Retention of structurally diverse drugs in human serum albumin chromatography and its potential to simulate plasma protein binding

被引：38

作者：

Chrysanthakopoulos, Marios ^{[1
]}

Giaginis, Costas ^{[1
]}

Tsantili-Kakoulidou, Anna ^{[1
]}

机构：

[1] Univ Athens, Sch Pharm, Dept Pharmaceut Chem, GR-15771 Athens, Greece

来源：

JOURNAL OF CHROMATOGRAPHY A | 2010年 / 1217卷 / 37期

关键词：

Biomimetic chromatography; Human serum albumin stationary phase; Plasma protein binding; Lipophilicity; Charged species; Linear free energy relationships; PERFORMANCE LIQUID-CHROMATOGRAPHY; IMMOBILIZED ARTIFICIAL MEMBRANE; CHIRAL STATIONARY PHASE; GRADIENT HPLC METHOD; LIPOPHILICITY ASSESSMENT; BASIC DRUGS; OCTANOL; HYDROPHOBICITY; PREDICTION; DISCOVERY;

D O I：

10.1016/j.chroma.2010.07.023

中图分类号：

Q5 [生物化学];

学科分类号：

071010 ; 081704 ;

摘要：

The retention behavior of 39 structurally diverse neutral, basic and acidic drugs was investigated on an HSA stationary phase using PBS buffer (pH 7.0) and acetonitrile or 2-propanol as organic modifiers. Extrapolated or directly measured log k(w) values as well as isocratic retention factors were correlated with plasma protein binding data taken from the literature. Retention factors determined in the presence of 10% acetonitrile led to high quality 1:1 correlation with apparent log K-HSA values. The derived reference equation was successfully validated using a secondary set of 24 drugs. Further analysis of HSA retention into more fundamental properties revealed the involvement of anionic species in solute-stationary phase interactions, expressed by the negatively charged fraction, besides the partitioning mechanism which was reflected by lipophilicity. Protonation of basic drugs, although less important, may also influence retention, leading to reduced partitioning into the HSA surface as a net effect, while it seems to have no effect on HSA binding. The above results were further confirmed by linear solvation energy relationships (LSER). (C) 2010 Elsevier B.V. All rights reserved.

引用

页码：5761 / 5768

页数：8

共 42 条

[21] ENANTIOSELECTIVE ASPECTS OF DRUG-ACTION AND DISPOSITION - THERAPEUTIC PITFALLS
JAMALI, F
MEHVAR, R
PASUTTO, FM
[J]. JOURNAL OF PHARMACEUTICAL SCIENCES, 1989, 78 (09) : 695 - 715
[22] QUANTITATIVE STRUCTURE-ENANTIOSELECTIVE RETENTION RELATIONSHIPS FOR THE CHROMATOGRAPHY OF 1,4-BENZODIAZEPINES ON A HUMAN SERUM-ALBUMIN BASED HPLC CHIRAL STATIONARY PHASE - AN APPROACH TO THE COMPUTATIONAL PREDICTION OF RETENTION AND ENANTIOSELECTIVITY
KALISZAN, R
NOCTOR, TAG
WAINER, IW
[J]. CHROMATOGRAPHIA, 1992, 33 (11-12) : 546 - 550
[23] Predicting plasma protein binding of drugs:: a new approach
Kratochwil, NA
Huber, W
Müller, F
Kansy, M
Gerber, PR
[J]. BIOCHEMICAL PHARMACOLOGY, 2002, 64 (09) : 1355 - 1374
[24] KROBOTH PD, 1984, CLIN PHARMACOL THER, V3, P379
[25] PARTITION COEFFICIENTS AND THEIR USES
LEO, A
HANSCH, C
ELKINS, D
[J]. CHEMICAL REVIEWS, 1971, 71 (06) : 525 - +
[26] ElogDoct:: A tool for lipophilicity determination in drug discovery.: 2.: Basic and neutral compounds
Lombardo, F
Shalaeva, MY
Tupper, KA
Gao, F
[J]. JOURNAL OF MEDICINAL CHEMISTRY, 2001, 44 (15) : 2490 - 2497
[27] MCMENAMY RH, 1958, J BIOL CHEM, V233, P1436
[28] Morris J.M., 2000, VIRTUAL SCREENING BI, P33
[29] MULLER WE, 1988, DRUG STEREOCHEMISTRY
[30] USE OF A HUMAN SERUM ALBUMIN-BASED STATIONARY PHASE FOR HIGH-PERFORMANCE LIQUID-CHROMATOGRAPHY AS A TOOL FOR THE RAPID-DETERMINATION OF DRUG PLASMA-PROTEIN BINDING
NOCTOR, TAG
DIAZPEREZ, MJ
WAINER, IW
[J]. JOURNAL OF PHARMACEUTICAL SCIENCES, 1993, 82 (06) : 675 - 676

← 1 2 3 4 5 →