PHARMACOKINETICS OF T-2588 IN PATIENTS WITH IMPAIRED RENAL FUNCTIONS
The pharmacokinetics of T-2525, an active form of a new oral cephem antibiotic T-2588, were studied in 4 healthy volunteers and 14 patients with various degrees of renal impairment after a single oral administration of 100 mg dose of T-2588. The endgeneous creatinine clearances (Ccr) of each subject...
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Published in: | CHEMOTHERAPY Vol. 34; no. Supplement2; pp. 150 - 157 |
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Main Authors: | , , , , , , , , , |
Format: | Journal Article |
Language: | Japanese |
Published: |
Japanese Society of Chemotherapy
30-04-1986
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Online Access: | Get full text |
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Summary: | The pharmacokinetics of T-2525, an active form of a new oral cephem antibiotic T-2588, were studied in 4 healthy volunteers and 14 patients with various degrees of renal impairment after a single oral administration of 100 mg dose of T-2588. The endgeneous creatinine clearances (Ccr) of each subject were used as indicator of renal function. Pharmacokinetic parameters were obtained following the one-compartment open model with lag phase in the absorption. The peak concentrations of T-2525 in serum were achieved 4 hours after administration without relation to the renal functions. The serum concentration of T-2525 increased in patients having the level of Ccr of 20 to 30ml/min. The mean serum half-life of T-2525 was calculated for 0. 83±0.02 hour in normal subjects and increased in patients along with increasing impairment of renal function. The excretion rate constant well correlated with Ccr (r=0.739, p<0.005). In normal subjects, 22.2±1.9% of the drug was excreted in the urine as T-2525 within the first 8 hours, and the urinary excretion rate declined gradually in patients as a degree of renal impairment advanced. In the patients with severely impaired renal function (Ccr of 20 to 30ml/min), the drug accumulation should be predicted by giving 100 mg oral dose of T-2588 repeated at interval of 8 hours, but not in patients who have the level of Ccr of 40 to 70ml/min. |
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ISSN: | 0009-3165 1884-5894 |
DOI: | 10.11250/chemotherapy1953.34.Supplement2_150 |