CROSS-REACTIVITIES OF CYCLOSPORINE-G (NVA(2) CYCLOSPORINE) AND METABOLITES IN CYCLOSPORINE-A IMMUNOASSAYS

被引：0

作者：

YATSCOFF, RW ^{[1
]}

LANGMAN, LJ ^{[1
]}

LEGATT, DF ^{[1
]}

机构：

[1] UNIV ALBERTA,DEPT LAB MED & PATHOL,EDMONTON T6G 2B7,AB,CANADA

来源：

CLINICAL CHEMISTRY | 1993年 / 39卷 / 06期

关键词：

INTERMETHOD COMPARISON; VARIATION; SOURCE OF; CYCLOSPORINE; CALIBRATION; MONITORING THERAPY; IMMUNOSUPPRESSIVE DRUGS;

D O I：

暂无

中图分类号：

R446 [实验室诊断]; R-33 [实验医学、医学实验];

学科分类号：

1001 ;

摘要：

Immunoassays of cyclosporin A (CsA) have been routinely used to measure CsG. We investigated the cross-reactivities of CsG and its metabolites, as well as the proportion CsG constitutes in relation to total drug measured, for six CsG metabolites (GM1, GM9, GM4N, GM1c, GM1c9, GM19) in the following CsA assays: Sandimmune selective RIA (SS), Sandimmune nonselective RIA (NS), Cyclotrac SP-RIA (CT), fluorescence polarization immunoassay (FPIA), and enzyme immunoassay (EMIT(TM)). The cross-reactivity of CsG in these assays was as follows: SS, FPIA, CT, approximately 100%; NS, approximately 40%; EMIT, < 2%. The cross-reactivities of CsG metabolites were investigated in all assays except EMIT and varied among metabolites and assays. The most significant variance was found with the NS assay, where most of the metabolites exhibited cross-reactivities of > 40%. In contrast, in the SS, FPIA, and CT assays, cross-reactivites of < 5% were observed for most of the metabolites. The ranking of cross-reactivites of CsG metabolites in the assays is SS = CT < FPIA < NS. The degree of cross-reactivity did not change significantly when the SS, CT, and FPIA assays were calibrated with CsG instead of CsA-whether parent CsG was present or not. The data suggest that the SS, CT, and FPIA methods would be suitable for the routine monitoring of CsG.

引用

页码：1089 / 1092

页数：4

共 13 条

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YATSCOFF, RW
HONCHARIK, N
LUKOWSKI, M
THLIVERIS, J
CHACKOWSKY, P
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CLINICAL CHEMISTRY, 1993, 39 (02) : 213 - 217
[2] COMPARISON OF CYCLOSPORINE-G (NVA(2)-CYCLOSPORINE) CONCENTRATIONS MEASURED IN WHOLE-BLOOD BY MONOCLONAL FLUORESCENCE POLARIZATION IMMUNOASSAY, MONOCLONAL RADIOIMMUNOASSAY, AND HPLC
ANNESLEY, TM
COOMBS, RC
ORSULAK, PJ
CLINICAL CHEMISTRY, 1993, 39 (06) : 1050 - 1053
[3] WHOLE-BLOOD CYCLOSPORINE-G IN RENAL-TRANSPLANT RECIPIENTS DETERMINED BY 2 IMMUNOASSAYS AND LIQUID-CHROMATOGRAPHY
MCBRIDE, JH
KIM, SS
DANOVITCH, GM
RODGERSON, DO
REYES, AF
OTA, MK
CLINICAL CHEMISTRY, 1993, 39 (07) : 1415 - 1419
[4] STEADY-STATE CONCENTRATION OF CYCLOSPORINE-G (OG37-325) AND ITS METABOLITES IN RENAL-TRANSPLANT RECIPIENTS
LANGMAN, LJ
LEICHTMAN, AB
WEITZEL, WF
YATSCOFF, RW
CLINICAL CHEMISTRY, 1994, 40 (04) : 613 - 616
[5] CRITICAL ANALYSIS OF THE TOXICITY AND ACTIVITY OF CYCLOSPORINE-A METABOLITES
GARRAFFO, R
THERAPIE, 1992, 47 (04): : 311 - 317
[6] ANALYSIS OF WHOLE-BLOOD CYCLOSPORINE-G BY LIQUID-CHROMATOGRAPHY IN RENAL-TRANSPLANT RECIPIENTS
MCBRIDE, JH
KIM, SS
JOURNAL OF CLINICAL LABORATORY ANALYSIS, 1995, 9 (04) : 238 - 242
[7] STIMULATION OF PLATELET-MITOGEN INDUCED PROSTAGLANDIN I-2 SYNTHESIS IN PERIODONTAL TISSUE OF CYCLOSPORINE-A TREATED PATIENTS
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SINZINGER, H
WIENER KLINISCHE WOCHENSCHRIFT, 1995, 107 (09) : 278 - 282
[8] Cyclosporine and its metabolites before and 2 h post-dose: comparative measurements of a monoclonal and a polyclonal immunoassay
Vyzantiadis, T
Belechri, AM
Memmos, D
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Papadimitriou, M
CLINICAL TRANSPLANTATION, 2003, 17 (03) : 231 - 233
[9] PARALLEL BLOOD-CONCENTRATIONS OF 2ND-GENERATION CYCLOSPORINE METABOLITES AND BILIRUBIN IN LIVER GRAFT RECIPIENTS
CHRISTIANS, U
KOHLHAW, K
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SCHOTTMANN, R
LINCK, A
RINGE, B
SEWING, KF
THERAPEUTIC DRUG MONITORING, 1995, 17 (05) : 487 - 498
[10] Comparison of predose vs 2-h postdose blood metabolites/cyclosporine ratios in kidney and liver transplant patients
Fernández-Marmiesse, A
Hermida, J
Tutor, JC
CLINICAL BIOCHEMISTRY, 2000, 33 (05) : 383 - 386

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