ARVs: What We Have and What is Coming

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ARVs: What We Have and What is Coming

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Title: ARVs: What We Have and What is Coming

1
ARVs What We Have and What is Coming

Michael Thompson PharmD, BCNSP
Professor of Pharmacy Practice
Florida AM University
Tallahassee, Florida

2
Disclosure of Financial Relationships

This speaker has no significant financial
relationships with commercial entities to
disclose.

This slide set has been peer-reviewed to ensure
that there are no conflicts of interest
represented in the presentation.
3
Lecture Objectives

Upon completion of this lecture the participant
should be able to
Identify currently available antiretroviral
agents and discuss
Mechanisms of action
Common Adverse Effects
Drug Interactions
New Drugs and Potential Effects on Current
Management

4
HIV Life Cycle
Fusion Inhibitors
Protease inhibitors (PIs)
NRTIs and NNRTI

From The Immunodeficiency Clinic - University
Health Network Website,www.tthhivclinic.com

5
ART Options

NRTIs (Nucleoside OR Nucleotide Reverse
Transcriptase Inhibitors, aka Nukes)
NNRTIs (Non-Nucleoside Reverse Transcriptase
Inhibitors, aka Non-Nukes)
PIs (Protease Inhibitors)
Fusion (or Entry Inhibitors)
ART agents in additional classes
currently in development
Vaccines against HIV in the distant
future?

6
Goal of Antiretroviral Therapy

To achieve maximum and durable suppression of HIV
replication
Interpreted to mean an HIV RNA level in plasma
that is less than the lower limit of quantization
(i.e. undetectable)
Increase in CD4 lymphocytes
Improved quality of life
Decreased morbidity and mortality

7
Goal of Therapy continued

Decreasing viral load below level of sensitivity
depends upon assay procedure
RTPCR (Amplicor)---
Versant----
Nuclisens---
Should be achieved within 16-24 weeks Should see
a 1log10 reduction within 8 weeks
Increase in CD4
Adequate suppression is an increase by 100-150
cells/mm3 per year

8
Tools to Achieve Goals

Maximal adherence to prescribed regimens
Rational sequencing of drugs
Resistance Testing

9
DHHS HIV Treatment Guidelines
Hit Hard, Hit Early CD4 20,000
Hit Hard, Hit Later CD4 55,000
Hit Hard, Hit Even Later CD4
100,000
10
Timeline of ARV Approvals
1987 Zidovudine
1987 1st NRTI Approved
1991 Didanosine 1992 Zalcitabine 1994
Stavudine
1995 1st PI
1995 Lamivudine, Invirase
1996 1st NNRTI
1996 Nevirapine, Ritonavir, Indinavir
1997 Delavirdine, Nelfinavir, Fortovase 1998
Abacavir, Efavirenz 1999 Amprenavir 2000
Lopinavir/ritonavir 2001 Tenofovir
2003 1st Fusion Inhibitor
2003 T-20, Atazanavir, Emtricitabine,
Fosamprenavir 2005 Tipranavir 2006 Darunavir
The Future Entry inhibitors, Integrase
inhibitors,chemokine receptor inhibitors, others
11
Nucleoside/Nucleotide Reverse Transcriptase
Inhibitors (NRTIs)
Agent
Approved

Zidovudine (AZT, ZDV, Retrovir?)
3/87
Didanosine (ddI, Videx?, Videx EC?) 10/91
Zalcitabine (ddC, Hivid?) 6/92
Stavudine (d4T, Zerit?) 6/94
Lamivudine (3TC, Epivir?) 11/95
Abacavir (ABC, Ziagen?) 12/98
Combivir? (AZT/3TC) 9/97
Trizivir? (AZT/3TC/ABC) 11/00
Tenofovir (TDF, Viread?) 10/01
Emtricitabine (FTC, Emtriva?) 7/03
Epzicom? (ABC/3TC) 8/04
Truvada? (FTC/TDF) 8/04

