Functional analysis of Kaposi's sarcoma-associated herpesvirus vFLIP expression reveals a new mode of IRES-mediated translation.

[primary effusion lymphoma]

Kaposi 's sarcoma -associated herpesvirus (KSHV ) is an oncogenic virus , the etiological agent of Kaposi 's sarcoma (KS ) and primary effusion lymphoma (PEL ). One of the key viral proteins that contributes to tumorigenesis is vFLIP , a viral homolog of the FLICE inhibitory protein . This KSHV protein interacts with the NFÎºB pathway to trigger the expression of antiapoptotic and proinflammatory genes and ultimately leads to tumor formation . The expression of vFLIP is regulated at the translational level by an internal ribosomal entry site (IRES ) element . However , the precise mechanism by which ribosomes are recruited internally and the exact location of the IRES has remained elusive . Here we show that a 252 -nt fragment directly upstream of vFLIP , within a coding region , directs translation . We have established its RNA structure and demonstrate that IRES activity requires the presence of eIF 4 A and an intact eIF 4 G . Furthermore , and unusually for an IRES , eIF 4 E is part of the complex assembled onto the vFLIP IRES to direct translation . These molecular interactions define a new paradigm for IRES-mediated translation .