RE: Simultaneous vs sequential for modeling parent AND metabolites in pop PK

The appropriate approach is to fit parent compound and the metabolites simultaneously, since it can help uniquely define the PK parameters, especially the CL. As we know that CL is a lumped parameter without metabolite information. Sequential estimation is the approach when there is no better way to solve the problem in simultaneous fitting due to numerical problem. This is different situation from PK-PD fitting. In the situation if PD has impact on PK, also, simultaneous fitting is the way to go. xiaofeng Xiaofeng Wang, PhD Oncology, Novartis (862)778-8856 (o) "Xiao, Alan" <[EMAIL PROTECTED]> Sent by: [EMAIL PROTECTED] 12/09/2008 01:30 PM To "Bachman, William" <[EMAIL PROTECTED]>, <[email protected]> cc Subject RE: [NMusers] Simultaneous vs sequential for modeling parent AND metabolites in pop PK Dear All, Thanks for your response and I'm sorry for the confusion. I'm talking about the sequential/simultaneous modeling to fit parent concentrations AND metabolites in pop PK, not about PD data at all. That is for sequential approach, you develop a model to fit the parent data first and then fix the PK parameters for parents to develop a model to fit the metabolite. While, for simultaneous approach, you develop a model to fit both parent and metabolites simultaneously (to simultaneously estimate parameters for both parent and metabolites). Alan