Variants encoding a restricted carboxy-terminal domain of SLC12A2 cause hereditary hearing loss in humans

Mutai, Hideki; Wasano, Koichiro; Momozawa, Yukihide; Kamatani, Yoichiro; Miya, Fuyuki; Masuda, Sawako; Morimoto, Noriko; Nara, Kiyomitsu; Takahashi, Satoe; Tsunoda, Tatsuhiko; Homma, Kazuaki; Kubo, Michiaki; Matsunaga, Tatsuo

doi:10.1371/journal.pgen.1008643

Cited by 41 publications

(42 citation statements)

References 61 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Because her fibroblasts were collected, genetic analysis revealed that she carried both her parent's mutations. Evidence is now mounting that de novo (single allele) mutations lead to neurodevelopmental deficits and cochlea-vestibular defects (McNeill et al, 2020;Mutai et al, 2020). Another patient with NKCC1 mutation deserves some attention in the context of this review article.…”

Section: Na + /Glucose Transporter (Sglt)mentioning

confidence: 99%

Sodium Transporters in Human Health and Disease

Gagnon

Delpire

2021

Front. Physiol.

View full text Add to dashboard Cite

Sodium (Na+) electrochemical gradients established by Na+/K+ ATPase activity drives the transport of ions, minerals, and sugars in both excitable and non-excitable cells. Na+-dependent transporters can move these solutes in the same direction (cotransport) or in opposite directions (exchanger) across both the apical and basolateral plasma membranes of polarized epithelia. In addition to maintaining physiological homeostasis of these solutes, increases and decreases in sodium may also initiate, directly or indirectly, signaling cascades that regulate a variety of intracellular post-translational events. In this review, we will describe how the Na+/K+ ATPase maintains a Na+ gradient utilized by multiple sodium-dependent transport mechanisms to regulate glucose uptake, excitatory neurotransmitters, calcium signaling, acid-base balance, salt-wasting disorders, fluid volume, and magnesium transport. We will discuss how several Na+-dependent cotransporters and Na+-dependent exchangers have significant roles in human health and disease. Finally, we will discuss how each of these Na+-dependent transport mechanisms have either been shown or have the potential to use Na+ in a secondary role as a signaling molecule.

show abstract

Section: Na + /Glucose Transporter (Sglt)mentioning

confidence: 99%

Sodium Transporters in Human Health and Disease

Gagnon

Delpire

2021

Front. Physiol.

View full text Add to dashboard Cite

show abstract

“…The shaker-with-syndactylism homozygotes are deaf and exhibit vestibular dysfunction [57,58]. So far, several human mutations of NKCC1 have been reported [59][60][61][62][63][64]. Patients with deletion in NKCC1 suffer from multiorgan failure [60] or global developmental delay, together with hearing loss, gastrointestinal abnormalities, and absent salivation (named Kilquist syndrome [59]), while a gain-of-function missense variant of NKCC1 has been linked to schizophrenia [62].…”

Section: Nkcc1 Functions Outside the Cnsmentioning

confidence: 99%

NKCC1, an Elusive Molecular Target in Brain Development: Making Sense of the Existing Data

Virtanen

Uvarov

Hübner

et al. 2020

Cells

View full text Add to dashboard Cite

Ionotropic GABA transmission is mediated by anion (mainly Cl−)-permeable GABAA receptors (GABAARs). In immature neurons, GABA exerts depolarizing and sometimes functionally excitatory actions, based on active uptake of Cl− by the Na-K-2Cl cotransporter NKCC1. While functional evidence firmly shows NKCC1-mediated ion transport in immature and diseased neurons, molecular detection of NKCC1 in the brain has turned out to be extremely difficult. In this review, we describe the highly inconsistent data that are available on the cell type-specific expression patterns of the NKCC1 mRNA and protein in the CNS. We discuss the major technical caveats, including a lack of knock-out-controlled immunohistochemistry in the forebrain, possible effects of alternative splicing on the binding of antibodies and RNA probes, and the wide expression of NKCC1 in different cell types, which make whole-tissue analyses of NKCC1 useless for studying its neuronal expression. We also review novel single-cell RNAseq data showing that most of the NKCC1 in the adult CNS may, in fact, be expressed in non-neuronal cells, especially in glia. As future directions, we suggest single-cell NKCC1 mRNA and protein analyses and the use of genetically tagged endogenous proteins or systematically designed novel antibodies, together with proper knock-out controls, for the visualization of endogenous NKCC1 in distinct brain cell types and their subcellular compartments.

show abstract

“…The affected individuals presented with severe hearing loss. 98 In the first family, a 7-month-old female infant and her twin brother shared a SLC12A2 c.2145C > G variant, resulting in p.Asp981Tyr mutation. In the second family, the affected individual carried a c.2930-2A > G mutation; which affects the splice acceptor site of exon 21.…”

Section: Slc12a2 Haplotype Insufficiency and Hearing Lossmentioning

confidence: 99%

“…Interestingly, all these variants were confined to exon 21 ( Figure 5 ). 98 In addition to the hearing loss, affected infants in two families had difficulties in holding their heads up, maintaining a sitting position, or walking, indicative of minor motor developmental delays. In a second study, we identified three individuals from two independent families with mutations in exon 21 associated with nonsyndromic bilateral sensorineural deafness ( Table 2 ).…”

Section: Slc12a2 Haplotype Insufficiency and Hearing Lossmentioning

confidence: 99%

NKCC1: Newly Found as a Human Disease-Causing Ion Transporter

2020

View full text Add to dashboard Cite

SUMMARY Among the electroneutral Na+-dependent chloride transporters, NKCC1 had until now evaded identification as a protein causing human diseases. The closely related SLC12A transporters, NKCC2 and NCC have been identified some 25 years ago as responsible for Bartter and Gitelman syndromes: two renal-dependent salt wasting disorders. Absence of disease was most surprising since the NKCC1 knockout mouse was shown in 1999 to be viable, albeit with a wide range of deleterious phenotypes. Here we summarize the work of the past five years that introduced us to clinical cases involving NKCC1. The most striking cases are of 3 children with inherited mutations, who have complete absence of NKCC1 expression. These cases establish that lack of NKCC1 causes deafness; CFTR-like secretory defects with mucus accumulation in lung and intestine; severe xerostomia, hypotonia, dysmorphic facial features, and severe neurodevelopmental disorder. Another intriguing case is of a patient with a dominant deleterious SLC12A2 allele. This de novo mutation introduced a premature stop codon leading to a truncated protein. This mutant transporter seems to exert dominant-negative effect on wild-type transporter only in epithelial cells. The patient who suffers from lung, bladder, intestine, pancreas, and multiple endocrine abnormalities has, however, normal hearing and cognition. Finally, new reports substantiate the haploinsufficiency prediction of the SLC12A2 gene. Cases with single allele mutations in SLC12A2 have been linked to hearing loss and neurodevelopmental disorders.

show abstract

Variants encoding a restricted carboxy-terminal domain of SLC12A2 cause hereditary hearing loss in humans

Cited by 41 publications

References 61 publications

Sodium Transporters in Human Health and Disease

Sodium Transporters in Human Health and Disease

NKCC1, an Elusive Molecular Target in Brain Development: Making Sense of the Existing Data

NKCC1: Newly Found as a Human Disease-Causing Ion Transporter

Contact Info

Product

Resources

About