1. COMPLICATIONS OF �ANTIRETROVIRAL THERAPY Michael Thompson PharmD, BCNSP
Faculty Florida/Caribbean AETC
Professor of Pharmacy Practice
College of Pharmacy
Florida A&M University
2. Disclosure of Financial Relationships This speaker has no significant financial relationships with commercial entities to disclose.
3. Objectives To review mechanisms of action of commonly used antiretroviral agents
To discuss common adverse effects associated with antiretroviral use
To discuss drug-drug interactions associated with antiretroviral use
Highlight the role of the clinician in prevention, detection and monitoring of adverse drug-related outcomes in patients receiving ARVs
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 Inhibitors
Entry Inhibitors
Integrase Inhibitors
6. Nucleoside/Nucleotide Reverse Transcriptase Inhibitors (NRTIs)
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
7. Non-Nucleoside Reverse �Transcriptase Inhibitors (NNRTIs)
Nevirapine (NVP, Viramune?) 6/96
Delavirdine (DLV, Rescriptor?) 4/97
Efavirenz (EFV, Sustiva?) 9/98
Etravirine (Intelence™) 1/08 We currently have 3 non-nucleoside reverse transcriptase inhibitors or NNRTI’s on the market. These are nevirapine, delavirdine and the most recently approved agent, efavirenz or Sustiva. Efavirenz was approved in September of 1998.We currently have 3 non-nucleoside reverse transcriptase inhibitors or NNRTI’s on the market. These are nevirapine, delavirdine and the most recently approved agent, efavirenz or Sustiva. Efavirenz was approved in September of 1998.
8. Protease Inhibitors (PIs)
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 Counting the two saquinavir formulations as one agent (although these formulations are not interchangeable, we now have 5 protease inhibitors or PI’s on the market. The most recently approved agent is amprenavir or Agenerase which was approved in April 1999.Counting the two saquinavir formulations as one agent (although these formulations are not interchangeable, we now have 5 protease inhibitors or PI’s on the market. The most recently approved agent is amprenavir or Agenerase which was approved in April 1999.
9. Fusion and Entry Inhibitors Agent Approved
Fusion Inhibitor
Enfuvirtide (T-20, Fuzeon?) 3/03
Entry Inhibitor (CCR5 Inhibitor)
Maraviroc (Selzentry™) 8/07
Counting the two saquinavir formulations as one agent (although these formulations are not interchangeable, we now have 5 protease inhibitors or PI’s on the market. The most recently approved agent is amprenavir or Agenerase which was approved in April 1999.Counting the two saquinavir formulations as one agent (although these formulations are not interchangeable, we now have 5 protease inhibitors or PI’s on the market. The most recently approved agent is amprenavir or Agenerase which was approved in April 1999.
10. 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!
11. Problems Associated �with Antiretrovirals Adverse Effects
Drug Interactions
Resistance
Genotyping
Phenotyping
12. Common Adverse �Effects of Antiretrovirals Lactic Acidosis
Hepatotoxicity
Hyperglycemia
Fat Maldistribution
Hyperlipidemia
Pancreatitis
Peripheral Neuropathy
Others (bone marrow suppression, gastric intolerance)
Common effects due to shared toxicity of mitochondria in human cells
13. Common Adverse Effects �of Antiretrovirals Lactic Acidosis
Thought to be secondary to mitochondrial damage; associated with hepatic steatosis
Increased risk in:
females,
obesity,
prolonged NRTI therapy,
nutritional depletion of cofactors/vitamins (riboflavin and thiamine)- required for normal mitochondrial function;
HIV itself (lower numbers of cellular mitochondria even prior to NRTI use)
14. Summary of NRTI Related �Lactic Acidosis NRTIs prevent DNA elongation and viral reproduction
Once incorporated into the viral DNA chain, their presence in the DNA halts transcription
These drugs unfortunately can also function as substrates for other enzymes like DNA polymerase gamma; this enzyme is involved in the replication of mitochondrial DNA
Disruption of DNA polymerase gamma is thought to result in a wide variety of adverse effects ranging from lactic acidosis to hepatic steatosis
15. Mechanism of Development of Lactic Acidosis in HAART
16. Lactic Acidosis Continued Symptoms: nonspecific GI complaints of nausea, abdominal pain, bloating, nausea and vomiting, diarrhea, anorexia, weakness, tachypnea, myalgia,paresthesia and weight loss with hepatomegaly
Labs: hyperlactemia, increased anion gap, elevated aminotransferases, LDH, lipase and amylase
Routine testing of lactic acid not recommended due to technical problems in reliably assaying for lactate
17. Adverse Effects: 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
18. Nevirapine Hepatotoxicity 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.
19. Protease Inhibitors can cause hepatoxicity at ANY time during therapy
Other antiretrovirals and hepatotoxicity
Co infection with Hepatitis C or B, alcohol and stavudine use can increase potential for toxicity
20. Adverse Effects Continued Hyperglycemia
Seen in Protease Inhibitors
Glucose intolerance and insulin resistance can occur without Diabetes
Fat maldistribution
Lipodystrophy is part of a metabolic syndrome that includes dyslipidemias, insulin resistance and accelerated bone loss
21. HAART Toxicities: Lipodystrophy Body habitus changes
Central fat accumulation
Peripheral fat wasting
Risk factors
Female gender
Older age
HAART
Protease Inhibitor use
22. Lipodystrophy
23. 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
24. Lipodystrophy: Unclear Etiology Mitochondrial toxicity?
Interference w/ adipocyte differentiation?
