Photoreceptor degeneration in two mouse models for congenital stationary night blindness type 2

Regus-Leidig H, Atorf J, Feigenspan A, Kremers J, Maw MA, Brandstätter JH (2014)

Publication Type: Journal article

Publication year: 2014

Journal

PLoS ONE Public Library of Science

Book Volume: 9

Pages Range: e86769

Journal Issue: 1

DOI: 10.1371/journal.pone.0086769

Abstract

Light-dependent conductance changes of voltage-gated Cav1.4 channels regulate neurotransmitter release at photoreceptor ribbon synapses. Mutations in the human CACNA1F gene encoding the ?1F subunit of Cav1.4 channels cause an incomplete form of X-linked congenital stationary night blindness (CSNB2). Many CACNA1F mutations are loss-of-function mutations resulting in non-functional Cav1.4 channels, but some mutations alter the channels' gating properties and, presumably, disturb Ca(2+) influx at photoreceptor ribbon synapses. Notably, a CACNA1F mutation (I745T) was identified in a family with an uncommonly severe CSNB2-like phenotype, and, when expressed in a heterologous system, the mutation was shown to shift the voltage-dependence of channel activation, representing a gain-of-function. To gain insight into the pathomechanism that could explain the severity of this disorder, we generated a mouse model with the corresponding mutation in the murine Cacna1f gene (I756T) and compared it with a mouse model carrying a loss-of-function mutation (?Ex14-17) in a longitudinal study up to eight months of age. In ?Ex14-17 mutants, the b-wave in the electroretinogram was absent, photoreceptor ribbon synapses were abnormal, and Ca(2+) responses to depolarization of photoreceptor terminals were undetectable. In contrast, I756T mutants had a reduced scotopic b-wave, some intact rod ribbon synapses, and a strong, though abnormal, Ca(2+) response to depolarization. Both mutants showed a progressive photoreceptor loss, but degeneration was more severe and significantly enhanced in the I756T mutants compared to the ?Ex14-17 mutants.

Authors with CRIS profile

Hanna Regus-Leidig Lehrstuhl für Tierphysiologie Jenny Atorf Department of Ophthalmology Andreas Feigenspan Professur für Neurobiologie Jan Kremers Professur für Experimentelle Augenheilkunde Johann Helmut Brandstätter Lehrstuhl für Tierphysiologie

Involved external institutions

University of Otago NZ New Zealand (NZ)

How to cite

APA:

Regus-Leidig, H., Atorf, J., Feigenspan, A., Kremers, J., Maw, M.A., & Brandstätter, J.H. (2014). Photoreceptor degeneration in two mouse models for congenital stationary night blindness type 2. PLoS ONE, 9(1), e86769. https://doi.org/10.1371/journal.pone.0086769

MLA:

Regus-Leidig, Hanna, et al. "Photoreceptor degeneration in two mouse models for congenital stationary night blindness type 2." PLoS ONE 9.1 (2014): e86769.

BibTeX: Download