Mutations in KCNH1 and ATP6V1B2 Cause Zimmermann-Laband Syndrome

Overview

Journal Nat Genet

Specialty Genetics

Date 2015 Apr 28

PMID 25915598

Citations 103

Authors

Fanny Kortum

Viviana Caputo

Christiane K Bauer

Lorenzo Stella

Andrea Ciolfi

Malik Alawi

Gianfranco Bocchinfuso

Elisabetta Flex

Stefano Paolacci

Maria Lisa Dentici

Paola Grammatico

Georg Christoph Korenke

Vincenzo Leuzzi

David Mowat

Lal D V Nair

Thi Tuyet Mai Nguyen

Patrick Thierry

Susan M White

Bruno Dallapiccola

Antonio Pizzuti

Philippe M Campeau

Marco Tartaglia

Kerstin Kutsche

Affiliations

Soon will be listed here.

Abstract

Zimmermann-Laband syndrome (ZLS) is a developmental disorder characterized by facial dysmorphism with gingival enlargement, intellectual disability, hypoplasia or aplasia of nails and terminal phalanges, and hypertrichosis. We report that heterozygous missense mutations in KCNH1 account for a considerable proportion of ZLS. KCNH1 encodes the voltage-gated K(+) channel Eag1 (Kv10.1). Patch-clamp recordings showed strong negative shifts in voltage-dependent activation for all but one KCNH1 channel mutant (Gly469Arg). Coexpression of Gly469Arg with wild-type KCNH1 resulted in heterotetrameric channels with reduced conductance at positive potentials but pronounced conductance at negative potentials. These data support a gain-of-function effect for all ZLS-associated KCNH1 mutants. We also identified a recurrent de novo missense change in ATP6V1B2, encoding the B2 subunit of the multimeric vacuolar H(+) ATPase, in two individuals with ZLS. Structural analysis predicts a perturbing effect of the mutation on complex assembly. Our findings demonstrate that KCNH1 mutations cause ZLS and document genetic heterogeneity for this disorder.

Citing Articles

Utilizing Spermatogenesis and Fertilization Mutants as a Model for Human Disease.

Perez S, Augustineli H, Marcello M J Dev Biol. 2025; 13(1).

PMID: 39982357 PMC: 11843878. DOI: 10.3390/jdb13010004.

V-ATPase Dysfunction in the Brain: Genetic Insights and Therapeutic Opportunities.

Falace A, Volpedo G, Scala M, Zara F, Striano P, Fassio A Cells. 2024; 13(17.

PMID: 39273013 PMC: 11393946. DOI: 10.3390/cells13171441.

Dominantly acting variants in ATP6V1C1 and ATP6V1B2 cause a multisystem phenotypic spectrum by altering lysosomal and/or autophagosome function.

Carpentieri G, Cecchetti S, Bocchinfuso G, Radio F, Leoni C, Onesimo R HGG Adv. 2024; 5(4):100349.

PMID: 39210597 PMC: 11465052. DOI: 10.1016/j.xhgg.2024.100349.

Neurocardiac pathologies associated with potassium channelopathies.

Singh V, Auerbach D Epilepsia. 2024; 65(9):2537-2552.

PMID: 39087855 PMC: 11702590. DOI: 10.1111/epi.18066.

Ancient eukaryotic protein interactions illuminate modern genetic traits and disorders.

Cox R, Papoulas O, Shril S, Lee C, Gardner T, Battenhouse A bioRxiv. 2024; .

PMID: 38853926 PMC: 11160598. DOI: 10.1101/2024.05.26.595818.