Idkaidek Nasir, Arafat Tawfiq
College of Pharmacy and Jordan Center for Pharmaceutical Research, University of Petra, Amman, Jordan.
Mol Pharm. 2012 Aug 6;9(8):2358-63. doi: 10.1021/mp300250r. Epub 2012 Jul 23.
The aims of this work were to study pharmacokinetics of randomly selected drugs in plasma and saliva samples in healthy human volunteers, and to introduce a Salivary Excretion Classification System. Saliva and plasma samples were collected for 3-5 half-life values of sitagliptin, cinacalcet, metformin, montelukast, tolterodine, hydrochlorothiazide (HCT), lornoxicam, azithromycin, diacerhein, rosuvastatin, cloxacillin, losartan and tamsulosin after oral dosing. Saliva and plasma pharmacokinetic parameters were calculated by noncompartmental analysis using the Kinetica program. Effective intestinal permeability (Peff) values were estimated by the Nelder-Mead algorithm of the Parameter Estimation module using the SimCYP program. Peff values were optimized to predict the actual average plasma profile of each drug. All other physicochemical factors were kept constant during the minimization processes. Sitagliptin, cinacalcet, metformin, tolterodine, HCT, azithromycin, rosuvastatin and cloxacillin had salivary excretion with correlation coefficients of 0.59-0.99 between saliva and plasma concentrations. On the other hand, montelukast, lornoxicam, diacerhein, losartan and tamsulosin showed no salivary excretion. Estimated Peff ranged 0.16-44.16 × 10(-4) cm/s, while reported fraction unbound to plasma proteins (fu) ranged 0.01-0.99 for the drugs under investigation. Saliva/plasma concentrations ratios ranged 0.11-13.4, in agreement with drug protein binding and permeability. A Salivary Excretion Classification System (SECS) was suggested based on drug high (H)/low (L) permeability and high (H)/low (L) fraction unbound to plasma proteins, which classifies drugs into 4 classes. Drugs that fall into class I (H/H), II (L/H) or III (H/L) are subjected to salivary excretion, while those falling into class IV (L/L) are not. Additional data from literature was also analyzed, and all results were in agreement with the suggested SECS. Moreover, a polynomial relationship with correlation coefficient of 0.99 is obtained between S* and C*, where S* and C* are saliva and concentration dimensionless numbers respectively. The proposed Salivary Excretion Classification System (SECS) can be used as a guide for drug salivary excretion. Future work is planned to test these initial findings, and demonstrate SECS robustness across a range of carefully selected (based on physicochemical properties) drugs that fall into classes I, II or III.
这项工作的目的是研究健康人类志愿者血浆和唾液样本中随机选择药物的药代动力学,并引入一种唾液排泄分类系统。口服给药后,收集西他列汀、西那卡塞、二甲双胍、孟鲁司特、托特罗定、氢氯噻嗪(HCT)、氯诺昔康、阿奇霉素、双醋瑞因、瑞舒伐他汀、氯唑西林、氯沙坦和坦索罗辛的唾液和血浆样本,采集时间为3 - 5个半衰期。使用Kinetica程序通过非房室分析计算唾液和血浆药代动力学参数。使用SimCYP程序通过参数估计模块的Nelder - Mead算法估计有效肠道渗透率(Peff)值。对Peff值进行优化以预测每种药物的实际平均血浆曲线。在最小化过程中,所有其他物理化学因素保持不变。西他列汀、西那卡塞、二甲双胍、托特罗定、HCT、阿奇霉素、瑞舒伐他汀和氯唑西林有唾液排泄,唾液和血浆浓度之间的相关系数为0.59 - 0.99。另一方面,孟鲁司特、氯诺昔康、双醋瑞因、氯沙坦和坦索罗辛未显示出唾液排泄。估计的Peff范围为0.16 - 44.16×10⁻⁴ cm/s,而所研究药物的血浆蛋白未结合分数(fu)报告范围为0.01 - 0.99。唾液/血浆浓度比范围为0.11 - 13.4,与药物蛋白结合和渗透率一致。基于药物的高(H)/低(L)渗透率和高(H)/低(L)血浆蛋白未结合分数,提出了一种唾液排泄分类系统(SECS),该系统将药物分为4类。属于I类(H/H)、II类(L/H)或III类(H/L)的药物会发生唾液排泄,而属于IV类(L/L)的药物则不会。还分析了来自文献的其他数据,所有结果均与所提出的SECS一致。此外,在S和C之间获得了相关系数为0.99的多项式关系,其中S和C分别是唾液和浓度无量纲数。所提出的唾液排泄分类系统(SECS)可作为药物唾液排泄的指导。计划未来的工作来测试这些初步发现,并证明SECS在一系列精心挑选的(基于物理化学性质)属于I类、II类或III类的药物中的稳健性。
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