Patients with rheumatoid arthritis and polymyositis treated with the immunosuppresive drug methotrexate (MTX) develop Epstein–Barr virus (EBV)-positive lymphomas more frequently than healthy individuals or similar patients treated with non-immunosuppressive drugs. Wen-hai Feng, Jeffrey I. Cohen et al. now report that MTX might promote EBV-positive lymphomas in these patients by a combination of immunosuppression and reactivation of latent EBV.

Latent infection is associated with cellular transformation of B cells, but the lytic form of infection, which leads to release of virus particles and death of the host cell, might also increase the number of latently EBV-infected B cells and increase the likelihood of malignancy. Using pharmacological doses of MTX, the authors showed that MTX induced lytic infection in an EBV-positive latently infected gastric carcinoma cell line (AGS-EBV-GFP) and in EBV-positive lymphoblastoid cell lines (LCLs). Other drugs used to treat rheumatoid arthritis did not have this effect.

To investigate whether MTX induced lytic EBV gene expression directly Feng and Cohen et al. transfected EBV-negative cells with the promoters of the early lytic viral proteins BZLF1 and BRLF1 linked to a reporter gene and treated them with MTX — the expression of the reporter gene more than doubled in both experiments. But is this expression accompanied by replication of lytic EBV DNA? Treatment of AGS-EBV-GFP cells with MTX increased the copies of the lytic EBV genome and this effect was inhibited by addition of the antiviral drug acyclovir. This induction of replication seems to be MTX specific, because gemcitabine, which also induced lytic viral gene expression, did not increase replication of EBV DNA. Furthermore, when drug-free medium was taken from MTX-treated AGS-EBV-GFP cells and used to infect an EBV-positive Burkitt's lymphoma cell line, GFP expresion was detected in the resulting infected cells, indicating that MTX had induced release of infectious virions.

So what effect does MTX have on EBV loads in patients with rheumatoid arthritis or polymyositis? The mean EBV load in 29 patients receiving treatment regimens including MTX was 40 EBV copies per 106 cellular genomes, compared with 5.1 EBV copies in the 12 patients on regimens that did not include MTX.

The authors conclude that the unique ability of MTX to induce EBV replication at the same time as suppressing the immune system might explain the association with EBV-positive lymphomas in patients who already have an increased risk of these malignancies. Whether MTX treatment of cancer patients has any effect on EBV reactivation or any link with EBV-associated tumours should be investigated.