Aberrant Compartment Formation by HSPB2 Mislocalizes Lamin A and Compromises Nuclear Integrity and Function

Federica F Morelli; Dineke S Verbeek; Jessika Bertacchini; Jonathan Vinet; Laura Mediani; Sandra Marmiroli; Giovanna Cenacchi; Milena Nasi; Sara De Biasi; Jeanette F Brunsting; Jan Lammerding; Elena Pegoraro; Corrado Angelini; Rossella Tupler; Simon Alberti; Serena Carra

doi:10.1016/j.celrep.2017.08.018

Aberrant Compartment Formation by HSPB2 Mislocalizes Lamin A and Compromises Nuclear Integrity and Function

Federica F Morelli, Dineke S Verbeek, Jessika Bertacchini, Jonathan Vinet, Laura Mediani, Sandra Marmiroli, Giovanna Cenacchi, Milena Nasi, Sara De Biasi, Jeanette F Brunsting, Jan Lammerding, Elena Pegoraro, Corrado Angelini, Rossella Tupler, Simon Alberti, Serena Carra^*

^*Corresponding author for this work

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

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Abstract

Small heat shock proteins (HSPBs) contain intrinsically disordered regions (IDRs), but the functions of these IDRs are still unknown. Here, we report that, in mammalian cells, HSPB2 phase separates to form nuclear compartments with liquid-like properties. We show that phase separation requires the disordered C-terminal domain of HSPB2. We further demonstrate that, in differentiating myoblasts, nuclear HSPB2 compartments sequester lamin A. Increasing the nuclear concentration of HSPB2 causes the formation of aberrant nuclear compartments that mislocalize lamin A and chromatin, with detrimental consequences for nuclear function and integrity. Importantly, phase separation of HSPB2 is regulated by HSPB3, but this ability is lost in two identified HSPB3 mutants that are associated with myopathy. Our results suggest that HSPB2 phase separation is involved in reorganizing the nucleoplasm during myoblast differentiation. Furthermore, these findings support the idea that aberrant HSPB2 phase separation, due to HSPB3 loss-of-function mutations, contributes to myopathy.

Original language	English
Pages (from-to)	2100-2115
Number of pages	16
Journal	Cell reports
Volume	20
Issue number	9
DOIs	https://doi.org/10.1016/j.celrep.2017.08.018
Publication status	Published - 29-Aug-2017

Keywords

HEAT-SHOCK-PROTEIN
DNA-DAMAGE RESPONSE
A-TYPE LAMINS
MUSCLE DIFFERENTIATION
CHROMATIN ORGANIZATION
CELLULAR SENESCENCE
MUSCULAR-DYSTROPHY
IN-VIVO
TRANSCRIPTION
DISEASE

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Morelli, F. F., Verbeek, D. S., Bertacchini, J., Vinet, J., Mediani, L., Marmiroli, S., Cenacchi, G., Nasi, M., De Biasi, S., Brunsting, J. F., Lammerding, J., Pegoraro, E., Angelini, C., Tupler, R., Alberti, S., & Carra, S. (2017). Aberrant Compartment Formation by HSPB2 Mislocalizes Lamin A and Compromises Nuclear Integrity and Function. Cell reports, 20(9), 2100-2115. https://doi.org/10.1016/j.celrep.2017.08.018

@article{0fba090fdcf641e9aaa7fe9479dec824,

title = "Aberrant Compartment Formation by HSPB2 Mislocalizes Lamin A and Compromises Nuclear Integrity and Function",

abstract = "Small heat shock proteins (HSPBs) contain intrinsically disordered regions (IDRs), but the functions of these IDRs are still unknown. Here, we report that, in mammalian cells, HSPB2 phase separates to form nuclear compartments with liquid-like properties. We show that phase separation requires the disordered C-terminal domain of HSPB2. We further demonstrate that, in differentiating myoblasts, nuclear HSPB2 compartments sequester lamin A. Increasing the nuclear concentration of HSPB2 causes the formation of aberrant nuclear compartments that mislocalize lamin A and chromatin, with detrimental consequences for nuclear function and integrity. Importantly, phase separation of HSPB2 is regulated by HSPB3, but this ability is lost in two identified HSPB3 mutants that are associated with myopathy. Our results suggest that HSPB2 phase separation is involved in reorganizing the nucleoplasm during myoblast differentiation. Furthermore, these findings support the idea that aberrant HSPB2 phase separation, due to HSPB3 loss-of-function mutations, contributes to myopathy.",

keywords = "HEAT-SHOCK-PROTEIN, DNA-DAMAGE RESPONSE, A-TYPE LAMINS, MUSCLE DIFFERENTIATION, CHROMATIN ORGANIZATION, CELLULAR SENESCENCE, MUSCULAR-DYSTROPHY, IN-VIVO, TRANSCRIPTION, DISEASE",

