Eukaryotic cells are equipped with an efficient quality control system to selectively eliminate misfolded and damaged proteins, and organelles. Abnormal polypeptides that escape from proteasome-dependent degradation and aggregate in the cytosol can be transported via microtubules to inclusion bodies called 'aggresomes', where misfolded proteins are confined and degraded by autophagy. Here, we show that Type 2 transglutaminase (TG2) knockout mice display impaired autophagy and accumulate ubiquitinated protein aggregates upon starvation. Furthermore, p62-dependent peroxisome degradation is also impaired in the absence of TG2. We also demonstrate that, under cellular stressful conditions, TG2 physically interacts with p62 and they are localized in cytosolic protein aggregates, which are then recruited into autophagosomes, where TG2 is degraded. Interestingly, the enzyme's crosslinking activity is activated during autophagy and its inhibition leads to the accumulation of ubiquitinated proteins. Taken together, these data indicate that the TG2 transamidating activity has an important role in the assembly of protein aggregates, as well as in the clearance of damaged organelles by macroautophagy.

D'Eletto, M., Farrace, M.g., Rossin, F., Strappazzon, F., Giacomo, G., Cecconi, F., et al. (2012). Type 2 transglutaminase is involved in the autophagy-dependent clearance of ubiquitinated proteins. CELL DEATH AND DIFFERENTIATION, 19(7), 1228-1238 [10.1038/cdd.2012.2].

Type 2 transglutaminase is involved in the autophagy-dependent clearance of ubiquitinated proteins

FARRACE, MARIA GRAZIA;Rossin, F;CECCONI, FRANCESCO;MELINO, GENNARO;PIACENTINI, MAURO
2012-07-01

Abstract

Eukaryotic cells are equipped with an efficient quality control system to selectively eliminate misfolded and damaged proteins, and organelles. Abnormal polypeptides that escape from proteasome-dependent degradation and aggregate in the cytosol can be transported via microtubules to inclusion bodies called 'aggresomes', where misfolded proteins are confined and degraded by autophagy. Here, we show that Type 2 transglutaminase (TG2) knockout mice display impaired autophagy and accumulate ubiquitinated protein aggregates upon starvation. Furthermore, p62-dependent peroxisome degradation is also impaired in the absence of TG2. We also demonstrate that, under cellular stressful conditions, TG2 physically interacts with p62 and they are localized in cytosolic protein aggregates, which are then recruited into autophagosomes, where TG2 is degraded. Interestingly, the enzyme's crosslinking activity is activated during autophagy and its inhibition leads to the accumulation of ubiquitinated proteins. Taken together, these data indicate that the TG2 transamidating activity has an important role in the assembly of protein aggregates, as well as in the clearance of damaged organelles by macroautophagy.
lug-2012
Pubblicato
Rilevanza internazionale
Articolo
Esperti anonimi
Settore BIO/10 - BIOCHIMICA
English
Animals; Transcription Factors; Autophagy; Humans; HEK293 Cells; Proteasome Endopeptidase Complex; Transglutaminases; Ubiquitinated Proteins; Mice; GTP-Binding Proteins; Mice, Knockout
D'Eletto, M., Farrace, M.g., Rossin, F., Strappazzon, F., Giacomo, G., Cecconi, F., et al. (2012). Type 2 transglutaminase is involved in the autophagy-dependent clearance of ubiquitinated proteins. CELL DEATH AND DIFFERENTIATION, 19(7), 1228-1238 [10.1038/cdd.2012.2].
D'Eletto, M; Farrace, Mg; Rossin, F; Strappazzon, F; Giacomo, G; Cecconi, F; Melino, G; Sepe, S; Moreno, S; Fimia, G; Falasca, L; Nardacci, R; Piacent...espandi
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2108/78440
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