Clinical Aspects of Treatment with Tipranavir
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Clinical Aspects of Treatment with Tipranavir Dr Kevin Curry Boehringer Ingelheim, Bracknell, UK
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Clinical Aspects of Treatment with Tipranavir. Dr Kevin Curry Boehringer Ingelheim, Bracknell, UK. Profile and Pharmacokinetics. Tipranavir Profile. The first in a new generation of PIs Non-peptidic structure: less Hydrogen bonds gives flexible binding - PowerPoint PPT Presentation
Transcript of Clinical Aspects of Treatment with Tipranavir
Clinical Aspects of Treatment with Tipranavir
Dr Kevin CurryBoehringer Ingelheim, Bracknell, UK
Profile and Pharmacokinetics
Tipranavir Profile
• The first in a new generation of PIs
• Non-peptidic structure: less Hydrogen bonds gives flexible binding
• Retains in vitro activity against >90% of HIV-1 strains resistant to first generation PIs
• Potent in vitro activity against wild-type HIV-1 and HIV-2 strains
Tipranavir Profile
• Wild Type EC90 0.5-1.0 M
• Target Cmin for multiple PI resistant HIV-1
– 20 µM
– 10x Protein adjusted EC90 for multiple PI resistant HIV-1
Tipranavir Pharmacokinetics
• TPV exhibits linear pharmacokinetics
• TPV exposure is markedly enhanced by rtv
• TPV is a potent inducer of CYP3A– This is overwhelmed by rtv
ARV Naïve PatientsMean (+SD) Plasma Concentrations on Day 11 (SEDDS Formulation)
Time (h)
TP
V C
once
ntra
tion
(µM
)
0
40
60
80
100
120
140
180
200
240
220
160
20
0 1 2 3 4 5 6 7 8 9 10 11 12
TPV 1,200 mg + rtv 200 mg bidTPV 300 mg + rtv 200 mg bidTPV 1,200 mg bid
Target Cmin
PharmacokineticsConclusions
• All doses of TPV/rtv (except 250/200) had
median Cmin >20 µM
• TPV induction of P450 3A4 was fully reversed by rtv co-administration
• rtv 200 provided more consistent P450 inhibition regardless of TPV dose
Studies in ARV Naïve PatientsBI 1182.3
ARV Naïve PatientsStudy Design
• HIV-1 RNA 5,000 copies/mL
• CD4 count 50 cells/mm3
• Treatment arms:
– TPV 1200mg (SEDDS) bid
– TPV 300 mg (SEDDS) + rtv 200 mg bid
– TPV 1200 mg (SEDDS) + rtv 200 mg bid
-2
-1.5
-1
-0.5
03 5 8 11 15
TPV 1200 mg bid
TPV 300 mg bid + rtv 200 mg bid
TPV 1200 mg bid + rtv 200 mg bid
Day on Therapy
HIV
-1 R
NA
(lo
g1
0 co
pie
s/m
L)
-1.44 log
-1.63 log
-0.77 log
ARV Naïve PatientsMean Changes in Viral Load
Studies in Multiple PI FailureBI 1182.2
Multiple PI FailuresStudy Design
• Open-label, parallel groups
• HIV-1+, multi-PI–experienced, NNRTI-naive adults
• History of 2 or more PI-containing regimens
–No wash-out period
–No genotype or phenotype eligibility criteria
• Primary endpoint
–Mean plasma HIV-1 RNA reduction at 48 weeks
Plasma HIV-1 RNA(log10 copies/mL)
CD4+ T cell count(cells/mm3)
4.51(3.87–5.21)
314(38–1067)
4.46(3.68–5.47)
290(41–610)
Low Dose High Dose
Number of subjects 19 22
Multiple PI FailuresBaseline Values
32%
95%
53%
63%55%
91%
68%
50%44%
93%
61%56%
0
20
40
60
80
100
IDV SQV NFV RTV
Per
cen
t P
rio
r E
xper
ien
ce (
N =
41)
Low Dose High Dose Total
Multiple PI FailuresPrior PI Experience
Low Dose High Dose
TPV HFC 1200 mg bid+ rtv 100 mg bid
TPV HFC 2400 mg bid+ rtv 200 mg bid
TPV SEDDS 500 mg bid+ rtv 100 mg bid
+ EFV 600 mg qd+ 1 new NRTI
TPV SEDDS 1000 mg bid+ rtv 100 mg bid
+ EFV 600 mg qd+ 1 new NRTI
Most patients initially took TPV 300 mg (HFC), then switched to TPV 250 mg soft-gel capsules (SEDDS) when these became available. 7/41 received SEDDS alone.
Multiple PI FailuresDosing
Low Dose, ITT-MCF
High Dose, ITT-MCFLow Dose, AT-OC
High Dose, AT-OC
0
20
40
60
80
100
4 8 16 24 48
Per
cent
BLQ
93.8%
78.9%78.6%
50.0%
0Number of patients below detection
10 14 15 15 1510 14 15 15 158 12 13 11 118 12 13 11 11
Weeks
Multiple PI FailuresViral Load Reduction: BLQ<400
• TPV 500/100 and 1000/100 effectively suppressed VL in multiple-PI–experienced patients at 48 weeks
• Patients taking 1000/100 had a higher incidence of adverse events, considered undesirable for chronic administration– The primary AEs seen for both doses were GI
• SEDDS formulation was better tolerated than the HFC formulation
Multiple PI FailuresConclusions
Adverse Event and Laboratory Profiles
TPV 1200 mg
N=10
TPV 300 mg+rtv 200 mg
N=10
TPV 1200 mg+rtv 200 mg
N=11
n (%) n (%) n (%)
Fatigue 1 (10%) 3 (30%) 0 (0%)
Diarrhea 6 (60%) 3 (30%) 7 (64%)
Nausea 1 (10%) 0 (0%) 6 (54%)
Vomiting 1 (10%) 1 (10%) 2 (18%)
ARV Naïve Patients (1182.3) Adverse Events
Gastrointestinal
Diarrhea59% (15/24 Grade
1)
Nausea 31%
Vomiting17%
Non-gastrointestinal
Headache 39%
Fatigue 29%
Dizziness 27%Abnormal 27% dreams
Insomnia 24%
NB. Not all these AEs were considered TPV-related
Multiple PI Failure (1182.2) Most Common Adverse Events
Low Dose High Dose
GGT, n (%) 6 (31.6) 4 (18.2)
ALT 2 (10.5) 5 (22.7)
AST 0 3 (13.6)
TG 4 (21.1) 4 (18.2)
Cholesterol 2 (10.5) 2 (9.1)
Multiple PI Failure (1182.2) Laboratory Abnormalities
Tipranavir Conclusions
Co-administration with low dose rtv substantially enhances PK
BID dosing with rtv 100/200 achieves target Cmin
TPV induction on CYP450 is neutralized by rtv
Promising efficacy in PI failure patients
TPV/rtv is generally well tolerated
- GI AEs are DAIDS Grade 1 to 2, self limited, or controllable with OTC medications
