Approccio terapeutico nel paziente pre-trattato

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Approccio terapeutico nel paziente pre-trattato

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Title: Approccio terapeutico nel paziente pre-trattato

1
Approccio terapeutico nel paziente pre-trattato

Ivano Mezzaroma
Dipartimento di Medicina Clinica
UOC Immunologia Clinica
Università di Roma La Sapienza

Roma, 24 marzo 2006
2
Reasons for Failure of Initial HAART

Inability to take regimen (or nonadherence) is
one primary reason for failure of initial therapy
Other causes have become more rare in current
practice
Inadequate potency
Interindividual pharmacologic variability ?
inadequate levels in some patients)
Drug-drug interactions now very rare causes

3
ICoNA Study Reasons for Failure of Initial HAART
8
Toxicity
n 25
Failure
Nonadherence
20
Other
n 61
58
n 182
14
n 44
d'Arminio Monforte A, et al. AIDS.
200014499-507.
4
Reasons for Failure Toxicity

Adverse effects are most common reason for
discontinuation
Develop a plan to help patients deal with side
effects
Minor common side effects may be as important
to the patient as major grade 3/4 events
Nausea, vomiting, abdominal discomfort or
cramping, and diarrhea are common reasons why
patients stop their medications
Most patients are asymptomatic when treatment is
started
Development of even minor symptoms can therefore
be distressing
Remind patients not to self-diagnose by
stopping one of their medications

5
Adherence

A major determinant of degree and duration of
viral suppression
Poor adherence associated with virologic failure
Optimal suppression requires 90-95 adherence
Suboptimal adherence is common

6
Predictors of Inadequate Adherence

Regimen complexity and pill burden
Poor clinician-patient relationship
Active drug use or alcoholism
Unstable housing
Mental illness (especially depression)
Lack of patient education
Medication adverse effects
Fear of medication adverse effects

7
Predictors of Good Adherence

Emotional and practical supports
Convenience of regimen
Understanding of the importance of adherence
Belief in efficacy of medications
Feeling comfortable taking medications in front
of others
Keeping clinic appointments
Severity of symptoms or illness

8
Improving Adherence

Establish readiness to start therapy
Provide education on medication dosing
Review potential side effects
Anticipate and treat side effects
Utilize educational aids including pictures,
pillboxes, and calendars

9
Improving Adherence

Simplify regimens, dosing, and food requirements
Engage family, friends
Utilize team approach with nurses, pharmacists,
and peer counselors
Provide accessible, trusting health care team

10
Adherence is Inversely Related to the Number of
Doses Per Day
Dose-timing adherence rates
Dose-taking adherence rates
P lt .001
P .008
P values not calculated
100
P .001
80
79
74
71
Mean dose-taking adherence ()
69
60
65
58
59
51
40
46
40
20
0
Overall
QD
BID
TID
QID
Overall
QD
BID
TID
QID
Studies of electronic monitoring of adherence

Dose-taking adherence appropriate number of
doses taken during the day (optimal adherence
variously defined as 70, 80, 90)
Dose-timing adherence doses taken at appropriate
time intervals, within 25 of the dosing interval
(e.g. BID should be taken 12 ? 3 hours apart)

Claxton et al., Clin Ther .20012312961310.
11
Patients Prefer QD Regimensto BID Regimens
68
of Patients ever forgetting to take HIV
medication
Patients ()
24
5
4 pills QD
1 morning, 1 evening
1 morning, 4 evening
Bass D, et al. XIV IAC, July 7-12, Barcelona,
2002, Abstract MoPe3290.
12
Changing TherapyConsiderations

Clinical status
HIV RNA level on 2 tests
CD4 T cell count
Remaining treatment options
Potential viral resistance
Medication adherence
Patient education

