Abstract

Homozygous PiZZ alpha1-antitrypsin deficiency is the most common genetic liver disease in children and is associated with chronic liver injury and hepatocellular carcinoma in adults. Liver injury results from the hepatotoxic effect of abnormally folded alpha1-AT Z which is unable to traverse the secretory pathway and accumulates in the ER of liver cells. It is unknown, however, why only 15% of the deficient population develop liver injury. In this project we have examined the hypothesis that this subset of the deficient population is more susceptible to liver injury by virtue of inherited traits or environmental factors which exaggerate the intracellular accumulation of alpha1-AT Z, or exaggerate the cellular pathologic sequelae of alpha1-AT Z accumulation. Two potential mechanisms have been identified and characterized. In the first, elastase-alpha1-AT complexes have been shown to mediate increases in synthesis of alpha1-AT and greater net accumulation of alpha1-AT Z in cells from PiZZ individuals. A specific pentapeptide neo-domain of alpha1-AT and a specific 8OkD cell surface polypeptide called the SEC receptor have been identified as the ligand and receptor responsible for this effect. Further detailed molecular/biochemical characterization of ligand and receptor as outlined in the current proposal will enhance the likelihood of pharmacologically blocking this receptor in PiZZ individuals, especially during alpha1-AT replacement therapy (protein or gene) for emphysema. Further characterization of this ligand-receptor interaction will also enhance our understanding of the local tissue response to inflammation for several reasons; 1) its regulatory effect allows for highly focussed and tightly controlled activity of limited proteolytic cascade pathways at sites of injury, for orderly initiation of tissue repair and for prevention of excessive connective tissue destruction around migrating cells and sprouting cell processes; 2) it mediates chemotaxis of neutrophils; 3) it may be involved in clearance/catabolism of serpin- enzyme complexes in vivo; 4) it may mediate some of the biologic effects of tachykinins and pathobiologic effects of amyloid-beta peptide. The second potential mechanism for susceptibility to liver injury in alpha1-AT deficiency was identified by examining the fate of the alpha1-AT Z in transfected skin fibroblast cell lines from PiZZ individuals with liver disease, lung disease or no apparent disease. The results indicate that there is a decrease in the rate of degradation of alpha1-AT Z in cells of PiZZ individuals with liver disease. Moreover, there is a decrease in interaction of this mutant alpha1-AT protein with a resident ER molecular chaperone, calnexin, In cells from PiZZ individuals with liver disease. More detailed molecular/biochemical studies of this defect in degradation as outlined in the current proposal will enhance the likelihood of predicting susceptibility to liver disease and developing specific pharmacological strategies for prevention of liver injury.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL037784-11
Application #
2378730
Study Section
Pathobiochemistry Study Section (PBC)
Project Start
1986-09-01
Project End
2000-02-29
Budget Start
1997-03-01
Budget End
1998-02-28
Support Year
11
Fiscal Year
1997
Total Cost
Indirect Cost

  Institution

Name
Washington University
Department
Pediatrics
Type
Schools of Medicine
DUNS #
062761671
City
Saint Louis
State
MO
Country
United States
Zip Code
63130

  Publications

Maurice, Nicholas; Perlmutter, David H (2012) Novel treatment strategies for liver disease due to ?1-antitrypsin deficiency. Clin Transl Sci 5:289-94
Hidvegi, Tunda; Ewing, Michael; Hale, Pamela et al. (2010) An autophagy-enhancing drug promotes degradation of mutant alpha1-antitrypsin Z and reduces hepatic fibrosis. Science 329:229-32
Perlmutter, D H (2009) Autophagic disposal of the aggregation-prone protein that causes liver inflammation and carcinogenesis in alpha-1-antitrypsin deficiency. Cell Death Differ 16:39-45
Scott, Craig M; Kruse, Kristina B; Schmidt, Bela Z et al. (2007) ADD66, a gene involved in the endoplasmic reticulum-associated degradation of alpha-1-antitrypsin-Z in yeast, facilitates proteasome activity and assembly. Mol Biol Cell 18:3776-87
Hidvegi, Tunda; Mirnics, Karoly; Hale, Pamela et al. (2007) Regulator of G Signaling 16 is a marker for the distinct endoplasmic reticulum stress state associated with aggregated mutant alpha1-antitrypsin Z in the classical form of alpha1-antitrypsin deficiency. J Biol Chem 282:27769-80
Perlmutter, David H (2006) The role of autophagy in alpha-1-antitrypsin deficiency: a specific cellular response in genetic diseases associated with aggregation-prone proteins. Autophagy 2:258-63
Perlmutter, David H (2006) Pathogenesis of chronic liver injury and hepatocellular carcinoma in alpha-1-antitrypsin deficiency. Pediatr Res 60:233-8
Kamimoto, Takahiro; Shoji, Shisako; Hidvegi, Tunda et al. (2006) Intracellular inclusions containing mutant alpha1-antitrypsin Z are propagated in the absence of autophagic activity. J Biol Chem 281:4467-76
Rudnick, David A; Perlmutter, David H (2005) Alpha-1-antitrypsin deficiency: a new paradigm for hepatocellular carcinoma in genetic liver disease. Hepatology 42:514-21
Hidvegi, Tunda; Schmidt, Bela Z; Hale, Pamela et al. (2005) Accumulation of mutant alpha1-antitrypsin Z in the endoplasmic reticulum activates caspases-4 and -12, NFkappaB, and BAP31 but not the unfolded protein response. J Biol Chem 280:39002-15

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