Literature DB >> 22484489

The family of mammalian small heat shock proteins (HSPBs): implications in protein deposit diseases and motor neuropathies.

Alessandra Boncoraglio1, Melania Minoia, Serena Carra.   

Abstract

A number of neurological and muscular disorders are characterized by the accumulation of aggregate-prone proteins and are referred to as protein deposit or protein conformation diseases. Besides some sporadic forms, most of them are genetically inherited in an autosomal dominant manner, although recessive forms also exist. Although genetically very heterogeneous, some of these diseases are the result of mutations in some members of the mammalian small heat shock protein family (sHSP/HSPB), which are key players of the protein quality control system and participate, together with other molecular chaperones and co-chaperones, in the maintenance of protein homeostasis. Thus, on one hand upregulation of specific members of the HSPB family can exert protective effects in protein deposit diseases, such as the polyglutamine diseases. On the other hand, mutations in the HSPBs lead to neurological and muscular disorders, which may be due to a loss-of-function in protein quality control and/or to a gain-of-toxic function, resulting from the aggregation-proneness of the mutants. In this review we summarize the current knowledge about some of the best characterized functions of the HSPBs (e.g. role in cytoskeleton stabilization, chaperone function, anti-aggregation and anti-apoptotic activities), also highlighting differences in the properties of the various HSPBs and how these may counteract protein aggregation diseases. We also describe the mutations in the various HSPBs associated with neurological and muscular disorders and we discuss how gain-of-toxic function mechanisms (e.g. due to the mutated HSPB protein instability and aggregation) and/or loss-of-function mechanisms can contribute to HSPB-associated pathologies. This article is part of a Directed Issue entitled: Small HSPs in physiology and pathology.
Copyright © 2012 Elsevier Ltd. All rights reserved.

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Year:  2012        PMID: 22484489     DOI: 10.1016/j.biocel.2012.03.011

Source DB:  PubMed          Journal:  Int J Biochem Cell Biol        ISSN: 1357-2725            Impact factor:   5.085


  28 in total

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Authors:  André-Patrick Arrigo
Journal:  Cell Stress Chaperones       Date:  2017-01-31       Impact factor: 3.667

2.  Structure and properties of chimeric small heat shock proteins containing yellow fluorescent protein attached to their C-terminal ends.

Authors:  Petr N Datskevich; Nikolai B Gusev
Journal:  Cell Stress Chaperones       Date:  2013-11-27       Impact factor: 3.667

Review 3.  Opportunities and challenges for molecular chaperone modulation to treat protein-conformational brain diseases.

Authors:  Herman van der Putten; Gregor P Lotz
Journal:  Neurotherapeutics       Date:  2013-07       Impact factor: 7.620

4.  HSPA1A-independent suppression of PARK2 C289G protein aggregation by human small heat shock proteins.

Authors:  Melania Minoia; Corien Grit; Harm H Kampinga
Journal:  Mol Cell Biol       Date:  2014-07-14       Impact factor: 4.272

5.  Rare Variants in MME, Encoding Metalloprotease Neprilysin, Are Linked to Late-Onset Autosomal-Dominant Axonal Polyneuropathies.

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Journal:  Am J Hum Genet       Date:  2016-09-01       Impact factor: 11.025

6.  Recurrent heat shock impairs the proliferation and differentiation of C2C12 myoblasts.

Authors:  Daniel J Bolus; Gobinath Shanmugam; Madhusudhanan Narasimhan; Namakkal S Rajasekaran
Journal:  Cell Stress Chaperones       Date:  2017-10-24       Impact factor: 3.667

Review 7.  Studying heat shock proteins through single-molecule mechanical manipulation.

Authors:  Dhawal Choudhary; Laura Mediani; Serena Carra; Ciro Cecconi
Journal:  Cell Stress Chaperones       Date:  2020-04-06       Impact factor: 3.667

Review 8.  The growing world of small heat shock proteins: from structure to functions.

Authors:  Serena Carra; Simon Alberti; Patrick A Arrigo; Justin L Benesch; Ivor J Benjamin; Wilbert Boelens; Britta Bartelt-Kirbach; Bianca J J M Brundel; Johannes Buchner; Bernd Bukau; John A Carver; Heath Ecroyd; Cecilia Emanuelsson; Stephanie Finet; Nikola Golenhofen; Pierre Goloubinoff; Nikolai Gusev; Martin Haslbeck; Lawrence E Hightower; Harm H Kampinga; Rachel E Klevit; Krzysztof Liberek; Hassane S Mchaourab; Kathryn A McMenimen; Angelo Poletti; Roy Quinlan; Sergei V Strelkov; Melinda E Toth; Elizabeth Vierling; Robert M Tanguay
Journal:  Cell Stress Chaperones       Date:  2017-03-31       Impact factor: 3.667

9.  The structured core domain of αB-crystallin can prevent amyloid fibrillation and associated toxicity.

Authors:  Georg K A Hochberg; Heath Ecroyd; Cong Liu; Dezerae Cox; Duilio Cascio; Michael R Sawaya; Miranda P Collier; James Stroud; John A Carver; Andrew J Baldwin; Carol V Robinson; David S Eisenberg; Justin L P Benesch; Arthur Laganowsky
Journal:  Proc Natl Acad Sci U S A       Date:  2014-04-07       Impact factor: 11.205

Review 10.  Different anti-aggregation and pro-degradative functions of the members of the mammalian sHSP family in neurological disorders.

Authors:  Serena Carra; Paola Rusmini; Valeria Crippa; Elisa Giorgetti; Alessandra Boncoraglio; Riccardo Cristofani; Maximillian Naujock; Melanie Meister; Melania Minoia; Harm H Kampinga; Angelo Poletti
Journal:  Philos Trans R Soc Lond B Biol Sci       Date:  2013-03-25       Impact factor: 6.237

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