The hematopoietic cell kinase (hck) is a member of the src family of tyrosine kinases, and is primarily expressed in myeloid cells. Hck expression increases with terminal differentiation in both monocyte/macrophages and granulocytes and is further augmented during macrophage activation. Recent evidence has implicated src-related tyrosine kinases in critical signaling pathways in other hematopoietic lineages. Herein we demonstrate that manipulation of the level of hck expression in the murine macrophage cell line BAC1.2F5 alters the responsiveness of these cells to activation by bacterial lipopolysaccharide (LPS) but does not affect survival or proliferation. Overexpression of an activated mutant of hck in BAC1.2F5 cells augments tumor necrosis factor (TNF) production in response to LPS, whereas inhibition of endogenous hck expression, by antisense oligonucleotides, interferes with LPS-mediated TNF synthesis. Together, these observations suggest that hck is an important component of the signal transduction pathways in activated macrophages.
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1 September 1993
Article|
September 01 1993
Hck tyrosine kinase activity modulates tumor necrosis factor production by murine macrophages.
B K English,
B K English
Department of Pediatrics, University of Tennessee, Memphis 38103.
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J N Ihle,
J N Ihle
Department of Pediatrics, University of Tennessee, Memphis 38103.
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A Myracle,
A Myracle
Department of Pediatrics, University of Tennessee, Memphis 38103.
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T Yi
T Yi
Department of Pediatrics, University of Tennessee, Memphis 38103.
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B K English
Department of Pediatrics, University of Tennessee, Memphis 38103.
J N Ihle
Department of Pediatrics, University of Tennessee, Memphis 38103.
A Myracle
Department of Pediatrics, University of Tennessee, Memphis 38103.
T Yi
Department of Pediatrics, University of Tennessee, Memphis 38103.
Online ISSN: 1540-9538
Print ISSN: 0022-1007
J Exp Med (1993) 178 (3): 1017–1022.
Citation
B K English, J N Ihle, A Myracle, T Yi; Hck tyrosine kinase activity modulates tumor necrosis factor production by murine macrophages.. J Exp Med 1 September 1993; 178 (3): 1017–1022. doi: https://doi.org/10.1084/jem.178.3.1017
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