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The gene, ELOVL4, is mutated in Stargardt-like macular dystrophy, a juvenile onset disorder. ELOVL4 is homologous to a fatty acid elongase presumably involved in the biosynthesis of docosahexaenoic acid, DHA.1 Humans can synthesise DHA from precursors in small amounts, which may not be sufficient for normal retinal function if intake is minimal.2
A 15 year old girl with Stargardt-like macular dystrophy and a mutation in ELOVL4 was given a dietary supplement of DHA on two occasions. A 7 day dietary history, prior to starting DHA supplementation, estimated her daily intake of DHA as 20 mg, in a diet of 1602 kcal. Beginning in April 2001, she was supplemented with 20 mg/kg body weight per day of DHA in capsules (Martek BioSciences, Columbia, MD, USA). Her functional response was determined by a VF-14 questionnaire,3 visual acuity testing, multifocal electroretinography (mfERG), and plasma phospholipid analysis.4
At baseline, fundus photography showed minimal macular changes (fig 1); however, the mfERG revealed significant macular dysfunction. A full field ERG performed in March 2000 revealed a reduction of approximately 30–40% in rod and cone responses, with the predominant effect on the b-wave amplitude in comparison with normative data (DTL electrode, dilated pupils, recorded according to ISCEV standards). No anomaly of latency was observed in either the mfERG or full field ERG recordings.
Peripheral blood samples were taken in a non-fasting state at the beginning of the study. Her baseline plasma DHA level was at the low end of the median for a North American diet, 24 μg/ml; whereas her omega-6 arachidonic acid was 76 μg/ml. Her plasma DHA level increased after 2 months of supplementation to 86 μg/ml (fig 2). She reported progressive subjective improvement in vision on the VF-14 questionnaire. Analysis of the mfERG tracings revealed that an improvement had occurred in amplitudes from the foveal and parafoveal regions of the macula (fig 2). For this study, we accepted the group average response of rings 1–2 (0–5°), and rings 3–5 (5–25°), derived from a 63 hexagon stimulus (Veris, San Mateo, CA, USA), as simulating the foveal and parafoveal responses respectively. Visual acuity improved from 20/200 to 20/100 only in her left eye with the DHA supplementation.
Unfortunately, she lost interest in the study, became non-compliant despite our encouragement, and was lost to follow up from August 2001 to the end of March 2002. She returned after perceiving that her vision had declined since halting the DHA supplementation. Repeat plasma DHA testing confirmed that her plasma DHA had dropped to levels approaching those from the beginning of the study (35 μg/ml, fig 2). Supplementation was once again initiated. After 4 months (July 2002), she showed the same improvements in visual function both subjectively (VF-14 score) and objectively (mfERG amplitudes, fig 2), coincident with an increase in plasma DHA.
The patient’s visual acuity again improved only in the left eye from 20/200 to 20/100. Another full field ERG was conducted in July 2002 to compare with the diagnostic series from March 2000. The amplitudes of the photopic b-wave and the scotopic b-wave both improved by 30%, averaging both eyes. The scotopic mixed rod-cone response showed increased amplitude of the a-wave by 85%, and b-wave by 46%, when responses from both eyes were averaged. These results could not be explained by intervisit variability and suggest the effect of DHA supplementation occurs beyond the macula, over the entire retina.
The patient’s young age, low dietary intake of DHA, and a mutation in ELOVL4 may have particularly predisposed her to an early macular degeneration. A longer experience with DHA supplementation in young patients with Stargardt-like macular dystrophy could determine if DHA supplementation can alter the natural history.
The technical assistance of Peggy Kaminski, OMT, YK Goh, PhD, and Ezekiel Weis, MD, is gratefully acknowledged.
Grant support: MSI Foundation, Alberta, Canada; University of Alberta Hospitals Foundation, Olive Young Fund; Royal Alexandra Hospital Foundation; Canadian Institutes for Health Research (MH Fellowship support).
Ethics: The health research ethics board of the University of Alberta approved this study and written consent was obtained before participation in the study
Conflict of interest: There are no financial agreements between any of the authors and Martek Biosciences, Columbia, MD, USA
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