SORL1 deficiency in human excitatory neurons causes APP-dependent defects in the endolysosome-autophagy network

Christy Hung; Eleanor Tuck; Victoria Stubbs; Sven J. van der Lee; Cora Aalfs; Resie van Spaendonk; Philip Scheltens; John Hardy; Henne Holstege; Frederick J. Livesey

doi:10.1016/j.celrep.2021.109259

SORL1 deficiency in human excitatory neurons causes APP-dependent defects in the endolysosome-autophagy network

Christy Hung
, Eleanor Tuck
, Victoria Stubbs
, Sven J. van der Lee
, Cora Aalfs
, Resie van Spaendonk
, Philip Scheltens
, John Hardy
, Henne Holstege
, Frederick J. Livesey^*

^*Corresponding author for this work

University College London
University of Cambridge
Electron Microscopy Center Amsterdam
Delft University of Technology
Hong Kong University of Science and Technology

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

Abstract

Dysfunction of the endolysosomal-autophagy network is emerging as an important pathogenic process in Alzheimer's disease. Mutations in the sorting receptor-encoding gene SORL1 cause autosomal-dominant Alzheimer's disease, and SORL1 variants increase risk for late-onset AD. To understand the contribution of SORL1 mutations to AD pathogenesis, we analyze the effects of a SORL1 truncating mutation on SORL1 protein levels and endolysosome function in human neurons. We find that truncating mutation results in SORL1 haploinsufficiency and enlarged endosomes in human neurons. Analysis of isogenic SORL1 wild-type, heterozygous, and homozygous null neurons demonstrates that, whereas SORL1 haploinsufficiency results in endosome dysfunction, complete loss of SORL1 leads to additional defects in lysosome function and autophagy. Neuronal endolysosomal dysfunction caused by loss of SORL1 is relieved by extracellular antisense oligonucleotide-mediated reduction of APP protein, demonstrating that PSEN1, APP, and SORL1 act in a common pathway regulating the endolysosome system, which becomes dysfunctional in AD.

Original language	English
Article number	109259
Journal	Cell reports
Volume	35
Issue number	11
DOIs	https://doi.org/10.1016/j.celrep.2021.109259
Publication status	Published - 15 Jun 2021

UN SDGs

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

SDG 3 Good Health and Well-being

Keywords

Alzheimer's disease
SORL1
amyloid precursor protein
autophagy
endosome
iPSC
lysosome

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10.1016/j.celrep.2021.109259

Cite this

@article{0a863bb50566405b82d09250cdb96d03,

title = "SORL1 deficiency in human excitatory neurons causes APP-dependent defects in the endolysosome-autophagy network",

abstract = "Dysfunction of the endolysosomal-autophagy network is emerging as an important pathogenic process in Alzheimer's disease. Mutations in the sorting receptor-encoding gene SORL1 cause autosomal-dominant Alzheimer's disease, and SORL1 variants increase risk for late-onset AD. To understand the contribution of SORL1 mutations to AD pathogenesis, we analyze the effects of a SORL1 truncating mutation on SORL1 protein levels and endolysosome function in human neurons. We find that truncating mutation results in SORL1 haploinsufficiency and enlarged endosomes in human neurons. Analysis of isogenic SORL1 wild-type, heterozygous, and homozygous null neurons demonstrates that, whereas SORL1 haploinsufficiency results in endosome dysfunction, complete loss of SORL1 leads to additional defects in lysosome function and autophagy. Neuronal endolysosomal dysfunction caused by loss of SORL1 is relieved by extracellular antisense oligonucleotide-mediated reduction of APP protein, demonstrating that PSEN1, APP, and SORL1 act in a common pathway regulating the endolysosome system, which becomes dysfunctional in AD.",

keywords = "Alzheimer's disease, SORL1, amyloid precursor protein, autophagy, endosome, iPSC, lysosome",

