New Drug Update: Whats in the pipeline

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New Drug Update: Whats in the pipeline

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Title: New Drug Update: Whats in the pipeline

1
New Drug UpdateWhats in the pipeline

Jean C. Lee, Pharm D, BCPS
McAuley Health Center
Saint Marys Health Care
Grand Rapids, MI

2
25 years of AIDS / 19 years of ARVs

Between 87 and 95, 4 antiretrovials were
launched.
Since 95, 24 new products have been introduced.

Aptivus
Truvada, Epzicom
Combivir
Viread
Epivir
Rescriptor
Hivid
Ziagen
Emtriva
Viramune
Sustiva
Trizivir
Zerit
Retrovir
Videx
87
91
92
94
95
96
97
98
99
00
88
89
90
01
02
03
93
04 05 06
RTI
Invirase
Viracept
Kaletra
Reyataz
NNRTI
Fortovase
Agenerase
Prezista
PI
Norvir
Multi-class Combination
Atripla
Crixivan
Lexiva
3
Whats in the Pipeline?
PI Brecanavir A-790742
NNRTI TMC-125 TMC-278 BILR 355
CXCR4 AMD 070 KRH 3955 KRH 3140
NRTI DAPD (Amdoxovir) Apricitabine GS9148
CCR5 Maraviroc Vicriviroc
Attachment / CD4 binding inhibitors TNX 355
Integrase Inhibitor MK 0518 GS 9137
Maturation Inhibitor PA-457 UK-201844
Fusion Inhibitor TRI-999 TRI-1144 T-651
4
NRTIs
5
Amdoxovir (DAPD)

(-)b-D-2,6-diaminopurine dioxolane
Guanosine analogue
Activity to HIV and HBV
PK
Half-life 7-8 hours
Suitable for bid dosing

D-diodolane guanine (DXG)
DAPD
Adenosine deaminase
Wang LH, et al. 8th CROI, Abstract 752 Wang LH,
et al. 7th CROI, Abstract 103
6
Amdoxovir Activity

Strains resistant to AZT/3TC, d4T/3TC (invitro)
Multi-NRTI resistant strains (codon 69ins)
Decreased susceptibility K65R and L74V

Lennerstrand J et al. 45th ICAAC. Abstract H-1092
7
DAPD-101 Study (Phase I)

Open label x 14 days, followed x 7 days

N90 VL 5000 250,000 copies/mL Naïve or
experienced x 6 mo
5 d/c from study
Experienced 49 Monotherapy (20) BID 200,
300, 500mg Add on (29) BID 300, 500mg
Naïve 41 Monotherapy BID 25, 100, 200, 300,
500mg QD 600mg

86 Male, 42 Caucasian, 39 African American
Mean age 38 years (19-57y)
BL CD4 362 cells/mm3 (49-1578), BL VL 4.53
log10 (3.02 5.79)

Thompson MA et al. AIDS 2005191607-15
8
DAPD-101 Study

Mean change from baseline in ART naïve and
experienced

Change in HIV-RNA from baseline (log10 copies/mL)
Thompson MA et al. AIDS 2005191607-15
9
Treatment experienced group

Add On Group
Median decrease from baseline
300mg -0.31 log10 copies/mL
500mg -0.65 log10 copies/mL (NS)
Monotherapy Add On Group
gt -0.5 log10 gt -1.0 log10
300mg 36 24
500mg 67 38
4 patients achieved lt400 copies/mL
3 in 500mg cohort

Thompson MA et al. AIDS 2005191607-15
10
Safety

43 (48) had 1 ADR (possibly related)
Most frequent ADR
Headache 11
Nausea 10
Diarrhea 10
No dose related ADRs
No reports of visual abnormalities

66 with 1 grade 1-4 treatment emergent lab
abnormality
Majority were Grade 1-2
None required dose adjustment
Grade 3-4 reports
Naïve 17
Experienced 28

Thompson MA et al. AIDS 2005191607-15
11
DAPD-150 Study
N18 Tx-experienced
Amdoxovir 300mg bid N8
Amdoxovir 500mg bid N10

Amdoxovir OBT 40 with gt 0.5 log10 copies/mL
decrease
11/18 discontinued
5 Lens opacities (visual acuity not affected)
4 Virological failure
2 Withdrew/ non-adherent

