RPE65

Leber Congenital Amaurosis

Clinical Characteristics

Ocular Features:

Leber congenital amaurosis is a collective term applied to multiple recessively inherited conditions with early-onset retinal dystrophy causing infantile or early childhood blindness. There are no established diagnostic criteria. First signs are usually noted before the age of 6 months. These consist of a severe reduction in vision accompanied by nystagmus, abnormal pupillary responses, and photophobia. Ametropia in the form of hyperopia is common. Keratoconus (and keratoglobus) is frequently found in older children but it is uncertain if this is a primary abnormality or secondary to eye rubbing as the latter is commonly observed. Repeated pressure on the eye may also be responsible for the relative enophthalmos often seen in these patients. The ERG is reduced or absent early and permanently. Final visual acuity is seldom better than 20/400 and perhaps one-third of affected individuals have no light perception. Some individuals experience a period of vision improvement.

The retina usually has pigmentary changes but these are not diagnostic. Retinal vessels are generally attenuated. The RPE may have a finely granulated appearance or, in some cases, whitish dots, and even 'bone spicules'.

Systemic Features:

A variety of metabolic and physical abnormalities have been reported with LCA but many publications are from the pre-genomic era and the significance of such associations remains uncertain. Most extraocular signs result from delays in mental development but it is uncertain what role, if any, that visual deprivation plays. Perhaps 20% of patients are mentally retarded or have significant cognitive deficits.

Genetics

Leber congenital amaurosis is genetically heterogeneous with at least 18 known gene mutations associated with the phenotype. It is also clinically heterogeneous both within and among families and this is the major obstacle to the delineation of individual clinicogenetic entities. As more patients are genotyped, it is likely that more precise genotype-phenotype correlations will emerge. At the present time, however, it is not possible to use clinical findings alone to distinguish individual conditions.

Below are links to the genotypic and phenotypic features of the 19 known types of LCA. All cause disease in the homozygous or compound heterozygous state.

LCA type OMIM# Locus Gene Symbol

LCA 1 204000 7p13.1 GUCY2D

LCA 2 204100 1p31 RPE65**

LCA 3 604232 14q31.3 SPATA7

LCA 4 604393 17p13.1 AIPL1

LCA 5 604537 6q14.1 LCA5

LCA 6 613826 14q11 RPGRIP1

LCA 7 613829 19q13.1 CRX*

LCA 8 613835 1q31-q32 CRB1

LCA 9 608553 1p36 NMNAT1

LCA 10 611755 12q21 CEP290

LCA 11 613837 7q31.3-q332 IMPDH1

LCA 12 610612 1q32.3 RD3

LCA 13 612712 14q24.1 RDH12

LCA 14 613341 4q31 LRAT

LCA 15 613843 6p21-31 TULP1

LCA 16 614186 2q37 KCNJ13

LCA 17 615360 8q22.1 GDF6

LCA 18 608133 6p21.1 PRPH2***

It is likely that more mutant genes will be identified since these are found in only about half of patients studied in large series.

*(Heterozygous mutations in CRX may also cause a cone-rod dystrophy).

**(Mutations in RPE65 has been described as also causing retinitis pigmentosa (RP20; 613794) with choroidal involvement.)

***Mutations in PRPH2 (RDS) has also been reported to cause retinitis pigmentosa 7, choroidal dystrophy, and vitelliform macular dystrophy (179605) among others.

Mutations in the GUCY2D gene seem to be the most common being present in about 21% of LCA patients with CRB1 next at 10%.

Pedigree:

Autosomal recessive

Treatment

Treatment Options:

Until recently, no treatment was available for LCA. However, results from early clinical trials with adeno-associated virus vector mediated gene therapy for RPE65 mutations in LCA 2 show promise. Subretinal placement of recombinant adeno-virus carrying RPE65 complementary DNA results in both subjective and objective improvements in visual function. Patients generally report subjective improvement in light sensitivity and visual mobility. Some recovery of rod and cone photoreceptor function has been documented. Studies have also documented an improvement in visual acuity, size of visual field, pupillary responses, and in the amouunt of nystagmus. More than 230 patients have now been treated and improvements seem to be maintained for at least 3 or more years. However, we have also learned that along with the enzymatic dysfunction of RPE65 that disrupts the visual cycle, there is also degeneration of photoreceptors which continues after treatment and the long term prognosis remains guarded. Multiple phase I clinical trials have demonstrated the safety of this approach and phase III trials are now underway.

It is crucial for patients to be enrolled early in sensory stimulation programs to ensure optimum neural development. For patients with residual vision, low vision aids can be beneficial. Vocational and occupational therapy should be considered for appropriate patients.

References

Article Title:

Leber congenital amaurosis/early-onset severe retinal dystrophy: clinical features, molecular genetics and therapeutic interventions

Kumaran N, Moore AT, Weleber RG, Michaelides M. Leber congenital amaurosis/early-onset severe retinal dystrophy: clinical features, molecular genetics and therapeutic interventions. Br J Ophthalmol. 2017 Jul 8. pii: bjophthalmol-2016-309975. doi: 10.1136/bjophthalmol-2016-309975. [Epub ahead of print] Review.

