Absence of HBV and HCV, HTLV-I and -II, and human herpes virus-8 activation after allogeneic RBC transfusion in patients with advanced HIV-1 infection.
Pubmed ID: 12662277
Journal: Transfusion
Publication Date: April 1, 2003
MeSH Terms: Humans, Acquired Immunodeficiency Syndrome, DNA, Viral, Prospective Studies, Virus Activation, Antibodies, Viral, Double-Blind Method, Erythrocyte Transfusion, Hepacivirus, Hepatitis B virus, Herpesvirus 8, Human, Human T-lymphotropic virus 1, Human T-lymphotropic virus 2, Viral Load
Grants: N01 HB 57115, N01 HB 57116, N01 HB 57117, N01 HB 57118, N01 HB 57119, N01 HB 57120, N01 HB 57121, N01 HB 57122, N01 HB 57123, N01 HB 57124, N01 HB 57125, N01 HB 57126, N01 HB 57127, RR 00046
Authors: Kalish LA, Busch MP, Lee TH, Murphy EL, Mohr BA, Laycock ME, Asmuth DM, Gallarda J, Giachetti C, Dollard SC, van der Horst CM, Grant RM
Cite As: Asmuth DM, Kalish LA, Laycock ME, Murphy EL, Mohr BA, Lee TH, Gallarda J, Giachetti C, Dollard SC, van der Horst CM, Grant RM, Busch MP, Viral Activation Transfusion Study Group. Absence of HBV and HCV, HTLV-I and -II, and human herpes virus-8 activation after allogeneic RBC transfusion in patients with advanced HIV-1 infection. Transfusion 2003 Apr;43(4):451-8.
Studies:
Abstract
BACKGROUND: The Viral Activation Transfusion Study was a prospective, randomized, double-blind comparison of transfusion with WBC-reduced versus non-WBC-reduced RBCs to HIV+ patients. The primary study characterized the effect of transfusion on HIV and CMV activation by monitoring viral load changes. The present study analyzed HBV, HCV, HTLV-I and -II, and human herpes virus-8 (HHV-8) viral load before and after transfusion to evaluate the further hypothesis that global immune stimulation following allogeneic RBC transfusion results in activation and increased viral proliferation of chronic viral infections other than HIV and CMV. STUDY DESIGN AND METHODS: Baseline samples from 519 to 523 subjects were screened for HBV, HCV, HTLV-I and -II, and HHV-8 infection, and baseline, serial weekly, and quarterly blood samples from infected subjects in the non-WBC-reduced arm were evaluated for changes from baseline in viral nucleic acid and ALT levels. RESULTS: Seroprevalence of HBV, HCV, HTLV-I and -II, and HHV-8 was 68, 25, 5, and 30 percent, respectively. No significant induction of HBV, HCV, HHV-8, or HTLV-I and -II viral replication following allogeneic transfusion of non-WBC-reduced blood was observed. A significant, albeit small, association was observed between transfusion and ALT. CONCLUSIONS: Based on these results and our previous finding that no adverse effect on HIV and CMV viral load and disease progression results from allogeneic transfusion, no evidence is found to support the selective use of WBC-reduced blood components for HIV-infected patients.