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Interferon-gamma is a major regulator of C1-inhibitor synthesis by human blood monocytes.

M Lotz and B L Zuraw
J Immunol November 15, 1987, 139 (10) 3382-3387;
M Lotz
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B L Zuraw
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Abstract

C1 inhibitor (C1INH) is the major control factor for the activation of the classical pathway of complement and for contact system activation. Hepatocytes and blood monocytes are known to synthesize this protease inhibitor. We studied the regulation of monocyte C1INH production by mediators that are generated during inflammatory responses. Purified blood monocytes spontaneously synthesized and secreted C1INH only after prolonged culture. In the presence of interferon (IFN)-gamma, C1INH was detectable within 24 hr and continued to be released at high levels throughout an 8-day culture period. Monocyte C1INH was newly synthesized and was functionally active as determined by forming stable complex with C1s. Other monocyte stimuli were either less potent (IFN-alpha, IFN-beta) or not capable of increasing C1INH release (lipopolysaccharide, interleukin 1, and tumor necrosis factor). The second component of complement, C2, was induced by IFN-gamma to a similar extent as C1INH. These findings demonstrate that IFN-gamma is a major regulator of monocyte C1INH production and may warrant consideration of IFN-gamma in the treatment of C1INH deficiency states.

  • Copyright © 1987 by American Association of Immunologists

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The Journal of Immunology
Vol. 139, Issue 10
15 Nov 1987
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Interferon-gamma is a major regulator of C1-inhibitor synthesis by human blood monocytes.
M Lotz, B L Zuraw
The Journal of Immunology November 15, 1987, 139 (10) 3382-3387;

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Interferon-gamma is a major regulator of C1-inhibitor synthesis by human blood monocytes.
M Lotz, B L Zuraw
The Journal of Immunology November 15, 1987, 139 (10) 3382-3387;
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Print ISSN 0022-1767        Online ISSN 1550-6606