PubMed ID:

28689169

Omics in Ophthalmology: Advances in Genomics and Precision

den Hollander AI. Omics in Ophthalmology: Advances in Genomics and Precision
Medicine for Leber Congenital Amaurosis and Age-Related Macular Degeneration.
Invest Ophthalmol Vis Sci. 2016 Mar 1;57(3):1378-87.

PubMed ID:

27010695

Autosomal-dominant Leber Congenital Amaurosis Caused by a Heterozygous CRX Mutation in a Father and Son

Arcot Sadagopan K, Battista R, Keep RB, Capasso JE, Levin AV. Autosomal-dominant Leber Congenital Amaurosis Caused by a Heterozygous CRX Mutation in a Father and Son. Ophthalmic Genet. 2013 Oct 4. [Epub ahead of print] PubMed PMID: 24093488.

PubMed ID:

24093488

Mutations in NMNAT1 cause Leber congenital amaurosis and identify a new disease

Koenekoop RK, Wang H, Majewski J, Wang X, Lopez I, Ren H, Chen Y, Li Y,
Fishman GA, Genead M, Schwartzentruber J, Solanki N, Traboulsi EI, Cheng J, Logan
CV, McKibbin M, Hayward BE, Parry DA, Johnson CA, Nageeb M; Finding of Rare
Disease Genes (FORGE) Canada Consortium, Poulter JA, Mohamed MD, Jafri H, Rashid
Y, Taylor GR, Keser V, Mardon G, Xu H, Inglehearn CF, Fu Q, Toomes C, Chen R.
Mutations in NMNAT1 cause Leber congenital amaurosis and identify a new disease
pathway for retinal degeneration. Nat Genet. 2012 Jul 29.

PubMed ID:

22842230

A dominant mutation in RPE65 identified by whole-exome sequencing causes retinitis pigmentosa with choroidal involvement

Bowne SJ, Humphries MM, Sullivan LS, Kenna PF, Tam LC, Kiang AS, Campbell M, Weinstock GM, Koboldt DC, Ding L, Fulton RS, Sodergren EJ, Allman D, Millington-Ward S, Palfi A, McKee A, Blanton SH, Slifer S, Konidari I, Farrar GJ, Daiger SP, Humphries P. A dominant mutation in RPE65 identified by whole-exome sequencing causes retinitis pigmentosa with choroidal involvement. Eur J Hum Genet. 2011 Oct;19(10):1074-81. Erratum in: Eur J Hum Genet. 2011 Oct;19(10):1109.

PubMed ID:

21654732

Treatment of leber congenital amaurosis due to RPE65 mutations by ocular subretinal injection of adeno-associated virus gene vector: short-term results of a phase I trial

Hauswirth WW, Aleman TS, Kaushal S, Cideciyan AV, Schwartz SB, Wang L, Conlon TJ, Boye SL, Flotte TR, Byrne BJ, Jacobson SG. Treatment of leber congenital amaurosis due to RPE65 mutations by ocular subretinal injection of adeno-associated virus gene vector: short-term results of a phase I trial. Hum Gene Ther. 2008 Oct;19(10):979-90.

PubMed ID:

18774912

Effect of gene therapy on visual function in Leber's congenital amaurosis

Bainbridge JW, Smith AJ, Barker SS, Robbie S, Henderson R, Balaggan K, Viswanathan A, Holder GE, Stockman A, Tyler N, Petersen-Jones S, Bhattacharya SS, Thrasher AJ, Fitzke FW, Carter BJ, Rubin GS, Moore AT, Ali RR. Effect of gene therapy on visual function in Leber's congenital amaurosis. N Engl J Med. 2008 May 22;358(21):2231-9.

PubMed ID:

18441371

Genotyping microarray (disease chip) for Leber congenital amaurosis: detection of modifier alleles

Zernant J, K?olm M, Dharmaraj S, den Hollander AI, Perrault I, Preising MN, Lorenz B, Kaplan J, Cremers FP, Maumenee I, Koenekoop RK, Allikmets R. Genotyping microarray (disease chip) for Leber congenital amaurosis: detection of modifier alleles. Invest Ophthalmol Vis Sci. 2005 Sep;46(9):3052-9.

PubMed ID:

16123401

Leber congenital amaurosis

Perrault I, Rozet JM, Gerber S, Ghazi I, Leowski C, Ducroq D, Souied E, Dufier JL, Munnich A, Kaplan J. Leber congenital amaurosis. Mol Genet Metab. 1999 Oct;68(2):200-8. Review.

PubMed ID:

10527670

Clinical phenotypes in carriers of Leber congenital amaurosis mutations

Galvin JA, Fishman GA, Stone EM, Koenekoop RK. Clinical phenotypes in carriers of Leber congenital amaurosis mutations. Ophthalmology. 2005 Feb;112(2):349-56. PubMed PMID: 15691574.

PubMed ID:

15691574

Recessive Mutations in KCNJ13, Encoding an Inwardly Rectifying Potassium Channel Subunit, Cause Leber Congenital Amaurosis

Sergouniotis PI, Davidson AE, Mackay DS, Li Z, Yang X, Plagnol V, Moore AT, Webster AR. Recessive Mutations in KCNJ13, Encoding an Inwardly Rectifying Potassium Channel Subunit, Cause Leber Congenital Amaurosis. Am J Hum Genet. 2011 Jul 15;89(1):183-90.

PubMed ID:

21763485

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