Stall in Canonical Autophagy-Lysosome Pathways Prompts Nucleophagy-Based Nuclear Breakdown in Neurodegeneration

Olga Baron; Adel Boudi; Catarina Dias; Michael Schilling; Anna Nölle; Gema Vizcay-Barrena; Ivan Rattray; Heinz Jungbluth; Wiep Scheper; Roland A. Fleck; Gillian P. Bates; Manolis Fanto

doi:10.1016/j.cub.2017.10.054

Stall in Canonical Autophagy-Lysosome Pathways Prompts Nucleophagy-Based Nuclear Breakdown in Neurodegeneration

Olga Baron
, Adel Boudi
, Catarina Dias
, Michael Schilling
, Anna Nölle
, Gema Vizcay-Barrena
, Ivan Rattray
, Heinz Jungbluth
, Wiep Scheper
, Roland A. Fleck
, Gillian P. Bates
, Manolis Fanto^*

^*Corresponding author for this work

King's College London
Guy's and St Thomas' NHS Foundation Trust
VU University
University College London

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

The terminal stages of neuronal degeneration and death in neurodegenerative diseases remain elusive. Autophagy is an essential catabolic process frequently failing in neurodegeneration. Selective autophagy routes have recently emerged, including nucleophagy, defined as degradation of nuclear components by autophagy. Here, we show that, in a mouse model for the polyglutamine disease dentatorubral-pallidoluysian atrophy (DRPLA), progressive acquirement of an ataxic phenotype is linked to severe cerebellar cellular pathology, characterized by nuclear degeneration through nucleophagy-based LaminB1 degradation and excretion. We find that canonical autophagy is stalled in DRPLA mice and in human fibroblasts from patients of DRPLA. This is evidenced by accumulation of p62 and downregulation of LC3-I/II conversion as well as reduced Tfeb expression. Chronic autophagy blockage in several conditions, including DRPLA and Vici syndrome, an early-onset autolysosomal pathology, leads to the activation of alternative clearance pathways including Golgi membrane-associated and nucleophagy-based LaminB1 degradation and excretion. The combination of these alternative pathways and canonical autophagy blockade, results in dramatic nuclear pathology with disruption of the nuclear organization, bringing about terminal cell atrophy and degeneration. Thus, our findings identify a novel progressive mechanism for the terminal phases of neuronal cell degeneration and death in human neurodegenerative diseases and provide a link between autophagy block, activation of alternative pathways for degradation, and excretion of cellular components. Golgi-mediated degradation and excretion of LaminB1 promote cell atrophy and death. Baron et al. demonstrate that a block in canonical autophagy signaling leads to activation of alternative clearance routes. Golgi-mediated degradation and excretion of nuclear LaminB1 finally result in terminal nuclear breakdown, cell atrophy, and death.

Original language	English
Pages (from-to)	3626-3642.e6
Journal	Current biology
Volume	27
Issue number	23
DOIs	https://doi.org/10.1016/j.cub.2017.10.054
Publication status	Published - 4 Dec 2017

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Keywords

Atrophin-1
autophagy
EPG5
neurodegeneration
nucleophagy
polyglutamine

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10.1016/j.cub.2017.10.054

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@article{bb22f191361e4215bb5e5c171dbd76ed,

title = "Stall in Canonical Autophagy-Lysosome Pathways Prompts Nucleophagy-Based Nuclear Breakdown in Neurodegeneration",

abstract = "The terminal stages of neuronal degeneration and death in neurodegenerative diseases remain elusive. Autophagy is an essential catabolic process frequently failing in neurodegeneration. Selective autophagy routes have recently emerged, including nucleophagy, defined as degradation of nuclear components by autophagy. Here, we show that, in a mouse model for the polyglutamine disease dentatorubral-pallidoluysian atrophy (DRPLA), progressive acquirement of an ataxic phenotype is linked to severe cerebellar cellular pathology, characterized by nuclear degeneration through nucleophagy-based LaminB1 degradation and excretion. We find that canonical autophagy is stalled in DRPLA mice and in human fibroblasts from patients of DRPLA. This is evidenced by accumulation of p62 and downregulation of LC3-I/II conversion as well as reduced Tfeb expression. Chronic autophagy blockage in several conditions, including DRPLA and Vici syndrome, an early-onset autolysosomal pathology, leads to the activation of alternative clearance pathways including Golgi membrane-associated and nucleophagy-based LaminB1 degradation and excretion. The combination of these alternative pathways and canonical autophagy blockade, results in dramatic nuclear pathology with disruption of the nuclear organization, bringing about terminal cell atrophy and degeneration. Thus, our findings identify a novel progressive mechanism for the terminal phases of neuronal cell degeneration and death in human neurodegenerative diseases and provide a link between autophagy block, activation of alternative pathways for degradation, and excretion of cellular components. Golgi-mediated degradation and excretion of LaminB1 promote cell atrophy and death. Baron et al. demonstrate that a block in canonical autophagy signaling leads to activation of alternative clearance routes. Golgi-mediated degradation and excretion of nuclear LaminB1 finally result in terminal nuclear breakdown, cell atrophy, and death.",

keywords = "Atrophin-1, autophagy, EPG5, neurodegeneration, nucleophagy, polyglutamine",

author = "Olga Baron and Adel Boudi and Catarina Dias and Michael Schilling and Anna N{\"o}lle and Gema Vizcay-Barrena and Ivan Rattray and Heinz Jungbluth and Wiep Scheper and Fleck, \{Roland A.\} and Bates, \{Gillian P.\} and Manolis Fanto",

year = "2017",

month = dec,

day = "4",

doi = "10.1016/j.cub.2017.10.054",

language = "English",

volume = "27",

pages = "3626--3642.e6",

journal = "Current biology",

issn = "0960-9822",

publisher = "Cell Press",

number = "23",

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TY - JOUR

T1 - Stall in Canonical Autophagy-Lysosome Pathways Prompts Nucleophagy-Based Nuclear Breakdown in Neurodegeneration

