TY - JOUR
T1 - Teicoplanin measurement in patients with renal failure
T2 - Comparison of fluorescence polarization immunoassay, microbiological assay, and high-performance liquid chromatographic assay
AU - Awni, W. M.
AU - St. Peter, W. L.
AU - Guay, D. R.P.
AU - Kenny, M. T.
AU - Matzke, G. R.
PY - 1991/11
Y1 - 1991/11
N2 - Characterization of antibiotic pharmacokinetics in patients with renal insufficiency may be complicated by interfering substances within the assay. We compared three different assays for teicoplanin in serum and dialysate of 10 hemodialysis and six continuous ambulatory peritoneal dialysis (CAPD) patients. The microbiological assay (micro) had a within-run and between-run coefficient of variation (%CV) of< 7.5% for concentrations ranging from 0.2 to 96 Üg/ml. The high-performance liquid chromatographic assay (HPLC) within-and between-run %CV was< 8% for concentrations ranging from 1 to 80 Üg/ml. The fluorescence polarization immunoassay (FPIA) within- and between-run %CV was< 7% for concentrations ranging from 5 to 100 Üg/ml. In serum of hemodialysis patients FPIA results were slightly higher than HPLC results: FPIA = 1.11 HPLC + 2.37 (0.975, n = 202), and FPIA concentrations in serum were also slightly higher than those measured by micro (FPIA = 1.21 micro – 1.57= 0.972, n = 161). The HPLC and micro serum results were also comparable in hemodialysis patients: micro = 0.92 HPLC + 2.89= 0.953, n = 160. However, in CAPD patients micro results were lower than HPLC results in serum (micro = 0.82 HPLC + 0.49= 0.981, n = 262). In peritoneal dialysate, HPLC values were 60% of the micro values. Thus, FPIA may be the optimal technique for therapeutic monitoring of teicoplanin in the clinical setting due to its simplicity, specificity, and good correlation to HPLC and micro.
AB - Characterization of antibiotic pharmacokinetics in patients with renal insufficiency may be complicated by interfering substances within the assay. We compared three different assays for teicoplanin in serum and dialysate of 10 hemodialysis and six continuous ambulatory peritoneal dialysis (CAPD) patients. The microbiological assay (micro) had a within-run and between-run coefficient of variation (%CV) of< 7.5% for concentrations ranging from 0.2 to 96 Üg/ml. The high-performance liquid chromatographic assay (HPLC) within-and between-run %CV was< 8% for concentrations ranging from 1 to 80 Üg/ml. The fluorescence polarization immunoassay (FPIA) within- and between-run %CV was< 7% for concentrations ranging from 5 to 100 Üg/ml. In serum of hemodialysis patients FPIA results were slightly higher than HPLC results: FPIA = 1.11 HPLC + 2.37 (0.975, n = 202), and FPIA concentrations in serum were also slightly higher than those measured by micro (FPIA = 1.21 micro – 1.57= 0.972, n = 161). The HPLC and micro serum results were also comparable in hemodialysis patients: micro = 0.92 HPLC + 2.89= 0.953, n = 160. However, in CAPD patients micro results were lower than HPLC results in serum (micro = 0.82 HPLC + 0.49= 0.981, n = 262). In peritoneal dialysate, HPLC values were 60% of the micro values. Thus, FPIA may be the optimal technique for therapeutic monitoring of teicoplanin in the clinical setting due to its simplicity, specificity, and good correlation to HPLC and micro.
KW - Fluorescence polarization immunoassay
KW - High-performance liquid chromatographic assay
KW - Microbiological assay
KW - Renal patients
KW - Teicoplanin
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U2 - 10.1097/00007691-199111000-00008
DO - 10.1097/00007691-199111000-00008
M3 - Article
C2 - 1837630
AN - SCOPUS:0025876175
SN - 0163-4356
VL - 13
SP - 511
EP - 517
JO - Therapeutic drug monitoring
JF - Therapeutic drug monitoring
IS - 6
ER -