Cytokines and Fibrogenesis

Scott L. Friedman

doi:10.1055/s-2007-1007105

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Semin Liver Dis 1999; 19(2): 129-140
DOI: 10.1055/s-2007-1007105

ORIGINAL ARTICLE

Cytokines and Fibrogenesis

Scott L. Friedman

Division of Liver Diseases, Mount Sinai School of Medicine, New York, New York

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Publication History

Publication Date:
17 March 2008 (online)

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ABSTRACT

Cytokines play a major role in the development of hepatic fibrosis, the wound-healing response of the liver to chronic injury. Major concepts in defining the role of cytokines in fibrogenesis include (1) Cytokines may be pro- or antifibrogenie; (2) autocrine, paracrine, and matrix-bound sources of cytokines are the most important; and (3) multiple mechanisms of cytokine regulation are essential to fine-tune their effects. The hepatic stellate cell is the key effector of the fibrotic response and both a principal source and target of cytokines. Activation of stellate cells connotes the conversion of a resting vitamin A-rich cell to one which is proliferative, contractile, fibrogenic, and devoid of vitamin A. The features of stellate cell activation provide a framework in which to understand how cytokines drive fibrosis. These features include (1) proliferation; (2) contractility; (3) fibrogenesis; (4) extracellular matrix degradation; (5) chemotaxis; (6) cytokine release; and (7) retinoid loss. The insights gained from illuminating the role of stellate cells has engendered realistic hopes for treating hepatic fibrosis through modulation of cytokine actions.

KEY WORDS

stellate cells - fibrogenesis - receptors

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