author = "Christy Hung and Eleanor Tuck and Victoria Stubbs and \{van der Lee\}, \{Sven J.\} and Cora Aalfs and \{van Spaendonk\}, Resie and Philip Scheltens and John Hardy and Henne Holstege and Livesey, \{Frederick J.\}",

note = "Funding Information: We would like to thank members of the F.J.L. group for technical support, especially Dr. Moritz Haneklaus for confirming the APOE genotype for the KOLF2 cell line. We also thank Dr. Steven Moore and Dr. Ayiba Momoh for kindly providing the APP-YFP construct as a template for cloning the APP:VN construct. C.H. is supported by a Race Against Dementia Fellowship , Alzheimer{\textquoteright}s Research UK ( ARUK-RADF2019A-007 ), and the NIHR Great Ormond Street Biomedical Research Centre . F.J.L.{\textquoteright}s group is supported by a Wellcome Trust Senior Investigator Award ( WT101052MA ), Great Ormond Street Children{\textquoteright}s Charity (Stem Cell Professorship), and Alzheimer{\textquoteright}s Research UK (Stem Cell Research Centre). J.H. is supported by the UK Dementia Research Institute , which receives its funding from DRI Ltd, funded by the UK Medical Research Council , Alzheimer's Society , and Alzheimer{\textquoteright}s Research UK ; Medical Research Council (award number MR/N026004/1 ); Wellcome Trust (award number 202903/Z/16/Z ); Dolby Family Fund ; and National Institute for Health Research University College London Hospitals Biomedical Research Centre . H.H. is a part of the EU Joint Programme-Neurodegenerative Disease Research (JPND) Working Group SORLA-FIX under the 2019 “Personalized Medicine” call (JPND2019-466-197, ZonMW 733051110). H.H. and S.L. are recipients of ABOARD, a public-private partnership receiving funding from ZonMW (\#73305095007) and Health\textasciitilde{}Holland, Topsector Life Sciences \& Health (PPP-allowance; \#LSHM20106). S.L. is recipient of ZonMW funding (\#733050512). Schematic illustrations were created with BioRender ( https://BioRender.com ). Funding Information: We would like to thank members of the F.J.L. group for technical support, especially Dr. Moritz Haneklaus for confirming the APOE genotype for the KOLF2 cell line. We also thank Dr. Steven Moore and Dr. Ayiba Momoh for kindly providing the APP-YFP construct as a template for cloning the APP:VN construct. C.H. is supported by a Race Against Dementia Fellowship, Alzheimer's Research UK (ARUK-RADF2019A-007), and the NIHR Great Ormond Street Biomedical Research Centre. F.J.L.?s group is supported by a Wellcome Trust Senior Investigator Award (WT101052MA), Great Ormond Street Children's Charity (Stem Cell Professorship), and Alzheimer's Research UK (Stem Cell Research Centre). J.H. is supported by the UK Dementia Research Institute, which receives its funding from DRI Ltd, funded by the UK Medical Research Council, Alzheimer's Society, and Alzheimer's Research UK; Medical Research Council (award number MR/N026004/1); Wellcome Trust (award number 202903/Z/16/Z); Dolby Family Fund; and National Institute for Health Research University College London Hospitals Biomedical Research Centre. H.H. is a part of the EU Joint Programme-Neurodegenerative Disease Research (JPND) Working Group SORLA-FIX under the 2019 ?Personalized Medicine? call (JPND2019-466-197, ZonMW 733051110). H.H. and S.L. are recipients of ABOARD, a public-private partnership receiving funding from ZonMW (\#73305095007) and Health\textasciitilde{}Holland, Topsector Life Sciences \& Health (PPP-allowance; \#LSHM20106). S.L. is recipient of ZonMW funding (\#733050512). Schematic illustrations were created with BioRender (https://BioRender.com). C.H. E.T. V.S. and F.J.L. conceived and designed the experiments. C.H. E.T. and V.S. performed the experiments. C.H. E.T. and V.S. analyzed the experiments. S.J.v.d.L. C.A. R.v.S. P.S. H.H. and J.H. provided genetic data and collected and provided donor fibroblasts. C.H. and F.J.L. wrote the manuscript with input from H.H. and J.H. The authors declare no competing interests. Publisher Copyright: {\textcopyright} 2021 The Authors Copyright: Copyright 2021 Elsevier B.V., All rights reserved.",

