rtfNCA: NCA output to rtf file
In ncar: Noncompartmental Analysis for Pharmacokinetic Report
rtfNCA R Documentation
NCA output to rtf file
Description
This output NCA result in a rtf file.
Usage
rtfNCA(fileName = "Temp-NCA.rtf", concData, key = "Subject", colTime = "Time",
colConc = "conc", dose = 0, adm = "Extravascular", dur = 0,
doseUnit = "mg", timeUnit = "h", concUnit = "ug/L", down="Linear",
R2ADJ = 0, MW = 0, SS = FALSE, iAUC = "", excludeDelta = 1)
Arguments
fileName
file name to save
concData
concentration data table
key
column names of concData to be shown in the output
colTime
column name for time
colConc
column name for concentration
dose
administered dose
adm
one of "Bolus" or "Infusion" or "Extravascular" to indicate drug administration mode
dur
duration of infusion
doseUnit
unit of dose
timeUnit
unit of time
concUnit
unit of concentration
down
either of "Linear" or "Log" to indicate the way to calculate AUC and AUMC
R2ADJ
Minimum adjusted R-square value to determine terminal slope automatically
MW
molecular weight of drug
SS
if steady-state, this should be TRUE. AUCLST (AUClast) is used instead of AUCIFO (AUCinf) for the calculation of Vz (VZFO, VZO), CL (CLFO, CLO), and Vdss (VSSO).
iAUC
interval AUC information in a dataframe with "Name", "Start", and "End" columns
excludeDelta
Improvement of R2ADJ larger than this value could exclude the last point. Default value 1 is for the compatibility with other software. Author recommends to use excludeDelta option with about 0.3.
Value
CMAX
maximum concentration, Cmax
CMAXD
dose normalized Cmax, CMAX / Dose, Cmax / Dose
TMAX
time of maximum concentration, Tmax
TLAG
time to observe the first non-zero concentration, for extravascular administration only
CLST
last positive concentration observed, Clast
CLSTP
last positive concentration predicted, Clast_pred
TLST
time of last positive concentration, Tlast
LAMZHL
half-life by lambda z, ln(2)/LAMZ
LAMZ
lambda_z negative of best fit terminal slope
LAMZLL
earliest time for LAMZ
LAMZUL
last time for LAMZ
LAMZNPT
number of points for LAMZ
CORRXY
correlation of log(concentration) and time
R2
R-squared
R2ADJ
R-squared adjusted
C0
back extrapolated concentration at time 0, for bolus intravascular administration only
AUCLST
AUC from 0 to TLST
AUCALL
AUC using all the given points, including trailing zero concentrations
AUCIFO
AUC infinity observed
AUCIFOD
AUCIFO / Dose
AUCIFP
AUC infinity predicted using CLSTP instead of CLST
AUCIFPD
AUCIFP / Dose
AUCPEO
AUC % extrapolation observed
AUCPEP
AUC % extrapolated for AUCIFP
AUCPBEO
AUC % back extrapolation observed, for bolus IV administration only
AUCPBEP
AUC % back extrapolation predicted with AUCIFP, for bolus IV administration only
AUMCLST
AUMC to the TLST
AUMCIFO
AUMC infinity observed using CLST
AUMCIFP
AUMC infinity determined by CLSTP
AUMCPEO
AUMC % extrapolated observed
AUMCPEP
AUMC % extrapolated predicted
MRTIVLST
mean residence time (MRT) to TLST, for intravascular administration
MRTIVIFO
mean residence time (MRT) infinity using CLST, for intravascular administration
MRTIVIFP
mean residence time (MRT) infinity using CLSTP, for intravascular administration
MRTEVLST
mean residence time (MRT) to TLST, for extravascular administration
MRTEVIFO
mean residence time (MRT) infinity using CLST, for extravascular administration
MRTEVIFP
mean residence time (MRT) infinity using CLSTP, for extravascular administration
VZO
volume of distribution determined by LAMZ and AUCIFO, for intravascular administration
VZP
volume of distribution determined by LAMZ and AUCIFP, for intravascular administration
VZFO
VZO for extravascular administration, VZO/F, F is bioavailability
VZFP
VZP for extravascular administration, VZP/F, F is bioavailability
CLO
clearance using AUCIFO, for intravascular administration
CLP
clearance using AUCIFP, for intravascular administration
CLFO
CLO for extravascular administration, CLO/F, F is bioavailability
CLFP
CLP for extravascular administration, CLP/F, F is bioavailability
VSSO
volume of distribution at steady state using CLST, for intravascular administration only
VSSP
volume of distribution at stead state using CLSTP, for intravascular administration only
Author(s)
Kyun-Seop Bae <k@acr.kr>
See Also
help, txtNCA, pdfNCA
Examples
#rtfNCA(fileName="NCA-Theoph.rtf", Theoph, key="Subject", colTime="Time",
# colConc="conc", dose=320, doseUnit="mg", timeUnit="h", concUnit="mg/L")
#rtfNCA(fileName="NCA-Theoph.rtf", Theoph, key=c("Subject", "Wt"), colTime="Time",
# colConc="conc", dose=320, doseUnit="mg", timeUnit="h", concUnit="mg/L")
#rtfNCA(fileName="NCA-Indometh.rtf", Indometh, key="Subject", colTime="time",
# colConc="conc", adm="Infusion", dur=0.5, dose=25, doseUnit="mg",
# timeUnit="h", concUnit="mg/L")
ncar documentation built on Nov. 19, 2023, 9:06 a.m.
R Package Documentation
Browse R Packages
We want your feedback!
Note that we can't provide technical support on individual packages. You should contact the package authors for that.
| rtfNCA | R Documentation |
NCA output to rtf file
Description
This output NCA result in a rtf file.
