Developing multiple high-throughput GLP methods for an investigational drug candidate in various matrices within a 96-well plate

被引：9

作者：

Zhang, Jun ^{[1
]}

Kim, Elaine J. ^{[1
]}

Ji, Qin C. ^{[1
]}

El-Shourbagy, Tawakol A. ^{[1
]}

机构：

[1] Abbott Labs, Dept Drug Anal, Abbott Pk, IL 60064 USA

来源：

RAPID COMMUNICATIONS IN MASS SPECTROMETRY | 2006年 / 20卷 / 24期

关键词：

D O I：

10.1002/rcm.2799

中图分类号：

Q5 [生物化学];

学科分类号：

071010 ; 081704 ;

摘要：

In early pharmaceutical product development, an investigational drug candidate is typically dosed to various species for toxicological and pharmacokinetic studies. Most of these studies require multiple analytical methods that have to be validated with good laboratory practice (GLP) prior to the application in regulated studies. Usually, these analytical methods are developed in either a serial or parallel approach. For either approach, the development of multiple analytical methods takes tremendous work from scientists and instruments, and thus is not cost-effective. In this respect, a new strategy has been developed for simultaneous GLP method development using liquid chromatographic separation and tandem mass spectrometric detection. This high-throughput approach allows system suitability, carryover, calibration curve, accuracy, precision, matrix effect and selectivity to be evaluated in one 96-well plate. The strategy has been successfully implemented for multiple investigational drug candidates at Abbott Laboratories. The methods developed with this strategy are accurate, precise, selective, robust and matrix-independent. As an example, ABT-279 was used to demonstrate the feasibility of this strategy. Copyright (c) 2006 John Wiley & Sons, Ltd.

引用

页码：3755 / 3760

页数：6

共 18 条

[1] Allanson JP, 1996, RAPID COMMUN MASS SP, V10, P811, DOI 10.1002/(SICI)1097-0231(199605)10:7<811::AID-RCM561>3.0.CO
[2] 2-Q
[3] Bonfiglio R, 1999, RAPID COMMUN MASS SP, V13, P1175, DOI 10.1002/(SICI)1097-0231(19990630)13:12<1175::AID-RCM639>3.3.CO
[4] 2-S
[5] HIGH-SPEED LIQUID-CHROMATOGRAPHY TANDEM MASS-SPECTROMETRY FOR THE DETERMINATION OF DRUGS IN BIOLOGICAL SAMPLES
COVEY, TR
LEE, ED
HENION, JD
[J]. ANALYTICAL CHEMISTRY, 1986, 58 (12) : 2453 - 2460
[6] FACTORS AFFECTING ELECTROSPRAY-IONIZATION OF EFFLUENTS CONTAINING TRIFLUOROACETIC-ACID FOR HIGH-PERFORMANCE LIQUID CHROMATOGRAPHY/MASS SPECTROMETRY
ESHRAGHI, J
CHOWDHURY, SK
[J]. ANALYTICAL CHEMISTRY, 1993, 65 (23) : 3528 - 3533
[7] DETERMINATION OF L-654,066, A NEW 5-ALPHA-REDUCTASE INHIBITOR IN PLASMA BY LIQUID-CHROMATOGRAPHY ATMOSPHERIC-PRESSURE CHEMICAL IONIZATION MASS-SPECTROMETRY
GILBERT, JD
OLAH, TV
BARRISH, A
GREBER, TF
[J]. BIOLOGICAL MASS SPECTROMETRY, 1992, 21 (07) : 341 - 346
[8] ATMOSPHERIC-PRESSURE IONIZATION MASS-SPECTROMETRY - DETECTION FOR THE SEPARATION SCIENCES
HUANG, EC
WACHS, T
CONBOY, JJ
HENION, JD
[J]. ANALYTICAL CHEMISTRY, 1990, 62 (13) : A713 - +
[9] Jemal M, 2000, BIOMED CHROMATOGR, V14, P422, DOI 10.1002/1099-0801(200010)14:6<422::AID-BMC25>3.0.CO
[10] 2-I

← 1 2 →