17 male, 18 Caucasian, median 40y
Median VL 4.41 log 10 copies/mL
Median CD4 326 cells/mm3
Background regimen optimized by investigator
Total 96 weeks, ongoing

Thompson M et al. 10th CROI, Abstract 554
12
ACTG 5118
Amdoxovir 300mg bid Placebo
T-20 OBR

Randomized, double-blinded, placebo controlled 24
week study
Study halted due to uncertainty of long term
development plan
Study was unblinded and subjects followed x 48
weeks
Data at 24 weeks reported (n18)
Baseline data
Median CD4 36 cells/mm3 (11-537)
Median VL 4.8 log10 copies/mL (3.5-6.3)
Average number of mutations NRTI 6 PI8
3 NNRTI resistance

Gripshover B et al. 12th CROI. Abstract 553
13
ACTG 5118 Efficacy / Safety (24wk)

Time-average AUC minus baseline
DAPD -1.1 log10 (95 CI 0.19-2.01)
Placebo -0.8 log10 (95 CI 0.15-1.45)
CD4 Response
DAPD 70 cells/mm3 (95 CI 35-105)
Placebo 54 cells/mm3 (95 CI 14-94)
Time to first ADR
no difference between groups
Mild decrease in CrCl - equal in both groups
No reports of ? lens opacity score

Gripshover B et al. 12th CROI. Abstract 553
14
ACTG 5165 DAPD Mycophenolate Mofetil
DAPD 500mg bid MMF Placebo N20
DAPD 500mg bid MMF 500mg bid N20
Vs.

Phase I/II, randomized, double-blinded placebo
controlled pilot study
Experienced patients
90 males, 55 Caucasian, 70 40-49y
BL VL 4.47 copies/mL
BL CD4 184 cells/mm3
Results
No difference between groups
DAPD -0.35 log10 copies/mL
DAPD MMF -0.24 log10 copies/mL
10 subjects with virological failure by week 2

Margolis D et al. 13th CROI. Abstract 517
15
Apricitabine SPD754

(-) dOTC (2-deoxy-3-oxa-4-thiocytidine)
Deoxycytidine analogue
Structurally similar to 3TC / FTC
Additive, slightly synergistic activity in
combination with other agents
Activity with strains with 184V and TAMS
PK supports bid dosing
Invitro data support low potential for
mitochondrial toxicity

Gu Z et al. Antimicrob Agents Chemother
200650625-31.
16
Apricitabine PK Study

Randomized, open-label, 3 way crossover
21 healthy volunteers

7 day washout
SPD754 600mg bid 3TC 300mg qd X 4 days
SPD754 600mg bid X 4 days
3TC 300mg qd X 4 days
Bethell R et al. 11th CROI. Abstract 138
17
Results

No difference in PK parameters
SPD754-TP ? 6-fold with 3TC
Interaction likely due to competition of same
phosphorylation enzymes

Bethell R et al. 11th CROI. Abstract 138
18
10 d Randomized Monotherapy trial
N63 Naïve patients CD4 gt250 cells/mm3 VL
5000-100,000 copies/mL
400mg / d 200mg bid N11
800mg /d 800mg qd 400mg bid N12
1200mg / d 1200mg qd 600mg bid N14
1600mg/d 800mg bid N13
Placebo N13
Cahn P et al. AIDS 2006201261-8
19
Results

All doses superior to placebo at day 7 and day 10
(plt0.001)
Reduction in plasma HIV-1 RNA

Log 10 HIV-1 RNA decline (copies/mL)
No clinically relevant changes in CD4 after 10 d
Cahn P et al. AIDS 2006201261-8
20
Results

All doses well tolerated
ADRs mild to moderate
Incidence similar in across all groups
Preliminary resistance results
No new mutations in RT likely to cause resistance

Cahn P et al. AIDS 2006201261-8
21
GS-9148 Nucleotide RTI

Cyclic adenosine monophosphate
Highly active against HIV-1 subtypes A - D
Mean EC50 13.1uM
Mitochondrial effects
Equivalent to TDF, ABC, FTC
Superior to d4T, ddI
Low lactate production
Low cytotoxicity to a variety of cell types,
including renal cells
PK supports once daily dosing

