Antiretroviral Drugs

Question 1

Nucleoside/-tide Reverse Transcritpase Inhibitors (NRTIs)

Answer 1

"Lam Did Stav Ten Zebras while Eating Aba's NRTIs"
Abacavir
Didanosine 
Emtricitabine
Lamivudine
Stavudine
Tenofovir
Zidovudine

Question 2

Nonnucleoside Reverse Transcriptase Inhibitors (NNRTIs)

Answer 2

“REN”

Rilpivirine, Efavirenz, Nevirapine,

Question 3

Protease Inhibitors

Answer 3

..NAVIR
Atazanavir
Darunavir
Indinavir
Lopinavir
Nelfinavir

Question 4

Entry Inhibitors

Answer 4

“MEn enter”

Enfuviritde, Maraviroc

Question 5

Integrase Inhibitor

Answer 5

“RED”

Dolutegravir, Elvitegravir, Raltegravir

Question 6

Pharmacokinetic enhancers

Answer 6

Cobicistat

Ritonavir

Question 7

NRTIs

MOA

Answer 7

Didanosine, Emtricitabine, Lamivudine, Stavudine, Tenofovir, Zidovudine

MOA: analogs of native ribosides (lack 3’OH)

• Phosphorylated by cellular enzyme and incorporated into viral DNA by reverse transcriptase
• Lack of 3’OH terminates DNA elongation ie. they are competitive inhibitors of reverse transcriptase
• Most have activity against HIV 2 (africa) as well as HIV 1 (Western world)

Question 8

NRTIs AE

Answer 8

> 1 NRTI causes toxicities to overlap

AE mainly due to inhibition of mitochondrial DNA polymerase: peripheral neuropathy, myopathy, lipoatrophy and lactic acidosis

Pancreatitis, myelosuppression and cardiomyopathy can also occur

Liver toxicity is rare but fatal (lactic acidosis, hepatomegaly with steatosis)

Zidovudine and stavudine may be particularly associated with dyslipidemia and insulin resistance

Question 9

NRTIs DI

Didansosine and Tenofovir

Answer 9

Tenofovir increases plasma didanosine levels ~ 60%.
doses of didansosine have to be reduced

NRTIs are not metabolized by cytochrome enzymes.

Question 10

Zidovudine (ZDV, AZT)
Nucleoside analog:
Pharmacokinetics:

Answer 10

Nucleoside Analog : Thymidine

Pharmacokinetics

• Oral
• Penetrates well across BBB
• Dosage adjustments required patients w/ cirrhosis

Question 11

Zidovudine (ZDV, AZT) AE:

CI:

Answer 11

AE:
Bone marrow suppression (neutropenia, anemia)
GI intolerance, headaches, insomnia

CI:
- Toxicity potentiated by coadmin. of probenecid, acetaminophen, lorazepam, indomethacin and cimetidine. (PLACI)

• Stavudine and ribavirin activated by same pathways (might reduce active levels of zidovudine)

Question 12

Stavudine (d4T): MOA/PK

what does it have high affinity for?

Answer 12

Strong inhibitor of beta and gama DNA polymerases (high affinity for mitochondrial DNA polymerase, which can lead to toxicity)

Nucleoside Analog:
Thymidine

PK: Oral, dosage adjustment required in renal insufficiency

Question 13

Stavudine AE

Answer 13

Peripheral neuropathy, lactic acidosis

Hyperlipidemia, neuromuscular weakness

Question 14

Didanosine (DDL)

Analogue?

Answer 14

Adenosine analogue

PK: Absorption best taken in fasting state (acid labile) or combined with antacid.

• penetrates into CSF
• Dosage adjustment acquired in renal insufficiency

Question 15

Didanosine (DDL) AE:

what does it have high affinity for?

Answer 15

High affinity for mitochondrial DNA polymerase
- Pancreatitis (esp. alcoholics and patients w/ hypertrigglyceridemia) - highest risk
Peripheral neuropathy, diarrheas, hepatic dysfunction
CNS effects

Question 16

Tenofovir (TDF)
Analog of?
Combos?

Answer 16

One of preferred NRTIs in currently recommended regimens

Nucleoside Analog
Adenosine

Fixed-dose combinations available
Tenofovir + emtricitabine
Tenofovir + emtricitabine + efavirenz

Question 17

Tenofovir (TDF) PK/AE

Answer 17

PK: taken w/ food to increase bioavailability
- Long t1/2 (can dose once daily)

AE: GI (nausea, diarrhea, vomiting, flatulence)

Question 18

Tenofovir (TDF) CI?

Answer 18

Serum creatinine monitored with renal insufficiency
Only NRTI with sig. drug interactions (increases didanosine concs. and dosage reductions are usually required)
- Decreases conc. of atazanavir (can be boosted with ritonavir.

Question 19

Lamivudine (3TC) MOA
what does it not affect?
ANALOG?
Resistance?
PK?
AE?

Answer 19

DOes not affect mitochondrial DNA synthesis or bone marrow precursor cells

CYTOSINE

High level of resistance with single amino substitutions.

dosage adjustment requirement w/ renal insufficiency

AE: Few significant (headache, dry mouth)

Question 20

Emtricitabine (FTC)
structurally related to?
ANALOG?
PK?
AE?

