RESUMO
Understanding and manipulation of surface impedance in graphene hybrid structure is a significant issue for applications of graphene-based optoelectronics devices. In order to achieve this purpose in the terahertz region, analytical expressions for the impedances of metasurface were derived, which allows us to easily understand the relationship between physical dimensions and impedance. Simulation results show an excellent agreement with the analytical predictions. In addition, we focus on the synthetic impedance when square patch and graphene sheet joined together, discuss the influence of the size of metasurface as well as chemical potentiality as for graphene on the synthetic impedance. Based on these results, a number of absorbers as well as optical devices can be designed that utilize impedance metasurfaces.
RESUMO
The bioavailability of clopidogrel bisulfate (CAS 135046-48-9) form I was compared with that of clopidogrel bisulfate form II in 12 male Sprague-Dawley rats. The rats, randomly divided into two groups, received a single oral dose of 8 mg/kg clopidogrel (CP) bisulfate form I and form II, respectively, under fasting condition. The plasma concentrations of CP and its inactive carboxylic acid metabolite (CAS 144457-28-3, IM) were simultaneously determined by a sensitive, specific LC-MS/MS method. The pharmacokinetic parameters included C(max), T(max), t1/2, AUC(0-t), AUC(0-infinity). The AUC(0-infinity) of CP was 13.78 +/- 0.67 and 11.46 +/- 1.98 ng/ mL x h for CP form I and form II, respectively. The AUC(0-infinity) of IM was 33.08 +/- 5.76 and 21.67 +/- 8.95 microg/mL x h for CP form I and form II, respectively. The maximum plasma concentration (C(max)) of CP was 3.81 +/- 0.54 ng/mL for CP form I and 3.18 +/- 0.31 ng/mL for CP form II, the C(max) of IM was 3.42 +/- 0.41 and 2.08 +/- 0.68 microg/ mL for the CP form I and form II, respectively. There was an obvious difference between form I and form II for C(max) and the area under the plasma concentration time curve for both CP and IM after a t-test. This study shows that CP form I has better bioavailability in rats than CP form II.
