Addition of capravirine to a three-drug regimen not beneficial in patients with NNRTI resistance

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Capravirine, a new nonnucleoside reverse transcriptase inhibitor (NNRTI), failed to control HIV better than placebo in a 48-week study of people with resistance to NNRTIs, according to a report at the Twelfth Conference on Retroviruses and Opportunistic Infections held in Boston, Massachusetts. However, a subgroup analysis suggested that a regimen including capravirine, nelfinavir, and two nucleoside reverse transcriptase inhibitors (NRTIs) had some activity against virus resistant to both zidovudine and lamivudine.

In vitro studies indicate that capravirine is able to inhibit some HIV strains resistant to current NNRTIs. Laboratory work also suggests that resistance to capravirine evolves more slowly than to other NNRTIs, Rick Pesano, MD, PhD reported.

The current trial randomised people taking a failing NNRTI regimen to receive 700mg or 1400mg of capravirine twice daily or placebo. All participants also received twice-daily nelfinavir and two NRTIs picked on the basis of treatment history and genotype. None of the 179 study participants had been previously treated with a protease inhibitor.

Glossary

placebo

A pill or liquid which looks and tastes exactly like a real drug, but contains no active substance.

diarrhoea

Abnormal bowel movements, characterised by loose, watery or frequent stools, three or more times a day.

log

Short for logarithm, a scale of measurement often used when describing viral load. A one log change is a ten-fold change, such as from 100 to 10. A two-log change is a one hundred-fold change, such as from 1,000 to 10.

statistical significance

Statistical tests are used to judge whether the results of a study could be due to chance and would not be confirmed if the study was repeated. If result is probably not due to chance, the results are ‘statistically significant’. 

reverse transcriptase

A retroviral enzyme which converts genetic material from RNA into DNA, an essential step in the lifecycle of HIV. Several classes of anti-HIV drugs interfere with this stage of HIV’s life cycle: nucleoside reverse transcriptase inhibitors and nucleotide reverse transcriptase inhibitors (NRTIs) and non-nucleoside reverse transcriptase inhibitors (NNRTIs). 

Trial enrollees had moderately advanced disease, with an average viral load around 4.4 log copies/mL and median CD4 counts of 206 cells/mm3 in the placebo group, 248 cells/mm3 in the 700-mg capravirine group, and 249 cells/mm3 in the 1400-mg capravirine group. Resistance to NRTIs and NNRTIs was similar across the study arms.

Pesano reported 48-week failure rates—defined as failure to reduce the viral load by 0.5 log by Week 4, or rebounding after a 0.5 log reduction—of 24% with placebo, 15% with 700 mg of capravirine, and 13% with 1400 mg, differences that were not statistically significant. The reductions in viral load from baseline to Week 48 also did not differ significantly: 2.1 logs, 2.3 logs, and 2.4 logs, respectively.

A 48-week noncompleter-equals-failure analysis determined that 58% of patients taking 1400 mg of capravirine twice daily had a viral load below 400 copies/ml, compared with 43% taking 700mg twice daily, and 46% taking placebo. These differences also fell short of statistical significance.

In a preplanned analysis of nonrandomised subgroups who began treatment with virus resistant to zidovudine and lamivudine, 54% in the 1400mg group had a viral load under 400 copies/ml at Week 48, compared with 36% taking 700mg, and 31% taking placebo. This trend was not statistically significant, however.

The better noncompleter response with 1400mg of capravirine partly reflects the high dropout rates in the other 2 arms—44% with placebo, 42% with 700mg capravirine, and 30% with 1400mg capravirine. Whereas 15% of patients stopped the 700mg dose because of side effects, 7% stopped the 1400-mg dose for that reason.

Diarrhoea affected 65% in the 1400mg group and 53% in the 700mg group. However, diarrhoea also was reported by 49% given placebo, and the incidence of diarrhea in all treatment arms may have been due to nelfinavir therapy. Rates of nausea were 35% with 1400mg, 27% with 700mg, and 20% with placebo.

Dr. Pesano noted that the high failure rates in all three study arms came as a surprise, since people started nelfinavir with no protease inhibitor experience and also began carefully chosen NRTIs. The study outcomes will be further scrutinized as the development of capravirine continues.

This content licensed to aidsmap by iMedOptions, publishers of http://clinicaloptions.com. Copyright iMedOptions, LLC, 2005

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References

Pesano R et al. 24-week safety, tolerability, and efficacy of capravirine as add-on therapy to nelfinavir and 2 nucleoside reverse transcriptase inhibitors in patients failing a nonnucleoside reverse transcriptase inhibitor-based regimen. Twelfth Conference on Retroviruses and Opportunistic Infections, Boston, abstract 555, 2005.