AU - Baron, Olga

AU - Boudi, Adel

AU - Dias, Catarina

AU - Schilling, Michael

AU - Nölle, Anna

AU - Vizcay-Barrena, Gema

AU - Rattray, Ivan

AU - Jungbluth, Heinz

AU - Scheper, Wiep

AU - Fleck, Roland A.

AU - Bates, Gillian P.

AU - Fanto, Manolis

PY - 2017/12/4

Y1 - 2017/12/4

N2 - The terminal stages of neuronal degeneration and death in neurodegenerative diseases remain elusive. Autophagy is an essential catabolic process frequently failing in neurodegeneration. Selective autophagy routes have recently emerged, including nucleophagy, defined as degradation of nuclear components by autophagy. Here, we show that, in a mouse model for the polyglutamine disease dentatorubral-pallidoluysian atrophy (DRPLA), progressive acquirement of an ataxic phenotype is linked to severe cerebellar cellular pathology, characterized by nuclear degeneration through nucleophagy-based LaminB1 degradation and excretion. We find that canonical autophagy is stalled in DRPLA mice and in human fibroblasts from patients of DRPLA. This is evidenced by accumulation of p62 and downregulation of LC3-I/II conversion as well as reduced Tfeb expression. Chronic autophagy blockage in several conditions, including DRPLA and Vici syndrome, an early-onset autolysosomal pathology, leads to the activation of alternative clearance pathways including Golgi membrane-associated and nucleophagy-based LaminB1 degradation and excretion. The combination of these alternative pathways and canonical autophagy blockade, results in dramatic nuclear pathology with disruption of the nuclear organization, bringing about terminal cell atrophy and degeneration. Thus, our findings identify a novel progressive mechanism for the terminal phases of neuronal cell degeneration and death in human neurodegenerative diseases and provide a link between autophagy block, activation of alternative pathways for degradation, and excretion of cellular components. Golgi-mediated degradation and excretion of LaminB1 promote cell atrophy and death. Baron et al. demonstrate that a block in canonical autophagy signaling leads to activation of alternative clearance routes. Golgi-mediated degradation and excretion of nuclear LaminB1 finally result in terminal nuclear breakdown, cell atrophy, and death.

AB - The terminal stages of neuronal degeneration and death in neurodegenerative diseases remain elusive. Autophagy is an essential catabolic process frequently failing in neurodegeneration. Selective autophagy routes have recently emerged, including nucleophagy, defined as degradation of nuclear components by autophagy. Here, we show that, in a mouse model for the polyglutamine disease dentatorubral-pallidoluysian atrophy (DRPLA), progressive acquirement of an ataxic phenotype is linked to severe cerebellar cellular pathology, characterized by nuclear degeneration through nucleophagy-based LaminB1 degradation and excretion. We find that canonical autophagy is stalled in DRPLA mice and in human fibroblasts from patients of DRPLA. This is evidenced by accumulation of p62 and downregulation of LC3-I/II conversion as well as reduced Tfeb expression. Chronic autophagy blockage in several conditions, including DRPLA and Vici syndrome, an early-onset autolysosomal pathology, leads to the activation of alternative clearance pathways including Golgi membrane-associated and nucleophagy-based LaminB1 degradation and excretion. The combination of these alternative pathways and canonical autophagy blockade, results in dramatic nuclear pathology with disruption of the nuclear organization, bringing about terminal cell atrophy and degeneration. Thus, our findings identify a novel progressive mechanism for the terminal phases of neuronal cell degeneration and death in human neurodegenerative diseases and provide a link between autophagy block, activation of alternative pathways for degradation, and excretion of cellular components. Golgi-mediated degradation and excretion of LaminB1 promote cell atrophy and death. Baron et al. demonstrate that a block in canonical autophagy signaling leads to activation of alternative clearance routes. Golgi-mediated degradation and excretion of nuclear LaminB1 finally result in terminal nuclear breakdown, cell atrophy, and death.

KW - Atrophin-1

KW - autophagy

KW - EPG5

KW - neurodegeneration

KW - nucleophagy

KW - polyglutamine

UR - https://www.scopus.com/pages/publications/85034652860

U2 - 10.1016/j.cub.2017.10.054

DO - 10.1016/j.cub.2017.10.054

M3 - Article

SN - 0960-9822

VL - 27

SP - 3626-3642.e6

JO - Current biology

JF - Current biology

IS - 23

ER -

Stall in Canonical Autophagy-Lysosome Pathways Prompts Nucleophagy-Based Nuclear Breakdown in Neurodegeneration

Abstract

UN SDGs

Keywords

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