13
Changing Therapy Treatment Regimen Failure

Virologic failure
Incomplete virologic response HIV RNA gt400
copies/mL after 24 wks, gt50 after 48 wks
Virologic rebound repeated detection of HIV RNA
after viral suppression
Immunologic failure
CD4 increase of lt25-50 cells/µL in first year of
therapy
CD4 decrease below baseline, on therapy
Clinical failure
occurrence of HIV-related events (after gt3 months
on therapy excludes immune reconstitution
syndromes)

14
Treatment Regimen Failure Assessment

Review antiretroviral history
Physical exam for signs of clinical progression
Assess adherence, tolerability, pharmacokinetic
issues
Resistance testing (while patient is on
therapy)
Identify treatment options

15
Treatment Regimen Failure Assessment

Possible causes
Suboptimal adherence
Medication intolerance
Pharmacokinetic issues
Suboptimal drug potency
Viral resistance
Approach depends on cause of regimen failure and
remaining antiretroviral options

16
Treatment Regimen Failure Assessment

Therapeutic options
Clarify goals If extensive resistance, viral
suppression may not be possible, but aim to
reestablish maximal virologic suppression
Remaining ARV options
Base treatment choices on expected efficacy,
tolerability, adherence, future treatment
options, past medication history, and resistance
testing

17
Virologic Failure Changing an ARV Regimen (1)

General principles
Prefer at least 2 fully active agents to design a
new regimen
Determined by ARV history and resistance testing
If 2 active agents are not available, consider
ritonavir-boosted PI plus optimized ARV
background, and/or reusing prior ARVs to provide
partial activity
Consider potent ritonavir-boosted PI and a drug
with a new mechanism of action (e.g., entry
inhibitor) plus an optimized ARV background may
have significant activity

18
Virologic Failure Changing an ARV Regimen (2)

General principles (2)
In general, 1 active drug should not be added to
a failing regimen because drug resistance is
likely to develop quickly. In some patients with
advanced HIV and few treatment options, this may
be considered to reduce the risk of immediate
clinical progression.
Consult with experts

19
Treatment-Experienced Patients Goals of Therapy

Limited prior treatment
Maximum viral suppression
Consider early change to prevent further
resistance mutations
Extensive prior treatment
Preservation of immune function
Prevention of clinical progression
Balance benefits of partial viral suppression
with risk of additional resistance mutations

20
Changing Therapy Treatment Options

Limited prior treatment with low HIV RNA
Intensification (e.g., tenofovir)
Pharmacokinetic (PK) enhancement
Change to new regimen

21
Changing Therapy Treatment Options

Limited prior treatment with single drug
resistance
Change 1 drug
PK enhancement
Change to new regimen

22
Changing Therapy Treatment Options

Limited prior treatment with gt1 drug resistance
Change drug classes and/or add new active drugs

23
Changing Therapy Treatment Options

Prior treatment with no resistance identified
Consider nonadherence or possibility that patient
was off medications at time of resistance test
Consider resuming same regimen or starting new
regimen and repeat resistance testing early (2-4
wks)

24
Changing Therapy Treatment Options

Extensive prior treatment with resistance
Avoid adding single active drug
Seek expert advice
If few or no treatment options, consider
continuing same regimen. Other possible
strategies
PK enhancement
Therapeutic drug monitoring
Retreatment with prior medications
Multidrug regimens (limited by complexity,
tolerability)
New ARV drugs, e.g., enfuvirtide, investigational
drugs
Treatment interruptions not recommended

25
Current Guidelines for Resistance Testing
DHHS1 IAS-USA2 EuroGuidelines 3
Primary Infection Recommend Recommend Recommend
PEP (Source Pt) Recommend
Chronic (lt 2 years) Consider Recommend Recommend/Consider
Treatment Failure Recommend Recommend Recommend
Pregnancy Recommend Recommend
Pediatric Recommend
Only if mother is viremic Only if mother was
viremic and on treatment at time of birth
1. DHHS. Guidelines for the Use of Antiretroviral
Agents in HIV-Infected Adults and Adolescents.
March 23, 2004. 2. Hirsch MS, et al. Clin Infect
Dis. 200337113-128. 3. Miller V, et al. AIDS.
200115309-320.
26
Testing for Drug Resistance

