Calpain released from dying hepatocytes mediates progression of acute liver injury induced by model hepatotoxicants

Liver injury is known to progress even after the hepatotoxicant is long gone and the mechanisms of progressive injury are not understood. We tested the hypothesis that hydrolytic enzymes such as calpain, released from dying hepatocytes, destroy the surrounding cells causing progression of injury. Ca...

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Bibliographic Details
Published in:Toxicology and applied pharmacology 2003-09, Vol.191 (3), p.211-226
Main Authors: Limaye, Pallavi B, Apte, Udayan M, Shankar, Kartik, Bucci, Thomas J, Warbritton, Alan, Mehendale, Harihara M
Format: Article
Language:English
Subjects:
Acetaminophen
Acetaminophen - metabolism
Acetaminophen - pharmacokinetics
Acetaminophen - toxicity
Animals
Biological and medical sciences
Blotting, Western
Ca 2
Calpain
Calpain - antagonists & inhibitors
Calpain - blood
Calpain - metabolism
Carbon Tetrachloride - metabolism
Carbon Tetrachloride - pharmacokinetics
Carbon Tetrachloride - toxicity
Carrier Proteins - metabolism
CCl 4
Chemical and Drug Induced Liver Injury
Cysteine Proteinase Inhibitors - pharmacology
Cytochrome P-450 CYP2E1 - metabolism
Cytochrome P-450 CYP2E1 Inhibitors
Death proteins
Dipeptides - pharmacology
Disease Progression
General aspects. Methods
Hepatocytes - enzymology
Immunohistochemistry
Inhibitor of calpain
Liver Diseases - blood
Liver Diseases - enzymology
Liver Diseases - pathology
Liver injury progression
Male
Medical sciences
Mice
Microfilament Proteins - metabolism
N-CBZ-Val-Phe-methyl ester
Necrosis
Random Allocation
Rats
Rats, Sprague-Dawley
Toxicology
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Summary:Liver injury is known to progress even after the hepatotoxicant is long gone and the mechanisms of progressive injury are not understood. We tested the hypothesis that hydrolytic enzymes such as calpain, released from dying hepatocytes, destroy the surrounding cells causing progression of injury. Calpain inhibitor, N-CBZ-VAL-PHE-methyl ester (CBZ), administered 1 h after a toxic but nonlethal dose of CCl 4 (2 ml/kg, ip) to male Sprague Dawley rats substantially mitigated the progression of liver injury (6 to 48 h) and also led to 75% protection against CCl 4-induced lethality following a lethal dose (LD75) of CCl 4 (3 ml/kg). Calpain leakage in plasma and in the perinecrotic areas increased until 48 h and decreased from 72 h onward paralleling progression and regression of liver injury, respectively, after CCl 4 treatment. Mitigation of progressive injury was accompanied by substantially low calpain in perinecrotic areas and in plasma after CBZ treatment. Normal hepatocytes incubated with the plasma collected from CCl 4-treated rats (collected at 12 h when most of the CCl 4 is eliminated) resulted in extensive cell death prevented by CBZ. Cell-impermeable calpain inhibitor E64 also protected against progression of CCl 4-induced liver injury, thereby confirming the role of released calpain in progression of liver injury. Following CCl 4 treatment, calpain-specific breakdown of α-fodrin increased, while it was negligible in rats receiving CBZ after CCl 4. Hepatocyte cell death in incubations containing calpain was completely prevented by CBZ. Eighty percent of Swiss Webster mice receiving a lethal dose (LD80) of acetaminophen (600 mg/kg, ip) survived if CBZ was administered 1 h after acetaminophen, suggesting that calpain-mediated progression of liver injury is neither species nor chemical specific. These findings suggest the role of calpain in progression of liver injury.
ISSN:0041-008X
1096-0333
DOI:10.1016/S0041-008X(03)00250-3