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Virological, immunological, and clinical impact of switching from protease inhibitors to nevirapine or to efavirenz in patients with human immunodeficiency virus infection and long-lasting viral suppression.

作者信息

Negredo Eugenia, Cruz Luís, Paredes Roger, Ruiz Lidia, Fumaz Carmina R, Bonjoch Anna, Gel Silvia, Tuldrà Albert, Balagué Montserrat, Johnston Susan, Arnó Albert, Jou Antoni, Tural Cristina, Sirera Guillem, Romeu Joan, Clotet Bonaventura

机构信息

Fundació Lluita contra la SIDA, Hospital Universitari Germans Trias i Pujol, Barcelona, Spain.

出版信息

Clin Infect Dis. 2002 Feb 15;34(4):504-10. doi: 10.1086/324629. Epub 2002 Jan 2.

DOI:10.1086/324629
PMID:11797178
Abstract

Seventy-seven subjects infected with human immunodeficiency virus were randomized to switch from protease inhibitor (PI) therapy to nevirapine therapy (group A; n=26) or to efavirenz therapy (group B; n=25) or to continue PI therapy (group C; n=26). At month 12, viral suppression had been maintained in 96% of patients in group A, 92% of patients in group B, and 92% of patients in group C. A significant increase in the CD4(+) level was observed in all 3 groups. In group A, lipid profiles improved, whereas levels of gamma-glutamiltransferase and alanine aminotransferase significantly increased; 1 subject interrupted treatment because of hepatotoxicity. In group B, an increase in gamma-glutamiltransferase levels was also observed, and 3 patients interrupted treatment because of central nervous system symptoms. Two patients in group C withdrew therapy. Quality of life significantly improved for groups A and B. In patients receiving effective PI-based therapy, the replacement of the PI with either nevirapine or efavirenz is safe and virologically effective.

摘要

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