Sangivamycin induces apoptosis by suppressing Erk signaling in primary effusion lymphoma cells.

[primary effusion lymphoma]

Sangivamycin , a structural analog of adenosine and antibiotic exhibiting antitumor and antivirus activities , inhibits protein kinase C and the synthesis of both DNA and RNA . Primary effusion lymphoma (PEL ) is an aggressive neoplasm caused by Kaposi 's sarcoma -associated herpesvirus (KSHV ) in immunosuppressed patients and HIV-infected homosexual males . PEL cells are derived from post-germinal center B cells , and are infected with KSHV . Herein , we asked if sangivamycin might be useful to treat PEL . We found that sangivamycin killed PEL cells , and we explored the underlying mechanism . Sangivamycin treatment drastically decreased the viability of PEL cell lines compared to KSHV-uninfected B lymphoma cell lines . Sangivamycin induced the apoptosis of PEL cells by activating caspase-7 and -9 . Further , sangivamycin suppressed the phosphorylation of Erk 1 /2 and Akt , thus inhibiting activation of the proteins . Inhibitors of Akt and MEK suppressed the proliferation of PEL cells compared to KSHV-uninfected cells . It is known that activation of Erk and Akt signaling inhibits apoptosis and promotes proliferation in PEL cells . Our data therefore suggest that sangivamycin induces apoptosis by inhibiting Erk and Akt signaling in such cells . We next investigated whether sangivamycin , in combination with an HSP 90 inhibitor geldanamycin (GA ) or valproate (valproic acid ), potentiated the cytotoxic effects of the latter drugs on PEL cells . Compared to treatment with GA or valproate alone , the addition of sangivamycin enhanced cytotoxic activity . Our data thus indicate that sangivamycin may find clinical utility as a novel anti-cancer agent targeting PEL .