Pro-inflammatory activation of the immune system during reconstitution?
25. Lipodystrophy Syndrome: �NRTIs versus PIs� We have attempted to create a model of the relationship between drug therapies and these clinical endpoints, which allows for ‘overlapping toxicities’ in which both drug classes contribute to a clinical endpoint (the example here being subcutaneous fat wasting), while suggesting that some clinical endpoints are strongly associated with either NRTIs or PIs, with little contribution from the other drug class...
In the case of NRTIs, there is no data currently available to suggest that PI therapy modifies the risk of hyperlactataemia. At the other end of the spectrum, PI therapy is strongly associated with risk of dyslipidaemia and insulin resistance.
As previously mentioned, there is now increasing evidence to support the concept that subcutaneous fat wasting represents a clinical endpoint where both NRTIs and PIs contribute significantly.
Antiretroviral therapy
Duration of treatment – Nucleoside RTIs
Protease inhibitors – Non-nucleoside RTIs
HIV disease course
Duration of infection – Viral load suppression
Disease progression – Immune reconstitution
Other potential risk factors
Age – Diet
Race – Host genetics
Gender – Mitochondrial toxicity
variety of clinical factors can predict the development and severity of fat redistribution in patients with HIV infection.��• These are data from the HIV Outpatient Study, which looked at 1077 patients visiting 8 clinics in 7 U.S. cities.1 Patients aged 40 and older were discovered to have an increased risk for developing these syndromes. Other time-dependent predictors were the duration of HIV infection and the number of months since the CD4 cell nadir.��• Treatment predictors were nucleoside use of greater than 8 months and protease inhibitor use of greater than 2 years’ duration. At the time of this study, non-nucleoside reverse transcriptase inhibitors (NNRTIs) were not widely used.��• Other predictors included the nadir CD4 percent and a body mass index loss of greater than 1.0 kg/m2.�
Gender differences are starting to emerge with the reporting of these syndromes. Whereas original observations were made mostly in men, Mulligan1 has tried to systematically examine the differences between men and women.��• Women are more likely to develop the lipohypertrophy-type syndromes, such as increased intra-abdominal and breast fat. They also have an increased prevalence in general when compared to men.��• On the other hand, men tend to experience more fat loss, particularly from their extremities. However, both men and women can experience any of these manifestations.��Reference:��1. Mulligan K. Abnormalities of body composition and lipids associated with HAART: pathogenesis, clinical manifestations, and case definitions. 7th Conference on Retroviruses and Opportunistic Infections, San Francisco, CA; Jan 30-Feb 2, 2000. Abstract S20.
We have attempted to create a model of the relationship between drug therapies and these clinical endpoints, which allows for ‘overlapping toxicities’ in which both drug classes contribute to a clinical endpoint (the example here being subcutaneous fat wasting), while suggesting that some clinical endpoints are strongly associated with either NRTIs or PIs, with little contribution from the other drug class...
In the case of NRTIs, there is no data currently available to suggest that PI therapy modifies the risk of hyperlactataemia. At the other end of the spectrum, PI therapy is strongly associated with risk of dyslipidaemia and insulin resistance.
As previously mentioned, there is now increasing evidence to support the concept that subcutaneous fat wasting represents a clinical endpoint where both NRTIs and PIs contribute significantly.
Antiretroviral therapy
Duration of treatment – Nucleoside RTIs
Protease inhibitors – Non-nucleoside RTIs
HIV disease course
Duration of infection – Viral load suppression
Disease progression – Immune reconstitution
Other potential risk factors
Age – Diet
Race – Host genetics
Gender – Mitochondrial toxicity
variety of clinical factors can predict the development and severity of fat redistribution in patients with HIV infection.
