Mutations in the nervous system–specific HSN2 exon of WNK1 cause hereditary sensory neuropathy type II

Shekarabi, Masoud; Girard, Nathalie; Rivière, Jean‐Baptiste; Dion, Patrick A.; Houle, Martin; Toulouse, André; Lafrenière, Ronald G.; Vercauteren, F.; Hince, Pascale; Laganière, Janet; Rochefort, Daniel; Faivre, Laurence; Samuels, Mark E.; Rouleau, Guy A.

doi:10.1172/jci34088

Cited by 79 publications

(145 citation statements)

References 46 publications

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“…92 Similarly, mutations in WNK1 could also alter NGF/TrkA signaling through its protein kinase activity, although abnormalities in kinase activity for particular substrates have not been examined in detail in mutant proteins that contain the pathogenic exon 8B. 93 Nevertheless, WNK1 activates Erk5, 94 and Erk5 is a critical mitogen-activated protein kinase required for retrograde NGF/TrkA survival signaling in NGF-dependent neurons. 95 Alterations in WNK1-mediated activation of Erk5 could lead to altered sensory and sympathetic neuron survival in HSAN2 caused by WNK1 mutations.…”

Section: Growth Factor Signalingmentioning

confidence: 99%

Axon Transport and Neuropathy

Tourtellotte

2016

The American Journal of Pathology

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Peripheral neuropathies are highly prevalent and are most often associated with chronic disease, side effects from chemotherapy, or toxic-metabolic abnormalities. Neuropathies are less commonly caused by genetic mutations, but studies of the normal function of mutated proteins have identified particular vulnerabilities that often implicate mitochondrial dynamics and axon transport mechanisms. Hereditary sensory and autonomic neuropathies are a group of phenotypically related diseases caused by monogenic mutations that primarily affect sympathetic and sensory neurons. Here, I review evidence to indicate that many genetic neuropathies are caused by abnormalities in axon transport. Moreover, in hereditary sensory and autonomic neuropathies. There may be specific convergence on gene mutations that disrupt nerve growth factor signaling, upon which sympathetic and sensory neurons critically depend. (Am J Pathol 2016, 186: 489e499; http://dx

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Section: Growth Factor Signalingmentioning

confidence: 99%

Axon Transport and Neuropathy

Tourtellotte

2016

The American Journal of Pathology

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“…An interesting recent study has reported that neuronal tissues express two distinct splice variants of WNK1, which possess an inserted sequence within the C-terminal non-catalytic domain that is expressed from distinct exons (termed exon 8b and exon HSN2) ( Fig. 1) (Shekarabi et al, 2008). Most importantly, this study reported that, human mutations that lie within exon HSN2 as well as in exon 6 of WNK1 resulted in an early-onset autosomal-recessive loss-of-pain-perception disorder termed hereditary sensory and autonomic neuropathy type II (HSANII) (Shekarabi et al, 2008).…”

Section: Key Features Of Wnk Isoformsmentioning

confidence: 99%

“…1) (Shekarabi et al, 2008). Most importantly, this study reported that, human mutations that lie within exon HSN2 as well as in exon 6 of WNK1 resulted in an early-onset autosomal-recessive loss-of-pain-perception disorder termed hereditary sensory and autonomic neuropathy type II (HSANII) (Shekarabi et al, 2008). The described mutations result in the truncation of a large region of the non-catalytic C-terminal domain of the WNK1 protein; this does not affect the kinase domain (Shekarabi et al, 2008).…”

Section: Key Features Of Wnk Isoformsmentioning

confidence: 99%

The regulation of salt transport and blood pressure by the WNK-SPAK/OSR1 signalling pathway

Richardson

Alessi

2008

Journal of Cell Science

270

323

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It has recently been shown that the WNK [with-no-K(Lysand NKCC2, which are targets for the commonly used bloodpressure-lowering thiazide-diuretic and loop-diuretic drugs. The finding that mutations in WNK1, WNK4, NCC and NKCC2 cause inherited blood-pressure syndromes in humans highlights the importance of these enzymes. We argue that these new findings indicate that SPAK and OSR1 are promising drug targets for the treatment of hypertension, because inhibiting these enzymes would reduce NCC and NKCC2 activity and thereby suppress renal salt re-absorption. We also discuss unresolved and controversial questions in this field of research.

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“…All immunohistochemistry and tissue preparations were performed as described previously (Howard et al, 2002;Shekarabi et al, 2008). A mix of anti-axonal markers SMI31 and SMI32 (Covance, each at 1:500), anti-glutamic acid decarboxylase (GAD67; Novus Biologicals, 1:200) followed by donkey antimouse Alexa Fluor 488 or anti-rabbit Alexa Fluor 488 (Molecular Probes, all at 1:1000) were used to label axons , and GABAergic neurons and synaptic terminals, respectively.…”

Section: ⌬18/⌬18mentioning

confidence: 99%

Loss of Neuronal Potassium/Chloride Cotransporter 3 (KCC3) Is Responsible for the Degenerative Phenotype in a Conditional Mouse Model of Hereditary Motor and Sensory Neuropathy Associated with Agenesis of the Corpus Callosum

Shekarabi

Moldrich²,

Rasheed³

et al. 2012

J. Neurosci.

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Disruption of the potassium/chloride cotransporter 3 (KCC3), encoded by the SLC12A6 gene, causes hereditary motor and sensory neuropathy associated with agenesis of the corpus callosum (HMSN/ACC), a neurodevelopmental and neurodegenerative disorder affecting both the peripheral nervous system and CNS. However, the precise role of KCC3 in the maintenance of ion homeostasis in the nervous system and the pathogenic mechanisms leading to HMSN/ACC remain unclear. We established two Slc12a6 Cre/LoxP transgenic mouse lines expressing C-terminal truncated KCC3 in either a neuron-specific or ubiquitous fashion. Our results suggest that neuronal KCC3 expression is crucial for axon volume control. We also demonstrate that the neuropathic features of HMSN/ACC are predominantly due to a neuronal KCC3 deficit, while the auditory impairment is due to loss of non-neuronal KCC3 expression. Furthermore, we demonstrate that KCC3 plays an essential role in inflammatory pain pathways. Finally, we observed hypoplasia of the corpus callosum in both mouse mutants and a marked decrease in axonal tracts serving the auditory cortex in only the general deletion mutant. Together, these results establish KCC3 as an important player in both central and peripheral nervous system maintenance.

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Mutations in the nervous system–specific HSN2 exon of WNK1 cause hereditary sensory neuropathy type II

Cited by 79 publications

References 46 publications

Axon Transport and Neuropathy

Axon Transport and Neuropathy

The regulation of salt transport and blood pressure by the WNK-SPAK/OSR1 signalling pathway

Loss of Neuronal Potassium/Chloride Cotransporter 3 (KCC3) Is Responsible for the Degenerative Phenotype in a Conditional Mouse Model of Hereditary Motor and Sensory Neuropathy Associated with Agenesis of the Corpus Callosum

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