[PDF][PDF] EBV persistence in memory B cells in vivo

GJ Babcock, LL Decker, M Volk, DA Thorley-Lawson - Immunity, 1998 - cell.com
GJ Babcock, LL Decker, M Volk, DA Thorley-Lawson
Immunity, 1998cell.com
Epstein-Barr virus establishes latency in vitro by activating human B cells to become
proliferating blasts, but in vivo it is benign. In the peripheral blood, the virus resides latently
in resting B cells that we now show are restricted to the sIgD− memory subset. However, in
tonsils the virus shows no such restriction. We propose that EBV indiscriminately infects B
cells in mucosal lymphoid tissue and that these cells differentiate to become resting memory
B cells that then enter the circulation. Activation to the blastoid stage of latency is an …
Abstract
Epstein-Barr virus establishes latency in vitro by activating human B cells to become proliferating blasts, but in vivo it is benign. In the peripheral blood, the virus resides latently in resting B cells that we now show are restricted to the sIgD memory subset. However, in tonsils the virus shows no such restriction. We propose that EBV indiscriminately infects B cells in mucosal lymphoid tissue and that these cells differentiate to become resting memory B cells that then enter the circulation. Activation to the blastoid stage of latency is an essential intermediate step in this process. Thus, EBV may persist by exploiting the mechanisms that produce and maintain long-term B cell memory.
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