Only rare cases of CHOP-induced Inhibitor Library nmr remission have been reported in patients simultaneously treated with HAART [13,14]. The induction of NF-κB in PEL cell lines has led to the investigation of proteasome inhibition in NF-κB-driven haematological malignancies. Bortezomib has recently been approved for the use in multiple myeloma and would seem an attractive therapy for PEL because of its intrinsic biology. Further antiviral approaches have been tried and in one patient the combination of interferon-alpha and AZT has been used with success [15]. Current clinical trials by
the NCI utilize a combination approach with antivirals, bortezomib and systemic chemotherapy. Further approaches include targeting latency phase genes such as LANA-1 see more using siRNAs to silence viral regulatory proteins and augmentation of host immunity against HHV8. We suggest that first-line treatment of PEL in HIV-infected individuals includes CHOP-like regimens. No comparative studies have been performed and there is no optimal gold-standard therapy (level of evidence
2C). Patients, where possible, should be entered into clinical trials that are testing novel targeted approaches (GPP). We recommend that chemotherapy regimens should be combined with HAART (level of evidence 1C). 1 Boulanger E, Gerard L, Gabarre J et al. Prognostic factors and outcome of human herpesvirus 8-associated primary effusion lymphoma in patients with AIDS. J Clin Oncol 2005; 23: 4372–4380. 2 Cotter MA 2nd, Robertson ES. The latency-associated nuclear antigen tethers the Kaposi’s sarcoma-associated herpesvirus genome to host chromosomes in body cavity-based lymphoma cells. Virology 1999; 264: 254–264. 3 Friborg J Jr, Kong W, Hottiger MO, Nabel GJ. p53 inhibition by the LANA protein of KSHV protects against cell death. Nature 1999; 402: 889–894. 4 Radkov SA, Kellam P, Boshoff C. The latent nuclear antigen of Kaposi sarcoma-associated herpesvirus targets the retinoblastoma-E2F pathway and with the oncogene Hras transforms primary rat cells.
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