Analysis of<i>CLCNKB</i>mutations at dimer‐interface, calcium‐binding site, and pore reveals a variety of functional alterations in ClC‐Kb channel leading to Bartter syndrome

Bignon, Yohan; Sakhi, Imène; Bitam, Sara; Bakouh, Naziha; Keck, Mathilde; Frachon, Nadia; Paulais, Marc; Planelles, Gabrielle; Teulon, Jacques; Andrini, Olga

doi:10.1002/humu.23962

Cited by 6 publications

(6 citation statements)

References 49 publications

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“…Thus, our data suggest that the Helix-O motions involved in transition to the outward-facing state are distinct from those postulated to facilitate inner-gate opening. While the mechanistic details linking Helix O-Q movements between outward-and inwardfacing states are currently unknown, it is of interest to note that many disease-causing mutations occur in this segment, in both CLC channels (Saviane et al, 1999;Pusch, 2002;Bignon et al, 2020) and transporters (Lourdel et al, 2012;Veeramah et al, 2013). In Helix O, for example, mutation of a highly conserved glycine residue occurring mid-helix can cause Dent's disease (CLC-5, (Smith et al, 2009)) or Bartter syndrome (CLC -Kb, (Lin et al, 2009)).…”

Section: Overall Conformational Change In Qqqmentioning

confidence: 99%

A CLC-ec1 mutant reveals global conformational change and suggests a unifying mechanism for the CLC Cl–/H+ transport cycle

Chavan

Cheng

Jiang

et al. 2020

eLife

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Among coupled exchangers, CLCs uniquely catalyze the exchange of oppositely charged ions (Cl– for H+). Transport-cycle models to describe and explain this unusual mechanism have been proposed based on known CLC structures. While the proposed models harmonize with many experimental findings, gaps and inconsistencies in our understanding have remained. One limitation has been that global conformational change – which occurs in all conventional transporter mechanisms – has not been observed in any high-resolution structure. Here, we describe the 2.6 Å structure of a CLC mutant designed to mimic the fully H+-loaded transporter. This structure reveals a global conformational change to improve accessibility for the Cl– substrate from the extracellular side and new conformations for two key glutamate residues. Together with DEER measurements, MD simulations, and functional studies, this new structure provides evidence for a unified model of H+/Cl– transport that reconciles existing data on all CLC-type proteins.

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Section: Overall Conformational Change In Qqqmentioning

confidence: 99%

A CLC-ec1 mutant reveals global conformational change and suggests a unifying mechanism for the CLC Cl–/H+ transport cycle

Chavan

Cheng

Jiang

et al. 2020

eLife

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“…20 In addition, tow cystathionineβsynthase domains located at the end of the carboxyl terminus have important roles in the function and/or expression of CLC-Kb, and eliminating these domains due to the mutation may abolish their functions. 1,20,21 It is noteworthy that this deletion has been previously reported in the compound heterozygote state. 22 This is the first time this mutation c.1332_1335delCTCT is reported in the homozygous state.…”

Section: Discussionmentioning

confidence: 64%

“…CLC‐Ka and CLC‐Kb belong to a large CLC gene family of chloride channels and are the most voltage‐gated Cl − channels located in the kidney and the inner ear cells. 1 , 8 CLC‐Kb operates as a homodimer associated with the regulatory Barttin subunit leading to reabsorption of Cl − at thick ascending limb (TAL) of loop of Henle. 8 , 9 This transmembrane protein is encoded by Cl − voltage‐gated channel Kb ( CLCNKB ) gene [OMIM #602023] which is situated on chromosome 1p36 and includes 20 exons.…”

Section: Introductionmentioning

confidence: 99%

“…CLC‐Ka and CLC‐Kb belong to a large CLC gene family of chloride channels and are the most voltage‐gated Cl − channels located in the kidney and the inner ear cells 1,8 . CLC‐Kb operates as a homodimer associated with the regulatory Barttin subunit leading to reabsorption of Cl − at thick ascending limb (TAL) of loop of Henle 8,9 .…”

Section: Introductionmentioning

confidence: 99%

“…

Bartter syndrome, BS, is a rare disease with a prevalence of 1 in 1,000,000 and a heterogeneous group of salt-wasting tubulopathies distinguished by polyuria, polydipsia, hypokalemia, metabolic alkalosis, renal salt loss with normal or low blood pressure and secondary hyperaldosteronism. [1][2][3] Genotypically, BS divided into at least 6 types results from loss of function mutations in different genes encoding the transporters involved in salt reabsorption at the TAL. [3][4][5] The type III BS appears in infancy to adolescence and has a wide spectrum of phenotype variability with a predominantly mild presentation.

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mentioning

confidence: 99%

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