year = "2021",

month = jun,

day = "15",

doi = "10.1016/j.celrep.2021.109259",

language = "English",

volume = "35",

journal = "Cell reports",

issn = "2211-1247",

publisher = "Cell Press",

number = "11",

}

TY - JOUR

T1 - SORL1 deficiency in human excitatory neurons causes APP-dependent defects in the endolysosome-autophagy network

AU - Hung, Christy

AU - Tuck, Eleanor

AU - Stubbs, Victoria

AU - van der Lee, Sven J.

AU - Aalfs, Cora

AU - van Spaendonk, Resie

AU - Scheltens, Philip

AU - Hardy, John

AU - Holstege, Henne

AU - Livesey, Frederick J.

N1 - Funding Information: We would like to thank members of the F.J.L. group for technical support, especially Dr. Moritz Haneklaus for confirming the APOE genotype for the KOLF2 cell line. We also thank Dr. Steven Moore and Dr. Ayiba Momoh for kindly providing the APP-YFP construct as a template for cloning the APP:VN construct. C.H. is supported by a Race Against Dementia Fellowship , Alzheimer’s Research UK ( ARUK-RADF2019A-007 ), and the NIHR Great Ormond Street Biomedical Research Centre . F.J.L.’s group is supported by a Wellcome Trust Senior Investigator Award ( WT101052MA ), Great Ormond Street Children’s Charity (Stem Cell Professorship), and Alzheimer’s Research UK (Stem Cell Research Centre). J.H. is supported by the UK Dementia Research Institute , which receives its funding from DRI Ltd, funded by the UK Medical Research Council , Alzheimer's Society , and Alzheimer’s Research UK ; Medical Research Council (award number MR/N026004/1 ); Wellcome Trust (award number 202903/Z/16/Z ); Dolby Family Fund ; and National Institute for Health Research University College London Hospitals Biomedical Research Centre . H.H. is a part of the EU Joint Programme-Neurodegenerative Disease Research (JPND) Working Group SORLA-FIX under the 2019 “Personalized Medicine” call (JPND2019-466-197, ZonMW 733051110). H.H. and S.L. are recipients of ABOARD, a public-private partnership receiving funding from ZonMW (#73305095007) and Health~Holland, Topsector Life Sciences & Health (PPP-allowance; #LSHM20106). S.L. is recipient of ZonMW funding (#733050512). Schematic illustrations were created with BioRender ( https://BioRender.com ). Funding Information: We would like to thank members of the F.J.L. group for technical support, especially Dr. Moritz Haneklaus for confirming the APOE genotype for the KOLF2 cell line. We also thank Dr. Steven Moore and Dr. Ayiba Momoh for kindly providing the APP-YFP construct as a template for cloning the APP:VN construct. C.H. is supported by a Race Against Dementia Fellowship, Alzheimer's Research UK (ARUK-RADF2019A-007), and the NIHR Great Ormond Street Biomedical Research Centre. F.J.L.?s group is supported by a Wellcome Trust Senior Investigator Award (WT101052MA), Great Ormond Street Children's Charity (Stem Cell Professorship), and Alzheimer's Research UK (Stem Cell Research Centre). J.H. is supported by the UK Dementia Research Institute, which receives its funding from DRI Ltd, funded by the UK Medical Research Council, Alzheimer's Society, and Alzheimer's Research UK; Medical Research Council (award number MR/N026004/1); Wellcome Trust (award number 202903/Z/16/Z); Dolby Family Fund; and National Institute for Health Research University College London Hospitals Biomedical Research Centre. H.H. is a part of the EU Joint Programme-Neurodegenerative Disease Research (JPND) Working Group SORLA-FIX under the 2019 ?Personalized Medicine? call (JPND2019-466-197, ZonMW 733051110). H.H. and S.L. are recipients of ABOARD, a public-private partnership receiving funding from ZonMW (#73305095007) and Health~Holland, Topsector Life Sciences & Health (PPP-allowance; #LSHM20106). S.L. is recipient of ZonMW funding (#733050512). Schematic illustrations were created with BioRender (https://BioRender.com). C.H. E.T. V.S. and F.J.L. conceived and designed the experiments. C.H. E.T. and V.S. performed the experiments. C.H. E.T. and V.S. analyzed the experiments. S.J.v.d.L. C.A. R.v.S. P.S. H.H. and J.H. provided genetic data and collected and provided donor fibroblasts. C.H. and F.J.L. wrote the manuscript with input from H.H. and J.H. The authors declare no competing interests. Publisher Copyright: © 2021 The Authors Copyright: Copyright 2021 Elsevier B.V., All rights reserved.