A nucleotide reverse transcriptase inhibitor
12
Non-Nucleoside Reverse Transcriptase Inhibitors
(NNRTIs)

Agent Approved
Nevirapine (NVP, Viramune?) 6/96
Delavirdine (DLV, Rescriptor?) 4/97
Efavirenz (EFV, Sustiva?) 9/98

13
Protease Inhibitors (PIs)

Agent
Approved
Saquinavir-HGC (SQV-HGC, Invirase?)
12/95
Ritonavir (RTV, Norvir?) 3/96
Indinavir (IDV, Crixivan?) 3/96
Nelfinavir (NFV, Viracept?) 3/97
Saquinavir-SGC (SQV-SGC, Fortovase?) 11/97
Amprenavir (APV, Agenerase?) 4/99
Lopinavir/ritonavir (KAL, Kaletra) 9/00
Atazanavir (ATV, Reyataz) 6/03
Fosamprenavir (fos-APV, Lexiva) 10/03
Tipranavir (TPV, Aptivus) 6/05
Darunavir (DRV, Prezista) 6/06

14
Fusion Inhibitor

Agent Approved
Enfuvirtide (T-20, Fuzeon?) 3/03

15
Multi-class Product

Atripla (emtricitabine/tenofovir/efavirenz)
Emtricitabine/tenofovir (Truvada) efavirenz
(Sustiva)
Approved July 12, 2006
First collaborative effort between 2 companies to
develop combination pill for HIV treatment
Not new drugs!

16
Choice of ARVs for Treatment of the ARV-Naïve
Patient1

Guidelines provided preferred and alternative PI
or NNRTI-based regimens for treatment-naïve
patients
Once patients have been a regimen, new regimens
are constructed with the use of resistance
testing, history of ARV use and tolerability
Refer to the AETC reference card for a list of
preferred and alternative regimens

1. October 10th, 2006 Department of Health and
Human Services Guidelines for the Use of
Antiretroviral Agents in HIV-infected Adult and
Adolescents Available at www.aidsinfo.nih.gov
17
Initial Treatment Preferred ComponentsDHHS
Guidelines October 11, 2006
NNRTI Option
NRTI Options
OR

Tenofovir emtricitabine
Zidovudine lamivudine

PI Options

Avoid in pregnant women and women with
significant pregnancy potential.
Emtricitabine can be used in place of
lamivudine and vice versa.

Department of Health and Human Services
Guidelines for the Use of Antiretroviral Agents
in HIV-infected Adult and Adolescents. Otoberr
10, 2006. Available at www.aidsinfonih.gov.
Accessed October 12, 2006.
18
Regimens NOT Recommended
19
Regimens NOT Recommended
20
Regimens NOT Recommended
21
Choice of ARVs for Treatment of the ARV-Naïve
Patient

ACTG 5095
Higher failure rates with Trizivir (21)
compared to Trizivir /efavirenz or
Combivir/efavirenz arms (11)

1. Gulick et al. 2nd IAS Conference. Paris,
France. July 13-16, 2003.
22
Problems Associated with Antiretrovirals

Adverse Effects
Drug Interactions
Resistance
Genotyping
Phenotyping

23
ARV Adverse Effects
24
NRTI Mitochondrial Toxicity

MOA Inhibition of mitochondial DNA polymerase-?,
? oxidative metabolism, ? ATP generation
Implicated in lactic acidosis with hepatic
steatosis
Other possible manifestations
Myopathy (AZT)
Neuropathy (d4T, ddI, ddC)
Lipoatrophy (d4T)
Pancreatitis (ddI)

25
HIV/HAART Toxicities Lactic Acidosis

Rare but potentially fatal syndrome linked to
prolonged use of NRTIs
Symptoms include lethargy, fatigue, abdominal
pain, respiratory distress
Etiology mitochondrial dysfunction, possibly due
to inhibition of key mitochondrial replication
enzyme by antiretroviral agents
Risk Factors
Stavudine and didanosine use, pregnancy, female
gender, obesity

