AI Article Synopsis
- Elevated levels of acute phase proteins (APR) in rats suppress acute inflammatory responses and are linked to liver fibrosis development.
- APR were induced through repeated epinephrine injections, leading to increased alpha 2-macroglobulin levels, which showed protective effects against liver damage.
- Rats with high APR levels experienced more severe fibrosis and cirrhosis after CCl4 treatment, despite showing lower initial hepatocellular damage, suggesting a complex role of APR in liver disease progression.
Article Abstract
High levels of acute phase proteins (acute phase reactants, APR) suppress acute inflammatory reactions in the rat. As many APR have antiprotease properties, including an anticollagenase activity, the effect of APR on the development of CCl4-induced liver fibrosis was investigated in rats. APR were provoked by repeated injections of epinephrine, inducing a broad spectrum of APR. This reaction can be monitored measuring alpha 2-macroglobulin levels in the rat (alpha 2-macrofetoprotein, alpha M FP). This protein was found to inhibit both acute galactosamine hepatitis and acute CCl4-induced liver toxicity. The animals with high levels of APR at the start of CCl4 treatment developed a more severe degree of fibrosis and cirrhosis than the control group in which no acute phase reaction was induced. Epinephrine alone had no such effects. Additionally, the APR positive group showed an initially lower degree of hepatocellular damage when compared to control animals. This uncoupling of liver cell damage and subsequent fibrosis may demonstrate that higher levels of APR might be important as to the development of cirrhosis, possibly based on the anticollagenase activity of these proteins.
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| http://dx.doi.org/10.1016/0014-4800(86)90066-3 | DOI Listing |
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