News

HIV-1C predicts virologic failure, especially with ritonavir-boosted PIs

View on the News

Adherence may trump viral factors

HIV-1 is diverse worldwide, but antiretroviral drug development has typically used subtype B as a standard. This study highlights the importance of doing studies in different populations representative of the global diversity of subtypes.

We acknowledge that failure rates might be relatively high in real-life settings, [in contrast to] a very low incidence of failure and protease-inhibitor–associated drug resistance in randomized controlled trials. However, a clinically important decreased enzyme affinity for protease inhibitors in HIV-1C will result in decreased susceptibility and will contribute to an increased risk of drug resistance mutations and failure, which currently is not observed in clinical practice.

In our opinion, substantiating impaired enzyme to protease inhibitor affinity as a cause of failure needs evidence of a significant reduction in phenotypic susceptibility and should be investigated further. Adherence is likely a more important predictor of virologic failure than are viral factors, but investigating this conclusively is challenging, given the difficulty of objective assessment of adherence. Other patient-related factors, in addition to adherence, might affect drug concentrations: Data are increasing for interindividual pharmacokinetic variability, which includes pharmacogenetics, concomitant drug interactions, and health and nutritional status of patients. Nevertheless, a better understanding of ritonavir-boosted lopinavir regimen failure remains a priority because these regimens are a last line for many patients in low-resource settings.

Dr. Gert U van Zyl and Dr. Eric H. Decloedt are in the division of medical virology at Stellenbosch University in Cape Town, South Africa. Dr. van Zyl reported receiving an honorarium from Abbvie; Dr. Decloedt reported no conflicts of interest. These comments are from their editorial accompanying the study (Lancet HIV. 2016 Mar 14. doi: 10.1016/S2352-3018[16]00040-0).


 

FROM THE LANCET HIV

References

Patients infected with HIV-1 subtype C failed antiretroviral therapy significantly earlier than did HIV-1B–infected patients, especially when they received ritonavir-boosted protease inhibitors instead of nonnucleoside reverse transcriptase inhibitors, according to a Swedish national cohort study.

“As low- and middle-income countries are poised to scale up second-line antiretroviral therapy containing ritonavir-boosted PIs [protease inhibitors], a concern is that PIs will be less efficient in patients with HIV-1C,” said Dr. Ujjwal Neogi of the Karolinska Institute in Stockholm and his associates. “Studies of new drugs such as integrase inhibitors should be done in patients with HIV-1C and other non-B subtypes, which are responsible for the greatest global HIV burden,” they wrote online in the Lancet HIV.

(Photo: Cynthia Goldsmith, CDC)

HIV-infected patients in low-income and middle-income countries often receive second-line boosted PI-based regimens, but few studies have rigorously looked at treatment response for the HIV-1C subtype, which causes most infections in countries such as Ethiopia, India, and South Africa, the investigators noted. They studied more than 99% of Sweden’s HIV-positive population to identify predictors of virologic failure. The dataset included 1,077 HIV-1B–infected patients and 596 HIV-1C–infected patients; 90% of the latter were immigrants (Lancet HIV. 2016 Mar 14. doi: 10.1016/S2352-3018[16]00023-0).

Predictors of primary virologic failure included higher baseline viral load (odds ratio, 1.8; 95% confidence interval, 1.5-2.2); subtype C infection (OR, 1.75; 1.1-2.9), and boosted PI-based regimens (OR, 1.55; 95% CI, 1.5-2.1). After adjustment for transmission route and duration of antiretroviral therapy, time to secondary virologic failure on boosted PI-based regimens was significantly earlier for HIV-1C–infected patients, compared with HIV-1B patients (hazard ratio, 1.8; 95% CI, 1.3-2.9). However, HIV-1 subtype did not significantly predict time to virologic failure for nonnucleoside reverse transcriptase inhibitor–based regimens.

“The poorer treatment outcome occurred in the patients with HIV-1C despite developed clinical care, modern laboratory monitoring, and focused adherence support at highly HIV-specialized infectious disease clinics in a high-income country,” the researchers wrote. Self-reported adherence to therapy did not differ by treatment regimen or HIV-1 subtype, although adherence data were available for only about a third of HIV-1C–infected patients, they added.

Homology-based molecular modeling also seemed to show a lower affinity between the PIs darunavir and lopinavir and the HIV-1C protease, compared with the HIV-1B protease, said the researchers. “Naturally occurring polymorphisms in HIV-1C protease might affect the binding of at least some protease inhibitors, potentially contributing to the differences we observed,” they concluded.

The study was funded by the Karolinska Institutet Research Foundation, Swedish Research Council, Stockholm County Council, Swedish Physicians against AIDS, National Institutes of Health, and University of Missouri. The investigators had no relevant financial disclosures.

Recommended Reading

HIV-positive life expectancy improves, but gap remains
MDedge Infectious Disease
Urine test use to guide treatment reduced TB mortality in HIV patients
MDedge Infectious Disease
When toenail onychomycosis can turn deadly
MDedge Infectious Disease
Privacy measure inadvertently suppresses substance abuse data
MDedge Infectious Disease
HIV research update: Early March 2016
MDedge Infectious Disease
Continuity of care can limit HIV deaths
MDedge Infectious Disease
Lifetime HIV infection risk declines, but some still at high risk
MDedge Infectious Disease
Sertraline improves Cryptococcus clearance in HIV meningitis
MDedge Infectious Disease
Pediatric infectious disease hospitalizations declined since 2000
MDedge Infectious Disease
HIV research update: Late March 2016
MDedge Infectious Disease