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Visual evoked potentials findings in non-affected subjects from a large Brazilian pedigree of 11778 Leber's hereditary optic neuropathy

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Date
2010-10-01
Author
Sacai, Paula Yuri [UNIFESP]
Salomão, Solange Rios [UNIFESP]
Carelli, Valerio
Pereira, Josenilson Martins [UNIFESP]
Belfort, Rubens [UNIFESP]
Sadun, Alfredo Arrigo
Berezovsky, Adriana [UNIFESP]
Type
Artigo
ISSN
0012-4486
Is part of
Documenta Ophthalmologica
DOI
10.1007/s10633-010-9241-2
Metadata
Show full item record
Abstract
To investigate pattern-reversal visual evoked potentials (PRVEP) in asymptomatic maternally and non-maternally related members from a large Brazilian 11778/ND4 LHON pedigree. Transient PRVEP for check sizes 15' and 60' were recorded from asymptomatic mutation carriers and non-mutant descendants of affected/non-affected males, all with best-corrected visual acuity of 20/20. A control group of spouses (off-pedigree) was also included. Parameters of N75, P100 and N135 latencies (ms) and N75-P100 peak-to-peak amplitude (mu V) as well as temporal dispersion (latency of N135-latency of N75) were determined. Longitudinal testing was obtained in a subseries of carriers in three annual consecutive visits. We tested 48 asymptomatic mutation carriers, 19 descendants of affected males, 9 descendants of non-affected males and 27 off-pedigrees, all of the latter being non-mutant. All non-mutant male descendants did not differ from off-pedigree controls. Statistically prolonged P100 latencies were found in mutation carriers (P = 0.0143) when compared with off-pedigrees for check sizes 15', as well as significantly larger temporal dispersions for both check size 15' (P = 0.0012) and check size 60' (P = 0.0271). Serial testing in 15 mutation carriers disclosed prolonged P100 latencies and larger temporal dispersion that did not change over time. Subclinical PRVEP abnormalities were detected in this large group of asymptomatic carriers of the 11778/ND4 LHON mutation from the same family, confirming and extending previous psychophysical and structural findings of a selective involvement of the parvocellular pathway. PRVEP is a useful test to characterize and monitor visual dysfunction in this devastating disease.
Citation
Documenta Ophthalmologica. Dordrecht: Springer, v. 121, n. 2, p. 147-154, 2010.
Keywords
Leber hereditary optic neuropathy
Visual evoked potentials
Optic nerve
Mitochondrial disease
11778 mutation
Sponsorship
International Foundation for Optic Nerve Disease-IFOND
URI
http://repositorio.unifesp.br/handle/11600/32946
Collections
  • Em verificação - Geral [8401]

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