P.Gln200Glu, a Putative Constitutively Active Mutant of Rod Alpha-transducin (GNAT1) in Autosomal Dominant Congenital Stationary Night Blindness

Overview

Journal Hum Mutat

Specialty Genetics

Date 2007 Jun 23

PMID 17584859

Citations 19

Authors

Viktoria Szabo

Hans-Jurgen Kreienkamp

Thomas Rosenberg

Andreas Gal

Affiliations

Soon will be listed here.

Abstract

Congenital stationary night blindness (CSNB) is a non-progressive Mendelian condition resulting from a functional defect in rod photoreceptors. A small number of unique missense mutations in the genes encoding various members of the rod phototransduction cascade, e.g. rhodopsin (RHO), cGMP phosphodiesterase beta-subunit (PDE6B), and transducin alpha-subunit (GNAT1) have been reported to cause autosomal dominant (ad) CSNB. While the RHO and PDE6B mutations result in constitutively active proteins, the only known adCSNB-associated GNAT1 change (p.Gly38Asp) produces an alpha-transducin that is unable to activate its downstream effector molecule in vitro. In a multigeneration Danish family with adCSNB, we identified a novel heterozygous C to G transversion (c.598C>G) in exon 6 of GNAT1 that should result in a p.Gln200Glu substitution in the evolutionarily highly conserved Switch 2 region of alpha-transducin, a domain that has an important role in binding and hydrolyzing GTP. Computer modeling based on the known crystal structure of transducin suggests that the p.Gln200Glu mutant exhibits impaired GTPase activity, and thereby leads to constitutive activation of phototransduction. This assumption is in line with our results of trypsin protection assays as well as previously published biochemical data on mutants of this glutamine in the GTPase active site of alpha-transducin following in vitro expression, and observations that inappropriately activating mutants of various members of the rod phototransduction cascade represent one of the major molecular causes of adCSNB.

Citing Articles

Structural view of G protein-coupled receptor signaling in the retinal rod outer segment.

Gulati S, Palczewski K Trends Biochem Sci. 2022; 48(2):172-186.

PMID: 36163145 PMC: 9868064. DOI: 10.1016/j.tibs.2022.08.010.

Clinical and Genetic Characteristics of Korean Congenital Stationary Night Blindness Patients.

Kim H, Joo K, Han J, Woo S Genes (Basel). 2021; 12(6).

PMID: 34064005 PMC: 8224030. DOI: 10.3390/genes12060789.

Photoreceptor phosphodiesterase (PDE6): activation and inactivation mechanisms during visual transduction in rods and cones.

Cote R Pflugers Arch. 2021; 473(9):1377-1391.

PMID: 33860373 PMC: 8376765. DOI: 10.1007/s00424-021-02562-x.

The molecular architecture of photoreceptor phosphodiesterase 6 (PDE6) with activated G protein elucidates the mechanism of visual excitation.

Irwin M, Gupta R, Gao X, Cahill K, Chu F, Cote R J Biol Chem. 2019; 294(51):19486-19497.

PMID: 31690623 PMC: 6926442. DOI: 10.1074/jbc.RA119.011002.

Coexistence of GNAT1 and ABCA4 variants associated with Nougaret-type congenital stationary night blindness and childhood-onset cone-rod dystrophy.

Hayashi T, Hosono K, Kurata K, Katagiri S, Mizobuchi K, Ueno S Doc Ophthalmol. 2019; 140(2):147-157.

PMID: 31583501 DOI: 10.1007/s10633-019-09727-1.