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Estimation Of Volume Of Distribution In Humans From High Throughput Hplc-Based Measurements Of Human Serum Albumin Binding And Immobilized Artificial Membrane Partitioning

JOURNAL OF MEDICINAL CHEMISTRY(2006)

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Abstract
The volume of distribution (VD) in humans of 179 known drug molecules (acids, bases, and neutrals) has been modeled using two biomimetic-binding measurements. The phospholipid binding (log K (IAM)) and the plasma protein binding (log K (HSA)) have been calculated from gradient HPLC retention times on immobilized artificial membrane (IAM) and on human serum albumin (HSA) columns, respectively. The log VD values showed good correlation with the compounds' relative binding to IAM and HSA as follows: log VD = 0.44 log K (IAM) -0.22 log K (HSA) -0.66; n = 179, r(2) = 0.76, s = 0.33, and F = 272. It was also observed that positively charged molecules bind relatively more to IAM, while negatively charged ones bind more to HSA, in line with the empirical observation that bases tend to have a larger volume of distribution than acids. These results suggest that with the help of these two simple high throughput HPLC-based biomimetic binding measurements an important in vivo drug disposition property can be estimated for use in early drug discovery.
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