Lymphoid hyperplasia and lymphoma in KSHV K1 transgenic mice.

[primary effusion lymphoma]

Growing evidence supports the involvement of human herpervirus 8 , Kaposi 's sarcoma associated herpesvirus (KSHV ), in the pathology of primary effusion lymphoma , multicentric Castleman 's disease , and Kaposi 's sarcoma , but the exact mechanism of KSHV contribution to the oncogenic process remains elusive . We studied transgenic mice expressing the ORF K 1 of KSHV , whose position in the KSHV genome corresponds to known lymphoproliferative genes of other herpesviruses . K 1 protein was previously shown to contain a constitutively active ITAM domain , involved in activation of Akt and pro-survival signaling , and to inhibit Fas-mediated apoptosis by interfering with binding of FasL . All this pointed to a possible role of K 1 in the pathogenesis of KSHV-associated cancers . K 1 transgenic mice (80 -90 %) developed lymphoid hyperplasia and splenomegaly at 8 and 10 months of age , 25 % had confirmed diagnosis of lymphoma , and 50 % developed abdominal and /or hepatic tumors by 18 months of age . Histological examination showed loss of splenic architecture and increased cellularity . Lymph nodes showed disrupted architecture with effaced follicles and other pathological changes , including signs of angiofollicular lymphoid hyperplasia . One of the livers showed signs of angiosarcoma . In summary , our histology results revealed pathological changes in K 1 transgenic mice similar to lymphoma , Castleman 's disease , and angiosarcoma , suggesting that K 1 may contribute to the development of KSHV-associated cancers .