Autophagy facilitates secretion and protects against degeneration of the Harderian gland

The epithelial derived Harderian gland consists of 2 types of secretory cells. The more numerous type A cells are responsible for the secretion of lipid droplets, while type B cells produce dark granules of multilamellar bodies. The process of autophagy is constitutively active in the Harderian glan...

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Autores principales: Koenig, Ulrich, Fobker, Manfred, Lengauer, Barbara, Brandstetter, Marlene, Resch, Guenter P, Gröger, Marion, Plenz, Gabriele, Pammer, Johannes, Barresi, Caterina, Hartmann, Christine, Rossiter, Heidemarie
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Taylor & Francis 2014
Materias:
Basic Science Research Papers
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4502725/
https://www.ncbi.nlm.nih.gov/pubmed/25484081
http://dx.doi.org/10.4161/15548627.2014.978221
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author Koenig, Ulrich
Fobker, Manfred
Lengauer, Barbara
Brandstetter, Marlene
Resch, Guenter P
Gröger, Marion
Plenz, Gabriele
Pammer, Johannes
Barresi, Caterina
Hartmann, Christine
Rossiter, Heidemarie
author_facet Koenig, Ulrich
Fobker, Manfred
Lengauer, Barbara
Brandstetter, Marlene
Resch, Guenter P
Gröger, Marion
Plenz, Gabriele
Pammer, Johannes
Barresi, Caterina
Hartmann, Christine
Rossiter, Heidemarie
author_sort Koenig, Ulrich
collection PubMed
description The epithelial derived Harderian gland consists of 2 types of secretory cells. The more numerous type A cells are responsible for the secretion of lipid droplets, while type B cells produce dark granules of multilamellar bodies. The process of autophagy is constitutively active in the Harderian gland, as confirmed by our analysis of LC3 processing in GFP-LC3 transgenic mice. This process is compromised by epithelial deletion of Atg7. Morphologically, the Atg7 mutant glands are hypotrophic and degenerated, with highly vacuolated cells and pyknotic nuclei. The mutant glands accumulate lipid droplets coated with PLIN2 (perilipin 2) and contain deposits of cholesterol, ubiquitinated proteins, SQSTM1/p62 (sequestosome 1) positive aggregates and other metabolic products such as porphyrin. Immunofluorescence stainings show that distinct cells strongly aggregate both proteins and lipids. Electron microscopy of the Harderian glands reveals that its organized structure is compromised, and the presence of large intracellular lipid droplets and heterologous aggregates. We attribute the occurrence of large vacuoles to a malfunction in the formation of multilamellar bodies found in the less abundant type B Harderian gland cells. This defect causes the formation of large tertiary lysosomes of heterologous content and is accompanied by the generation of tight lamellar stacks of endoplasmic reticulum in a pseudo-crystalline form. To test the hypothesis that lipid and protein accumulation is the cause for the degeneration in autophagy-deficient Harderian glands, epithelial cells were treated with a combination of the proteasome inhibitor and free fatty acids, to induce aggregation of misfolded proteins and lipid accumulation, respectively. The results show that lipid accumulation indeed enhanced the toxicity of misfolded proteins and that this was even more pronounced in autophagy-deficient cells. Thus, we conclude autophagy controls protein and lipid catabolism and anabolism to facilitate bulk production of secretory vesicles of the Harderian gland.
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spelling pubmed-45027252015-11-11 Autophagy facilitates secretion and protects against degeneration of the Harderian gland Koenig, Ulrich Fobker, Manfred Lengauer, Barbara Brandstetter, Marlene Resch, Guenter P Gröger, Marion Plenz, Gabriele Pammer, Johannes Barresi, Caterina Hartmann, Christine Rossiter, Heidemarie Autophagy Basic Science Research Papers The epithelial derived Harderian gland consists of 2 types of secretory cells. The more numerous type A cells are responsible for the secretion of lipid droplets, while type B cells produce dark granules of multilamellar bodies. The process of autophagy is constitutively active in the Harderian gland, as confirmed by our analysis of LC3 processing in GFP-LC3 transgenic mice. This process is compromised by epithelial deletion of Atg7. Morphologically, the Atg7 mutant glands are hypotrophic and degenerated, with highly vacuolated cells and pyknotic nuclei. The mutant glands accumulate lipid droplets coated with PLIN2 (perilipin 2) and contain deposits of cholesterol, ubiquitinated proteins, SQSTM1/p62 (sequestosome 1) positive aggregates and other metabolic products such as porphyrin. Immunofluorescence stainings show that distinct cells strongly aggregate both proteins and lipids. Electron microscopy of the Harderian glands reveals that its organized structure is compromised, and the presence of large intracellular lipid droplets and heterologous aggregates. We attribute the occurrence of large vacuoles to a malfunction in the formation of multilamellar bodies found in the less abundant type B Harderian gland cells. This defect causes the formation of large tertiary lysosomes of heterologous content and is accompanied by the generation of tight lamellar stacks of endoplasmic reticulum in a pseudo-crystalline form. To test the hypothesis that lipid and protein accumulation is the cause for the degeneration in autophagy-deficient Harderian glands, epithelial cells were treated with a combination of the proteasome inhibitor and free fatty acids, to induce aggregation of misfolded proteins and lipid accumulation, respectively. The results show that lipid accumulation indeed enhanced the toxicity of misfolded proteins and that this was even more pronounced in autophagy-deficient cells. Thus, we conclude autophagy controls protein and lipid catabolism and anabolism to facilitate bulk production of secretory vesicles of the Harderian gland. Taylor & Francis 2014-11-11 /pmc/articles/PMC4502725/ /pubmed/25484081 http://dx.doi.org/10.4161/15548627.2014.978221 Text en © 2015 The Author(s). Published with license by Taylor & Francis http://creativecommons.org/licenses/by-nc/3.0/ This is an Open Access article distributed under the terms of the Creative Commons Attribution-Non-Commercial License (http://creativecommons.org/licenses/by-nc/3.0/), which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited. The moral rights of the named author(s) have been asserted.
spellingShingle Basic Science Research Papers
Koenig, Ulrich
Fobker, Manfred
Lengauer, Barbara
Brandstetter, Marlene
Resch, Guenter P
Gröger, Marion
Plenz, Gabriele
Pammer, Johannes
Barresi, Caterina
Hartmann, Christine
Rossiter, Heidemarie
Autophagy facilitates secretion and protects against degeneration of the Harderian gland
title Autophagy facilitates secretion and protects against degeneration of the Harderian gland
title_full Autophagy facilitates secretion and protects against degeneration of the Harderian gland
title_fullStr Autophagy facilitates secretion and protects against degeneration of the Harderian gland
title_full_unstemmed Autophagy facilitates secretion and protects against degeneration of the Harderian gland
title_short Autophagy facilitates secretion and protects against degeneration of the Harderian gland
title_sort autophagy facilitates secretion and protects against degeneration of the harderian gland
topic Basic Science Research Papers
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4502725/
https://www.ncbi.nlm.nih.gov/pubmed/25484081
http://dx.doi.org/10.4161/15548627.2014.978221
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