26. Lipodystrophy:� Treatment Options Switch patient to NNRTI regimen
Anti-hyperglycemic agents
Metformin and Thiazolidindiones
Growth hormone
27. Lipodystrophy Illustrations
28. Severe Wasting
29. Treatment of Facial Wasting�
30. Example of Buffalo Hump
31. Other Adverse Effects Pancreatitis
Bleeding in Hemophiliacs
Skin Rash/Dermatologic Effects
Examples
NNRTIs (nevirapine, efavirenz)
NRTIs (abacavir)
Others
32. Steven Johnson Syndrome or Toxic Epidermal Necrolysis http://www.fromthewilderness.com/images/stevenJohnsonSyndrome2.jpghttp://www.fromthewilderness.com/images/stevenJohnsonSyndrome2.jpg
33. Drug Interactions
34. Understanding Drug Interactions with Antiretrovirals Mechanisms of Drug Interactions: Pharmacokinetic Interactions
These interactions affect:
Absorption of drugs
Distribution of drugs
Metabolism
Elimination of drugs
Considered clinically significant if there is more than a 30% change in the blood levels or area under the concentration curve
35. Interactions Affecting Drug Metabolism Most Common Cytochrome P450 is an enzyme system containing many enzyme families
The majority of interactions reported involve CYP3A4
Medications can induce OR inhibit the action of enzymes responsible for their own metabolism or the metabolism of other drugs
Inducing enzymes result in lower drug levels; Inhibiting enzymes result in increased levels
37. Drug Interactions: HAART Nucleoside and Nucleotide drugs not eliminated via cytochrome P450 therefore these interactions are minimal
Drug interactions here may occur via other mechanisms (eg GI absorption, renal elimination)
38. Non-nucleoside 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
Etravirine is an inducer of CYP3A4 (inhibits CYP2C, and CYP2C19)
39. 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
Tipranavir can also be an inducer
40. Other classes Fusion inhibitors and integrase inhibitors are not metabolized by these systems
41. 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
42. Food Effects Continued.. Ritonavir
Take with food; increases bioavailability
Indinavir
Food decreases levels by 77% (not a problem if boosted with ritonavir)
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
43. 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
44. Effect of Buffering Agents �on PI Concentrations Mechanism
PI absorption is related to its solubility properties
For weak bases-solubility increases in gastric acid
When pH is less acidic, PIs become less soluble to varying degrees
ion-trapping mechanisms will cause acidic compounds (weak bases) to accumulate in alkaline compartmentsion-trapping mechanisms will cause acidic compounds (weak bases) to accumulate in alkaline compartments
45. Effect of Buffering Agents �on Gastric pH Buffering agents
Proton-pump inhibitors (PPIs)
Histamine-2 (H2) blockers
Antacids
calcium carbonate and magnesium hydroxide in didanosine buffered tablets (Videx)
Duration of action
Decrease in gastric acidity varies by drug class
PPI > H2 blockers > antacids � 24 - 72h 10 – 12h a few hours
46. Effect of Buffering Agents on Antiretroviral Drug Absorption Didanosine (ddI)
Contains buffering agents that can affect absorption of:
Atazanavir
Tetracyclines
Quinolones
Itraconazole
Proton Pump Inhibitors, H2 antagonists and Antacids
Atazanavir absorption decreased
Note manufacturer’s dosing recommendation as follows
47. Dosing Recommendations for Use of PPIs with Atazanivir Treatment Naïve Patients
PPI max dose equal to 20mg omeprazole given 12 hrs before atazanvir 300mg with ritonavir 100mg
Treatment Experienced Patients
Avoid use as per manufacturer’s recommendations
48. 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
49. Antiretroviral Interactions Continued Tenofovir and Atazanavir
Atazanavir levels are decreased
Tenofovir concentrations increased
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
50. Other Interactions: Maraviroc When given with strong CYP3A inhibitors (with or without CYP3A inducers) including PIs (except tipranavir/ritonavir), delavirdine 150 mg twice daily
With NRTIs, tipranavir/ritonavir, nevirapine, and other drugs that are not strong CYP3A inhibitors or CYP3A inducers 300 mg twice daily (i.e. that do not have a net CYP3A inhibition or induction effect)
With CYP3A inducers including efavirenz (without a strong CYP3A inhibitor) 600 mg twice daily
51. 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
53. Drug Interactions with Antiretrovirals Antifungal agents
Review of specific agents with dosage adjustments
Antilipidemic agents
Selection of proper agents to avoid interactions. Avoid: simvastatin (Zocor®) and lovastatin (Lescol®)
Dosage adjustment: when using rosuvastatin (Crestor®) with lopinavir, do not exceed 10 mg/day of rosuvastatin
Antimycobacterial agents
Major interactions to consider
Management Issues
54. Drug Interactions Continued Anticonvulsants
Carbamazepine, Phenobarbital and Phentyoin
Effect on serum concentrations of ARV
Concomitant effects on anticonvulsant levels
55. Drug Interactions Herbal Products
St John’s Wort
Kava Kava
Other herbals that cause hepatotoxicity
Other herbal products to consider
56. Role of the Clinician in Drug Interaction �Detection and Prevention Question patients concerning
Nonprescription Drug Usage
Herbal and Natural Product Usage
Use appropriate literature sources to obtain reliable and consistent information
www.aidsinfo.nih.gov
www.hivinsite.com
www.hiv-druginteractions.org
Prescribing information on web
Communication among providers is key
57. Summary Talk with patients to stress adherence to therapy
Review all medications with patients
Function in an interdisciplinary environment
61. 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 oxidative phosphorylation)
62. 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
63. Facial Wasting
64. Adverse Effects Clinical Features of Peripheral Fat Loss
Peripheral fat loss in face, limbs, buttocks
Accumulation of fat centrally in abdomen and breast and over dorsocervical spine (buffalo hump)
Dyslipidemia
Elevation in triglyceride and cholesterol levels
Can respond to antihyperlipidemics
