Literature DB >> 1715569

Mouse macrophage clones immortalized by retroviruses are functionally heterogeneous.

L Pirami1, B Stockinger, S B Corradin, M Sironi, M Sassano, P Valsasnini, M Righi, P Ricciardi-Castagnoli.   

Abstract

Murine macrophage clones were generated from thymus, spleen, brain, and bone marrow by in vitro immortalization with recombinant retroviruses carrying an avian v-myc oncogene. The cloned cell lines express F4/80 molecules, exert phagocytosis, have nonspecific esterase activity, and express class II molecules after interferon gamma activation. The macrophage clones are diploid and their karyotypes have remained stable for greater than 3 years in culture. After the macrophage clones were activated, their pattern of cytokine production was investigated. Functional heterogeneity in cytokine transcription was demonstrated: one of six liposaccharide-activated macrophages was unable to transcribe interleukin 1 alpha, whereas all of the liposaccharide-activated clones were able to transcribe tumor necrosis factor alpha. Interleukin 6 production was detected in three of six clones. The production of nitrite and tumor necrosis factor alpha as effector molecules of cytotoxicity was detected in all clones, thus showing that a single macrophage can exert more than one cytotoxic mechanism. The results indicate that immortalized and cloned macrophages have a differentially regulated expression of cytokine genes, adding further evidence for the existence of functional heterogeneity among cloned macrophages. This heterogeneity seems to derive from differentiation-related mechanisms rather than from external constraints.

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Year:  1991        PMID: 1715569      PMCID: PMC52337          DOI: 10.1073/pnas.88.17.7543

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  28 in total

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4.  Plasma membrane-associated tumor necrosis factor. A non-integral membrane protein possibly bound to its own receptor.

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6.  Release of reactive nitrogen intermediates and reactive oxygen intermediates from mouse peritoneal macrophages. Comparison of activating cytokines and evidence for independent production.

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7.  Cell-associated tumor necrosis factor (TNF) as a killing mechanism of activated cytotoxic macrophages.

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8.  Activation of the M-CSF gene in mouse macrophages immortalized by retroviruses carrying a v-myc oncogene.

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9.  Macrophage cytotoxicity: role for L-arginine deiminase and imino nitrogen oxidation to nitrite.

Authors:  J B Hibbs; R R Taintor; Z Vavrin
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