Recommended in case of virologic failure, to
determine role of resistance and maximize the
number of active drugs in a new regimen
Combine with obtaining a drug history and
maximizing drug adherence
Research supports use in certain settings
Perform while patient is taking ART (or within 4
weeks of regimen discontinuation)

27
Drug Resistance Testing Limitations

Lack of uniform quality assurance
Relatively high cost
Insensitivity for minor viral species (lt10-20)

28
Interruption of Antiretroviral Therapy

Intolerable side effects
Drug interactions
First trimester pregnancy
Poor adherence
Unavailability of drugs
Many other possible causes

29
Interruption of Antiretroviral Therapy Planned

Structured (supervised) treatment interruption
(STI)
Insufficient data to recommend STI research
ongoing
Possible risks decline in CD4 count, disease
progression, increase in HIV transmission,
development of resistance
Possible benefits reduction in drug toxicities,
preservation of future treatment options

30
Interruption of Antiretroviral Therapy Planned

Several scenarios
Patients who started ART during acute HIV
infection
Optimal duration of treatment is unknown studies
ongoing
Women who started ART during pregnancy to
decrease risk of mother-to-child transmission
If pretreatment CD4 is above currently
recommended ART starting levels and patient
wishes to stop therapy after delivery

31
Interruption of Antiretroviral Therapy Planned

Patients with chronic infection with viral
suppression and CD4 above levels recommended for
starting therapy
Started ART with CD4 above currently recommended
starting levels
Started ART at lower CD4 but now with stable CD4
above recommended starting levels
Small short-term prospective clinical trials
suggest safety long-term studies ongoing
CD4 decline after treatment interruption is
related to pretreatment CD4 nadir

32
Interruption of Antiretroviral Therapy Planned

Patients with treatment failure, extensive ARV
resistance, and few available treatment options
Partial virologic suppression from ART has
clinical benefit
Not recommended outside clinical trial setting

33
Interruption of Antiretroviral Therapy

Stop all antiretroviral medications at once
efavirenz and nevirapine have long half-lives
consider stopping these before other agents
In patients with hepatitis B who are treated with
emtricitabine, lamivudine, or tenofovir,
discontinuation of these may cause hepatitis
exacerbation
Monitor closely

34
Optimal Use of Boosted PIs in Treatment-Experience
d Patients
35
Goals of Therapy With MDR HIV

Patients with access to 2 active agents
Complete viral suppression
Patients with access to lt 2 active agents
Reduce viral load by 1 log10 copies/mL
Stabilize CD4 cell counts
Minimize drug toxicity
Minimize mortality
Minimize accumulation of additional mutations
that could cause resistance to drugs in
development

36
Saquinavir/Ritonavir

MaxCmin studies
Large, multinational, randomized trials comparing
boosted SQV with other boosted PIs in drug-naive
and drug-experienced patients also receiving 2
NRTIs and/or NNRTIs
MaxCmin 1 IDV/RTV 800/100 mg BID vs SQV/RTV
1000/100 mg BID1
Similar rate of virologic failure between
treatments at Week 48 (27 vs 25)
Adverse events more frequent in IDV/RTV arm
When switching from randomized treatment because
of toxicity considered as failure, SQV/RTV
superior (49 vs 34, P .009)
MaxCmin 2 LPV/RTV 400/100 mg BID vs SQV/RTV
1000/100 mg BID2
Found LPV/RTV superior at Week 48
Risk of virologic failure and treatment
discontinuation greater in SQV/RTV arm

1. Dragsted UB, et al. J Infect Dis.
2003188635-642. 2. Youle M, et al. IAS 2003.
Abstract LB23.
37
CONTEXT FPV/RTV vs LPV/RTV in PI-Experienced
Patients