Cihlar T et al. 13th CROI Abstract 45 Ray A et
al. 13th CROI. Abstract 498
22
Unique resistance profile

Susceptibility
Full K65R other RT mutations, M184V, L74V
? with T69ins TAMS M184V
3.16 fold reduced with Q151M complex
Selects for rare K70E/N mutation in vitro

Cihlar T et al. 13th CROI Abstract 45 Ray A et
al. 13th CROI. Abstract 498
23
NNRTIs
24
Etravirine (TMC-125)

Diarylpyrimidine derivative with activity against
NNRTI resistant HIV-1
Molecular flexibility allows to accommodate
mutational changes in the binding pocket
EC50 for WT HIV-1 1.4 nM
Little or no loss of activity with key NNRTI
resistant variants
Strong in vitro activity (IC50 lt10nM)
Variants with K103N, V106A, Y181C, G190A/S

Andries et al. Antimicrob Agents Chemother
2004484680-6
25
Etravirine activity in naïve(A) experienced(B)
patients
Gruzdev B et al. AIDS 2003172487-94 Gazzard BG
et al. AIDS 200317F49-54
26
Etravirine PK

Metabolized by 3A4 , glucuronidation
TPV/r ? Etravirine exposure by 76
Coadministration not recommended
New 100mg formulation to be used
200mg bid 800mg bid

Scholler M et al. 3rd IAS. Abstract
TuPe3.1B11 Scholler M et al. 13th CROI. Abstract
583
27
Etravirine Comparison to PI based regimen
2 NRTI PI

PI naïve failing NNRTI regimen
Data analyzed at Week 12

vs.
2 NRTI Etravirine

After enrollment of first 54 patients at week 12
Proportion of patients achieving or maintaining
lt50 copies/mL favored the PI-based control group
Study was prematurely discontinued in Nov 2005

www.tibotec.com/news/detail/jhtml?itemnamenews_09
. Accessed Aug 1, 2006
28
Study C223 TMC125 in PatientsWith NNRTI and PI
Resistance
HIV RNA Change at 24 Weeks

Phase IIb study (n240)
HIV RNA 4.7 log10 copies/mL
CD4 99 cells/mm3
NNRTI resistance (fold change)
Efavirenz 41.4
Nevirapine 61.3
gt3 PI resistance mutations
Treatment arms
Active control
Best available regimen from licensed agents
TMC125 400 or 800 mg bid background regimen
Investigator selected NRTIs lopinavir/r
enfuvirtide

Active control
-0.19
-1.04
TMC125 400 mg bid
Log10 Copies/mL
-1.188
TMC125 800 mg bid
0 4 8 12 16
20 24
Weeks
CD4 Cell Count (cells/mm3)
TMC125 400 mg bid
48
Change From Baseline
47
TMC125 800 mg bid
18
Active control
0 4 8 12 16
20 24
Weeks
Plt0.05 vs active control.
Nadler J, et al. 10th EACS. Dublin, 2005.
Abstract LBPS3.7A.
29
C223 48 week results

patients achieving HIV-1 RNA lt400 copies/mL

Plt0.05 Plt0.001
?CD4 TMC125 (58-61cells/mm3) Control (13
cells/mm3) Common ADR diarrhea, rash, ISR,
pyrexia
Cohen C et al. 12th British HIV Association.
Abstract P2
30
Effect of Baseline Resistance on Response to
Etravirine

Each of the following mutations, always in
combination with up to 4 other mutations, was
associated with a mean FC gt 10
K101P, V179E, V179F, Y181I, Y181V, G190S, M230L
For V179E, V179F, G190S or M230L, the additional
mutations always included Y181C when the FC gt 10
No single NNRTI drug resistance mutation was
associated with FC gt 10
Required multiple mutations ( 4)

Vingerhoets J, et al. J Virol. 20057912773-12782
. Vingerhoets J, et al. CROI 2006. Abstract 154.
31
Study C203 Safety of TMC125 inPatients With
NNRTI and PI Resistance
Montaner J, et al. 10th EACS. Dublin, 2005.
Abstract LBPS3.7B.
32
Pilot study TMC 114 plus Etravirine 3 and 4
class ARV experienced patients

N 10 on novel combination of 114 / Etravirine
OB
PK No impact on 114/r levels modest reduction
on Etravirine levels
Week 12 Median -2.76 log decline
All gt 2 log decline
All had VL lt 400 c/mL
Median (range) CD4 increase was 87 (83-171)
cells/mm3
No SAE, lab events
Possible drug related AE mild diarrhea, HA, rash
All resolve with continuous dosing.