Answer 20

lamivudine
One of the prefered NRTIs in currently recommended regimens
Nucleoside analogue: Cytosine
PK: One a day admin.
AE: Hyperpigmentation of palms and soles (occurs most frequently in dark-skinned)

Question 21

Abacavir (ABC)
ANALOG?
RESISTANCE?
AE?

Answer 21

Nucleotide analog:
Guanosine

Resistance:
- HIV resistance requires several mutations and tends to develop slowly.

AE: GI, headache, dizzinesss
- 5% - hypersensitivity reation (one or more of rash, GI, malaise, respiratory distress).

• Sensitized individuals shoud NEVER be rechallenged!!!!! Can be genetically screened

Question 22

Non-Nucleoside Reverse transcriptase inhibitors (NNRTIs) MOA?

Answer 22

MOA

• Highly selective, noncompetitive inhibitors of HIV 1 RT
• Bind at distinct sites away from active sites (NNRTI pocket)
• All NNRTIs bind within the same pocket
• All result in inhibition of RNA and DNA dependent DNA polymerase.
• DO NOT require phosphoryation by cellular enzyms***

Question 23

Advantages of NNRTIs

Answer 23

lack of effect on host blood-forming elements

lack of cross resistance with NRTIs (binding sites are distinct)

Question 24

Disadvantages of NNRTIs

Answer 24

Cross-resistance w/ NNRTIs
Drug interaction
HIGH incidence of hypersensitivity reactions (eg. rash)

Question 25

NNRTIs AE

Answer 25

SKin rash (including stevens-johnson syndrome)
GI intolerance
ALL are CYP3A4 substrates and can act as inducers, inhibitors or both of CYPs.

Question 26

Nevirapine (NVP) Pharmacokinetics

AE?

Answer 26

excreted in urine as metabolites (CYP 3A4 and CYP 2B6)

AE: Potential severe hepatotoxicity ( DON’T use in women w/ CD4+ counts >250 and men >400)
RASH (16%), dermalogic effects (stevens johnson syndrome and toxic epiderml necrolysis)

14 day titration at 1/2 dose is mandatory to reduce risk of serrious epidermal reactions.

Question 27

Nevirapine (NVP)

what enzyme does it induce?

Answer 27

Inducer of CYP 3A4
Increases metabolism of PIs (no dosage adjustment necssary), oral contracpetives, Ketoconazole, methadone, metronidazole, quinidine, theophylline and warfarin).

Question 28

Efavirenz (EFV)
clinical appliations?
PK?

Answer 28

results in increased CD4+ counts and decreased viral load
Not a first line agent in new guidelines (2015)

PK:
Oral, t1/2 >40hrs (once a day dosing)
Extensively metabolized to inactive products

Question 29

Efavirenz (EFV) AE?

Answer 29

High rate of CNS toxicity (50%): dizziness, headache, vivid dreams, loss of concentration- possible association with suicidality.

RASH (25%)

Increased triglycerides, HDL and total cholesterol (lipid levels must be monitored at beginning of and during therapy).

Question 30

Efavirenz (EFV) CI:

Answer 30

Potent inhibitor of CYP 450 enzymes.

Pregnancy (D) (can be used after 1st trimester if considered best choice)

Question 31

Rilpivirine PK/AE

Answer 31

Oral, extensively metabolized to inactive products

AE: RASH, INSOMNIA, DEPRESSION, INCREASED Live enzymes!

Question 32

Protease Inhibitors (PIs) MOA

Answer 32

Reversible inhibitors of aspartyl protease of HIV
- inhibition prevents viral maturation and results in production of non-infectious virions!

DO NOT require intracellular activation
Active against both HIV-1 and HIV-2

Question 33

Protease Inhibitors (PIs) PK?

Answer 33

Poor oral bioavailability
High fat meals increase (nelfinavir) or decrease (indinabir) bioavailabilty
- Substrate for CYP 3A4 (most require enhancing w/ a PK enhancer).
- Substrates for P-glycoprotein pump
- Bound to plasma proteins (alpha1-acid glycoprotein which can increase in response to trauma and surgery).

Question 34

Protease Inhibitors AE

Answer 34

Parathesias, nausea, vomiting diarrhea

• disturbances in lipid metabolism (diabetes, hypertriglycerodemia, hypercholesterolemia)
• Chronic admin –> fat redistribution and accumulation resulting in central obesity, dorsocervical fat enlargement, peripheral and facial wasting, breat enlargement and a cushingoid appearance.***

Question 35

Protease Inhibitors DI:

Answer 35

• Potent inhibitors and substrates of CYP isoforms:
  eg, rhabdomyolysis (simvastatin or lovastatin), excessive sedation (midazolam or triazolam), respiratory depression (fentanyl)
• Warfarin, sildenafil and phenytoin require dosage adjustments
• Rifampin and st. johns wort are CI.

Question 36

Entry/fusion inhibitors
Fusion inhibitor?
Entry inhibitor?

