A Randomized, Double‐Blind Trial of Valaciclovir Prophylaxis for Cytomegalovirus Disease in Patients with Advanced Human Immunodeficiency Virus Infection | Zendy

Judith Feinberg | Zendy; Shelley Hurwitz | Zendy; David A. Cooper | Zendy; Fred R. Sattler | Zendy; Rob Roy MacGregor | Zendy; William Powderly | Zendy; Gary N. Holland | Zendy; Paul Griffiths | Zendy; Richard B. Pollard | Zendy; M Youle | Zendy; M John Gill | Zendy; F. J. Holland | Zendy; Maureen Power | Zendy; Susan Owens | Zendy; Dion F. Coakley | Zendy; John Fry | Zendy; Mark A. Jacobson | Zendy

Open Access

A Randomized, Double‐Blind Trial of Valaciclovir Prophylaxis for Cytomegalovirus Disease in Patients with Advanced Human Immunodeficiency Virus Infection

Author(s) -

Judith Feinberg,

Shelley Hurwitz,

David A. Cooper,

Fred R. Sattler,

Rob Roy MacGregor,

William Powderly,

Gary N. Holland,

Paul Griffiths,

Richard B. Pollard,

M Youle,

M John Gill,

F. J. Holland,

Maureen Power,

Susan Owens,

Dion F. Coakley,

John Fry,

Mark A. Jacobson

Publication year - 1998

Publication title -

the journal of infectious diseases (online. university of chicago press)/the journal of infectious diseases

Language(s) - English

Resource type - Journals

eISSN - 1537-6613

pISSN - 0022-1899

DOI - 10.1086/513804

Subject(s) - valaciclovir , medicine , discontinuation , human cytomegalovirus , cytomegalovirus , herpesviridae , viral disease , aciclovir , randomized controlled trial , gastroenterology , immunology , virology , virus , surgery

Cytomegalovirus (CMV) disease is a common complication of advanced human immunodeficiency virus (HIV) infection. Administration of oral valaciclovir, a valine ester of acyclovir, achieves sufficient plasma acyclovir levels to inhibit many clinical isolates. Acyclovir has been associated with enhanced survival in AIDS but not with CMV disease prevention. CMV-seropositive patients (1227) with CD4 cell counts <100/mm3 were enrolled in a randomized, double-blind trial. Valaciclovir, 8 g/day, was compared with acyclovir, 3.2 or 0.8 g/day, for CMV prevention; all three arms were compared for survival. The confirmed CMV disease rate was 11.7% among valaciclovir recipients and 17.5% in the pooled acyclovir arms, a 33% reduction in risk. Time to confirmed CMV disease was significantly longer for the valaciclovir group (P = .03). A trend toward earlier mortality for valaciclovir recipients was seen (P = .06). Toxicity and earlier medication discontinuation were more common in this group. Valaciclovir significantly reduces the risk of CMV disease. Further exploration of a better-tolerated dose is warranted.

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