26
Mechanism of Development of Lactic Acidosis in
HAART
27
Mechanism of NRTI Associated Lactic Acidosis
Specifics

During normal glycolysis, glucose is converted to
pyruvate in the cytosol and is transferred into
the mitochondria
Once the pyruvate is in the mitochondria, most of
it is converted into acetylcoenzyme A, which in
turn enters the tricarboxylic acid cycle to form
NADH (nicotinamide adenine dinucleotide)
NADH is used by the mitochondria to produce ATP
through oxidative phosphorylation Dna polymerase
is inhibited in the presence of NRTIs which
diminishes mitochondrial function (especially
oxidatiave phosphorylation)

28
continued

Pyruvate and NADH accumulate and the conversion
of pyruvate to lactate is enhanced
Impaired oxidation leads to decreased fatty acid
oxidation resulting in accumulation of free fatty
acids
Free fatty acids are converted to triglycerides
and accumulate in liver causing hepatic steatosis

29
Adverse Effects Hepatotoxicity

Hepatotoxicity
Defined as 3 to 5 times increase in serum
transaminases with or without clinical hepatitis
All marketed NNRTIs and Protease Inhibitors have
been associated with elevations in transaminases
Of the NNRTIs, nevirapine has highest incidence
of hepatoxicity and patients should be monitored
especially throughout the first 18 weeks
Patients with hepatitis B and C may be at
increased risk.
The two week lead in with nevirapine may reduce
incidence of hepatotoxicity. Patients should be
monitored every 2 weeks for the first month then
monthly for the first 18 weeks. If rash occurs,
patients should be monitored for hepatotoxicity
as well.

30
Adverse Effects Hepatotoxicity

Protease Inhibitors can cause hepatoxicity at ANY
time during therapy
Co infection with Hepatitis C or B, alcohol and
stavudine use can increase potential for toxicity

31
Hepatotoxicity

RTV use linked to increased risk of severe
hepatotoxicity
Increased LFTs observed with all PIs
More common in pts with chronic viral hepatitis
(HBV, HCV)
Data do not support withholding PIs from
co-infected patients with HBV or HCV

Sulkowski, JAMA 2000 28374
32
Adverse Effects NRTIs

Abacavir - hypersensitivity reaction
Didanosine - GI intolerance, pancreatitis,
peripheral neuropathy (PN)
Emtricitabine hyperpigmentation, skin
discoloration
Stavudine - PN, pancreatitis, lipodystrophy,
dyslipidemia
Tenofovir - headache, GI intolerance, renal
impairment
Zidovudine - headache, GI intolerance, bone
marrow suppression

Black Box Warning- Lactic acidosis and hepatic
steatosis. Pregnant women may be at increased
risk for lactic acidosis and liver damage when
treated with stavudine didanosine. This
combination should be avoided in pregnant women,
if possible.
33
Abacavir hypersensitivity

Black Box Warning
Occurs in 5-8 of people taking abacavir
Most common symptoms
Fever, rash, nausea, fatigue, GI and URI symptoms
Onset usually first two weeks of therapy
Can be fatal if continued or restarted and should
NEVER re-challenged
Patient counseling and follow-up mandatory

34
Adverse Effects NNRTIs

All NNRTIs
Rash
Increased liver function tests
Nevirapine
Hepatotoxicity (CD4 250? and 400 ?)
Rash including Stevens-Johnson syndrome
Use caution in discontinuing in patients on
tenofovir, lamivudine, or emtricitabine, in HBV
co-infected patients
Efavirenz
Neuropsychiatric effects (vivid dreams,
nightmares, hallucinations, dizziness)
Teratogenic in non-human primates (Pregnancy
Category D)

35
Steven Johnson Syndrome or Toxic Epidermal
Necrolysis
http//www.fromthewilderness.com/images/stevenJohn
sonSyndrome2.jpg
36
Adverse Effects PIs

All PIs
GI intolerance
Dyslipidemia
Insulin resistance and diabetes
Lipodystrophy
Elevated liver function tests
Possible increased bleeding risk in hemophiliacs
Drug-drug interactions

