Sequestration of Mutated {alpha}1-Antitrypsin Into Inclusion Bodies Is a Cell Protective Mechanism to Maintain Endoplasmic Reticulum Function

doi:10.1091/mbc.E07-06-0587

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MBC in Press, published online ahead of print November 28, 2007
Mol. Biol. Cell 10.1091/mbc.E07-06-0587

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Articles by Granell, S.

Articles by Baldini, G.

Submitted on June 21, 2007
Revised on October 18, 2007
Accepted on November 16, 2007

Sequestration of Mutated ${alpha}$ 1-Antitrypsin Into Inclusion Bodies Is a Cell Protective Mechanism to Maintain Endoplasmic Reticulum Function

Susana Granell,* Giovanna Baldini, ${dagger}$ Sameer Mohammad,* Vanessa Nicolin, ${dagger}$ Paola Narducci, ${dagger}$ Brian Storrie, ${ddagger}$ and Giulia Baldini*

^*Department of Biochemistry and Molecular Biology and Department of Physiology and Biophysics, University of Arkansas for Medical Sciences, Little Rock, AR 72205; Dipartimento Universitario Clinico di Biomedicina, Universita’ degli Studi di Trieste, Trieste I-34138, Italy

Monitoring Editor: Thomas Sommer

A variant ${alpha}$ 1-antitrypsin withE342K mutation has a high tendency to form intracellular polymersand is associated with liver disease. In the hepatocyte of individualscarrying the mutation, ${alpha}$ 1-antitrypsin localizes both to the endoplasmicreticulum (ER) and to membrane-surrounded inclusion bodies (IBs).It is unclear whether the IBs contribute to cell toxicity orare protective to the cell. We found that in hepatoma cells,mutated ${alpha}$ 1-antitrypsin exited the ER and accumulated in IBs thatwere negative for autophagosomal and lysosomal markers, containedseveral ER components, but not calnexin. Mutated ${alpha}$ 1-antitrypsininduced IBs also in neuroendocrine cells, showing that formationof these organelles is not cell-type specific. In the presenceof IBs, ER function was largely maintained. Increased levelsof calnexin, but not of protein disulphide isomerase, inhibitedformation of IBs and lead to retention of mutated ${alpha}$ 1-antitrypsinin the ER. In hepatoma cells, shift of mutated ${alpha}$ 1-antitrypsinlocalization to the ER by calnexin overexpression lead to cellshrinkage, ER stress and impairment of the secretory pathwayat the ER level. We conclude that segregation of mutated ${alpha}$ 1-antitrypsinfrom the ER to the IBs is a protective cell response to maintaina functional secretory pathway.

Address correspondence to: Giulia Baldini (Gbaldini{at}uams.edu)

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Sequestration of Mutated 1-Antitrypsin Into Inclusion Bodies Is a Cell Protective Mechanism to Maintain Endoplasmic Reticulum Function

Sequestration of Mutated ${alpha}$ 1-Antitrypsin Into Inclusion Bodies Is a Cell Protective Mechanism to Maintain Endoplasmic Reticulum Function