Antiretrovirals for final

Question 1

Zidovudine (Azidothymidine or AZT)

Answer 1

Class NRTI

MOA: termination. The inhibitor binds to the DNA chain and terminates the production of DNA. Require phosphorylation by cellular enzymes to the triphosphate to be active.

Resistance - Resistance to one may may result in resistance to another within the class.

General adverse events - Potentially fatal syndrome of lactic acidosis with hepatic steatosis, probably due to mitochondrial toxicity. Associated with fat redistribution and hyperlipidemia.

Specific adverse events - Granulocytopenia and anemia in up to 45% of treated patients (monitor at 2 week intervals), CNS disturbances (severe headache, nausea, insomnia, and malaise)

Question 2

Lamivudine

Answer 2

Class - NRTI

MOA: termination. The inhibitor binds to the DNA chain and terminates the production of DNA. Require phosphorylation by cellular enzymes to the triphosphate to be active.

Resistance - Resistance to one may may result in resistance to another within the class.

General adverse events - Potentially fatal syndrome of lactic acidosis with hepatic steatosis, probably due to mitochondrial toxicity. Associated with fat redistribution and hyperlipidemia.

Probably the best tolerated of NRTIs. Also active vs. Hep. B.

Question 3

Abacavir

Answer 3

Class - NRTI

MOA: termination. The inhibitor binds to the DNA chain and terminates the production of DNA. Require phosphorylation by cellular enzymes to the triphosphate to be active.

Resistance - Resistance to one may may result in resistance to another within the class.

General adverse events - Potentially fatal syndrome of lactic acidosis with hepatic steatosis, probably due to mitochondrial toxicity. Associated with fat redistribution and hyperlipidemia.

Specific Adverse Events: Hypersensitivity reactions.

Question 4

Emtricitabine

Answer 4

Class - NRTI

MOA: termination. The inhibitor binds to the DNA chain and terminates the production of DNA. Require phosphorylation by cellular enzymes to the triphosphate to be active.

Resistance - Resistance to one may may result in resistance to another within the class.

General adverse events - Potentially fatal syndrome of lactic acidosis with hepatic steatosis, probably due to mitochondrial toxicity. Associated with fat redistribution and hyperlipidemia.

Probably the best tolerated of NRTIs. Also active against Hep. B.

Question 5

Tenofovir

Answer 5

Class - NRTI

MOA: termination. The inhibitor binds to the DNA chain and terminates the production of DNA. Require phosphorylation by cellular enzymes to the triphosphate to be active.

Adverse Events: Most common is nausea, vomiting, diarrhea and potential for renal failure. Potentially fatal syndrome of lactic acidosis with hepatic steatosis, probably due to mitochondrial toxicity

Specific A.E. - Renal toxicity.

Question 6

Etravirine

Answer 6

Class - NNRTI

MOA - NNRTIs bind directly to the reverse transcriptase at a site distinct from that of the NRTI. The enzyme cannot then produce viral DNA. Do not require phosphorylation for activity and are primarily effective against HIV-1.

Resistance - No cross resistance with NNRTIs and NRTIs and protease inhibitors.

General Adverse Events - Varying levels of GI intolerance and skin rash.

Specific Adverse Events - Rash, nausea, peripheral neuropathy

PK: CYP 450 - Drug interactions. They can be inducers, inhibitors, or mixed inducers/inhibitors.

Question 7

Efavirenz

Answer 7

Class - NNRTI

Class - NNRTI

MOA - NNRTIs bind directly to the reverse transcriptase at a site distinct from that of the NRTI. The enzyme cannot then produce viral DNA. Do not require phosphorylation for activity and are primarily effective against HIV-1.

Resistance - No cross resistance with NNRTIs and NRTIs and protease inhibitors.

General Adverse Events - Varying levels of GI intolerance and skin rash.

Specific Adverse Events - CNS effects (vivid dreams, nightmares, and hallucinations)

PK: CYP 450 - Drug interactions. They can be inducers, inhibitors, or mixed inducers/inhibitors.