37
Adverse Effects PIs

Amprenavir, fosamprenavir, darunavir
sulfonamide derivative potential for cross
hypersensitivity with other sulfa drugs
Amprenavir oral solution CI, in pregnancy,
children
renal failure, patients treated with disulfiram
or metronidazole
Atazanavir - hyperbilirubinemia, PR interval
prolongation
Indinavir nephrolithiasis, alopecia,
paronychia, cheilitis, dermatitis,
hyperbilirubinemia, HA, asthenia, blurred vision
Lopinavir/ritonavir ??? diarrhea

38
Adverse Effects PIs

Nelfinavir - ??? diarrhea
Saquinavir- GI intolerance
Tipranavir rash (contains sulfonamide
derivative), hepatotoxicity, ??? lipids,
associated with reports of fatal and non-fatal
intracranial hemorrhage

39
Lipodystrophy
40
HAART Toxicities Lipodystrophy

Body habitus changes
Central fat accumulation
Peripheral fat wasting
Risk factors
Female gender
Older age
HAART
Protease Inhibitor use

41
Lipodystrophy
http//www.thebody.com/pinf/wise_words/mar05/lipod
ystrophy.html?m89o
42
Proposed Case Definition of Lipodystrophy

Primary Characteristics
Age 40 years
HIV infection 4 years
AIDS (Class C)
Increased waist hip ratio
Decreased HDL
Change in anion gap

Secondary Characteristics
Increased total cholesterol
Increased triglycerides
Decreased lactate

http//www.hivforum.org/publications/Lipodystro
phy.pdf
http//www.med.unsw.edu.au/nchecr
43
Lipodystrophy Unclear Etiology

Mitochondrial toxicity?
Interference w/ adipocyte differentiation?
Pro-inflammatory activation of the immune system
during reconstitution?

44
Lipodystrophy Syndrome NRTIs versus PIs
PIs
NRTIs d4TZDV
Intra-abdominal fat Cholesterol
TG Insulin resistance
Lactic acid
SC fat wasting TG Buffalo hump
John M, et al. Antiviral Ther. 200169-20.
45
Lipodystrophy Treatment Options

Switch PI to NNRTI or to all NRTI regimen
Anti-hyperglycemic agents
Metformin and Thiazolidindiones
Growth hormone

46
Lipodystrophy Illustrations
Buffalo hump
Facial wasting
Crix belly
http//www.hivandhepatitis.com/recent/lipo/fataccu
mulation/1.htmlbuf
47
Severe Wasting
http//bayloraids.org/atlas/images/14.jpg
48
Facial Wasting
http//www.emedicine.com/derm/topic877.htmsection
pictures
49
Treatment of Facial WastingSculptra
http//www1.sculptra.com/US/hcp/Works.jsp
50
Bone Disorders in HIV Disease

Osteonecrosis
Death of bone tissue as resulting from
circulatory insufficiency
Usually involves femoral heads
Increased frequency with introduction of HAART
Diagnosis imagining
Treatment surgical joint replacement
Osteoporosis
Bone demineralization
Small reports of osteopenia and osteoporosis seen
mainly with PI regimens
Diagnosis X-ray or DEXA
Treatment consider bisphosphonate drug with
frank osteoporosis

51
HIV/HAART Toxicities Lipid Abnormalities

Low HDL, high LDL and TGs
Hypertriglyceridemia risk of pancreatitis
Generally treated w/ fibrates and/or statins
Inconsistent results from switch studies
Beware of drug interactions, risk of myositis
Avoid lovastatin or simvastatin

Guidelines for the Evaluation and Management of
Dyslipidemia in Human Immunodeficiency Virus
(HIV) Infected Adults Receiving Antiretroviral
Therapy Recommendations of the HIV Medicine
Association of the Infectious Disease Society of
America and the Adult AIDS Clinical Trials Group.
Clin Infect Dis. 200337613-627 (Available
online at http//www.idsociety.org/Content/Navigat
ionMenu/Resources/HIVMA/Practice_Guidelines2/Pract
ice_Guidelines.htm)
52
HIV/HAART Toxicities Insulin Resistance

