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Neuropsychology and magnetic resonance correlation in Parkinson´s disease mild cognitive impairment: Case-control study

L.F.R. Vasconcellos, M. Adachi, D. Greca, M. Cruz, A.L. Malak, H. Charchat-Fichman, J.S. Pereira (Rio de Janeiro, Brazil)

Meeting: 2016 International Congress

Abstract Number: 1347

Keywords: Cognitive dysfunction, Magnetic resonance imaging(MRI), Parkinsonism

Session Information

Date: Wednesday, June 22, 2016

Session Title: Cognitive disorders

Session Time: 12:00pm-1:30pm

Location: Exhibit Hall located in Hall B, Level 2

Objective: Evaluate the relationship between magnetic resonance (MRI) abnormalities and neuropsychological assessment in Parkinson s disease mild cognitive impairment (PD-MCI) and controls with mild cognitive impairment (CO-MCI).

Background: The recognition and treatment of cognitive impairment are increasingly emphasized in the care of PD. PD-MCI is one of the most important risk factor related to dementia. Global Cerebral Atrophy (CGA), Medial Temporal Atrophy (MTA) and white matter hyperintensities could be found more frequently in Parkinson s disease dementia. We evaluated if these structural changes could be related with neuropsychological pattern of PD-MCI comparing with CO-MCI.

Methods: 75 PD and 88 controls (CO) were evaluated, 50 PD and 61 CO were excluded because didn t have MRI scan, presented one or more findings that could be related to cognitive impairment (use of benzodiazepine or anticholinergic, MRI or blood abnormalities) or fulfilled criteria for dementia or depression. The assessment consists of: neurology examination, Hoehn-Yahr, UPDRS, PDQ 39, Schwab-England, Beck scale, L-dopa dose, neuropsychological battery, Global Cerebral Atrophy (GCA), medial temporal atrophy (MTA), Evans Index, and Fazekas scale (FS).

Results: Both groups were classified by neuropsychological assessment in amnestic or non- amnestic. No differences were observed on several demographic data.

Sample characteristics
Variables DP Amnestic MCI n=13 mean (sd) DP Nonamnestic MCI n=12 mean (sd) Control Amnestic MCI n=18 mean (sd) Control Nonamnestic MCI n=9 mean (sd) p-value
Age (years) 60.23 (7.132) 58.92 (6.908) 60.72 (6.323) 60.89 (6,451) 0.781 (a)
Education Level (years) 9.23 (4.126) 10.25 (2.864) 12.72 (3.893) 13.22 (4.147) 0.031(a)
Sex % (male / female) 53.8 / 46.2 83.3 / 16.7 27.8 / 72.2 11.1 / 88.9  
MMSE 27.31 (1.601) 27.83 (1.337) 27.89 (1.278) 27.89 (1.269) 0.651(a)
MoCA 23.00 (2.915) 24.00 (3.191) 22.94 (2.754) 23.89 (3.180) 0.710(a)
BDI 8.38 (5.591) 5.33 (4.438) 7.50 (5.159) 8.22 (3.232) 0.404(a)
Years since diagnosis (months) 64.62 (31.574) 68.00 (37.717) – – 0.809(b)
Levodopa dosage equivalence (Mg) 636.31 (292.665) 1783.75 (4060.456) – – 0.350(b)
UPDRS-III 18.54 (9.421) 15.92 (5.791) – – 0.088(b)
PDQ39 (total) 28.50 (14.112) 19.55 (10.914) – – 0.408(b)
Schwab-England 83.08 (7.511) 88.33 (3.892) – – 0.039(b)
Cerebrovascular risk factor % 38.5 25.0 38.9 66.7  
Smoking % (sim / não) 38.5 / 61.5 83.3 / 16.7 5.6 / 94.4 11.1 / 88.9  
Global Cerebral Atrophy % (score 0/1/2/3) 46.2 / 46.2 / 7.7/0.0 50.0 / 50.0 / 0.0/0.0 33.3 / 44.4 / 5.6/0.0 55.6 / 44.4 / 0.0/0.0  
MTA % (score 0/1/2/3/4) 46.2 / 46.2 / 7.7/0.0/0.0 58.3 / 41.7 / 0.0/0.0/0.0 61.1 / 33.3 / 5.6/0.0/0.0 55.6 / 44.4 / 0.0/0.0/0.0  
FAZEKAS % (score 0/1/2/3) 38.5 / 46.2 / 7.7 / 7.7 58.3 / 25.0 / 8.3 / 8.3 38.9 / 38.9 / 11.1 / 55.6 11.1 / 55.6 / 33.3 / 0.0  
(a) One-way ANOVA; (b) t-test
” PD-MCI amnestic group presented worse results on memory and executive function followed by PD-MCI non amnestic.

