HTLV-I Activates Complement Leading to Increased Binding to Complement Receptor-Positive Cells

This investigation was performed to determine whether HTLV-I can activate complement, since previous studies show that complement activation by some viruses, including HTV-1, can enhance binding to, and infection of complement receptor-positive (CR⁺) cells. Complement treatment increased binding of HTLV-I to CR⁺ HPB-ALL cells by approximately 5-fold. In contrast, increased binding was not observed with H9 cells, which lack CR. Heat inactivation or EDTA treatment of complement blocked this increased binding while EGTA treatment only partially blocked binding. Anti-CR2 antibody significantly blocked binding of complementtreated HTLV-I to HPB-ALL cells. Since previous studies showed that HIV-1 could activate complement, activation of complement by this virus was compared with HTLV-I. It was observed that binding of HTLV-I to HPB-ALL cells was enhanced by highly dilute complement (≥ 1:810) while HIV-1 required much higher concentrations of complement (≥1:30), indicating that HTLV-I is a much stronger complement activator. Treatment with complement transiently increased the ability of HTLV-I to infect CR⁺ cell lines as judged by provirus formation (4- to 8-fold increase) and p24 production (5- to 10-fold increase). In contrast, complement treatment did not increase infection of CR^- cells. In conclusion this study shows that HTLV-I activates complement leading to increased binding to, and transiently increased infection of, CR⁺ cells. This complement-mediated increased binding of HTLV-I may dramatically affect viral trafficking and immunological reactivity of virus in vivo.