Greater number of virologic failures in FPV/RTV
arms compared with LPV/RTV arm
Once-daily arm underperformed compared with
twice-daily arms
Twice-daily FPV/RTV failed to meet
protocol-defined threshold for noninferiority to
LPV/RTV

70
61
58
60
50
50
46
50
37
40
Viral Suppression ()
30
20
10
0
LPV/RTV Twice Daily
FPV/RTV Once Daily
FPV/RTV Twice Daily
Intent-to-treat, missing equals failure analysis
Elston RC, et al. IAC 2004. Abstract MoOrB1055.
38
Lopinavir/Ritonavir

LPV/RTV vs NFV, plus d4T/3TC, in treatment-naive
patients1
67 vs 52 of patients had viral load lt 50
copies/mL at Week 48 (P lt .001)
In patients with viral load gt 400 copies/mL,
frequency of emergent PI-associated mutations
significantly lower with boosted PI
Supports theory that boosted PIs offer greater
genetic barrier to emergent resistance than
unboosted PIs
BMS 043 LPV/RTV vs ATV, plus NRTIs, in
PI-experienced patients2
LPV/RTV showed -0.3 log10 copies/mL greater
reduction in viral load than unboosted ATV at
Week 24 (P .0032)

1. Walmsley S, et al. N Engl J Med.
20023462039-2046. 2. Nieto-Cisneros L, et al.
Antivir Ther. 20038(suppl1)S212. Abstract 117.
39
In Combination Therapy, Only The Active Drugs
Count

Early HAART in NRTI-experienced patients often
amounted to serial monotherapy
New drugs (eg, PIs) added to a failing NRTI-based
regimen
Less sustained responses with only 1 active drug
TORO results demonstrated applicability of this
principle to the use of enfuvirtide (ENF)
Several recent studies demonstrate that in
triple-class-experienced patients, combining ENF
an active boosted PI improves response rate

40
TORO Virologic Response to Enfuvirtide OB
Regimen
Arastéh K, et al. IAC 2004. Abstract MoOrB1058.
41
TORO Importance of Combining ENF With an Active
Boosted PI
Miralles GD, et al. IDSA 2004. Abstract 921.
42
TORO Impact of Number of Active Agents on
Response
Henry K, et al. IAS 2002. Abstract LbOr19B.
43
RESIST-1 Response to TPV/r vs CPI/r
Hicks C, et al. ICAAC 2004. Abstract 1137a.
44
RESIST Impact of Enfuvirtide on Virologic
Response

ENF use comparable in both arms
27.1 TPV/r
22.2 CPI/r
ENF use improved treatment response in both arms
However, TPV/r superior to CPI/r with or without
ENF

Deeks S, et al. IAS 2005. Abstract WeFo0201.
45
Relationship of TPV Score to TPV Phenotype
Results and Response
Valdez H, et al. Resistance Workshop 2005.
Abstract 27.
46
POWER 1 Virologic Response to TMC114/r
Katlama C, et al. IAS 2005. Abstract WeOaLB0102.

47
POWER 1 Subgroup Analyses of Response to
TMC114/r 600/100 BID
Katlama C, et al. IAS 2005. Abstract WeOaLB0102.
48
TMC125 in Treatment-Experienced Patients

Open, phase 2a study
16 HIV-infected men
Failing efavirenz or nevirapine
Resistance to efavirenz
CD4 cell count 389 cells/mm3
Viral load 10,753 copies/mL
TMC125 900 mg BID continue NRTIs for 7 days
After 7 days, median 0.9-log decrease in viral
load

Gazzard BG, et al. AIDS. 200317F49-F54.
49
CCR5 Inhibitors in Development
1. Lalezari J, et al. ICAAC 2004. Abstract
H-1137b. 2. Schurmann D, et al. CROI 2004.
Abstract 140LB. 3. Pozniak AL, et al. ICAAC
2003. Abstract H-443.
50
Treatment Strategies in Experienced Patients
Role of NRTIs

