A knock-in/knock-out mouse model of HSPB8-associated distal hereditary motor neuropathy and myopathy reveals toxic gain-of-function of mutant Hspb8

Delphine Bouhy; Manisha Juneja; Istvan Katona; Anne Holmgren; Bob Asselbergh; Vicky De Winter; Tino Hochepied; Steven Goossens; Jody J Haigh; Claude Libert; Chantal Ceuterick-de Groote; Joy Irobi; Joachim Weis; Vincent Timmerman

doi:10.1007/s00401-017-1756-0

A knock-in/knock-out mouse model of HSPB8-associated distal hereditary motor neuropathy and myopathy reveals toxic gain-of-function of mutant Hspb8

Acta Neuropathol. 2018 Jan;135(1):131-148. doi: 10.1007/s00401-017-1756-0. Epub 2017 Aug 5.

Authors

Delphine Bouhy¹, Manisha Juneja¹, Istvan Katona², Anne Holmgren¹, Bob Asselbergh³, Vicky De Winter¹, Tino Hochepied^{4

5}, Steven Goossens^{5

6

7}, Jody J Haigh^{5

8}, Claude Libert⁷, Chantal Ceuterick-de Groote⁹, Joy Irobi¹⁰, Joachim Weis², Vincent Timmerman¹¹

Affiliations

¹ Peripheral Neuropathy Research Group, Department of Biomedical Sciences and Institute Born Bunge, University of Antwerp, Universiteitsplein 1, 2610, Antwerpen, Belgium.
² Institute of Neuropathology, RWTH Aachen University Hospital, Aachen, Germany.
³ VIB Center for Molecular Neurology, University of Antwerp, Antwerpen, Belgium.
⁴ Transgenic Mouse Core Facility, VIB Inflammation Research Center, Gent, Belgium.
⁵ Department of Biomedical Molecular Biology, Ghent University, Gent, Belgium.
⁶ Cancer Research Institute Ghent (CRIG), Ghent University, Gent, Belgium.
⁷ VIB Inflammation Research Center, Ghent University, Gent, Belgium.
⁸ Mammalian Functional Genetics Laboratory, Division of Blood Cancers, Australian Centre for Blood Diseases, Monash University, Melbourne, VIC, 3004, Australia.
⁹ Laboratory of Neuromuscular Pathology, Institute Born-Bunge and Translational Neurosciences, University of Antwerp, Antwerpen, Belgium.
¹⁰ Neurofunctional Genomics, Biomedical Research Institute (BIOMED), Hasselt University/Transnational University Limburg, School of Life Sciences, Diepenbeek, Belgium.
¹¹ Peripheral Neuropathy Research Group, Department of Biomedical Sciences and Institute Born Bunge, University of Antwerp, Universiteitsplein 1, 2610, Antwerpen, Belgium. vincent.timmerman@uantwerpen.be.

Abstract

Mutations in the small heat shock protein B8 gene (HSPB8/HSP22) have been associated with distal hereditary motor neuropathy, Charcot-Marie-Tooth disease, and recently distal myopathy. It is so far not clear how mutant HSPB8 induces the neuronal and muscular phenotypes and if a common pathogenesis lies behind these diseases. Growing evidence points towards a role of HSPB8 in chaperone-associated autophagy, which has been shown to be a determinant for the clearance of poly-glutamine aggregates in neurodegenerative diseases but also for the maintenance of skeletal muscle myofibrils. To test this hypothesis and better dissect the pathomechanism of mutant HSPB8, we generated a new transgenic mouse model leading to the expression of the mutant protein (knock-in lines) or the loss-of-function (functional knock-out lines) of the endogenous protein Hspb8. While the homozygous knock-in mice developed motor deficits associated with degeneration of peripheral nerves and severe muscle atrophy corroborating patient data, homozygous knock-out mice had locomotor performances equivalent to those of wild-type animals. The distal skeletal muscles of the post-symptomatic homozygous knock-in displayed Z-disk disorganisation, granulofilamentous material accumulation along with Hspb8, αB-crystallin (HSPB5/CRYAB), and desmin aggregates. The presence of the aggregates correlated with reduced markers of effective autophagy. The sciatic nerve of the homozygous knock-in mice was characterized by low autophagy potential in pre-symptomatic and Hspb8 aggregates in post-symptomatic animals. On the other hand, the sciatic nerve of the homozygous knock-out mice presented a normal morphology and their distal muscle displayed accumulation of abnormal mitochondria but intact myofiber and Z-line organisation. Our data, therefore, suggest that toxic gain-of-function of mutant Hspb8 aggregates is a major contributor to the peripheral neuropathy and the myopathy. In addition, mutant Hspb8 induces impairments in autophagy that may aggravate the phenotype.

Keywords: Autophagy; HSPB8; Myofibrillar myopathy; Peripheral neuropathy.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Atrophy / metabolism
Atrophy / pathology
Autophagy / physiology
Disease Models, Animal
Distal Myopathies / metabolism*
Distal Myopathies / pathology
Female
Gain of Function Mutation*
HSP20 Heat-Shock Proteins / genetics*
HSP20 Heat-Shock Proteins / metabolism*
Heat-Shock Proteins
Mice, Transgenic
Mitochondria / metabolism
Mitochondria / pathology
Molecular Chaperones
Muscle Proteins / genetics*
Muscle Proteins / metabolism*
Muscle, Skeletal / metabolism
Muscle, Skeletal / pathology
Myopathies, Structural, Congenital / metabolism*
Myopathies, Structural, Congenital / pathology
Peripheral Nervous System Diseases / metabolism*
Sciatic Nerve / metabolism
Sciatic Nerve / pathology

Substances

HSP20 Heat-Shock Proteins
Heat-Shock Proteins
Hspb8 protein, mouse
Molecular Chaperones
Muscle Proteins

Supplementary concepts

Myofibrillar Myopathy