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In terms of parameter precision, the scenario incorporating data only within one dosing interval showed the worst results (V p /F = 313%, Q/F = 64.3%). Some scenarios including early trough samples yielded comparable outcomes (V p /F = 18.4%, Q/F = 32.1%) to the extended full-PK sampling scenario (V p /F = 15.9%, Q/F = 30.3%), which was the best case. The quality of distribution-related parameters was the major difference between scenarios. Conclusion In multiple-dose studies on drugs with delayed distributional equilibrium, information

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