Boffito M, et al. 13th CROI, Denver, CO, February
5-8, 2006. Abst. 575c
33
TMC-278

Diarylpyrimidine NNRTI
EC50 for WT HIV-1 0.5nM
Little / no loss of activity with resistant virus
EC50 2.7nM (L100I K103N)
Active against 89 of 1500 resistant isolates
EC50 lt10nM
EFV 33 NVP 0
T1/2 34-55h
QD dosing
Minimal renal clearance

de Bethune MP et al. 12th CROI. Abstract 556
34
TMC-278 PK

Given with food
Provides modest ? in exposure (45)
Metabolized by CYP3A4
Rifampin ? AUC by 80
Ketoconazole ? AUC by 50

Hoetelmans R et al. 3rd IAS. Abstract
TuPe3.1B10 van Heeswijk R et al. 7th
International Workshop on Clinical Pharmacology o
f HIV Treatment. Abstract 74
35
TMC-278 Drug interactions

PK not affected when combined with TDF
TDF exposure ? by 24
Not clinically relevant
No dose adjustment necessary
Interaction with LPV/r cap
TMC278 AUC ? 52
No effect on LPV/r

Hoetelmans R et al. 3rd IAS. Abstract
WePe3.3C15 Hoetelmans R et al. 10th EAC. Abstract
PE4.3/1
36
TMC-278 Monotherapy study
HIV infected, naïve CD4 75-500 cells/mm3 VL
gt5000 copies/mL N47
Oral solution Treatment x 7 d Follow up x 30d
Placebo N11
TMC278 150mg/d N9
TMC278 25mg/d N-9
TMC278 100mg/d N9
TMC278 50mg/d N9
100 male, 94 Caucasian, Median VL 4.5
copies/mL (3.5-5.9) Median CD4 292 cells/mm3
(29-590)
Goebel F et al. 12th CROI. Abstract 160
37
Similar efficacy with all doses

Median change -1.2 (all groups)

Plt0.01
Median CD4 ? of 55 cells/mm3 after 7 days No
NNRTI resistant mutations detected at day 8
Goebel F et al. 12th CROI. Abstract 160
38
Safety Tolerability

Mild ADRs
TMC278 22 events Placebo 7 events
Primarily grade 1 ADR
1 grade 3 nausea
1 grade 1 rash on day 3 (resolved on day 7)

Goebel F et al. 12th CROI. Abstract 160
39
PIs
40
Brecanavir GW-640385

Non-peptidic PI
Binds tightly to HIV protease
IC50 WT 1.1 nM
Active against highly PI resistant variants
Low oral bioavailability
Use with RTV

Hazen R et al. 2nd IAS. Abstract 541 Reddy S et
al. 43rd ICAAC. Abstract A-1800
41
Study HPR10006

Brecanavir/rtv 300/100mg bid 2NRTIs (AZT,d4T,
ddI, 3TC, FTC)
48-week study
N31
6 had PI resistance
HIV RNA 4.71 log10 copies/mL
CD4 311 cells/mm3
HIV RNA change
(log10 copies/mL)
PI sensitive -3.3
PI resistant -2.2
HIV RNA ()
lt400 copies/mL 81
lt50 copies/mL 77
CD4 gain (cells/mm3) 84

Ward D, et al. 45th ICAAC. Washington, DC, 2005.
Abstract H-412.
42
Study HPR10006

At week 24
4 discontinuations
Most common ADRs
Fatigue 13
Nausea 10
Dyspepsia 10
? CK 10
? TG 6

Ward D, et al. 45th ICAAC. Washington, DC, 2005.
Abstract H-412.
43
Drug Interaction data TDF

N35 healthy volunteers
All meds were well tolerated
CrCl ? by 15mL/min
BCV/r inhibition of active tubular secretion may
account for some of the decreased TDF clearance
(-30)
No TDF dosage adjustment is required

