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Allelic variance between GRM6 mutants, Grm6nob3 and Grm6nob4 results in differences in retinal ganglion cell visual responses.

Authors :
Maddox DM
Vessey KA
Yarbrough GL
Invergo BM
Cantrell DR
Inayat S
Balannik V
Hicks WL
Hawes NL
Byers S
Smith RS
Hurd R
Howell D
Gregg RG
Chang B
Naggert JK
Troy JB
Pinto LH
Nishina PM
McCall MA
Source :
The Journal of physiology [J Physiol] 2008 Sep 15; Vol. 586 (18), pp. 4409-24. Date of Electronic Publication: 2008 Aug 07.
Publication Year :
2008

Abstract

An electroretinogram (ERG) screen identified a mouse with a normal a-wave but lacking a b-wave, and as such it was designated no b-wave3 (nob3). The nob3 phenotype mapped to chromosome 11 in a region containing the metabotropic glutamate receptor 6 gene (Grm6). Sequence analyses of cDNA identified a splicing error in Grm6, introducing an insertion and an early stop codon into the mRNA of affected mice (designated Grm6(nob3)). Immunohistochemistry of the Grm6(nob3) retina showed that GRM6 was absent. The ERG and visual behaviour abnormalities of Grm6(nob3) mice are similar to Grm6(nob4) animals, and similar deficits were seen in compound heterozygotes (Grm6(nob4/nob3)), indicating that Grm6(nob3) is allelic to Grm6(nob4). Visual responses of Grm6(nob3) retinal ganglion cells (RGCs) to light onset were abnormal. Grm6(nob3) ON RGCs were rarely recorded, but when they were, had ill-defined receptive field (RF) centres and delayed onset latencies. When Grm6(nob3) OFF-centre RGC responses were evoked by full-field stimulation, significantly fewer converted that response to OFF/ON compared to Grm6(nob4) RGCs. Grm6(nob4/nob3) RGC responses verified the conclusion that the two mutants are allelic. We propose that Grm6(nob3) is a new model of human autosomal recessive congenital stationary night blindness. However, an allelic difference between Grm6(nob3) and Grm6(nob4) creates a disparity in inner retinal processing. Because the localization of GRM6 is limited to bipolar cells in the On pathway, the observed difference between RGCs in these mutants is likely to arise from differences in their inputs.

Details

Language :
English
ISSN :
1469-7793
Volume :
586
Issue :
18
Database :
MEDLINE
Journal :
The Journal of physiology
Publication Type :
Academic Journal
Accession number :
18687716
Full Text :
https://doi.org/10.1113/jphysiol.2008.157289