Mutations in a new photoreceptor-pineal gene on 17p cause Leber congenital amaurosis

Melanie M. Sohocki; Sara J. Bowne; Lori S. Sullivan; Seth Blackshaw; Constance L. Cepko; Annette M. Payne; Shomi S. Bhattacharya; Shagufta Khaliq; S. Qasim Mehdi; David G. Birch; Wilbur R. Harrison; Frederick F.B. Elder; John R. Heckenlively; Stephen P. Daiger

doi:10.1038/71732

Mutations in a new photoreceptor-pineal gene on 17p cause Leber congenital amaurosis

Melanie M. Sohocki, Sara J. Bowne, Lori S. Sullivan, Seth Blackshaw, Constance L. Cepko, Annette M. Payne, Shomi S. Bhattacharya, Shagufta Khaliq, S. Qasim Mehdi, David G. Birch, Wilbur R. Harrison, Frederick F.B. Elder, John R. Heckenlively, Stephen P. Daiger

Research output: Contribution to journal › Article › peer-review

223 Scopus citations

Abstract

Leber congenital amaurosis (LCA, MIM 204000) accounts for at least 5% of all inherited retinal disease and is the most severe inherited retinopathy with the earliest age of onset. Individuals affected with LCA are diagnosed at birth or in the first few months of life with severely impaired vision or blindness, nystagmus and an abnormal or flat electroretinogram (ERG). Mutations in GUCY2D fief. 3), RPE65 (ref. 4) and CRX (ref. 5) are known to cause LCA, but one study identified disease-causing GUCY2D mutations in only 8 of 15 families whose LCA locus maps to 17p13.1 (ref. 3), suggesting another LCA locus might be located on 17p13.1. Confirming this prediction, the LCA in one Pakistani family mapped to 17p13.1, between D17S849 and D17S960 - a region that excludes GUCY2D. The LCA in this family has been designated LCA4 (ref. 6). We describe here a new photoreceptor/pineal-expressed gene, AIPL1 (encoding aryl-hydrocarbon interacting protein-like 1), that maps within the LCA4 candidate region and whose protein contains three tetratricopeptide (TPR) motifs, consistent with nuclear transport or chaperone activity. A homozygous nonsense mutation at codon 278 is present in all affected members of the original LCA4 family. AIPL1 mutations may cause approximately 20% of recessive LCA, as disease-causing mutations were identified in 3 of 14 LCA families not tested previously for linkage.

Original language	English (US)
Pages (from-to)	79-83
Number of pages	5
Journal	Nature genetics
Volume	24
Issue number	1
DOIs	https://doi.org/10.1038/71732
State	Published - 2000
Externally published	Yes

ASJC Scopus subject areas

Genetics

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Sohocki, M. M., Bowne, S. J., Sullivan, L. S., Blackshaw, S., Cepko, C. L., Payne, A. M., Bhattacharya, S. S., Khaliq, S., Mehdi, S. Q., Birch, D. G., Harrison, W. R., Elder, F. F. B., Heckenlively, J. R., & Daiger, S. P. (2000). Mutations in a new photoreceptor-pineal gene on 17p cause Leber congenital amaurosis. Nature genetics, 24(1), 79-83. https://doi.org/10.1038/71732

@article{28b7606e39e041809d1f0338c2c868f5,

title = "Mutations in a new photoreceptor-pineal gene on 17p cause Leber congenital amaurosis",

abstract = "Leber congenital amaurosis (LCA, MIM 204000) accounts for at least 5% of all inherited retinal disease and is the most severe inherited retinopathy with the earliest age of onset. Individuals affected with LCA are diagnosed at birth or in the first few months of life with severely impaired vision or blindness, nystagmus and an abnormal or flat electroretinogram (ERG). Mutations in GUCY2D fief. 3), RPE65 (ref. 4) and CRX (ref. 5) are known to cause LCA, but one study identified disease-causing GUCY2D mutations in only 8 of 15 families whose LCA locus maps to 17p13.1 (ref. 3), suggesting another LCA locus might be located on 17p13.1. Confirming this prediction, the LCA in one Pakistani family mapped to 17p13.1, between D17S849 and D17S960 - a region that excludes GUCY2D. The LCA in this family has been designated LCA4 (ref. 6). We describe here a new photoreceptor/pineal-expressed gene, AIPL1 (encoding aryl-hydrocarbon interacting protein-like 1), that maps within the LCA4 candidate region and whose protein contains three tetratricopeptide (TPR) motifs, consistent with nuclear transport or chaperone activity. A homozygous nonsense mutation at codon 278 is present in all affected members of the original LCA4 family. AIPL1 mutations may cause approximately 20% of recessive LCA, as disease-causing mutations were identified in 3 of 14 LCA families not tested previously for linkage.",

author = "Sohocki, {Melanie M.} and Bowne, {Sara J.} and Sullivan, {Lori S.} and Seth Blackshaw and Cepko, {Constance L.} and Payne, {Annette M.} and Bhattacharya, {Shomi S.} and Shagufta Khaliq and Mehdi, {S. Qasim} and Birch, {David G.} and Harrison, {Wilbur R.} and Elder, {Frederick F.B.} and Heckenlively, {John R.} and Daiger, {Stephen P.}",

