Mutations in C8orf37, Encoding a Ciliary Protein, are Associated with Autosomal-Recessive Retinal Dystrophies with Early Macular Involvement

Estrada-Cuzcano, Alejandro; Neveling, Kornelia; Kohl, Susanne; Banin, Eyal; Rotenstreich, Ygal; Sharon, Dror; Falik‐Zaccai, Tzipora C.; Hipp, Stephanie; Roepman, Ronald; Wissinger, Bernd; Letteboer, Stef J.F.; Mans, Dorus A.; Blokland, Ellen A.W.; Kwint, Michael; Gijsen, Sabine; Huet, Ramon A. C. van; Collin, Rob W.J.; Scheffer, Hans; Veltman, Joris A.; Zrenner, Eberhart; Hollander, Anneke I. den; Klevering, B. Jeroen; Cremers, Frans P.M.

doi:10.1016/j.ajhg.2011.11.015

Cited by 73 publications

(79 citation statements)

References 34 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Refer to Table S1 for further details. Novel uncharacterised proteins are still being discovered to play a role in such processes, such as C8orf37, a ciliary protein which is mutated in CORD and RP 232 and C2orf71, a ciliary protein mutated in RP in humans and progressive retinal atrophy in several breeds of dog. 233,234 While our understanding of primary cilia and specialized sensory cilia such as the photoreceptor has advanced greatly in the past two decades, there still remains much to discover.…”

Section: Future Perspectives and Challengesmentioning

confidence: 99%

The role of primary cilia in the development and disease of the retina

2013

View full text Add to dashboard Cite

Section: Future Perspectives and Challengesmentioning

confidence: 99%

The role of primary cilia in the development and disease of the retina

2013

View full text Add to dashboard Cite

“…1-3 CRD can manifest under a variety of inheritance models, though the autosomal recessive mode of inheritance is the most prevalent. To date, eight genes responsible for autosomal recessive CRD have been identified: ABCA4 (OMIM#601691), 4 ADAM9 (OMIM#602713), 5 C8orf37 (OMIM#614477), 6 CERKL (OMIM#608381), 7 EYS (OMIM#612424), 8 RPGRIP1 (OMIM#605446), 9 RAB28 (OMIM#612994) 10 and TULP1 (OMIM#602280). 11 However, the known variants do not account for all cases of CRD.…”

Section: Introductionmentioning

confidence: 99%

Homozygous missense variant in the human CNGA3 channel causes cone-rod dystrophy

et al. 2014

Self Cite

View full text Add to dashboard Cite

We assessed a large consanguineous Pakistani family (PKAB157) segregating early onset low vision problems. Funduscopic and electroretinographic evaluation of affected individuals revealed juvenile cone-rod dystrophy (CRD) with maculopathy. Other clinical symptoms included loss of color discrimination, photophobia and nystagmus. Whole-exome sequencing, segregation and haplotype analyses demonstrated that a transition variant (c.955T4C; p.(Cys319Arg)) in CNGA3 co-segregated with the CRD phenotype in family PKAB157. The ability of CNGA3 channel to influx calcium in response to agonist, when expressed either alone or together with the wild-type CNGB3 subunit in HEK293 cells, was completely abolished due to p.Cys319Arg variant. Western blotting and immunolocalization studies suggest that a decreased channel density in the HEK293 cell membrane due to impaired folding and/or trafficking of the CNGA3 protein is the main pathogenic effect of the p.Cys319Arg variant. Mutant alleles of the human cone photoreceptor cyclic nucleotide-gated channel (CNGA3) are frequently associated with achromatopsia. In rare cases, variants in CNGA3 are also associated with cone dystrophy, Leber's congenital amaurosis and oligo cone trichromacy. The identification of predicted p.(Cys319Arg) missense variant in CNGA3 expands the repertoire of the known genetic causes of CRD and phenotypic spectrum of CNGA3 alleles.

show abstract

“…Three of these genes initially have been associated with ACHM, a form of cone dysfunction that can develop into COD. Eighteen genes have been associated with ar CRD (ABCA4, 17 ADAM9, 18 C8orf37, 19 CDHR1, 20,21 CERKL, 22 CNGB3, 23 CRB1, 24 CRX, 24 EYS, 25 FSCN2, 26 GUCY2D, 27 KCNV2, 14 PDE6C, 23 POC1B, 28,29 PROM1, 30 RAB28, 31 RPE65, 24 RPGRIP1, 23 and TULP1 16 ). In both disorders, mutations in these genes explain disease in an estimated 21% (COD) and 25% (CRD) of patients.…”

mentioning

confidence: 99%