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Dissection of Autophagosome Formation Using Apg5-Deficient Mouse Embryonic Stem Cells

In macroautophagy, cytoplasmic components are delivered to lysosomes for degradation via autophagosomes that are formed by closure of cup-shaped isolation membranes. However, how the isolation membranes are formed is poorly understood. We recently found in yeast that a novel ubiquitin-like system, t...

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Autores principales: Mizushima, Noboru, Yamamoto, Akitsugu, Hatano, Masahiko, Kobayashi, Yoshinori, Kabeya, Yukiko, Suzuki, Kuninori, Tokuhisa, Takeshi, Ohsumi, Yoshinori, Yoshimori, Tamotsu
Formato: Texto
Lenguaje:English
Publicado: The Rockefeller University Press 2001
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2195787/
https://www.ncbi.nlm.nih.gov/pubmed/11266458
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author Mizushima, Noboru
Yamamoto, Akitsugu
Hatano, Masahiko
Kobayashi, Yoshinori
Kabeya, Yukiko
Suzuki, Kuninori
Tokuhisa, Takeshi
Ohsumi, Yoshinori
Yoshimori, Tamotsu
author_facet Mizushima, Noboru
Yamamoto, Akitsugu
Hatano, Masahiko
Kobayashi, Yoshinori
Kabeya, Yukiko
Suzuki, Kuninori
Tokuhisa, Takeshi
Ohsumi, Yoshinori
Yoshimori, Tamotsu
author_sort Mizushima, Noboru
collection PubMed
description In macroautophagy, cytoplasmic components are delivered to lysosomes for degradation via autophagosomes that are formed by closure of cup-shaped isolation membranes. However, how the isolation membranes are formed is poorly understood. We recently found in yeast that a novel ubiquitin-like system, the Apg12-Apg5 conjugation system, is essential for autophagy. Here we show that mouse Apg12-Apg5 conjugate localizes to the isolation membranes in mouse embryonic stem cells. Using green fluorescent protein–tagged Apg5, we revealed that the cup-shaped isolation membrane is developed from a small crescent-shaped compartment. Apg5 localizes on the isolation membrane throughout its elongation process. To examine the role of Apg5, we generated Apg5-deficient embryonic stem cells, which showed defects in autophagosome formation. The covalent modification of Apg5 with Apg12 is not required for its membrane targeting, but is essential for involvement of Apg5 in elongation of the isolation membranes. We also show that Apg12-Apg5 is required for targeting of a mammalian Aut7/Apg8 homologue, LC3, to the isolation membranes. These results suggest that the Apg12-Apg5 conjugate plays essential roles in isolation membrane development.
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spelling pubmed-21957872008-05-01 Dissection of Autophagosome Formation Using Apg5-Deficient Mouse Embryonic Stem Cells Mizushima, Noboru Yamamoto, Akitsugu Hatano, Masahiko Kobayashi, Yoshinori Kabeya, Yukiko Suzuki, Kuninori Tokuhisa, Takeshi Ohsumi, Yoshinori Yoshimori, Tamotsu J Cell Biol Original Article In macroautophagy, cytoplasmic components are delivered to lysosomes for degradation via autophagosomes that are formed by closure of cup-shaped isolation membranes. However, how the isolation membranes are formed is poorly understood. We recently found in yeast that a novel ubiquitin-like system, the Apg12-Apg5 conjugation system, is essential for autophagy. Here we show that mouse Apg12-Apg5 conjugate localizes to the isolation membranes in mouse embryonic stem cells. Using green fluorescent protein–tagged Apg5, we revealed that the cup-shaped isolation membrane is developed from a small crescent-shaped compartment. Apg5 localizes on the isolation membrane throughout its elongation process. To examine the role of Apg5, we generated Apg5-deficient embryonic stem cells, which showed defects in autophagosome formation. The covalent modification of Apg5 with Apg12 is not required for its membrane targeting, but is essential for involvement of Apg5 in elongation of the isolation membranes. We also show that Apg12-Apg5 is required for targeting of a mammalian Aut7/Apg8 homologue, LC3, to the isolation membranes. These results suggest that the Apg12-Apg5 conjugate plays essential roles in isolation membrane development. The Rockefeller University Press 2001-02-19 /pmc/articles/PMC2195787/ /pubmed/11266458 Text en © 2001 The Rockefeller University Press This article is distributed under the terms of an Attribution–Noncommercial–Share Alike–No Mirror Sites license for the first six months after the publication date (see http://www.rupress.org/terms). After six months it is available under a Creative Commons License (Attribution–Noncommercial–Share Alike 4.0 Unported license, as described at http://creativecommons.org/licenses/by-nc-sa/4.0/).
spellingShingle Original Article
Mizushima, Noboru
Yamamoto, Akitsugu
Hatano, Masahiko
Kobayashi, Yoshinori
Kabeya, Yukiko
Suzuki, Kuninori
Tokuhisa, Takeshi
Ohsumi, Yoshinori
Yoshimori, Tamotsu
Dissection of Autophagosome Formation Using Apg5-Deficient Mouse Embryonic Stem Cells
title Dissection of Autophagosome Formation Using Apg5-Deficient Mouse Embryonic Stem Cells
title_full Dissection of Autophagosome Formation Using Apg5-Deficient Mouse Embryonic Stem Cells
title_fullStr Dissection of Autophagosome Formation Using Apg5-Deficient Mouse Embryonic Stem Cells
title_full_unstemmed Dissection of Autophagosome Formation Using Apg5-Deficient Mouse Embryonic Stem Cells
title_short Dissection of Autophagosome Formation Using Apg5-Deficient Mouse Embryonic Stem Cells
title_sort dissection of autophagosome formation using apg5-deficient mouse embryonic stem cells
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2195787/
https://www.ncbi.nlm.nih.gov/pubmed/11266458
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