Progression to frank diabetes mellitus possible
Monitor with fasting glucose values
Improvement often seen with switching out of
PI-based regimens
Some success w/ metformin (Glucophage)

53
Mechanisms of Drug Interactions
54
Why are HIV/AIDS Patients at Risk?

Use of 3 and 4 drug antiretroviral regimens
Multiple agents for treatment/prevention of
various opportunistic infections
Patient living longer and being treated for other
chronic diseases (e.g. diabetes, CAD)
Many antiretroviral agents have a profound effect
on the cytochrome P450 enzyme system

55
Factors Affecting Concentration of Antiviral
Drug at its Site of Action
Absorption
Metabolism
CYPs P-gp
Oral AdministrationDrug (tablet/capsule)
Dissolution
GI MUCOSA
CYP3A4/5 CYP2B6 CYP2C19 P-gp
SYSTEMIC CIRCULATION
PIs NNRTIs
ProteinBoundDrug
FreeDrug
Distribution
TISSUES Bound Drug Free Drug

TARGET CELL
NRTIs (Intracellular Phosphorylation)
Protease Inhibitors
NNRTIs

Excretion
URINE BILE
http//www.clinicaloptions.com/
56
Effect of ARVs on Drug Metabolism
3A4
2C19
2D6
2C9
1A2
2E1
2A6
2B6
2C8
Inhibited by ATV
Fichtenbaum CJ. Clin Pharmacokinet.
2002411195-1211 Product labels.
57
Other Inhibitors and Inducers of Drug Metabolism

Rifampin
Rifabutin
Phenobarbital
Carbamazepine
Phenytoin
Cimetidine
Omeprazole
Fluoxetine

Clarithromycin
Erythromycin
Non-DHP CCBs
Azole Antifungals
Isoniazid
Ciprofloxacin
Grapefruit juice
Amiodarone

58
Drug Interactions HAART

Nucleoside and Nucleotide drugs not eliminated
via cytP450 therefore these interactions are
minimal
Drug interactions here may occur via other
mechanisms (e.g GI absorption, renal elimination)

59
Effects of Food on Absorption of Antiretrovirals

Didanosine
Levels decrease by 55
Take ½ hour before or 2 hours after meals
Efavirenz
Empty stomach, food increases levels as high as
39-79
Amprenavir
High fat meal decreases blood levels
Can take with food but avoid high fat
f-Amp not affected as much

60
Food Effects continued..

Ritonavir
Take with food increases bioavailability
Indinavir
Food decreases levels by 77 (unless boosted)
Take 1 hr before or 2 hr after or may take with
skim milk or low fat meal
Nelfinavir
Levels increase 2-3 fold with food Take with food

61
Food Effects continued..

Saquinavir (eg Fortovase, Invirase)
Levels increase 6-fold if taken with food
Take with or up to 2 hours after a meal as sole
PI or with RTV
Lopinavir/Ritonavir (Kaletra)
Take with food
AUC increased when taken with food

62
Examples of Noted Interactions Between
Antiretrovirals

Efavirenz and Nevirapine
Decrease atazanavir levels
Tenofovir and ddI
ddI levels are elevated (exact mechanism not
known fully)
Recommend 250mg ddI-EC (60 kg)
Some reports to suggest decreased virologic
control when this combination used as NRTI
backbone with EFV or NVP

63
Antiretroviral Interactions continued

Tenofovir and atazanavir
Atazanavir levels are decreased
Tenofovir concentrations increase
Atazanavir should be boosted with RTV when
combined
Does not seem to be clinically significant with
PIs such as lopinavir/ritonavir (Kaletra)
Tenofovir may compete for tubular secretion for
wide variety of drugs as well

64
Nonnucleoside Interactions

Drugs involved
Efavirenz can induce or inhibit CYP3A4 (most
often acts as an inducer and can also induce
others)
Nevirapine acts as an inducer to CYP3A4
Delavirdine acts as an inhibitor of CYP3A4

