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Aggregation of TAR-DNA-binding protein 43 (TDP-43) and of its fragments TDP-25 and TDP-35 occurs in amyotrophic lateral sclerosis (ALS). TDP-25 and TDP-35 act as seeds for TDP-43 aggregation, altering its function and exerting toxicity. Thus, inhibition of TDP-25 and TDP-35 aggregation and promotion of their degradation may protect against cellular damage. Upregulation of HSPB8 is one possible approach for this purpose, since this chaperone promotes the clearance of an ALS associated fragment of TDP-43 and is upregulated in the surviving motor neurones of transgenic ALS mice and human patients. We report that overexpression of HSPB8 in immortalized motor neurones decreased the accumulation of TDP-25 and TDP-35 and that protection against mislocalized/truncated TDP-43 was observed for HSPB8 in Drosophila melanogaster. Overexpression of HSP67Bc, the functional ortholog of human HSPB8, suppressed the eye degeneration caused by the cytoplasmic accumulation of a TDP-43 variant with a mutation in the nuclear localization signal (TDP-43-NLS). TDP-43-NLS accumulation in retinalcells was counteracted by HSP67Bc overexpression. According with this finding, downregulation of HSP67Bc increased eye degeneration, an effect that is consistent with the accumulation of high molecular weight TDP-43 species and ubiquitinated proteins. Moreover, we report a novel Drosophila model expressing TDP-35, and show that while TDP-43 and TDP-25 expression in the fly eyes causes a mild degeneration, TDP-35 expression leads to severe neurodegeneration as revealed by pupae 5 lethality; the latter effect could be rescued by HSP67Bc overexpression. Collectively, our data demonstrate that HSPB8 upregulation mitigates TDP fragment mediated toxicity, in mammalian neuronal cells and flies.

The Chaperone HSPB8 Reduces the Accumulation of Truncated TDP-43 Species in Cells and Protects Against TDP-43-Mediated Toxicity / V. Crippa, M.E. Cicardi, N. Ramesh, S.J. Seguin, M. Ganassi, I. Bigi, C. Diacci, E. Zelotti, M. Baratashvili, J.M. Gregory, C.M. Dobson, C. Cereda, U.B. Pandey, A. Poletti, S. Carra. - In: HUMAN MOLECULAR GENETICS. - ISSN 0964-6906. - 25:18(2016), pp. 3904-3924. [10.1093/hmg/ddw232]

The Chaperone HSPB8 Reduces the Accumulation of Truncated TDP-43 Species in Cells and Protects Against TDP-43-Mediated Toxicity

V. Crippa
Primo
;M.E. Cicardi
Secondo
;A. Poletti
Penultimo
;
2016

Abstract

Aggregation of TAR-DNA-binding protein 43 (TDP-43) and of its fragments TDP-25 and TDP-35 occurs in amyotrophic lateral sclerosis (ALS). TDP-25 and TDP-35 act as seeds for TDP-43 aggregation, altering its function and exerting toxicity. Thus, inhibition of TDP-25 and TDP-35 aggregation and promotion of their degradation may protect against cellular damage. Upregulation of HSPB8 is one possible approach for this purpose, since this chaperone promotes the clearance of an ALS associated fragment of TDP-43 and is upregulated in the surviving motor neurones of transgenic ALS mice and human patients. We report that overexpression of HSPB8 in immortalized motor neurones decreased the accumulation of TDP-25 and TDP-35 and that protection against mislocalized/truncated TDP-43 was observed for HSPB8 in Drosophila melanogaster. Overexpression of HSP67Bc, the functional ortholog of human HSPB8, suppressed the eye degeneration caused by the cytoplasmic accumulation of a TDP-43 variant with a mutation in the nuclear localization signal (TDP-43-NLS). TDP-43-NLS accumulation in retinalcells was counteracted by HSP67Bc overexpression. According with this finding, downregulation of HSP67Bc increased eye degeneration, an effect that is consistent with the accumulation of high molecular weight TDP-43 species and ubiquitinated proteins. Moreover, we report a novel Drosophila model expressing TDP-35, and show that while TDP-43 and TDP-25 expression in the fly eyes causes a mild degeneration, TDP-35 expression leads to severe neurodegeneration as revealed by pupae 5 lethality; the latter effect could be rescued by HSP67Bc overexpression. Collectively, our data demonstrate that HSPB8 upregulation mitigates TDP fragment mediated toxicity, in mammalian neuronal cells and flies.
English
motoneuron direases; amyotrophic lateral sclerosis; ALS, protein misfolding; protein aggregation; autophagy; proteasome; chaperones; HSPB8; BAG3
Settore BIO/13 - Biologia Applicata
Articolo
Esperti anonimi
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2016
HUMAN MOLECULAR GENETICS
25
18
3904
3924
21
Pubblicato
Periodico con rilevanza internazionale
Centro Interdipartimentale di Eccellenza per le Malattie Neurodegenerative CEND
crossref
WOS:000395806000002
2-s2.0-85014348474
27466192
Aderisco
info:eu-repo/semantics/article
The Chaperone HSPB8 Reduces the Accumulation of Truncated TDP-43 Species in Cells and Protects Against TDP-43-Mediated Toxicity / V. Crippa, M.E. Cicardi, N. Ramesh, S.J. Seguin, M. Ganassi, I. Bigi, C. Diacci, E. Zelotti, M. Baratashvili, J.M. Gregory, C.M. Dobson, C. Cereda, U.B. Pandey, A. Poletti, S. Carra. - In: HUMAN MOLECULAR GENETICS. - ISSN 0964-6906. - 25:18(2016), pp. 3904-3924. [10.1093/hmg/ddw232]
partially_open
Prodotti della ricerca::01 - Articolo su periodico
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262
Article (author)
no
V. Crippa, M.E. Cicardi, N. Ramesh, S.J. Seguin, M. Ganassi, I. Bigi, C. Diacci, E. Zelotti, M. Baratashvili, J.M. Gregory, C.M. Dobson, C. Cereda, U.B. Pandey, A. Poletti, S. Carra
01 - Articolo su periodico
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2434/425869
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