Nursing Pharmacology: Antiviral Drugs
Entry Inhibitors
Antiretroviral Drugs Used in Treating HIV Infection
→Entry Inhibitors:
HIV viral entry may be inhibited by two drugs classified as "entry inhibitors" and these agents act by different mechanisms.6
One agent, enfuvirtide (Fuzeon) prevents viral and cell membrane fusion, a process mediated by molecular interactions between viral gp41 and the target cell surface binding site CD4.
The second agent, maraviroc (Selzentry or Celsentri), is classified as a chemokine receptor inhibitor, binding to host cell CCR5 receptors with the consequent effect of preventing HIV viral gp120 protein association.6
The drug enfuvirtide, derived from gp41, binds to gp41 in a way that prevents the structural change needed for fusion.
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Enfuviritide (Fuzeon) is a synthetic peptide consisting of 36 amino acids.6
Part of its amino acid sequence was modelled based on the sequence of the transmembrane gp41 HIV-1 protein important in viral membrane fusion with the target cell membrane.
Enfuviritide exhibits selectivity against HIV-1 laboratory and clinical variants; moreover, this drug is not active against HIV-2.
The mechanism of anti-HIV activity was determined associated with inhibition of HIV-mediated membrane fusion.
Enfuviritide exhibits a unique pharmacodynamic anti-retroviral mechanism, blocking the interaction between the N36 and C34 sequences of the gp41 glycoprotein.6
The peptide inhibition is due to association in the hydrophobic groove associated with the N36 coil.
Because of its distinctive mechanism of antiretroviral action, enfuviritide may continue to exhibit antiretroviral activity in patients in which their viral isolates exhibit resistance to antiretroviral drugs associated with other classes.
However, HIV-enfuvirtide resistance may develop as a result of mutations in the enfuvirtide- gp41 binding domain.
Patients exhibiting virologic failure while on enfuvirtide treatment usually (94%) present with mutations in this gp41 region (in vitro).
Single amino acid substitutions at one of two common mutation sites may increase resistance by 450 fold in laboratory tests.
However, clinical resistance typically presents with two or more amino acid alterations.
Enfuviritide (Fuzeon) was as of 2011 the only approved antiretroviral agent requiring parenteral administration, with the bioavailability of subcutaneously administered enfuvirtide estimated at about 80% compared to the IV dose.6
The approximate elimination half-life (t½) of the parenteral drug is about four hours, thus requiring twice-daily dosing.
Adverse effects:6
Injection site reactions represent the most prominent adverse effect with nearly all patients exhibiting injection site pain, erythema and induration.
About 5% of patients discontinue therapy due to these local reactions.
Clinical indications:6
Enfuvirtide (Fuzeon) is FDA-approved only for use in those adults exhibiting HIV replication despite ongoing antiretroviral drug treatment.
Adding enfuvirtide to and optimize antiretroviral treatment plan increases the fraction of patients with undetectable plasma HIV-1 RNA concentrations evaluated after six months of treatment.
The magnitude of this effect is described as an increase from about 6% of patients with undetectable plasma HIV-1 RNA to about 16%.
In this consideration undetectable plasma HIV-1 RNA is defined as <50 copies/cc.
Mutations and Resistance to Enfuvirtide:
Resistance to enfuvirtide is mediated by mutations in the enfuvirtide binding region of the gp41 subunits of the HIV envelope protein complex.
A functional Gp41 transmembrane protein is required for host cell infection.
Patients experiencing virologic failure during enfuvirtide treatment typically (>90) exhibited gp41 mutations.6
"High-level" clinical resistance often involves 2 or more amino acid mutations,.6
Pharmacokinetics:
Enfuvirtide is administered parenterally e.g. subcutaneously or by intravenous administration.12
Administration may require twice-daily injections; however, the location of the subcutaneous injection site does not appear to influence drug pharmacokinetics.6
Enfuvirtide half-life is about 4 hours after a single 90-mg subcutaneous dose within associated apparent clearance of about 30 ml/h/kg.11
Adverse Effects:
Local injection site reactions represent the most common adverse effect associated with enfuvirtide treatment.12
This reaction is characterized by "painful erythematous nodules".
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This adverse reaction only rarely necessitates drug discontinuation.
Headache, dizziness, insomnia nausea represent other side effects that may occur.
Furthermore, enfuvirtide hypersensitivity reactions may also rarely present.
The principal laboratory abnormality following enfuvirtide administration is an eosinophilia. Drug-drug interactions that would require dosage adjustment have not been noted.12
Therapeutics:
Enfuvirtide (Fuzeon) has received FDA approval for use in treatment-experienced adults presenting with significant, continuing HIV replication in the face of continuing standard antiretroviral treatment.6
Beneficial response with enfuvirtide is more likely to occur in those patients receiving at least two other effective antiretroviral agents in the protocol.
For several reasons including administration convenience, cutaneous toxicity described above, and cost, enfuvirtide is usually given only to those patients who have "failed all other feasible antiretroviral regimens".6
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