65
NRTI Drug Interactions

Zidovudine
Agents that cause additive bone marrow
suppression (i.e. ganciclovir, flucytosine,
pentamidine)
Antagonism with stavudine (competition for
intracellular activation)
Didanosine (ddI)
Inhibition of absorption of other agents due to
ddI buffer in Videx (FQs, tetracyclines,
dapsone, ketoconazole, indinavir, delavirdine)
Ribavirin significantly ? ddI levels-do not use
together

66
NNRTI Drug Interactions

All NNRTIs are metabolized by the CYP3A4 enzyme
Delavirdine can inhibit CYP3A4 enzyme
Nevirapine can induce CYP3A4
Efavirenz can inhibit or induce CYP3A4 enzyme

67
NRTI Drug Interactions

Zidovudine
Agents that cause additive bone marrow
suppression (i.e. ganciclovir, flucytosine,
pentamidine)
Antagonism with stavudine (competition for
intracellular activation)
Didanosine (ddI)
Inhibition of absorption of other agents due to
ddI buffer in Videx (FQs, tetracyclines,
dapsone, ketoconazole, indinavir, delavirdine)
Ribavirin significantly ? ddI levels-do not use
together

68
NRTI Drug Interactions

Didanosine, Stavudine, Zalcitabine
Agents causing additive neurotoxicity
(vincristine, cisplatin, isoniazid)
Agents causing additive pancreatoxicity (alcohol,
pentamidine, valproic acid)
Abacavir
Metabolized by alcohol dehydrogenase (alcohol can
increase abacavir levels and toxicity)

69
Protease Inhibitor Interactions

All PIs inhibit CYP3A4
Ritonavir is the most potent inhibitor while
Saquinavir is the least potent
Ritonavir can inhibit other cytochrome P450
inhibitors and can induce CYP1A2
Note Fusion inhibitors not metabolized by these
systems

70
Drugs That Should Not Be Given With PIs

Simvastatin
Lovastatin
Astemizole
Terfenadine
Cisapride
Pimozide
Bepridil

St. Johns Wort
Rifampin (except ritonavir)
Rifapentine
Midazolam
Triazolam
Ergot alkaloids

Additionally the following should not be given
with ritonavir amiodarone, flecainide,
propafenone, quinidine
Proton pump inhibitors and Irinotecan should not
be used with atazanavir

71
Medications Contraindicated with Protease
Inhibitors
72
Rifabutin Use with PIs
73
Interaction Between Atazanavir Omeprazole

N 48 HIV(-) subjects
ATV exposures substantially reduced by
coadministration with OMP 40 mg
Not corrected by increased ATV dose or 8 oz cola
OMP exposures not significantly altered
Effect of OMP 20 mg (OTC dose) not known
Do not coadminister

Agarwala S, et al. CROI 2005. Abstract 658.
74
Fluticasone and Ritonavir (Flovent and Flonase)

Fluticasone induced Cushings Syndrome
Fluticasone is a 3A4 substrate and RTV a 3A4
inhibitor

Gupta SK. CID 200235e69-e71
75
Drug Interactions with Drugs Used in Treating
Addiction

Methadone
Efavirenz and nevirapine decreases methadone
levels Delavirdine effects unknown
Abacavir decreases methadone clearance
Methadone decreases stavudine levels but
increases zidovudine
PIs decrease levels and patients can have
symptoms of withdrawal

76
ARV Interactions with Recreational Drugs
77
ARV Interactions with Recreational Drugs
78
Herbal and Nutraceutical Interactions with CYP450
3A4 Isoenzyme

Echinacea
Garlic pills
Grapefruit juice
Seville orange juice
Milk thistle
St. Johns wort

Will alter the metabolism of substrates of 3A4
system. Interactions have clinical significance
http//www.prn.org/prn_nb_cntnt/vol7/num1/pau_sum.
htm
79
Drug Interaction Resources