Reevaluation of Dystrophin Localization in the Mouse Retina

Wersinger, Eric; Bordais, Agnès; Schwab, Yannick; Sène, Abdoulaye; Bénard, Romain; Alunni, Violaine; Sahel, José‐Alain; Rendón, Álvaro; Roux, Michel J.

doi:10.1167/iovs.11-7519

Cited by 28 publications

(51 citation statements)

References 39 publications

(33 reference statements)

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“…We found ERG changes corresponding with the recently reported differential expression of Dp isoforms between retinal subnetworks in animal models, with Dp427 allied more with cone pathways and Dp260 with rods. 19 We recognise now that ERG b-wave amplitude mainly depends on depolarisation of on-bipolar cells, 40 rather than potassium channels on the Müller glial cells, 41 which are altered in the Dp71-null mouse models of DMD. This explains why ERGs reported in DMD patients differ from some previously predicted DMD mouse knockout models.…”

Section: Discussionmentioning

confidence: 87%

“…Dp427, Dp260 and Dp140 are located in photoreceptor terminals, whereas Dp71 is expressed in Müller glia cells. [16][17][18][19][20] Recently, Dp427, Dp260 and Dp140 expressions have been identified in inner retinal layer neurons as well; Dp427 was expressed proportionately more at cone than rod synapses, in bipolar cells and some amacrine cells. 19 Mutations downstream of exon 30, which affect Dp260 expression, are associated with an abnormal scotopic electroretinogram (ERG) waveform [21][22][23][24] and some impairment of red-green colour vision.…”

Section: Introductionmentioning

confidence: 99%

“…[16][17][18][19][20] Recently, Dp427, Dp260 and Dp140 expressions have been identified in inner retinal layer neurons as well; Dp427 was expressed proportionately more at cone than rod synapses, in bipolar cells and some amacrine cells. 19 Mutations downstream of exon 30, which affect Dp260 expression, are associated with an abnormal scotopic electroretinogram (ERG) waveform [21][22][23][24] and some impairment of red-green colour vision. 25 In light of the recent retinal expression studies, we sought to explore the clinical ERG as a potential biomarker of CNS dystrophin expression associated with different DMD genotypes and recorded ERGs to a wide range of flash strengths in a cohort of individuals with a range of mutations across the DMD gene.…”

Section: Introductionmentioning

confidence: 99%

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Ocular and neurodevelopmental features of Duchenne muscular dystrophy: a signature of dystrophin function in the central nervous system

Ricotti

Jägle²,

Theodorou

et al. 2015

Eur J Hum Genet

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Multiple isoforms of dystrophin (Dp427, Dp260, Dp140, Dp71) are expressed differentially in the central nervous system (CNS) including the retinal layers. Disruption of these protein products is responsible for cognitive dysfunction, electroretinogram (ERG) abnormalities and behavioural disorders in Duchenne muscular dystrophy (DMD). We studied the ocular characteristics and neuropsychiatric profile of 16 DMD boys. The ISCEV standard, full-field flash ERGs were assessed. Intellectual ability and behavioural disturbances were measured. All genotypes were associated with mildly abnormal photopic ERG a:b-wave amplitude ratios. In addition, we identified the following genotype/phenotype correlations: boys with mutations upstream of exon 30 (ie, isolated Dp427 altered expression) showed normal scotopic a:b ratios, abnormal photopic oscillatory potential OP2 and normal scotopic OP2. Conversely, all boys with DMD mutations downstream of exon 30 showed profoundly 'negative' scotopic ERGs (a:b ratios 41). In these patients, the involvement of Dp260 isoform resulted in the absence of slow rod pathway signalling in15 Hz scotopic flicker ERGs. These boys had abnormal scotopic OP2 and normal photopic OP2. Finally, children with mutations also affecting Dp71 were associated with more pronounced electronegative ERGs. When correlating ERGs to neurodevelopmental outcome, we found a positive correlation between negative scotopic ERGs and neurodevelopmental disturbances, and the most severe findings were in boys with Dp71 disruption. These findings suggest a strong association between DMD mutations affecting different DMD isoforms with characteristically abnormal scotopic ERGs and severe neurodevelopmental problems. The role of the ERG as a potential biomarker for dystrophin function in the CNS and response to novel genetic therapies warrants further exploration.

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Section: Discussionmentioning

confidence: 87%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Ocular and neurodevelopmental features of Duchenne muscular dystrophy: a signature of dystrophin function in the central nervous system

Ricotti

Jägle²,

Theodorou

et al. 2015

Eur J Hum Genet

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“…Besides Dp260, the predominant retinal gene products of dystrophin found in the outer plexiform layer (OPL), 3 the full protein Dp427, and shorter DMD gene products Dp140 and Dp71 are also found at various locations in the retina (reviewed in Ref. 4).…”

mentioning

confidence: 99%

Asymmetrical Functional Deficits of ON and OFF Retinal Processing in the mdx^3Cv Mouse Model of Duchenne Muscular Dystrophy

Tsai

Barboni

Nagy

et al. 2016

Invest. Ophthalmol. Vis. Sci.