Ford SL et al. 45th ICAAC. Washington DC.
Abstract A-1198 Ford SL et al. 7th International
Workshop on Clinical Pharmacology of HIV Therapy.
Lisbon, Portugal. Abstract 38
44
Drug Interactions

Minimal interaction with LPV/r
BCV/r and ATV exposure ?
Higher frequency of Grade 4 ?bilirubin for BCV/r
ATV
Clinical significance unknown
May require reduction of ATV dose

Ford SL et al. 7th International Workshop on
Clinical Pharmacology of HIV Therapy. Lisbon,
Portugal. Abstract 51 Ford SL et al. 7th
International Workshop on Clinical Pharmacology
of HIV Therapy. Lisbon, Portugal. Abstract 76
45
Integrase Inhibitors
46
HIV Integrase Mechanism
www.clinicaloptions.com/hiv
47
MK-0518

Metabolized by glucuronidation (UGT1A1)
Potential interaction with atazanavir
Not a CYP450 metabolite or inhibitor
No expected significant interactions with most
antiretrovirals
Cannot be boosted by ritonavir

www.merck.com/newsroom/press_releases/reasearch_an
d_development/2006_0209.html
48
MK-0518 Monotherapy study
N35 VL 5000 CD4 100 Treatment naive
MK 0518 600mg bid N8
Placebo N7
MK 0518 100mg bid N7
MK 0518 400mg bid N6
MK 0518 200mg bid N7
All arms similar at baseline Mean BL VL 4.7
copies/mL, CD4 425 cells/mm3 Fewer with AIDS
dx in placebo arm
Morales-Ramirez JO, et al. 10th EACS. Dublin,
2005. Abstract LBPS1/6.
49
HIV RNA Change at Day 10
HIV RNA Change at Day 10
50-57 lt400 copies/mL 13-29 lt50 copies/mL
-0.2
Log10 Copies/mL
-1.7
-1.9
-2.0
-2.2
100 200 400 600 Placebo
MK-0518 (mg bid)
Morales-Ramirez JO, et al. 10th EACS. Dublin,
2005. Abstract LBPS1/6.
50
MK-0518

Generally well tolerated
No serious ADR or discontinuations
All events mild, transient
No grade 3 / 4 lab abnormalities
1 patient with ?ALT at day 5, resolved at day 10
Most common ADR
Dizziness
Headache
Fatigue

Morales-Ramirez JO, et al. 10th EACS. Dublin,
2005. Abstract LBPS1/6.
51
MK-0518 Phase IIb (Protocol 005)
N167 VL 5000 CD4 50 Resistant to 1 NRTI,
NNRTI, PI
Multicenter, randomized, double blind
MK 0518 600mg bid OBR N42
Placebo OBR N7
MK 0518 200mg bid OBR N42
MK 0518 400mg bid OBR N42

Treatment arms similar at baseline
Mean duration of HAART 9-11 yrs
Mean VL 4.6-4.8 log10 copies/mL Mean CD4
220-283 cells/mm3
Use of ENF in OBR 33 to 38
Patients with no active PIs in OBR 84 to 98

Grinsztejn B, et al. 13th CROI, Denver, CO,
February 5-8, 2006. Abst. 159LB
52
MK-0518 Efficacy Results (Wk 16)

Change in HIV-RNA
MK 0518 -2.0 log10 copies/mL
Placebo -0.8 log10 copies/mL

Change in CD4
MK 0518 400mg 600mg arms
100 cells/mm3
Placebo 200mg arms
25 cells/mm3

Grinsztejn B, et al. 13th CROI, Denver, CO,
February 5-8, 2006. Abst. 159LB
53
MK-0518 Virologic Suppression Through Week 16
Grinsztejn B, et al. 13th CROI, Denver, CO,
February 5-8, 2006. Abst. 159LB
54
MK-0518 Adverse Events

ADRs similar to placebo
Most common ADR
Diarrhea, nausea, fatigue, ISRs, headache,
pruritus
Occurring in gt5 of 2 patients per arm

Grinsztejn B, et al. 13th CROI, Denver, CO,
February 5-8, 2006. Abst. 159LB
55
MK-0518 Adverse Events