note = "Funding Information: We thank the LCA families for participation; O.L. June, C. Inglehearn, J. McHale and D. Hughbanks-Wheaton for expert assistance; and R. McInnes and D. Ing for providing the retinal northern blot. Supported by grants from the Foundation Fighting Blindness and the George Gund Foundation, the William Stamps Farish Fund, the M.D. Anderson Foundation, the John S. Dunn Research Foundation and by grant EY07142 from the National Eye Institute-National Institutes of Health (M.M.S., S.J.B., L.S.S. and S.P.D.) S.S.B. acknowledges support of the Medical Research Council (grant ref: G9301094) and the Wellcome Trust (grant ref: 049571/Z/96/Z) for research funding.",

year = "2000",

doi = "10.1038/71732",

language = "English (US)",

volume = "24",

pages = "79--83",

journal = "Nature genetics",

issn = "1061-4036",

publisher = "Nature Publishing Group",

number = "1",

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TY - JOUR

T1 - Mutations in a new photoreceptor-pineal gene on 17p cause Leber congenital amaurosis

AU - Sohocki, Melanie M.

AU - Bowne, Sara J.

AU - Sullivan, Lori S.

AU - Blackshaw, Seth

AU - Cepko, Constance L.

AU - Payne, Annette M.

AU - Bhattacharya, Shomi S.

AU - Khaliq, Shagufta

AU - Mehdi, S. Qasim

AU - Birch, David G.

AU - Harrison, Wilbur R.

AU - Elder, Frederick F.B.

AU - Heckenlively, John R.

AU - Daiger, Stephen P.

N1 - Funding Information: We thank the LCA families for participation; O.L. June, C. Inglehearn, J. McHale and D. Hughbanks-Wheaton for expert assistance; and R. McInnes and D. Ing for providing the retinal northern blot. Supported by grants from the Foundation Fighting Blindness and the George Gund Foundation, the William Stamps Farish Fund, the M.D. Anderson Foundation, the John S. Dunn Research Foundation and by grant EY07142 from the National Eye Institute-National Institutes of Health (M.M.S., S.J.B., L.S.S. and S.P.D.) S.S.B. acknowledges support of the Medical Research Council (grant ref: G9301094) and the Wellcome Trust (grant ref: 049571/Z/96/Z) for research funding.

PY - 2000

Y1 - 2000

N2 - Leber congenital amaurosis (LCA, MIM 204000) accounts for at least 5% of all inherited retinal disease and is the most severe inherited retinopathy with the earliest age of onset. Individuals affected with LCA are diagnosed at birth or in the first few months of life with severely impaired vision or blindness, nystagmus and an abnormal or flat electroretinogram (ERG). Mutations in GUCY2D fief. 3), RPE65 (ref. 4) and CRX (ref. 5) are known to cause LCA, but one study identified disease-causing GUCY2D mutations in only 8 of 15 families whose LCA locus maps to 17p13.1 (ref. 3), suggesting another LCA locus might be located on 17p13.1. Confirming this prediction, the LCA in one Pakistani family mapped to 17p13.1, between D17S849 and D17S960 - a region that excludes GUCY2D. The LCA in this family has been designated LCA4 (ref. 6). We describe here a new photoreceptor/pineal-expressed gene, AIPL1 (encoding aryl-hydrocarbon interacting protein-like 1), that maps within the LCA4 candidate region and whose protein contains three tetratricopeptide (TPR) motifs, consistent with nuclear transport or chaperone activity. A homozygous nonsense mutation at codon 278 is present in all affected members of the original LCA4 family. AIPL1 mutations may cause approximately 20% of recessive LCA, as disease-causing mutations were identified in 3 of 14 LCA families not tested previously for linkage.

AB - Leber congenital amaurosis (LCA, MIM 204000) accounts for at least 5% of all inherited retinal disease and is the most severe inherited retinopathy with the earliest age of onset. Individuals affected with LCA are diagnosed at birth or in the first few months of life with severely impaired vision or blindness, nystagmus and an abnormal or flat electroretinogram (ERG). Mutations in GUCY2D fief. 3), RPE65 (ref. 4) and CRX (ref. 5) are known to cause LCA, but one study identified disease-causing GUCY2D mutations in only 8 of 15 families whose LCA locus maps to 17p13.1 (ref. 3), suggesting another LCA locus might be located on 17p13.1. Confirming this prediction, the LCA in one Pakistani family mapped to 17p13.1, between D17S849 and D17S960 - a region that excludes GUCY2D. The LCA in this family has been designated LCA4 (ref. 6). We describe here a new photoreceptor/pineal-expressed gene, AIPL1 (encoding aryl-hydrocarbon interacting protein-like 1), that maps within the LCA4 candidate region and whose protein contains three tetratricopeptide (TPR) motifs, consistent with nuclear transport or chaperone activity. A homozygous nonsense mutation at codon 278 is present in all affected members of the original LCA4 family. AIPL1 mutations may cause approximately 20% of recessive LCA, as disease-causing mutations were identified in 3 of 14 LCA families not tested previously for linkage.

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Mutations in a new photoreceptor-pineal gene on 17p cause Leber congenital amaurosis

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