Glutamate secretion and metabotropic glutamate receptor 1 expression during Kaposi's sarcoma-associated herpesvirus infection promotes cell proliferation.

[primary effusion lymphoma]

Kaposi 's sarcoma associated herpesvirus (KSHV ) is etiologically associated with endothelial Kaposi 's sarcoma (KS ) and B-cell proliferative primary effusion lymphoma (PEL ), common malignancies seen in immunocompromised HIV-1 infected patients . The progression of these cancers occurs by the proliferation of cells latently infected with KSHV , which is highly dependent on autocrine and paracrine factors secreted from the infected cells . Glutamate and glutamate receptors have emerged as key regulators of intracellular signaling pathways and cell proliferation . However , whether they play any role in the pathological changes associated with virus induced oncogenesis is not known . Here , we report the first systematic study of the role of glutamate and its metabotropic glutamate receptor 1 (mGluR 1 ) in KSHV infected cell proliferation . Our studies show increased glutamate secretion and glutaminase expression during de novo KSHV infection of endothelial cells as well as in KSHV latently infected endothelial and B-cells . Increased mGluR 1 expression was detected in KSHV infected KS and PEL tissue sections . Increased c-Myc and glutaminase expression in the infected cells was mediated by KSHV latency associated nuclear antigen 1 (LANA -1 ). In addition , mGluR 1 expression regulating host RE-1 silencing transcription factor /neuron restrictive silencer factor (REST /NRSF ) was retained in the cytoplasm of infected cells . KSHV latent protein Kaposin A was also involved in the over expression of mGluR 1 by interacting with REST in the cytoplasm of infected cells and by regulating the phosphorylation of REST and interaction with Î²-TRCP for ubiquitination . Colocalization of Kaposin A with REST was also observed in KS and PEL tissue samples . KSHV infected cell proliferation was significantly inhibited by glutamate release inhibitor and mGluR 1 antagonists . These studies demonstrated that elevated glutamate secretion and mGluR 1 expression play a role in KSHV induced cell proliferation and suggest that targeting glutamate and mGluR 1 is an attractive therapeutic strategy to effectively control the KSHV associated malignancies .