Usage
rtfNCA(fileName = "Temp-NCA.rtf", concData, key = "Subject", colTime = "Time",
colConc = "conc", dose = 0, adm = "Extravascular", dur = 0,
doseUnit = "mg", timeUnit = "h", concUnit = "ug/L", down="Linear",
R2ADJ = 0, MW = 0, SS = FALSE, iAUC = "", excludeDelta = 1)
Arguments
fileName |
file name to save |
concData |
concentration data table |
key |
column names of concData to be shown in the output |
colTime |
column name for time |
colConc |
column name for concentration |
dose |
administered dose |
adm |
one of |
dur |
duration of infusion |
doseUnit |
unit of dose |
timeUnit |
unit of time |
concUnit |
unit of concentration |
down |
either of |
R2ADJ |
Minimum adjusted R-square value to determine terminal slope automatically |
MW |
molecular weight of drug |
SS |
if steady-state, this should be TRUE. AUCLST (AUClast) is used instead of AUCIFO (AUCinf) for the calculation of Vz (VZFO, VZO), CL (CLFO, CLO), and Vdss (VSSO). |
iAUC |
interval AUC information in a dataframe with "Name", "Start", and "End" columns |
excludeDelta |
Improvement of R2ADJ larger than this value could exclude the last point. Default value 1 is for the compatibility with other software. Author recommends to use |
Value
CMAX |
maximum concentration, Cmax |
CMAXD |
dose normalized Cmax, CMAX / Dose, Cmax / Dose |
TMAX |
time of maximum concentration, Tmax |
TLAG |
time to observe the first non-zero concentration, for extravascular administration only |
CLST |
last positive concentration observed, Clast |
CLSTP |
last positive concentration predicted, Clast_pred |
TLST |
time of last positive concentration, Tlast |
LAMZHL |
half-life by lambda z, ln(2)/LAMZ |
LAMZ |
lambda_z negative of best fit terminal slope |
LAMZLL |
earliest time for LAMZ |
LAMZUL |
last time for LAMZ |
LAMZNPT |
number of points for LAMZ |
CORRXY |
correlation of log(concentration) and time |
R2 |
R-squared |
R2ADJ |
R-squared adjusted |
C0 |
back extrapolated concentration at time 0, for bolus intravascular administration only |
AUCLST |
AUC from 0 to TLST |
AUCALL |
AUC using all the given points, including trailing zero concentrations |
AUCIFO |
AUC infinity observed |
AUCIFOD |
AUCIFO / Dose |
AUCIFP |
AUC infinity predicted using CLSTP instead of CLST |
AUCIFPD |
AUCIFP / Dose |
AUCPEO |
AUC % extrapolation observed |
AUCPEP |
AUC % extrapolated for AUCIFP |
AUCPBEO |
AUC % back extrapolation observed, for bolus IV administration only |
AUCPBEP |
AUC % back extrapolation predicted with AUCIFP, for bolus IV administration only |
AUMCLST |
AUMC to the TLST |
AUMCIFO |
AUMC infinity observed using CLST |
AUMCIFP |
AUMC infinity determined by CLSTP |
AUMCPEO |
AUMC % extrapolated observed |
AUMCPEP |
AUMC % extrapolated predicted |
MRTIVLST |
mean residence time (MRT) to TLST, for intravascular administration |
MRTIVIFO |
mean residence time (MRT) infinity using CLST, for intravascular administration |
MRTIVIFP |
mean residence time (MRT) infinity using CLSTP, for intravascular administration |
MRTEVLST |
mean residence time (MRT) to TLST, for extravascular administration |
MRTEVIFO |
mean residence time (MRT) infinity using CLST, for extravascular administration |
MRTEVIFP |
mean residence time (MRT) infinity using CLSTP, for extravascular administration |
VZO |
volume of distribution determined by LAMZ and AUCIFO, for intravascular administration |
VZP |
volume of distribution determined by LAMZ and AUCIFP, for intravascular administration |
VZFO |
VZO for extravascular administration, VZO/F, F is bioavailability |
VZFP |
VZP for extravascular administration, VZP/F, F is bioavailability |
CLO |
clearance using AUCIFO, for intravascular administration |
CLP |
clearance using AUCIFP, for intravascular administration |
CLFO |
CLO for extravascular administration, CLO/F, F is bioavailability |
CLFP |
CLP for extravascular administration, CLP/F, F is bioavailability |
VSSO |
volume of distribution at steady state using CLST, for intravascular administration only |
VSSP |
volume of distribution at stead state using CLSTP, for intravascular administration only |
Author(s)
Kyun-Seop Bae <k@acr.kr>
See Also
help, txtNCA, pdfNCA
Examples
#rtfNCA(fileName="NCA-Theoph.rtf", Theoph, key="Subject", colTime="Time",
# colConc="conc", dose=320, doseUnit="mg", timeUnit="h", concUnit="mg/L")
#rtfNCA(fileName="NCA-Theoph.rtf", Theoph, key=c("Subject", "Wt"), colTime="Time",
# colConc="conc", dose=320, doseUnit="mg", timeUnit="h", concUnit="mg/L")
#rtfNCA(fileName="NCA-Indometh.rtf", Indometh, key="Subject", colTime="time",
# colConc="conc", adm="Infusion", dur=0.5, dose=25, doseUnit="mg",
# timeUnit="h", concUnit="mg/L")
R Package Documentation
Browse R Packages
We want your feedback!
Note that we can't provide technical support on individual packages. You should contact the package authors for that.
Embedding an R snippet on your website
Add the following code to your website.
For more information on customizing the embed code, read Embedding Snippets.