author = "Morelli, {Federica F} and Verbeek, {Dineke S} and Jessika Bertacchini and Jonathan Vinet and Laura Mediani and Sandra Marmiroli and Giovanna Cenacchi and Milena Nasi and {De Biasi}, Sara and Brunsting, {Jeanette F} and Jan Lammerding and Elena Pegoraro and Corrado Angelini and Rossella Tupler and Simon Alberti and Serena Carra",

year = "2017",

month = aug,

day = "29",

doi = "10.1016/j.celrep.2017.08.018",

language = "English",

volume = "20",

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Morelli, FF, Verbeek, DS, Bertacchini, J, Vinet, J, Mediani, L, Marmiroli, S, Cenacchi, G, Nasi, M, De Biasi, S, Brunsting, JF, Lammerding, J, Pegoraro, E, Angelini, C, Tupler, R, Alberti, S & Carra, S 2017, 'Aberrant Compartment Formation by HSPB2 Mislocalizes Lamin A and Compromises Nuclear Integrity and Function', Cell reports, vol. 20, no. 9, pp. 2100-2115. https://doi.org/10.1016/j.celrep.2017.08.018

TY - JOUR

T1 - Aberrant Compartment Formation by HSPB2 Mislocalizes Lamin A and Compromises Nuclear Integrity and Function

AU - Morelli, Federica F

AU - Verbeek, Dineke S

AU - Bertacchini, Jessika

AU - Vinet, Jonathan

AU - Mediani, Laura

AU - Marmiroli, Sandra

AU - Cenacchi, Giovanna

AU - Nasi, Milena

AU - De Biasi, Sara

AU - Brunsting, Jeanette F

AU - Lammerding, Jan

AU - Pegoraro, Elena

AU - Angelini, Corrado

AU - Tupler, Rossella

AU - Alberti, Simon

AU - Carra, Serena

PY - 2017/8/29

Y1 - 2017/8/29

N2 - Small heat shock proteins (HSPBs) contain intrinsically disordered regions (IDRs), but the functions of these IDRs are still unknown. Here, we report that, in mammalian cells, HSPB2 phase separates to form nuclear compartments with liquid-like properties. We show that phase separation requires the disordered C-terminal domain of HSPB2. We further demonstrate that, in differentiating myoblasts, nuclear HSPB2 compartments sequester lamin A. Increasing the nuclear concentration of HSPB2 causes the formation of aberrant nuclear compartments that mislocalize lamin A and chromatin, with detrimental consequences for nuclear function and integrity. Importantly, phase separation of HSPB2 is regulated by HSPB3, but this ability is lost in two identified HSPB3 mutants that are associated with myopathy. Our results suggest that HSPB2 phase separation is involved in reorganizing the nucleoplasm during myoblast differentiation. Furthermore, these findings support the idea that aberrant HSPB2 phase separation, due to HSPB3 loss-of-function mutations, contributes to myopathy.

AB - Small heat shock proteins (HSPBs) contain intrinsically disordered regions (IDRs), but the functions of these IDRs are still unknown. Here, we report that, in mammalian cells, HSPB2 phase separates to form nuclear compartments with liquid-like properties. We show that phase separation requires the disordered C-terminal domain of HSPB2. We further demonstrate that, in differentiating myoblasts, nuclear HSPB2 compartments sequester lamin A. Increasing the nuclear concentration of HSPB2 causes the formation of aberrant nuclear compartments that mislocalize lamin A and chromatin, with detrimental consequences for nuclear function and integrity. Importantly, phase separation of HSPB2 is regulated by HSPB3, but this ability is lost in two identified HSPB3 mutants that are associated with myopathy. Our results suggest that HSPB2 phase separation is involved in reorganizing the nucleoplasm during myoblast differentiation. Furthermore, these findings support the idea that aberrant HSPB2 phase separation, due to HSPB3 loss-of-function mutations, contributes to myopathy.

KW - HEAT-SHOCK-PROTEIN

KW - DNA-DAMAGE RESPONSE

KW - A-TYPE LAMINS

KW - MUSCLE DIFFERENTIATION

KW - CHROMATIN ORGANIZATION

KW - CELLULAR SENESCENCE

KW - MUSCULAR-DYSTROPHY

KW - IN-VIVO

KW - TRANSCRIPTION

KW - DISEASE

U2 - 10.1016/j.celrep.2017.08.018

DO - 10.1016/j.celrep.2017.08.018

M3 - Article

C2 - 28854361

SN - 2211-1247

VL - 20

SP - 2100

EP - 2115

JO - Cell reports

JF - Cell reports

IS - 9

ER -