期刊
CANCER CHEMOTHERAPY AND PHARMACOLOGY
卷 57, 期 3, 页码 275-281出版社
SPRINGER
DOI: 10.1007/s00280-005-0058-8
关键词
MS-275; histone deacetylase inhibitor; protein binding; equilibrium dialysis
MS-275 (MS-27- 275; 3-pyridylmethyl-N-{4[(2-aminophenyl)-carbamoyl]-benzyl-carbamate) is a histone deacetylase inhibitor under clinical development as an anticancer agent. Here, we examined the role of protein binding as a possible determinant of the pharmacokinetic behavior of MS-275. The distribution of MS-275 in plasma was studied in vitro using equilibrium dialysis and ex vivo in five cancer patients receiving the drug orally at a dose of 10 mg/m(2). The dialysis method uses a tracer amount of [G-H-3]MS-275 on a 96-well microdialysis plate with a 5-kDa cut-off membrane, and requires 250 mu l sample. The time to equilibrium was established to be within 5 h, and the mean unbound fraction of MS-275 (f(u)) over a presumed therapeutic concentration range in healthy volunteer human plasma was 0.188 +/- 0.0075 as compared to 0.168 +/- 0.0144 in cancer patients. The binding was concentration-independent, indicating a low affinity, possibly non-specific and non-saturable process. MS-275 was found to bind in decreasing order to plasma > alpha(1)-acid glycoprotein > albumin. Among 19 tested drugs, a slightly increased fu was observed in the presence of only ibuprofen (f(u), 0.236 +/- 0.001) and metoclopramide (f(u), 0.270 +/- 0.042), suggesting weakly competitive displacement from protein-binding sites (P < 0.01). Compared to humans, f(u) was significantly higher in plasma from mouse (0.376), rat (0.393), rabbit (0.355), dog (0.436), and pig (0.439) (P < 0.01), which may explain, in part, the species-dependent pharmacokinetic pro. le of MS-275 observed previously.
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