Literature DB >> 23572034

Temporal macular thinning associated with X-linked Alport syndrome.

Faisal Ahmed1, Kandon K Kamae, Denise J Jones, Margaret M Deangelis, Gregory S Hageman, Martin C Gregory, Paul S Bernstein.   

Abstract

IMPORTANCE: Optical coherence tomography (OCT) findings of temporal macular thinning are important in the diagnosis and prognosis of X-linked Alport syndrome (XLAS).
OBJECTIVES: To report OCT findings and severity of temporal macular thinning in a cohort with XLAS and to correlate these and other ocular findings with mutation genotype.
DESIGN: Patients with XLAS underwent genotyping for COL4A5 mutations and complete eye examinations with retinal imaging using spectral domain OCT and fundus photography. Temporal macular thinning was calculated from OCT measurements by comparing the ratio of the retinal thickness of the temporal to the nasal subfields with a published normative database.
SETTING: University departments of ophthalmology and nephrology. PARTICIPANTS: Thirty-two patients from 24 families. MAIN OUTCOME AND MEASURES: Temporal thinning index calculated from spectral domain OCT scans.
RESULTS: All study patients had a mutation associated with the X-linked COL4A5 gene. Eleven different mutations were identified. Eleven of 32 patients (34%) expressed the L1649R mutation. Of a total of 63 eyes with available OCT scans, 44 (70%) had severe pathological temporal macular thinning. The L1649R mutation was associated with the least amount of severe temporal macular thinning and later onset of renal failure. CONCLUSIONS AND RELEVANCE: Temporal macular thinning is a prominent sign associated with XLAS, suggesting that OCT measurements are essential in the diagnosis and prognosis of the disease. The L1649R mutation in the COL4A5 gene causes a relatively mild form of XLAS characterized by late-onset renal failure and less frequent, severe temporal macular thinning relative to other COL4A5 mutations. The pathological basis for the retinal abnormalities of XLAS remains to be established.

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Year:  2013        PMID: 23572034      PMCID: PMC3746023          DOI: 10.1001/jamaophthalmol.2013.1452

Source DB:  PubMed          Journal:  JAMA Ophthalmol        ISSN: 2168-6165            Impact factor:   7.389


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