Answer 36

Fusion inhibitor:
- Emfuvirtide
Entry inhibitor
- Maraviroc

Question 37

Enfuvirtide (T-20)
whats special about Enfuvirtide
MOA?

Answer 37

• First approved drug that inhibits viral fusion
• Approved for use in treatment-experienced adults
with evidence of HIV replication**
• No activity against HIV-2

MOA
• Structurally similar to gp41 (HIV protein mediates
membrane fusion)

• Binds to GP41**subunit of the viral envelope glycoprotein,
preventing ability of virion to fuse cell membrane

Question 38

Enfutvirtide (T-20) PK/AE

Answer 38

Pharmacokinetics
• Parenteral admin. only

Adverse Effects
• Injection-related (3% discontinue)
• Hypersensitivity reactions & eosinophilia rarely
• No drug interactions with other antiretrovirals have
been noted

Question 39

MARAVIROC MOA

AE?

Answer 39

Binds specifically to CCR5**

Blocks HIV entry (only CCR5 tropic viruses can be treated with MARAVIROC doesnt work with CXCR4)

Well tolerated, risk of hepato toxicicity

Metabolized by CYP 3A4

Question 40

Integrase Strand Transfer Inhibitors (INSTI’s)

Clinical applications?

Answer 40

Clinical Applications Clinical Applications
• In combination with other antiretrovirals, INSTI’s are
approved for treatment-experienced and treatment-naive
patients with evidence of viral replication

• Currently most popular antiretroviral class due to good
side-effect profile and favorable effects on lipid
metabolism

Question 41

Dolutegravir PK?
AE
DI?

Answer 41

Pharmacokinetics
• Primarily eliminated by glucoronidatoin via UGT1A1
enzyme but some contribution from CYP 3A4.

Adverse Effects Adverse Effects
• Well tolerated (nausea, headache, diarrhea)
• Some reports of organ dysfunction (if so, discontinue
drug)

Drug Interactions
• Can occur due to CYP3A interactions

Question 42

Elvitegravir
PK?
AE?
DI?

Answer 42

Pharmacokinetics
• Primarily metabolized by CYP3A enzymes
• May require ‘enhancing’ with a PK enhancer (Cobicistat)

Adverse Effects
• Well tolerated ( nausea, headache, diarrhea)

Drug Interactions
• Can occur due to CYP interactions

Question 43

Raltegravir
Pk?
AE?
DI?

Answer 43

Pharmacokinetics
• Primarily eliminated by glucoronidation via UGT1A1
enzyme

Adverse Effects
• Well tolerated (nausea, headache, diarrhea)
• Can cause increases in creatine phosphokinases
DI i rug Interactions
• Rifampin, tipranavir & efavirenz may decrease [raltegravir]
• PPI’s may increase [raltegraivr]

Question 44

Pharmacokinetic enhancers

MOA?

Answer 44

• Ritonavir (protease inhibitor)- never used a a protease inhibitor, mostly enhancer
• Cobicistat

MOA
• Potent inhibitors of CYP 3A4
• Increase plasma concentrations of ARV allowing for
lower and/or less frequent dosing
• Improve tolerability of ARV

Question 45

Ritonavir

how is it used?

Answer 45

Used in combo with most protease inhibitors (NOT nelfinavir

Never used alone

Question 46

Cobicistat

Answer 46

Used commonly in combination with the INSTI elvitegravir

Also found in combo w/ darunavir and atazanavir

Question 47

Current recommendations for Tx-naive patients:

Regimens

Answer 47

1. 2*NRTI + INSTI

2. 2*NRTI + PI

Question 48

Current recommendations for Tx-naive patients:

Selection based on:

Answer 48

• Avoiding the use of 2 agents of the same nucleotide
analog
• Avoiding overlapping toxicities and genotypic and
phenotypic characteristics of the virus
• Patient factors such as disease symptoms and concurrent
illnesses
• Impact of drug interactions; and
• Ease of adherence to a frequently complex administration
regimen

Question 49

Current recommendations for Tx-naive patients:

Prefered regimens

Answer 49

INSTI - based regimens

1. Raltegravir + tenofovir + emtricitabine
2. Dolutegravir + tenofovir + emtricitabine

PI-based regimen
1. Ritonavir-boosted darunavir + tenofovir + emticitabine

Question 50

Current recommendations for Infant born to HIV infected mother:

Answer 50

Zidovudine (start immediately after birth and administer for 6 weeks)

Question 51

HIV prophylaxis following a needle stick

Answer 51

Postexposure prophylaxis:

regimen containing atleast 3 antiretroviral drugs

Raltegravir + tenofovir + emtricitabine

for 28 days and can be stopped if source is shown to be HIV negative

Question 52

What Vaccines are recommeded for all HIV patients

Answer 52

Strep. Pneumoniae
Hep A
Hep B
Influenza

Question 53

What Vaccines are CI’d in HIV+ patients w/ CD4+ count

Answer 53

Live vaccines eg,
MMR
Varicella and
Zoster
other vaccines may be administered w/out regard to the patients CD4+