5 Serious ADRs reported
Acute pancreatitis (secondary to OBT, 200mg)
Lipoatrophy (blinded)
Anemia, metabolic acidosis, renal insufficiency,
death (blinded)
Hepatomegaly, fever (600 mg arm)
Lacunar infarction (placebo arm)
Low frequency Grade 3 / 4 lab abnormalities

Grinsztejn B, et al. 13th CROI, Denver, CO,
February 5-8, 2006. Abst. 159LB
56
GS-9137 / JTK-303

Dihydroquinoline carboxylic acid
Strand transfer inhibitor
Structurally resembles quinolones
Activity
Inhibits HIV-1 replication in 8 subtypes (A-G,O)
Synergistic 3TC
Additive AZT, TDF, EFV, IDV, NFV

T1/2 5-6h
Food ? Cmax, AUC by 3 fold
Metabolized by CYP 3A
Moderate inducer of 3A
RTV ? exposure by 20 fold
Increasing T1/2 to 9h
Other drug interactions unknown

Sato M et al. J Med Chem 2006491506-8 Matsuzaki
Y et al. 13th CROI Denver, CO. Abstract 508
Kawaguchi I et al. 13th CROI Denver, CO. Abstract
580 DeJesus E et al. 13th CROI Denver, CO.
Abstract 160LB
57
Integrase Inhibitor GS-9137

Phase IIa, 10-day monotherapy, placebo controlled
N 40 HIV patients
Naïve (n15)
Off treatment (n25)
GS-9137 dosing
200, 400, 800 mg BID
800 mg QD
50 mg RTV 100 mg QD
Dose-dependent response
RTV boosting allowed lower, once-daily GS-9137
dosing
No serious adverse events

Once-daily dosing with ritonavir to be
investigated in phase II trial with experienced
patients

DeJesus E, et al. 13th CROI, Denver, CO, February
5-8, 2006. Abst. 160LB
58
Steady State PK
protein binding adjusted, wild type virus
DeJesus E, et al. 13th CROI, Denver, CO, February
5-8, 2006. Abst. 160LB
59
GS-9137 generally well tolerated

No serious ADRs
Similar frequency ADR, lab abnormalities
Mild diarrhea, nausea, headache, fatigue
Fatigue greater frequency in GS 9137 groups
No changes in QT interval
Grade 3/4 abnormalities

GS 9137 ? TG ? amylase
Placebo ? aminotransferase ? amylase ? CK
DeJesus E, et al. 13th CROI, Denver, CO, February
5-8, 2006. Abst. 160LB
60
Maturation Inhibitor
61
Bevirimat PA-457

Butulinic acid derivative
Phase II trials
Disrupts the final step in the processing of HIV
Gag protein.
Inhibits the conversion of the capsid precursor
(p25) to mature capsid protein (p24)
Release of non-infectious viral particles and the
termination of viral replication
Mutations conferring resistance to PA-457 map to
the p25 to p24 cleavage site

Li F et al. Proc Natl Acad Sci 200310013555-60
62
Viral Budding and Maturation Mechanism and
Inhibition
www.Clincialoptions.com/hiv
63
Bevirimat

IC50 for WT 10.3nM
Active against WT drug resistant HIV-1
Inactive against HIV-2
Synergy in combination with ARVs
Strongest with AZT
Half-life 60h
Suitable for QD dosing
Not metabolized or significantly inhibit CYP450
enzymes
Does not interact with human PGP

Li F et al. Proc Natl Acad Sci 200310013555-60 O
gundele A et al. 3rd IAS. Abstract
TuPe3.1B01 Martin DE et al. 11th CROI San
Francisco, CA. Abstract 545 Kilgore N et al. 13th
CROI Denver, CO. Abstract 509
64
Phase II 10-Day Dosing Study

Phase II monotherapy study
33 treatment-naïve patients
Baseline
HIV RNA 4.73 log10 copies/mL
CD4 441 cells/mm3
Randomized groups
Placebo
PA-457 25, 50, 100, 200 mg qd
No evidence of resistance
ADRs mild to moderate
Mostly GI
No grade 3/4 adverse events
1 poorly controlled HTN lacunar stroke ? related