Evidence for partial activity of NRTIs even with
key resistance mutations present, eg, 3TC and d4T
M184V can confer improved phenotypic
susceptibility to TDF and ZDV in viruses with
TAMs and K65R
TDF and D-d4FC active against virus strains with
TAMs
Both can select for K65R ZDV shows
hypersusceptibility
Strategic use of NRTI combinations possible
TDF - FTC - ZDV
TDF - ZDV - D-d4FC

1. Walmsley S, et al. CROI 2005. Abstract 580. 2.
Ruiz L, et al. CROI 2005. Abstract 679.
51
3TC Alone vs Treatment Interruption in Patients
Failing 3TC-Based HAART
Mean CD4 Decrease (ITT)
Mean VL Increase (ITT)
Weeks
2.0
3TC
TI
4
12
24
36
48
P .0015
0
1.5
-50
Mean Change in HIV-1 RNA (log10 copies/mL)
1.0
-100
Mean Change in CD4 Cell Count (cells/mm3)
-150
0.5
-200
-250
0
P NS
4
12
24
36
48
-300
Weeks

In contrast to treatment interruption arm, 3TC
alone resulted in
Smaller recovery in replication capacity
No further selection of resistance mutations

Castagna A, et al. IAS 2005. Abstract WeFo0204.
52
When To Use a New Drug, and When to Wait

Is there at least 1 new class available, and if
so, will it be well protected?
What is the expected prognosis with continued
nonsuppressive therapy?
What are the resistance consequences of continued
nonsuppressive therapy?
How can I maintain the right mutations without
allowing the wrong ones to emerge?
When will new drugs be available, and will they
be active against the patients virus?

53
Options If New Drugs Are Not Available

Multidrug salvage therapy ("mega-HAART")
Difficult due to problems with tolerability and
interactions
Dual-boosted PI therapy
SQV (1000 mg BID) LPV/r (400/100 mg BID)
encouraging responses at Week 48 (noncomparative
studies)
Can have intolerable GI effects ? risk of lipid
abnormalities
Pharmacologic interactions not always predictable
Nonsuppressive regimens
Risk of emergence of new resistance mutations
Potentially less response when new drugs approved
in same class

54
Options If New Drugs Are Not Available (cont)

Switch to a holding regimen
Maximal negative impact on viral fitness (ie,
replication capacity)
Minimal risk of added resistance
Monotherapy with 3TC or FTC
Over 6 months, lower virologic rebound and less
CD4 loss
M184V linked to other mutations, reduce emergence
of WT virus
Treatment interruption (TI)
No clear evidence of improved response after TI
Risk of rapid CD4 cell decline and increased
risk of OIs
Potentially dangerous in advanced disease (CD4 lt
200)

55
Continued Therapy in Patients With Virologic
Failure A Delicate Balance
Accumulate new mutations Develop resistance to
drugs in development
Maintain mutations Decrease fitness Delay
progression
56
Optimizing Adherence

Optimal adherence plays a pivotal role in
sustaining efficacy of ART
Influenced greatly by patient motivation and
knowledge but also by convenience and
tolerability of treatment regimen
Minimizing pill count and size, frequency of
dosing, and dietary requirements important in
supporting higher levels of adherence
Reducing adverse effects of therapy vital to
increased adherence
Most boosted PIs administered twice daily
ATV dosed once daily, but reduced efficacy with
extensive PI resistance
Less toxic, more convenient boosted PI regimens
can improve adherence, but cannot replace ongoing
patient education and adherence monitoring within
clinic

57
Pharmacology of Boosted PIs

High PI concentration can inhibit drug-resistant
virus and increase genetic barrier to wild-type
virus
RTV boosting improves exposure, increases
activity against resistant virus, improves
durability in naive patients
However, increased exposure may increase
toxicities
RTV inhibits cytochrome P450 isoenzymes such as
CYP 3A4
In addition to boosting PIs, other drugs patient
may be taking can be affected by this inhibition
Other drugs that inhibit or induce CYP 3A4 may
affect PI levels
EFV commonly used NNRTI that induces CYP3A4
Use of EFV in patients receiving boosted PIs may
cause drop in PI level and loss of activity if PI
dosage not increased appropriately

