Mutations in HspB1 and hereditary neuropathies

Muranova, Lydia K.; Sudnitsyna, Maria V.; Strelkov, S.V.; Gusev, Nikolai B.

doi:10.1007/s12192-020-01099-9

Cited by 16 publications

(29 citation statements)

References 91 publications

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“…Dysregulation of the activity or expression of HSP27 can result in debilitating diseases, including cancers (Ciocca & Calderwood, 2005; Straume et al, 2012), neurodegenerative diseases (Outeiro et al, 2006), and neuropathies (Evgrafov et al, 2004). More than 30 heritable HSP27 mutations are implicated in Charcot‐Marie‐Tooth (CMT) disease (Nefedova et al, 2015; Adriaenssens et al, 2017; Echaniz‐Laguna et al, 2017; Muranova et al, 2020; Vendredy et al, 2020), a group of neuropathies that affects ca . 1 in 2,500 individuals and is the most common inherited disorder involving the peripheral nervous system (Barisic et al, 2008; Timmerman et al, 2014).…”

Section: Introductionmentioning

confidence: 99%

A weakened interface in the P182L variant of HSP27 associated with severe Charcot‐Marie‐Tooth neuropathy causes aberrant binding to interacting proteins

et al. 2021

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HSP27 is a human molecular chaperone that forms large, dynamic oligomers and functions in many aspects of cellular homeostasis. Mutations in HSP27 cause Charcot‐Marie‐Tooth (CMT) disease, the most common inherited disorder of the peripheral nervous system. A particularly severe form of CMT disease is triggered by the P182L mutation in the highly conserved IxI/V motif of the disordered C‐terminal region, which interacts weakly with the structured core domain of HSP27. Here, we observed that the P182L mutation disrupts the chaperone activity and significantly increases the size of HSP27 oligomers formed in vivo, including in motor neurons differentiated from CMT patient‐derived stem cells. Using NMR spectroscopy, we determined that the P182L mutation decreases the affinity of the HSP27 IxI/V motif for its own core domain, leaving this binding site more accessible for other IxI/V‐containing proteins. We identified multiple IxI/V‐bearing proteins that bind with higher affinity to the P182L variant due to the increased availability of the IxI/V‐binding site. Our results provide a mechanistic basis for the impact of the P182L mutation on HSP27 and suggest that the IxI/V motif plays an important, regulatory role in modulating protein–protein interactions.

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Section: Introductionmentioning

confidence: 99%

A weakened interface in the P182L variant of HSP27 associated with severe Charcot‐Marie‐Tooth neuropathy causes aberrant binding to interacting proteins

et al. 2021

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“…4 Heat shock proteins (HSPs) are a group of ubiquitously expressed molecular chaperons with crucial roles in the response to cellular stress, proteostasis, and apoptosis. 7,9 The relative specificity of HSP27 mutations for peripheral nerves, and, potentially, for muscle, 10,11 has not yet been explained, but it may implicate HSPs involvement in cell-specific functions, such as cytoskeletal integrity. 12 HSPs structure 13 is highly conserved through evolution and is characterized by the presence of a hydrophobic N-terminal region with a phosphorylation domain (WDFP) which is critical for protein oligomerization, an α-crystallin domain containing β-sheets and mediating dimer formation, and a flexible C-terminal region ( Figure 1C).…”

Section: Discussionmentioning

confidence: 99%

“…4,5 Following the original description by Evgrafov et al, 4 more than 18 pathogenic mutations spanning across the whole HSPB1 gene have been reported. 6,7 As a result, the ability to diagnose CMT2F/dHMN2 and understand the genotypephenotype correlations that could inform about the natural history of the disease are rapidly expanding.…”

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confidence: 99%

A novel HSPB1 mutation associated with a late onset CMT2 phenotype: Case presentation and systematic review of the literature

Taga

Cornblath

2020

J Peripheral Nervous Sys

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Mutations in the HSPB1 gene are associated with Charcot‐Marie‐Tooth (CMT) disease type 2F (CMT2F) and distal hereditary motor neuropathy type 2 (dHMN2). More than 18 pathogenic mutations spanning across the whole HSPB1 gene have been reported. Three family members with a novel p.P57S (c.169C>T) HSPB1 mutation resulting in a late onset axonal neuropathy with heterogeneous clinical and electrophysiological features are detailed. We systematically reviewed published case reports and case series on HSPB1 mutations. While a genotype‐phenotype correlation was not obvious, we identified a common phenotype, which included adult onset, male predominance, motor more frequently than sensory involvement, distal and symmetric distribution with preferential involvement of plantar flexors, and a motor and axonal electrophysiological picture.

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“…In cases of irreversibly impaired polypeptides, HspB1, together with the other chaperones, can promote their ubiquitination and proteasomal degradation machinery [ 60 , 61 ]. In unstressed cells, different oligomeric and phosphorylated forms of HspB1 [ 62 , 63 ] interact with numerous different client proteins in order to modulate their maturation, activity or half-life [ 31 , 64 , 65 ]. In humans, HspB1 mutants can cause neuronal pathologies, such as distal hereditary motor neuropathy and hereditary peripheral neuropathy, also known as Charcot–Marie–Tooth disease type 2F [ 66 , 67 ].…”

Section: Small Hsps As Modulators Of Cftrmentioning

confidence: 99%

Small Hsps as Therapeutic Targets of Cystic Fibrosis Transmembrane Conductance Regulator Protein

Simon

Aissat

Degrugillier

et al. 2021

IJMS

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Human small heat shock proteins are molecular chaperones that regulate fundamental cellular processes in normal and pathological cells. Here, we have reviewed the role played by HspB1, HspB4 and HspB5 in the context of Cystic Fibrosis (CF), a severe monogenic autosomal recessive disease linked to mutations in Cystic Fibrosis Transmembrane conductance Regulator protein (CFTR) some of which trigger its misfolding and rapid degradation, particularly the most frequent one, F508del-CFTR. While HspB1 and HspB4 favor the degradation of CFTR mutants, HspB5 and particularly one of its phosphorylated forms positively enhance the transport at the plasma membrane, stability and function of the CFTR mutant. Moreover, HspB5 molecules stimulate the cellular efficiency of currently used CF therapeutic molecules. Different strategies are suggested to modulate the level of expression or the activity of these small heat shock proteins in view of potential in vivo therapeutic approaches. We then conclude with other small heat shock proteins that should be tested or further studied to improve our knowledge of CFTR processing.

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Mutations in HspB1 and hereditary neuropathies

Cited by 16 publications

References 91 publications

A weakened interface in the P182L variant of HSP27 associated with severe Charcot‐Marie‐Tooth neuropathy causes aberrant binding to interacting proteins

A weakened interface in the P182L variant of HSP27 associated with severe Charcot‐Marie‐Tooth neuropathy causes aberrant binding to interacting proteins

A novel HSPB1 mutation associated with a late onset CMT2 phenotype: Case presentation and systematic review of the literature

Small Hsps as Therapeutic Targets of Cystic Fibrosis Transmembrane Conductance Regulator Protein

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