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Study of memory deficit in Alzheimer’s disease by means of complexity analysis of fNIRS signal

DOI:10.1117/1.nph.5.1.011010 期刊:Neurophotonics 出版年份:2017 更新时间:2025-09-09 09:28:46
摘要: Working memory deficit is a signature of Alzheimer’s disease (AD). The free and cued selective reminding test (FCSRT) is a clinical test that quantifies memory deficit for AD diagnosis. However, the diagnostic accuracy of FCSRT may be increased by accompanying it with neuroimaging. Since the test requires doctor–patient interaction, brain monitoring is challenging. Functional near-infrared spectroscopy (fNIRS) could be suited for such a purpose because of the fNIRS flexibility. We investigated whether the complexity, based on sample entropy and multiscale entropy metrics, of the fNIRS signal during FCSRT was correlated with memory deficit in early AD. fNIRS signals were recorded over the prefrontal cortex of healthy and early AD participants. Group differences were tested through Wilcoxon–Mann–Whitney test (p < 0.05). At group level, we found significant differences for Brodmann areas 9 and 46. The results, although preliminary, demonstrate the feasibility of performing ecological studies on early AD with fNIRS. This approach may provide a potential neuroimaging-based method for diagnosis of early AD, viable at the doctor’s office level, improving test-based diagnosis. The increased entropy of the fNIRS signal in early AD suggests the opportunity for further research on the neurophysiological status in AD and its relevance for clinical symptoms.
作者: David Perpetuini,Roberta Bucco,Michele Zito,Arcangelo Merla
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Investigating the correlation between the complexity of fNIRS signals during FCSRT and memory deficit in early Alzheimer’s disease.

The study demonstrates the feasibility of using fNIRS and complexity analysis to discriminate between healthy individuals and AD patients during ecological protocols. Significant differences in entropy metrics were found in Brodmann areas 9 and 46 during the delayed free recall phase, suggesting dysregulation in neurological patterns in AD. This approach could support traditional clinical diagnosis of AD.

The study's limitations include a limited sample size and the restricted length of the fNIRS signal due to the test’s structure and ecological features. The short duration of the rest phase may have prevented the detection of differences during this period.

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