Once a day administration.

Question 8

Atazanavir

Answer 8

Class - Protease Inhibitor

MOA: These drugs prevent protease action required for maturation of the fully assembled virus. As the virus is budding, proteolytic cleavage occurs. Without this cleavage, the virus is not infectious.

General Adverse Events:

• GI disturbances
• Hepatotoxicity
• Hyperglycemia and insulin resistance
• Dyslipidemia
• Cardiac conduction abnormalities
• Peripheral lipoatrophy and central fat accumulation

PK - Metabolized by and inhibit hepatic CYP3A4

Given with Ritonavir booster

Question 9

Darunavir

Answer 9

Class - Protease Inhibitor

MOA: These drugs prevent protease action required for maturation of the fully assembled virus. As the virus is budding, proteolytic cleavage occurs. Without this cleavage, the virus is not infectious.

General Adverse Events:

• GI disturbances
• Hepatotoxicity
• Hyperglycemia and insulin resistance
• Dyslipidemia
• Cardiac conduction abnormalities
• Peripheral lipoatrophy and central fat accumulation

PK - Metabolized by and inhibit hepatic CYP3A4

Given w/ Ritonavir booster

Question 10

Ritonavir

Answer 10

Class - Protease Inhibitor

MOA: These drugs prevent protease action required for maturation of the fully assembled virus. As the virus is budding, proteolytic cleavage occurs. Without this cleavage, the virus is not infectious.

General Adverse Events:

• GI disturbances
• Hepatotoxicity
• Hyperglycemia and insulin resistance
• Dyslipidemia
• Cardiac conduction abnormalities
• Peripheral lipoatrophy and central fat accumulation

PK -Metabolized by and inhibit hepatic CYP3A4

High doses of the protease inhibitor ritonavir are poorly tolerated. However, it is used at lower doses to increase the serum concentrations of other protease inhibitors, and decrease the dosage frequency of other PIs. Ritonavir is a potent inhibitor of CYP3A4 which is the cytochrome that metabolizes a number of the other PIs and decreases their effectiveness.

Question 11

Enfuviritide

Answer 11

Class - Fusion Inhibitor

MOA -Binds to gp41 and prevents the conformational change needed for fusion.

PK - Subcutaneous administration twice daily.

Adverse effects - High incidence of local reactions with pain erythema, induration, nodules, and cysts. Rare systemic hypersensitivity. Higher incidence of bacterial pneumonia.

Active against HIV resistant to other classes of antiretrovirals (last resort drug)

Question 12

Raltegravir

Answer 12

Class - Integrase Inhibitor (or Integrase Strand Transfer Inhibitors, INSTI)

MOA - . By binding integrase, it inhibits strand transfer, the final step of provirus integration.

PK: Fewer drug drug interactions than PI or NNRTI based regimens.

Question 13

Maroviroc

Answer 13

Class - CCR5 Antagonist

MOA: Specifically and selectively blocks host CCR5

Question 14

Cobicistat

Answer 14

Pharmacokinetic enhancer that inhibits CYP3A4 as well as certain intestinal transport proteins and can also act as a booster of protease inhibitors. It is not a protease inhibitor itself.

Question 15

HAART

Answer 15

Highly Active Antiretroviral Therapy

Generally reference to therapy with RTIs in combination with PI. Long term use of combination anti-retroviral therapy is associated with secondary effects, the most prevalent being HAART lipodystrophy.

HAART Lipodystrophy:

• Estimated to affect 25-50%
• Wasting of subcutaneous fat
• Central adiposity
• Hyperlipidemia, insulin resistance, and DM
• Most often seen with use of NRTIs + PI, but also seen with single NRTI treatment.

Question 16

Truvada

Answer 16

tenofovir and emtricitabine

Used as PrEP (pre exposure prophylaxis) –> use for HIV negative spouses, sex workers, and IV drug users.