlin 5.2 software. The analysis of variance showed that the two formulations did not demonstrate bioequivalence using a 90% confidence interval range (80% - 120%) of Cmax, AUC0-t, and AUC0-∞. No significant difference in Tmax was found at the 0.95 significance level using the Wilcoxon signed-rank test. D-Optimal Experimental Design provided definitive direction for an optimal formulation of capsules containing enteric-coated pellets of lansoprazole loaded within the coating of pellets that provided similar bioequivalence to Gastevin.

三七总皂苷肠溶微丸的包衣液处方优选

目的:优选三七总皂苷肠溶微丸的包衣液处方。方法:采用单因素法,考察不同包衣材料比例、溶剂系统、包衣材料浓度、着色剂和增塑剂等对肠溶微丸外观、收得率、释放度等的影响,优化包衣液处方。结果:三七总皂苷肠溶微丸包衣液处方为尤特奇(EUDRAGIT)L100∶S100:1∶4,溶于75%乙醇后总浓度为6%,柠檬酸三乙酯相对尤特奇树脂用量为20%,柠檬黄用量为0.03%。结论:按优选出的包衣液处方制备的肠溶微丸表面光滑,圆整度好,色泽光鲜,收得率高,释放度符合要求。

三七总皂苷肠溶微丸和三七总皂苷对家兔动脉粥样硬化预防作用比较

目的:比较三七总皂苷(panax notoginsenoside,PNS)肠溶微丸和三七总皂苷对家兔实验性动脉粥样硬化的预防作用。方法:50只家兔随机分为空白对照组、动脉粥样硬化(atherosclerosis,AS)模型组、PNS原料药组、注射用血栓通(冻干)组和PNS肠溶微丸组,耳缘静脉注射牛血清白蛋白250 mg.kg-1后(空白对照组除外),分别喂食普通饲料+生理盐水、高脂饲料+生理盐水、高脂饲料+PNS原料药(30 mg.kg-1.d-1,ig)、高脂饲料+血栓通(15 mg.kg-1.d-1,肌肉注射)和高脂饲料+PNS肠溶微丸(30 mg.kg-1.d-1,ig)。于12周末耳缘静脉取血测定血脂含量,摘取主动脉观察病理学改变。结果:给药12周后,PNS原料药组、注射用血栓通(冻干)组和PNS肠溶微丸组能显著降低家兔总胆固醇(T-CHO),甘油三酯(TG)和低密度脂蛋白胆固醇(LDL-C)水平(P<0.01),升高高密度脂蛋白胆固醇(HDL-C)水平(P<0.01);注射用血栓通(冻干)组和PNS肠溶微丸组降低T-CHO,TG和LDL-C的效果优于PNS原料药组(P<0.01),升高HDL-C水平优于PNS原料药组(P<0.01);PNS肠溶微丸组降低LDL-C效果优于注射用血栓通(冻干)组(P<0.01)。主动脉病理结果表明:注射用血栓通(冻干)组和PNS肠溶微丸组均能减轻主动脉内膜病变程度(P<0.01),且两者差异没有统计学意义;PNS肠溶微丸组减轻主动脉内膜病变程度优于PNS原料药组(P<0.01)。结论:三七总皂苷肠溶微丸和三七总皂苷原料药均能降低AS模型家兔的血脂水平和减轻主动脉内膜病变程度,且前者预防作用优于后者。

三七总皂苷生物黏附微丸体外黏附性及在人工胃液中留存量考察

目的探讨不同生物黏附材料对三七总皂苷(PNS)微丸体外黏附性和在人工胃液中留存的影响。方法选择不同生物黏附材料,并进行相应组合制备PNS生物黏附微丸,通过组织留存量法测定PNS生物黏附微丸的体外黏附性,并采用HPLC测定黏附微丸在人工胃液中释放一定时间后留存于微丸中的PNS(三七皂苷R1,人参皂苷Rg1,人参皂苷Rb1)含量。结果以壳聚糖和壳聚糖-卡波姆组合为生物黏附材料制备的微丸在人工胃液中2 h留存量最大,分别是(27.60±7.45)%和(19.80±3.55)%(R1);(27.01±5.49)%和(19.67±1.39)%(Rg1);(47.07±6.26)%和(51.08±7.44)%(Rb1)。HPMC和HPMC-卡波姆组合黏附性最好,其次是壳聚糖和壳聚糖-卡波姆组合。结论以壳聚糖和壳聚糖-卡波姆组合为生物黏附材料制备的生物黏附微丸对PNS在人工胃液中降解具有一定的保护作用,且黏附性较好。

三七总皂苷肠溶微丸对动脉粥样硬化家兔肝脏的影响

目的研究三七总皂苷(PNS)肠溶微丸对动脉粥样硬化(AS)模型家兔肝细胞的影响。方法建立家兔AS模型,连续ig给予PNS原料药及不同剂量的PNS肠溶微丸,阳性药血栓通注射剂(冻干)采用肌肉注射给药。分别给予相应的药物干预后,通过测定各组兔肝脏脂肪变性的分级程度、肝系数,同时进行HE染色观察肝组织病理改变并进行结果分析,评价肝脏损伤程度和药物对AS模型家兔肝细胞的影响。结果与模型组比较,PNS肠溶微丸低剂量能明显降低肝脏脂肪变性及AS模型家兔的肝系数;PNS肠溶微丸低剂量的效果优于PNS原料药组。结论 PNS原料药及其制剂均能显著减轻肝脏脂肪变性程度及降低肝系数,且PNS肠溶微丸低剂量优于PNS原料药及血栓通注射剂(冻干)。