RE: enzyme turnover
Khaled,
You seem need another parameter. KENZ cannot be both a creation and a
death rate for A(3) (i.e. [mg/h] and [1/h]). Also, it is confusing the
way you use both masses and concentrations in your interaction terms. Do
you intend CL24 to be L h-1 mg-1?
John
John C Lukas
Strategic Consulting Services
Pharsight Corp.
line: + 33 492 726 495
cell: + 33 626 496 777
Quoted reply history
________________________________
From: [EMAIL PROTECTED] [mailto:[EMAIL PROTECTED]
On Behalf Of Khaled Nm
Sent: Wednesday, February 13, 2008 2:08 PM
To: [email protected]
Subject: [NMusers] enzyme turnover
Dear nmuser,
I had analyzed data set of a CYP- inhibitor agent using NONMEM ADVAN 6.
A two-comp. model was used to describe the parent and its metabolite
data sets sid by side to a hypothetical enzyme compartment. All
estimates are fine except the KENZ (enzyme turnover rate was about (2
hr-1) which is 100-fold the published value. my code is
$DES
C2=A(2)/V2 ; for parent
C4=A(4)/V4 ; for metab
DADT(1)= -KA*A(1)
DADT(2)=KA*A(1) - CL24*A(3)*C2
DADT(3)= KENZ - KENZ*A(3) - KIRR *C2 *A(3)
DADT(4)=CL24*A(3)*C2 - CL40*C4
If i use the Emax and IC50 mode, the result is similar. what is wrong
with my code ?
All suggesion are wellcome.
Regards
Khaled
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