HIV RNA Change at Day 10
-0.03
-0.05
-0.17
-0.48
P0.004
-1.03
Log10 Copies/mL
Plt0.0001
25 50 100 200
Placebo Bevirimat
Beatty G, et al. 45th ICAAC. Washington, DC,
2005. Abstract H-416d
65
General Entry inhibitors
66
HIV-1 Entry Inhibitors
67
HIV-1 Entry Inhibitors TNX-355

Humanized oral monoclonal Ab 5A8
IgG subtype 4
Recognizes unique epitope in domain 2 of the CD4
receptor
Inhibits post-HIV-CD4binding entry step
In vitro
Active against R5, X4-tropic HIV
Synergistic activity with ENF
Single dose showed at least -1.1log10 and dose
dependent increase in CD4.

Kuritzkes D, et al. J Infect Dis.
2004189286-291. Godofsky E, et al. ICAAC 2005.
Abstract LB26.
68
TNX-355 24 week interim results

48-week phase II study
3-class experienced (n82)
Treatment arms
OBR vs. TNX-355 OBR
15 mg/kg IV q2wks
10 mg/kg IV qwk x 8 wks, then 10 mg/kg q2wks
CD4 response
OBR 5 cells/mm3
10mg/kg 9 cells/mm3
15mg/kg 51 cells/mm3
Well tolerated, no serious ADR related to drug,
no ISRs
Results sustained to Wk 48

Norris D, et al. 45th ICAAC. Washington, DC,
2005. Abstract LB2-26 Tanox Inc. News Release May
2, 2006.
69
CCR5 Inhibitors
70
Vicriviroc

SCH-D / SCH 417690
Piperazine based CCR5 antagonist
Orally bioavailable 80
IC50 0.1 3 nM
Phase 1 trials showed -1.6 log10 VL reduction
T1/2 27h

Chen et al. 9th CROI, Seattle, WA. Abstract
396-T Schuermann D et al. 3rd IAS Rio de Janeiro,
Brazil. Abstract TuOa0205 Schurmann D, et al.
11th CROI, San Francisco, CA. Abstract 140LB.
71
PK Interactions Vicriviroc

Metabolized via CYP 3A4

Sansone A, et al. PK Workshop 2005. Abstract 85.
2. Sansone A, et al. PK Workshop 2005. Abstract
84. 3. Saltzman M, et al. IAS 2005. Abstract
TuPe3.1B05. 4. Saltzman M, et al. IAS 2005.
Abstract TuPe3.1B08.

72
14 day Monotherapy study
Phase II study, randomized, placebo-controlled
trial

N 92
Treatment-naive subjects CCR5-tropic virus
CD4 count gt 150 cells/mm³
HIV-1 RNA 3000 copies/mL
No baseline resistance to regimen compounds

Greaves W, et al. CROI 2006. Abstract 161LB.
73
Late Virologic Breakthrough

Median follow-up 31.8 weeks (1.0-53.8)
Resistance profile at breakthrough
22/26 had evaluable genotypes
22/22 had M184V/I
1 had M41L
No change in vicriviroc IC50 noted with virologic
breakthrough
Serious ADR
Vicriviroc 10-12
Placebo 4
Grade 3/ 4 ADR similar rate
DSMB ended this study

Greaves W, et al. CROI 2006. Abstract 161LB.
74
Maraviroc UK-427,857

Maraviroc inhibits HIV-1 gp120 binding to CCR5
coreceptor, thereby preventing gp160-CCR5
mediated cell-cell fusion
Maraviroc demonstrated no antagonistic effects
when coadministered with other antiretroviral
agents

Dorr P et al. Antimicrob Agents Chemother
2005494721-32
75
Maraviroc

Selective reversible binding to CCR5 receptor
2nM antiviral IC90 activity
Cross clade potency
Active against current class resistant HIV but
not CXCR4 virus
HIV strains resistant to Maraviroc does not lead
to class resistance

Westby et al. 12th CROI, Boston, MA. Abstract 96
76
Maraviroc PK

T1/2 13-17h
50 reduction in exposure with food
No effect on antiviral activity
Metabolized by CYP3A4
Does not inhibit or induce CYP450 enzymes