58
Pharmacology of Boosted PIs (cont)

Boosted PIs should not be combined until clinical
trials have determined potential for drug-drug
interactions
Non-HIV medications also interact with boosted
PIs
Rifampin can greatly reduce PI levels
Boosted PIs can dangerously increase
concentration of sildenafil
Must caution patients taking boosted PIs about
taking any new medications and address potential
interactions accordingly
Therapeutic drug monitoring (TDM) remains
somewhat controversial issue in routine
management of ART-treated patients
PI drug levels correlate with efficacy and
toxicities, but ability to effectively improve
patient care by measuring PI levels and adjusting
dosage unproven

59
Manipulating Dosage of Boosted PIs With
Ritonavir A Delicate Balance
Impact on adherence Risk of increased toxicity
Improves exposure Greater activity against
resistant virus
60
Boosted PIs and Drug Resistance

PIs may select for unique resistance patterns,
but multiple mutations are associated with
cross-resistance, reduced PI susceptibility
In PI-experienced patients, use whichever PI has
most remaining activity at appropriately high
exposure, utilizing RTV boosting
Optimizing other drugs in ARV regimen vital to
success of boosted PI in treatment-experienced
patients
Patients who have failed multiple prior regimens
have usually acquired widespread NRTI and NNRTI
resistance
To benefit from a new boosted PI, it is crucial
to add drug from a new class, such as fusion
inhibitor, ENF
Demonstrated in TORO, RESIST, and POWER studies

61
Appropriate Goals and Strategies for Highly
Experienced Patients

Primary ART goal for all HIV patients complete
viral suppression
Even in patients with multiple prior failures,
combination of boosted PI and ENF may reduce
HIV-1 RNA to undetectable levels
When complete HIV-1 RNA suppression cannot be
obtained, maintaining immunologic function,
preventing clinical deterioration are goals of
ART
Drug selection should be based on utility against
resistant virus, tolerability in patient
Patients with widespread resistance to all but 1
drug class and intact immune function, clinical
status may employ holding strategy
Stop ARVs, or only drug classes where resistance
already widespread, and monitor CD4 cell counts,
clinical status closely
Save remaining drug class for later when new
drugs to which patients virus remains sensitive
may become available

62
Summary and Implications

Boosted PIs key component of regimens for
drug-experienced patients
Data suggest LPV/RTV superior to SQV/RTV in
drug-experienced patients
Due to poor pharmacologic characteristics,
IDV/RTV seldom used
NFV not used as boosted PI due to poor
augmentation by RTV

63
Summary and Implications (cont)

Virologic potency of FPV/RTV appears lt LPV/RTV in
experienced patients
Efficacy of ATV/RTV appears comparable to LPV/RTV
in experienced patients with limited PI
resistance, but inferior with widespread
resistance
TPV/RTV demonstrated virologically and
immunologically superior to LPV/RTV, SQV/RTV, or
APV/RTV in heavily pretreated patients
TMC114/RTV improves treatment outcomes in
patients with extensive drug experience relative
to comparator boosted PIs
No comparative data on TMC114/RTV vs TPV/RTV

64
Summary and Implications (cont)

Adherence crucial to success of ART
Manipulation of dosages should be carefully
considered with boosted PIs
Trade-offs between convenience, toxicity, and
efficacy
Boosted PIs cleared from body predominantly
through hepatic metabolism
Clinical studies of specific drug combinations
required to delineate drug-drug interactions
Should not combine boosted PIs before potential
drug-drug interactions determined

65
Summary and Implications (cont)

PIs show reduction in susceptibility to viruses
with multiple mutations
Use PI likely to provide most remaining activity
at appropriately high exposure, with RTV
Optimizing other drugs in regimen vital to
success of boosted PI
Crucial to add drug from new class whenever
possible
Goal of therapy for HIV-infected patients
complete viral suppression
If not possible, maintain immunologic function
and prevent clinical deterioration