Performance of Patients and Controls in the Neuropsychological Tests (raw scores)
Neuropsychological Tests DP Amnestic MCI n=13 mean (sd) DP Nonamnestic MCI n=12 mean (sd) p-value (a) Control Amnestic MCI n=18 mean (sd) Control Nonamnestic MCI n=9 mean (sd) p-value(a) PS
MI(b;1) 5.08 (1.038) 6.50 (1.508) 0.013 5.33 (1.188) 5.78 (1.202) 0.377 Storage of information that occurs passively (i.e., without conscious effort). MEMORY
M1(b;2) 6.92 (1.320) 8.25 (1.055) 0.011 8.11 (1.023) 8.78 (1.302) 0.202 Visual short-term memory MEMORY
M2(b;3) 8.92 (0.862) 9.25 (0.754) 0,323 8.56 (1.542) 9.67 (0.500) 0.011 Visual learning MEMORY
M5(b;4) 7.00 (2.345) 8.75 (0.754) 0.022 8.39 (1.243) 8.89 (1.054) 0.288 Visual long-term memory MEMORY
A6(c;6) 3.85 (2.410) 8.75 (2.491) < 0.001 7.22 (3.135) 9.78 (3.153) 0.064 Verbal memory MEMORY
A7(c;7) 4.00 (2.121) 9.25 (2.417) < 0.001 7.00 (3.881) 10.56 (3.005) 0.016 Verbal long-term memory MEMORY
LOT(c;8) 11.54 (5.487) 21.33 (7.228) 0.001 17.67 (8.260) 20.33 (6.124) 0.355 Verbal learning MEMORY
RI(c;9) 0.49 (0.275) 0.76 (0.203) 0.010 0,75 (0.286) 0.83 (0.132) 0.343 Interference MEMORY and EXECUTIVE FUNCTIONS
Recognition(c;10) 4.62 (4.053) 11.08 (2.811) < 0.001 6.28 (4.417) 12.33 (2.646) < 0.001 Recognition memory MEMORY
TMT A(d) 71.83 (18.914) 68.06 (18.895) 0.641 53.39 (17.431) 40.13 (9.040) 0.017 Processing Speed EXECUTIVE FUNCTIONS
FAS(f) 25.62 (6.449) 35.08 (8.458) 0.005 31.83 (7.710) 33.22 (5.191) 0.585 Phonemic verbal fluency EXECUTIVE FUNCTIONS
(a)t-Test; (b)Figures Memory Test – Nitrini (1994); (1)MI = incidental memory; (2)M1= number of figures recalled after 1-minute visualization;(3)M2= Learning; (4)M5= recall of memorized figures after 5 minutes; (c)Rey Auditory Verbal Learning Test – Malloy-Diniz (2007); (5)B1=retrieval of words included in the interference list of 15 new substantives; (6)A6= number of words memorized from list A without reread; (7)A7 = number of words memorized from list A, without reread, after 20-minute interval; (8)LOT=leaning curve of the wordsduring attempts A1 to A5; (9)RI= Retroactive Interference (A6/A5); (10)correct answers in recognitive list; (d)TMT A = trail making test – trail A (time in seconds); (e)FVS=semantic verbal fluency (animals); (f)FAS=phonemic verbal fluency (letters F, A and S)
” More severe motor impairment (UPDRS) presented worse scores in attention and memory. MRI variables: GCA correlates with executive function (EF) in PD amnestic & non amnestic, MTA with EF & memory (Me) in PD amnestic & CO amnestic, Fazekas with EF, Me & attention (AT) in PD amnestic & PD non amnestic, Evans Index with Me in all four groups, AT in PD amnestic & Language in PD non amnestic.

Conclusions: Structural abnormalities in MRI were more common in PD-MCI than MCI-CO. PD group presented more prominent impairment than control. MRI could be more useful in PD-MCI than MCI-CO and could reflect irreversible structural changes beyond basal ganglia in PD. Burton EJ, McKeith IG, Burn DJ et al. Cerebral atrophy in Parkinson s disease with and without dementia. Brain. 2004;127:791-800. Yarnall AJ, Rochester L, Burn DJ. Mild cognitive impairment in Parkinson s disease. Age Ageing. 2013;42(5):567-76.

To cite this abstract in AMA style:

L.F.R. Vasconcellos, M. Adachi, D. Greca, M. Cruz, A.L. Malak, H. Charchat-Fichman, J.S. Pereira. Neuropsychology and magnetic resonance correlation in Parkinson´s disease mild cognitive impairment: Case-control study [abstract]. Mov Disord. 2016; 31 (suppl 2). https://www.mdsabstracts.org/abstract/neuropsychology-and-magnetic-resonance-correlation-in-parkinsons-disease-mild-cognitive-impairment-case-control-study/. Accessed May 11, 2025.
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