Abel S et al. 10th CROI. Boston, MA. Abstract
547 Fatkenheuer G et al. XV IAC. Bangkok,
Thailand. Abstract TuPeB4489
77
Maraviroc PK Interactions

No interaction between MVC and tipranavir/ritonavi
r1
Maraviroc AUC doubled with lopinavir/ritonavir2
? MVC dose by 50 when given with most PIs
Maraviroc AUC ? 50 with efavirenz2
? Cmax with NVP

Abel S, et al. EACS 2005. Abstract
LBPE4.3/15. Muirhead G, et al. CROI 2005.
Abstract 663.
78
10d Monotherapy-dose ranging study

Randomization of 80 HIV infected patients with
CCR5 tropic virus
CD4 gt250 cells/mm3
VL gt5000 copies/mL

Doses gt100mg/d had gt 1.0 log10 decrease
Small ? CD4 count with all doses
61/63 had CCR5 tropic virus at BL remained CCR5
tropic at follow up
1 reverted to CCR5 topic at day 40
1 persisted gt6 mo post study with no evidence of
clinical progression

Fatkenheuer G et al. XV IAC. Bangcock, Thailand.
Abstract TuPeB4489
79
Maraviroc well tolerated

Majority ADRs mild moderate
Asthenia, headache, dizziness
2 discontinuations, not treatment related
No clinically significant lab abnormalities or
effects on QT interval
Postural hypotension dose limiting AE in phase I
study
Higher rates vs. placebo with doses 600mg
Sporadic, clinically relevant ?transaminases
No dose relationship or elevation in bilirubin

Fatkenheuer G et al. XV IAC. Bangcock, Thailand.
Abstract TuPeB4489 McHale et al. 3rd IAS. Rio de
Janerio, Brazil. Oral TuOa0204
80
1 case of Hepatotoxicity

AZT/3TC Maraviroc 300mg qd
HCV ()
Undetectable HCV RNA
Radiologic evidence of underlying stenosis
Meds for hypergammaglobinemia and () ANA
Rash hepatotoxicity after 4 doses
Maraviroc d/cd, other potentially hepatotoxic
meds were continued (INH, TMP/SMX, acetaminophen,
LPV/r)
Liver transplant

Pfizer Inc. Press Release. December 3, 2005.
81
Maraviroc in Treatment naïve

Once daily dosing arm in treatment naïve subjects
was terminated due to inferior performance
relative to EFV based control arm.
Ongoing studies in R5 experienced and R5/X4
experienced patients

82
CXCR4 Inhibitors

Slower development than R5 inhibitors
No naturally occurring mutations leading to
absence of CXCR4
Deletion of CVCR4 ligand is lethal in mice
AMD3100 halted due to QT prolongation
AMD070 in currently in studies
Dose related increase in WBC
Preclinical studies KRH-3955 / KRH-3140
Active against X4 virus
Increase in WBC

Schols D et al. 12th CROI. Boston, MA. Abstract
545 Tanaka Y et al. 13th CROI. Denver, CO.
Abstract 49LB
83
CCR5 / CXCR4 tropism
84
Chemokine Coreceptor Antagonists

HIV can enter the cell via various chemokine
coreceptors
R5 vs X4 virus
Mixed and dual-tropic populations
Start with CCR5 virus, over time change to CXCR4
virus
? Progression of disease
Relationship between viral tropism and disease
progression

85
Prevalence of Coreceptor Tropism

Demarest J, et al. ICAAC 2004. Abstract H-1136.
2. Brumme ZL, et al. J Infect Dis.
2005192466-474. 3. Moyle GJ, et al. J Infect
Dis. 2005191866-872. 4. Melby T, et al.
CROI 2006. Abstract 233.
5. Wilkin T, et al. CROI 2006. Abstract 655.

86
HIV Tropism and Disease Progression
Courtesy GSK interactive CD "Exploring an
allosteric world CCR5 entry inhibitors and HIV"
87
Baseline CD4 strongest predictor of X4 phenotype
Harrigan PR et al. XV IAC. Bangkok, Thailand.
Abstract MoPeB3117
88
Dual tropism Emergence With Maraviroc
Lewis ME, et al. ICAAC 2004. Abstract 584b.
89
Challenges with CCR5 / CXCR4 inhibitors