Drug-drug interactions may result in toxicity,
treatment failure, or loss of effectiveness and
can significantly affect a patient's clinical
outcome.
An understanding of the fundamental mechanisms
of HIV drug-drug interactions may allow for the
early detection or avoidance of troublesome
regimens and prudent management if they develop.
Although HIV drug interactions are usually
thought of as detrimental, resulting in a loss of
therapeutic effect or toxicity, some drug
interactions such as ritonavir boosted protease
inhibitor-based antiretroviral treatments are
beneficial and are commonly used in clinical
practice.

67
Enzyme Inhibition and Induction
Drug Enzyme Inhibition Enzyme Induction
Atazanavir
Delavirdine
Efavirenz
Fosamprenavir
Indinavir
Lopinavir/ritonavir1
Tipranavir/ritonavir1
Nelfinavir
Nevirapine
Ritonavir
Saquinavir2
1. Assessment also reflects the effects of
ritonavir. 2. Saquinavir can inhibit P450 3A4 in
vitro, but this is not generally manifested
clinically.
Modified from Flexner CW. http//clinicaloptions.
com/2004PK
68
Tenofovir Interactions
Impact of Coadministration on Exposure (AUC)
Plasma levels
69
Issues with Didanosine Tenofovir Efavirenz

TEDDI trial confirms previous reports of higher
rate of virologic failure in patients receiving
ddI TDF EFV 1
VF 25 after 12 weeks of TDF ddI EFV
EFADITE study stably suppressed pts who switched
to TDF ddI EFV or continued current regimen
2
Viral suppression maintained in most patients
However, CD4 ? on TDF ddI EFV
Median change in CD4 at Yr 1, -25 vs 46 in
controls (P .007)
Significantly larger CD4 declines in pts on high
vs low ddI doses

1. van Lunzen J, et al. IAS 2005. Abstract
TuPp0306. 2. Barrios A, et al. IAS 2005. Abstract
WePe12.3C16.
70
Small Reductions in Renal Function With Tenofovir
vs Other NRTIs
120

Small but statistically significant ? in CLCr
with TDF
Clinical significance unclear
Not grounds to exclude TDF for pts at risk for
renal dysfunction (dose adjust in renal
insufficiency)
Other studies
GFR detects more patients with mild renal
impairment than serum creatinine2
10 of TDF pts w/ Gr 3 GFR
MACS TDF associated with lower GFR3

100
Normal range 80-120 mL/min
80
CLCr (mL/min)
60
40
P lt .05 change from baseline for TDF vs NRTI
20
0
0
90
180
270
360
Days
Last CLCr on treatment carried forward if
treatment stopped
1. Gallant J, et al. CID 2005401194-8. 2.
Becker S, et al. CROI 2005. Abstract 819. 3.
Reisler R, et al. CROI 2005. Abstract 818.
71
Low Rate of Renal Events in Tenofovir Clinical
Dataset

Retrospective analysis of TDF Expanded Access
Program and postmarketing data after 4 years of
TDF availability

Serious Renal Adverse Events in EAP and Postmarketing Databases Serious Renal Adverse Events in EAP and Postmarketing Databases Serious Renal Adverse Events in EAP and Postmarketing Databases Serious Renal Adverse Events in EAP and Postmarketing Databases
Event EAP N 10343/3700 PY EAP N 10343/3700 PY Postmarketing 455,392 PY
Cases/100,000 PY Reporting Rate/100,000 PY
Renal failure 0.3 865 24.2
Fanconi/tubular disorder/hypophosphatemia/glycosuria lt 0.1 270 22.4
Elevated serum creatinine, BUN lt 0.1 189 5.1

Risk factors for serious renal adverse events
included sepsis or serious infection, history of
renal disease, late-stage HIV, concomitant
nephrotoxic medications, and hypertension