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Citation: Tsai TI, Barboni MTS, Nagy BV, et al. Asymmetrical functional deficits of ON and OFF retinal processing in the mdx 3Cv mouse model of Duchenne muscular dystrophy. Invest Ophthalmol Vis Sci. 2016;57:5788-5798. DOI:10.1167/ iovs.16-19432 PURPOSE. The dystrophin mouse mutant mdx 3Cv exhibits scotopic electroretinograpic (ERG) abnormalities, which resemble clinical changes observed in Duchenne muscular dystrophy (DMD) patients. In the present study, ERGs obtained from mdx 3Cv and their wild-type littermates under scotopic, mesopic, and photopic conditions were analyzed to provide further insight on the affected retinal pathways, and to compare them with human data. METHODS.Electroretinograms of mdx 3Cv (n ¼ 9) and age-matched C57BL/6J mice (n ¼ 10) included the scotopic full-field flash (for outer retinal deficits in rod pathway), scotopic threshold response (for inner retinal integrity), photopic flash, sinusoidal flicker (for outer retinal deficits in cone pathway), mesopic rapid-on/-off sawtooth flicker, and photopic longduration flash measurements (for separate ON-/OFF-responses under different conditions). RESULTS.The mdx 3Cv mice exhibited diminished and delayed scotopic and photopic ERGs, particularly in their b-wave and oscillatory potentials. Interestingly, homologues to the a-and b-wave of the mesopic ON-response were affected in their peak/trough times but not in their amplitude, whereas changes to both features were uncovered for photopic ON-response and sinusoidal flicker. Mesopic and photopic OFF-components were within the norm.CONCLUSIONS. Abnormal scotopic and photopic flash ERGs were observed in mdx 3Cv , which corroborate with deficits that are likely restricted to the level of photoreceptor-to-bipolar cell transmission. Further overlaps between mdx 3Cv mice and DMD patients exist, including asymmetrical ON versus OFF ERG alterations under mesopic versus photopic vision. In mice, ON-pathway function is compromised, whereas the OFF-pathway is spared.Keywords: Duchenne muscular dystrophy, dystrophin, electrophysiology, mouse model D ystrophin is a 427-kDa protein (Dp427), in which nonsense mutations in its gene (dmd) can cause Duchenne muscular dystrophy (DMD), a lethal, X-linked recessive muscle degenerative disease that primarily affects male children. 1 Shorter gene products of the protein, also transcribed by dmd, are present in different tissues.2 The retina, for example, is a tissue where extensive expressions of the dystrophin proteins occur. Besides Dp260, the predominant retinal gene products of dystrophin found in the outer plexiform layer (OPL), 3 the full protein Dp427, and shorter DMD gene products Dp140 and Dp71 are also found at various locations in the retina (reviewed in Ref. 4).Mouse strains lacking single or multiple dystrophin gene products have provided different models to study the mechanisms underlying electroretinographic (ERG) abnormalities in DMD patients. 5 Varying degrees of retinal dysfunction are associated with different dmd mutations. 6 Dp71, for example...

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“…A Dp260 é mais expressa na CNE seguida da Dp140 e da Dp427. E o oposto ocorre na CNI que tem mais Dp427 expressa seguida das Dp140 e Dp260 (Wersinger et al, 2011). Estes resultados mostram que a distrofina não está restrita a retina externa, portanto pode afetar diferentes funções visuais.…”

Section: Distrofia Muscular De Duchenne (Dmd)unclassified

Avaliação das vias do sistema visual por eletrorretinograma e testes psicofísicos na Distrofia Muscular de Duchenne e na Diabetes Mellitus tipo 1

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Reevaluation of Dystrophin Localization in the Mouse Retina

Cited by 28 publications

References 39 publications

Ocular and neurodevelopmental features of Duchenne muscular dystrophy: a signature of dystrophin function in the central nervous system

Ocular and neurodevelopmental features of Duchenne muscular dystrophy: a signature of dystrophin function in the central nervous system

Asymmetrical Functional Deficits of ON and OFF Retinal Processing in the mdx^3Cv Mouse Model of Duchenne Muscular Dystrophy

Avaliação das vias do sistema visual por eletrorretinograma e testes psicofísicos na Distrofia Muscular de Duchenne e na Diabetes Mellitus tipo 1

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Reevaluation of Dystrophin Localization in the Mouse Retina

Cited by 28 publications

References 39 publications

Ocular and neurodevelopmental features of Duchenne muscular dystrophy: a signature of dystrophin function in the central nervous system

Ocular and neurodevelopmental features of Duchenne muscular dystrophy: a signature of dystrophin function in the central nervous system

Asymmetrical Functional Deficits of ON and OFF Retinal Processing in the mdx3Cv Mouse Model of Duchenne Muscular Dystrophy

Avaliação das vias do sistema visual por eletrorretinograma e testes psicofísicos na Distrofia Muscular de Duchenne e na Diabetes Mellitus tipo 1

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Asymmetrical Functional Deficits of ON and OFF Retinal Processing in the mdx^3Cv Mouse Model of Duchenne Muscular Dystrophy