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AIDS:
10 March 2000 - Volume 14 - Issue 4 - pp 357-366
Clinical

Adherence to protease inhibitors, HIV-1 viral load, and development of drug resistance in an indigent population

Bangsberg, David R.; Hecht, Frederick M.; Charlebois, Edwin D.; Zolopa, Andrew R.; Holodniy, Mark; Sheiner, Lewis; Bamberger, Joshua D.; Chesney, Margaret A.; Moss, Andrew

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Abstract

Objective: To examine the relationship between adherence, viral suppression and antiretroviral resistance in HIV-infected homeless and marginally housed people on protease inhibitor (PI) therapy.

Design and setting: A cross-sectional analysis of subjects in an observational prospective cohort systematically sampled from free meal lines, homeless shelters and low-income, single-room occupancy (SRO) hotels.

Participants: Thirty-four HIV-infected people with a median of 12 months of PI therapy.

Main outcomes: Adherence measured by periodic unannounced pill counts, electronic medication monitoring, and self-report; HIV RNA viral load; and HIV-1 genotypic changes associated with drug resistance.

Results: Median adherence was 89, 73, and 67% by self-report, pill count, and electronic medication monitor, respectively. Thirty-eight per cent of the population had over 90% adherence by pill count. Depending on the measure, adherence explained 36-65% of the variation in concurrent HIV RNA levels. The three adherence measures were closely related. Of 20 genotyped patients who received a new reverse transcriptase inhibitor (RTI) when starting a PI, three had primary protease gene substitutions. Of 12 genotyped patients who received a PI without a new RTI, six had primary protease gene substitutions (P < 0.03).

Conclusion: A substantial proportion of homeless and marginally housed individuals had good adherence to PI therapy. A strong relationship was found between independent methods of measuring adherence and concurrent viral suppression. PI resistance was more closely related to the failure to change RTI when starting a PI than to the level of adherence.

© 2000 Lippincott Williams & Wilkins, Inc.

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