Nelson M, et al. CROI 2006. Abstract 781.
72

Vari Autori sostengono la necessita di
monitorare strettamente e per periodi lunghi la
funzione renale nei pazienti in terapia con
tenofovir e di valutare il rischio di interazioni
con altri farmaci.
Nelle linee linee-guida per la gestione delle
disfunzioni renali nei pazienti con HIV tenofovir
viene citato tra i farmaci potenzialmente
nefrotossici (tenofovir-related
nephrotoxicity), con raccomandazione di misurare
regolarmente la funzione renale nei soggetti con
filtrazione glomerulare lt 90 ml/min per 1.73m2.
Viene specificato che la maggior parte dei casi
di tossicita renale sono stati osservati in
pazienti in terapia con tenofovir PI boosted
con ritonavir.
EMEA ha ritenuto opportuno che GS informi
(tramite Dear Doctor Letter) i Medici della
necessità di uno stretto monitoraggio della
funzione renale nei pazienti in terapia con
tenofovir e della necessità di aggiustamenti
posologici e/o della frequenza di
somministrazione.

73
Tipranavir interazioni con ARVs (3)
Nessuna modifica della dose è necessaria quando
tipranavir/r (500/200 mg BID) è co-somministrato
con

NRTIs
Tenofovir
NNRTIs
Nevirapina riduce tipranavir AUC del 15 e Cmin
di lt5 ma nessuna modifica della dose è
necessaria
Efavirenz non ha effetti su tipranavir/r PK
quando associato con 200 mg BID di ritonavir

74
Tipranavir interazioni con ARVs (2)

Co-somministrazione di tipranavir/r (500/200 mg)
con amprenavir/r, lopinavir/r o saquinavir/r ha
rivelato una significativa riduzione dei livelli
di Cmin dopo 4 settimane di (1182.51)
Amprenavir 56
Lopinavir 55
Saquinavir 81
Le concentrazioni plasmatiche di TPV aumentano in
presenza di amprenavir/r e lopinavir/r ma non
saquinavir/r
Nessuna modifica della dose è raccomandata per
queste associazioni.sono controindicate!

75
Open issues on antiretroviral drug interactions

Treatment of opioid dependence and coinfection
with HIV and hepatitis C virus in
opioid-dependent patients The importance of drug
interactions between opioids and antiretroviral
agents.
McCance-Katz-E-F. Clinical Infectious Diseases
2005, 41/1 SUPPL. (S89-S95)
Pharmacokinetic interaction between chemotherapy
for non-Hodgkin's lymphoma and protease
inhibitors in HIV-1-infected patients.
Cruciani-M, Gatti-G, Vaccher-E, Di-Gennaro-G,
Cinelli-R, Bassetti-M, Tirelli-U, Bassetti-D.
Journal of Antimicrobial Chemotherapy 2005, 55/4
(546-549).
Natural health product-HIV drug interactions A
systematic review.
Mills-E, Montori-V, Perri-D, Phillips-E,
Koren-G. International Journal of STD and AIDS
2005, 16/3 (181-186).
Antiviral hepatitis and antiretroviral drug
interactions
Christian Perronne Journal of Hepatology 44
(2006) 119125
Hormonal contraceptive use and the effectiveness
of highly active antiretroviral therapy.
Chu-Jaclyn-H, Gange-Stephen-J, Anastos-Kathryn,
Minkoff-Howard, Cejtin-Helen, Bacon-Melanie,
Levine-Alexandra, Greenblatt-Ruth-M. American
journal of epidemiology, 2005, 161-9, p.881-90.

76
Summary

Not all drug-drug interactions can be predicted
Clinical significance cannot be excluded simply
on the basis of magnitude of change in
concentrations
Knowledge of drug concentrations will contribute
to an understanding of the overall effects of an
antiretroviral regimen
Pharmacologic characteristics of combination
antiretroviral regimens need to be sufficiently
understood prior to use in HIV-infected pts