COMPARISON OF SINGLE-DOSE AND STEADY-STATE NADOLOL PLASMA-CONCENTRATIONS

被引:12
|
作者
KRUKEMYER, JJ
BOUDOULAS, H
BINKLEY, PF
LIMA, JJ
机构
[1] UNIV TENNESSEE,CTR HLTH SCI,COLL PHARM,DEPT CLIN PHARM,MEMPHIS,TN 38163
[2] OHIO STATE UNIV,COLL PHARM,DEPT PHARM PRACTICE,COLUMBUS,OH 43210
[3] OHIO STATE UNIV,COLL MED,DIV CARDIOL,COLUMBUS,OH 43210
来源
PHARMACEUTICAL RESEARCH | 1990年 / 7卷 / 09期
关键词
high-performance liquid chromatography (HPLC); nadolol; nonlinearity; pharmacokinetics; β-blocker;
D O I
10.1023/A:1015954108734
中图分类号
O6 [化学];
学科分类号
0703 ;
摘要
The pharmacokinetics of nadolol have been previously reported to be linear between single and steady-state dosing. Data from a study in our laboratory suggested greater than expected β-blockade with nadolol at steady state. Because the early potency studies were single-dose studies, we hypothesized there was a nonlinearity in nadolol pharmacokinetics which produced higher than expected plasma concentrations at steady state. Six normal volunteers from the previous study (steady state) volunteered to participate in the single-dose study. Plasma concentrations were determined for 24 hr following a single dose of nadolol, 80 mg. A simple, inexpensive, and accurate method for determination of nadolol in plasma or serum by HPLC with fluorometric detection is described. The AUCo–tau at steady state was greater than the AUC0–∞ following a single dose in five of the six subjects. The mean ratio of AUCss/AUCsd was 2.54. This value would be unity in the presence of linear pharmacokinetics. We conclude that the principle of superposition is not applicable for nadolol. © 1990, Plenum Publishing Corporation. All rights reserved.
引用
收藏
页码:953 / 956
页数:4
相关论文
共 50 条
  • [21] THE RELATIONSHIP OF STEADY-STATE HEPARIN INFUSIONS TO SINGLE-DOSE ADMINISTRATIONS
    MANION, CV
    COMP, PC
    WHITSETT, TL
    TAYLOR, F
    CLINICAL PHARMACOLOGY & THERAPEUTICS, 1981, 29 (02) : 264 - 264
  • [22] PHARMACOKINETICS OF THE ANTIARRHYTHMIC AGENT TIRACIZINE - STEADY-STATE KINETICS IN COMPARISON WITH SINGLE-DOSE KINETICS
    BERNDT, A
    OERTEL, R
    TERHAAG, B
    RICHTER, K
    GRAMATTE, T
    BIOPHARMACEUTICS & DRUG DISPOSITION, 1995, 16 (05) : 427 - 441
  • [23] PREDICTION OF PLASMA-CONCENTRATIONS OF MIANSERIN AND DESMETHYLMIANSERIN AT STEADY-STATE FROM THOSE AFTER AN INITIAL DOSE OF MIANSERIN
    OTANI, K
    MIHARA, K
    OKADA, M
    TANAKA, O
    KANEKO, S
    FUKUSHIMA, Y
    THERAPEUTIC DRUG MONITORING, 1993, 15 (02) : 118 - 121
  • [24] DIGOXIN TABLET BIOAVAILABILITY - SINGLE-DOSE AND STEADY-STATE ASSESSMENT
    PREIBISZ, JJ
    BUTLER, VP
    LINDENBA.J
    ANNALS OF INTERNAL MEDICINE, 1974, 81 (04) : 469 - 474
  • [25] SINGLE-DOSE AND STEADY-STATE PHARMACOKINETICS OF TOMOXETINE IN NORMAL SUBJECTS
    FARID, NA
    BERGSTROM, RF
    ZIEGE, EA
    PARLI, CJ
    LEMBERGER, L
    JOURNAL OF CLINICAL PHARMACOLOGY, 1985, 25 (04): : 296 - 301
  • [26] SINGLE-DOSE AND STEADY-STATE PHARMACOKINETICS OF FLUNARIZINE IN EPILEPTIC PATIENTS
    TREIMAN, DM
    DEGIORGIO, CM
    KAPETANOVIC, IM
    KUPFERBERG, HJ
    EPILEPSIA, 1986, 27 (05) : 649 - 649
  • [27] A COMPARISON OF ABSORPTION RATE MODELS IN THE PREDICTION OF STEADY-STATE PLASMA-CONCENTRATIONS DURING ORAL THEOPHYLLINE ADMINISTRATION
    PATERSON, CME
    HUDSON, SA
    JEFFERSON, GC
    JOURNAL OF CLINICAL PHARMACY AND THERAPEUTICS, 1987, 12 (01) : 39 - 46
  • [28] PREDICTABILITY OF VERAPAMIL STEADY-STATE PLASMA-LEVELS FROM SINGLE-DOSE DATA EXPLAINED
    WAGNER, JG
    CLINICAL PHARMACOLOGY & THERAPEUTICS, 1984, 36 (01) : 1 - 4
  • [29] MEAN STEADY-STATE PLASMA-CONCENTRATIONS OF LABETALOL IN PATIENTS UNDERGOING ANTIHYPERTENSIVE THERAPY
    SANDERS, GL
    ROUTLEDGE, PA
    WARD, A
    DAVIES, DM
    RAWLINS, MD
    BRITISH JOURNAL OF CLINICAL PHARMACOLOGY, 1979, 8 : S153 - S155
  • [30] URINARY DESIPRAMINE HYDROXYLATION INDEX AND STEADY-STATE PLASMA-CONCENTRATIONS OF IMIPRAMINE AND DESIPRAMINE
    SPINA, E
    ARENA, A
    PISANI, F
    THERAPEUTIC DRUG MONITORING, 1987, 9 (02) : 129 - 133
12345