Electrophysiological correlates of selective attention: A lifespan comparison

<p>Abstract</p> <p>Background</p> <p>To study how event-related brain potentials (ERPs) and underlying cortical mechanisms of selective attention change from childhood to old age, we investigated lifespan age differences in ERPs during an auditory oddball task in four age groups including 24 younger children (9–10 years), 28 older children (11–12 years), 31 younger adults (18–25), and 28 older adults (63–74 years). In the Unattend condition, participants were asked to simply listen to the tones. In the Attend condition, participants were asked to count the deviant stimuli. Five primary ERP components (N1, P2, N2, P3 and N3) were extracted for deviant stimuli under Attend conditions for lifespan comparison. Furthermore, Mismatch Negativity (MMN) and Late Discriminative Negativity (LDN) were computed as difference waves between deviant and standard tones, whereas Early and Late Processing Negativity (EPN and LPN) were calculated as difference waves between tones processed under Attend and Unattend conditions. These four secondary ERP-derived measures were taken as indicators for change detection (MMN and LDN) and selective attention (EPN and LPN), respectively. To examine lifespan age differences, the derived difference-wave components for attended (MMN and LDN) and deviant (EPN and LPN) stimuli were specifically compared across the four age groups.</p> <p>Results</p> <p>Both primary and secondary ERP components showed age-related differences in peak amplitude, peak latency, and topological distribution. The P2 amplitude was higher in adults compared to children, whereas N2 showed the opposite effect. P3 peak amplitude was higher in older children and younger adults than in older adults. The amplitudes of N3, LDN, and LPN were higher in older children compared with both of the adult groups. In addition, both P3 and N3 peak latencies were significantly longer in older than in younger adults. Interestingly, in the young adult sample P3 peak amplitude correlated positively and P3 peak latency correlated negatively with performance in the Identical Picture test, a marker measure of fluid intelligence.</p> <p>Conclusion</p> <p>The present findings suggest that patterns of event-related brain potentials are highly malleable within individuals and undergo profound reorganization from childhood to adulthood and old age.</p

Anormalidades do potencial evocado visual por padrão reverso em pacientes com esclerose múltipla definida Pattern reversal visual evoked potential abnormalities in patients with defined multiple sclerosis

O potencial evocado visual por padrão reverso, obtido por padrões de 14' e 28', foi analisado retrospectivamente em 28 pacientes com diagnóstico de esclerose múltipla definida. Observamos respostas anormais em 27/28 (96,4%) pacientes, em 31/36 (86%) dos olhos considerados sintomáticos e em 16/20 (80%) dos ollhos assintomáticos. Classificando os achados em cada olho segundo as respostas obtidas aos dois estímulos, observamos uma possível relação entre essa classificação e a gravidade de comprometimento visual pela doença. Detectamos em alguns olhos anormalidades isoladas do N75 e também de P100 apenas à estimulação de 28'. Dessa forma, a técnica empregada foi considerada sensível e pôde definir inclusive comprometimento visual subclínico. Entretanto, não teve sensibilidade absoluta para detectar anormalidades em alguns olhos sintomáticos. O tipo de resposta aos estímulos empregados pode sugerir o grau de extensão de envolvimento do sistema visual pela doença. Os achados mostram ainda o envolvimento irregular e predominante das fibras mais centrais da visão pela esclerose múltipla, e sugerem processadores neurais distintos e paralelos para as respostas aos dois padrões utilizados.<br>The pattern reversal visual evoked potential with checks of 14' and 28' was restropectivelly studied in 28 patients with definite multiple sclerosis. We observed abnormal responses in 27/28 (96.4%) patients, in 31/36 (86%) of symptomatic eyes, and in 16/20 (80%) of asymptomatic eyes. When we classified the abnormalities in each eye according to the findings obtained with each check, there was a correlation between the pattern of abnormalities and the severity of visual involvement. Occasionally there were isolated abnormalities of N75 or only in P100 obtained with 28' checks. In conclusion the methodology applied was very sensible in detecting abnormalities in visual pathway. We could classify the findings in each eye and correlate them with the severity of visual involvement. The findings showed uneven distribution of lesions in visual pathway, affecting preferentially the central vision afferents