HIV Infections Clinical Trial
Official title:
Randomized Multicenter Study to Compare Starting Nevirapine at the Full Dose With Dose Escalation in Patients Who Require Efavirenz to be Withdrawn Due to Adverse Reactions
This study aims to compare the trough plasma concentrations of nevirapine after 7 days of treatment at the full dose from baseline with dose escalation in patients taking efavirenz who switch to nevirapine due to neuropsychiatric adverse reactions.
The prognosis for HIV infection changed radically after 1996 thanks to the arrival of
protease inhibitors (PI), which, when combined with 2 nucleoside analogue reverse
transcriptase inhibitors (NRTI) formed the so-called highly active antiretroviral therapy
(HAART). HAART led to a considerable decrease in the incidence and mortality of
opportunistic infections and made HIV infection a chronic condition and not necessarily the
progressive, irreversible, and fatal disease it was before 1996. The initial euphoria led
people to believe that HAART could cure the disease, but it was soon clear that eradication
of the virus was impossible and that treatment would have to be continued indefinitely.
Chronic treatment became more difficult because of the frequent onset of adverse events or
extremely complex regimens with a high pill burden that had to be administered several times
per day, often with dietary restrictions.1,2 In this context, adherence was difficult,
efficacy was far from optimal, and the patient's quality of life was noticeably reduced. The
subsequent appearance of non-nucleoside analogue reverse transcriptase inhibitors
(NNRTI)—nevirapine and efavirenz—considerably improved some of the disadvantages of PIs.
Today, the combination of 2 NRTIs and an NNRTI is considered the regimen of choice when
starting antiretroviral therapy. Efavirenz is considered the gold standard for initial
antiretroviral therapy and is widely used in clinical practice.
More than half of the patients who start treatment with efavirenz present adverse effects,
although these are generally well tolerated and decrease with time. Approximately 3%-8% of
patients have to suspend efavirenz due to adverse effects, which are mainly
neuropsychiatric. In these cases, efavirenz is usually replaced by nevirapine.
Nevirapine is a substrate and potent inducer of the hepatic cytochrome P450 enzyme system
(CYP3A4 and others) and continuous administration leads to progressive autoinduction of its
own metabolism. The recommended dose is 200 mg every 12 hours. If this dose is administered
from the start of treatment, the plasma concentrations reached during the first few days are
much higher than those reached later. Therefore, and because the toxicity of nevirapine is
associated with its plasma concentrations, the recommended initial dose is 200 mg/d for the
first 14 days followed by 200 mg every 12 hours indefinitely. There are no specific
recommendations on dosage when nevirapine replaces efavirenz; therefore, it is administered
at increasing doses according to the summary of product characteristics.
Efavirenz is also a potent inducer of CYP3A4 and increases the metabolism of other drugs
that use this metabolic pathway. Enzyme induction is by increased synthesis of the enzymes
involved, with the result that, when the inducer is suspended, the enzyme induction effect
persists for a few days until the excess enzymes are catabolized. Furthermore, the half-life
of efavirenz is very long. Consequently, the plasma concentrations fall progressively for
more than a week after the drug is withdrawn. Therefore, when efavirenz is replaced by
nevirapine, the residual enzyme induction that persists might lead to a fall in the plasma
concentrations of nevirapine. Given that NNRTIs have a low genetic barrier for the
development of resistance, the fall in plasma concentrations of nevirapine for the 14 days
during which it is administered at 200 mg/d can generate resistance mutations and virologic
failure.
When efavirenz is switched for nevirapine, it is unknown whether nevirapine should be
started at increasing standard doses (200 mg/d for the first 14 days plus 200 mg bid
thereafter) or at the full dose (200 mg every 12 hours) as a consequence of the enzyme
induction caused by efavirenz.
Currently available data do not enable us to make a recommendation on the dose with which
treatment with nevirapine can be started in patients who required efavirenz to be withdrawn
and for whom nevirapine was chosen as an alternative. Nevertheless, despite small sample
sizes, preliminary studies suggest that this strategy could be effective and safe.
Therefore, randomized clinical trials that enable us to evaluate this strategy appropriately
are necessary
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Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label
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