PY - 2021/6/15

Y1 - 2021/6/15

N2 - Dysfunction of the endolysosomal-autophagy network is emerging as an important pathogenic process in Alzheimer's disease. Mutations in the sorting receptor-encoding gene SORL1 cause autosomal-dominant Alzheimer's disease, and SORL1 variants increase risk for late-onset AD. To understand the contribution of SORL1 mutations to AD pathogenesis, we analyze the effects of a SORL1 truncating mutation on SORL1 protein levels and endolysosome function in human neurons. We find that truncating mutation results in SORL1 haploinsufficiency and enlarged endosomes in human neurons. Analysis of isogenic SORL1 wild-type, heterozygous, and homozygous null neurons demonstrates that, whereas SORL1 haploinsufficiency results in endosome dysfunction, complete loss of SORL1 leads to additional defects in lysosome function and autophagy. Neuronal endolysosomal dysfunction caused by loss of SORL1 is relieved by extracellular antisense oligonucleotide-mediated reduction of APP protein, demonstrating that PSEN1, APP, and SORL1 act in a common pathway regulating the endolysosome system, which becomes dysfunctional in AD.

AB - Dysfunction of the endolysosomal-autophagy network is emerging as an important pathogenic process in Alzheimer's disease. Mutations in the sorting receptor-encoding gene SORL1 cause autosomal-dominant Alzheimer's disease, and SORL1 variants increase risk for late-onset AD. To understand the contribution of SORL1 mutations to AD pathogenesis, we analyze the effects of a SORL1 truncating mutation on SORL1 protein levels and endolysosome function in human neurons. We find that truncating mutation results in SORL1 haploinsufficiency and enlarged endosomes in human neurons. Analysis of isogenic SORL1 wild-type, heterozygous, and homozygous null neurons demonstrates that, whereas SORL1 haploinsufficiency results in endosome dysfunction, complete loss of SORL1 leads to additional defects in lysosome function and autophagy. Neuronal endolysosomal dysfunction caused by loss of SORL1 is relieved by extracellular antisense oligonucleotide-mediated reduction of APP protein, demonstrating that PSEN1, APP, and SORL1 act in a common pathway regulating the endolysosome system, which becomes dysfunctional in AD.

KW - Alzheimer's disease

KW - SORL1

KW - amyloid precursor protein

KW - autophagy

KW - endosome

KW - iPSC

KW - lysosome

UR - https://www.scopus.com/pages/publications/85107990896

U2 - 10.1016/j.celrep.2021.109259

DO - 10.1016/j.celrep.2021.109259

M3 - Article

C2 - 34133918

SN - 2211-1247

VL - 35

JO - Cell reports

JF - Cell reports

IS - 11

M1 - 109259

ER -

SORL1 deficiency in human excitatory neurons causes APP-dependent defects in the endolysosome-autophagy network

Abstract

UN SDGs

Keywords

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