Author: McIntyre, Kim W.; Natuk, Robert J.; Biron, Christine A.; Kase, Kenneth; Greenberger, Joel; Welsh, Raymond M.
Title: Blastogenesis of Large Granular Lymphocytes in Nonlymphoid Organs Cord-id: 540gkpel Document date: 1988_6_1
ID: 540gkpel
Snippet: High numbers of large granular lymphocytes (LGL) accumulate in the livers and peritoneal cavities of mice during the course of viral infection. Accumulation of natural killer (NK) cells at day 3 postinfection (p.i.) was shown to be radiationâ€sensitive, implying that proliferation was required for this response. Accumulation occurred in splenectomized mice, indicating that the spleen, known to be an organ for mature NK cell proliferation, was not the major source for liver and peritoneal NK/LGL
Document: High numbers of large granular lymphocytes (LGL) accumulate in the livers and peritoneal cavities of mice during the course of viral infection. Accumulation of natural killer (NK) cells at day 3 postinfection (p.i.) was shown to be radiationâ€sensitive, implying that proliferation was required for this response. Accumulation occurred in splenectomized mice, indicating that the spleen, known to be an organ for mature NK cell proliferation, was not the major source for liver and peritoneal NK/LGL. Significant percentages (> 25%) of the LGL found in the liver and peritoneal cavity following viral infection or interferon induction with polyâ€inosinic:poryâ€cytidylic acid were defined morphologically as blasts (large cells with prominent nucleoli and intensely basophilic cytoplasms containing azurophilic granules). Most blast LGL at day 3 p.i. were sensitive to administration of antiâ€asialo GM(1) serum in vivo, were Lytâ€2(â€), and were enriched in populations that lysed NK cellâ€sensitive targets in vitro, indicating that these were NK/LGL. At day 3 p.i., leukocytes from the liver and peritoneal cavity incorporated (3)Hâ€thymidine and bound to and killed NK cellâ€sensitive targets in singleâ€cell cytotoxicity assays. These data suggest that NK/LGL undergo at least one round of division in the liver and peritoneal cavity during viral infection. In contrast, blast LGL at day 7 p.i. were resistant to in vivo treatments with antiâ€asialo GM(1) serum, were Lytâ€2(+), and were enriched in populations of cells that killed virusâ€infected histocompatible targets, indicating that they were cytotoxic T lymphocytes (CTL). These results suggest that both NK/LGL and CTL/LGL are capable of blastogenesis and presumed proliferation at sites of virus infection, providing a means for the in situ augmentation of a host's cellâ€mediated antiviral defenses.
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