Addenbrooke’s cognitive examination III: diagnostic utility for detecting mild cognitive impairment and dementia in Parkinson’s disease

Sousa, Nariana Mattos Figueiredo; Brucki, Sonia Maria Dozzi

doi:10.1055/s-0042-1758448

Abstract

Background

Cognitive deficit in Parkinson disease (PD) is an important cause of functional disability in these patients and early detection, with sensitive instruments, can contribute to longitudinal monitoring.

Objective

To investigate the diagnostic accuracy, sensitivity, and specificity of the Addenbrooke’s Cognitive Examination-III in patients with PD, using the comprehensive neuropsychological battery as reference method.

Methods

Cross-sectional, observational, case-control study. Setting: rehabilitation service. A total of 150 patients and 60 healthy controls matched for age, sex, and education. For level I assessment, Addenbrooke Cognitive Examination (ACE-III) was used. Level II assessment used a comprehensive neuropsychological battery of standardized tests for this population. All patients remained in on-state during the study. The diagnostic accuracy of the battery was investigated through the receiver operating characteristic (ROC) analysis.

Results

The clinical group was divided into 3 subgroups: normal cognition in Parkinson’s disease (NC-PD-16%), mild cognitive impairment due to Parkinson’s disease (MCI-PD-69.33%), and dementia due to Parkinson’s disease (D-PD-14.66%). ACE-III optimal cutoff scores for detecting MCI-PD and D-PD were 85/100 (sensitivity 58.65%, specificity 60%) and 81/100 points (sensitivity 77.27%, specificity 78.33%), respectively. Age was inversely associated with the performance of the scores (totals and domains of the ACE-III), while the level of education had a significantly positive correlation in the performance of these scores.

Conclusions

ACE-III is a useful battery for assessing the cognitive domains and to differentiate individuals with MCI-PD and D-PD from healthy controls. Future research, in a community setting, is necessary to provide discriminatory capacity of ACE-III in the different severities of dementia.

Keywords:
Parkinson Disease; Cognitive Dysfunction; Dementia; Neuropsychological Tests

Resumo

Antecedentes

O déficit cognitivo na doença de Parkinson (DP) é uma importante causa de incapacidade funcional nestes pacientes e a detecção precoce, com instrumentos sensíveis, pode contribuir para o acompanhamento longitudinal.

Objetivo

Investigar a acurácia diagnóstica, sensibilidade e especificidade do Exame Cognitivo de Addenbrooke-II em pacientes com DP, usando uma bateria neuropsicológica ampla como método de referência.

Métodos

Estudo transversal, observacional, caso-controle. Local: serviço de reabilitação. Um total de 150 pacientes e 60 controles saudáveis pareados por idade, sexo e escolaridade. Para avaliação do nível I, foi utilizada a Addenbrooke Cognitive Examination (ACE-III). A avaliação do nível II utilizou o exame neuropsicológico, com testes padronizados para esta população. Todos os pacientes estavam na fase “on” da medicação. A acurácia diagnóstica da bateria foi investigada por meio da análise do receiver operating characteristic (ROC, na sigla em inglês).

Resultados

O grupo clínico foi dividido em 3 subgrupos: cognição normal na DP (CN-DP-16%), comprometimento cognitivo leve devido à DP (CCL-DP-69,33%) e demência devido à DP (D-DP-14,66%). As notas de corte ideais da ACE-III para detectar CCL-DP e D-DP foram 85/100 (sensibilidade 58,65%, especificidade 60%) e 81/100 pontos (sensibilidade 77,27%, especificidade 78,33%), respectivamente. A idade associou-se inversamente com o desempenho dos escores (totais e domínios da ACE-III), enquanto a faixa de escolaridade apresentou correlação significativamente positiva no desempenho destes escores.

Conclusões

A ACE-III é uma bateria útil para avaliação de domínios cognitivos e diferenciar indivíduos com CCL-DP e D-DP de controles saudáveis. Pesquisas futuras, em ambiente comunitário, são necessárias para fornecer capacidade discriminatória da ACE-III nos diferentes estágios da demência.

Palavras-chave:
Doença de Parkinson; Disfunção Cognitiva; Demência; Testes Neuropsicológicos

INTRODUCTION

Parkinson disease (PD) is a progressive neurodegenerative condition initially described as a movement disorder, characterized by symptoms such as tremor, stiffness, bradykinesia, and postural instability.¹1 Lees AJ, Hardy J, Revesz T. Parkinson’s disease. Lancet 2009;373 (9680):2055-2066. Doi: 10.1016/S0140-6736(09)60492-X
https://doi.org/10.1016/S0140-6736(09)60... Since the initial stages of the disease, ~ 20 to 30% of patients have some cognitive impairment,²2 Emre M, Aarsland D, Brown R, et al. Clinical diagnostic criteria for dementia associated with Parkinson’s disease. Mov Disord 2007; 22(12):1689-1707, quiz 1837. Doi: 10.1002/mds.21507
https://doi.org/10.1002/mds.21507... which is an important cause of functional disability in these patients.³3 Cerasa A, Gioia MC, Salsone M, et al. Neurofunctional correlates of attention rehabilitation in Parkinson’s disease: an explorative study. Neurol Sci 2014;35(08):1173-1180. Doi: 10.1007/s10072-014-1666-z
https://doi.org/10.1007/s10072-014-1666-... ,⁴4 Kulisevsky J, Pagonabarraga J. Cognitive impairment in Parkinson’s disease: tools for diagnosis and assessment. Mov Disord 2009;24(08):1103-1110. Doi: 10.1002/mds.22506
https://doi.org/10.1002/mds.22506...

Part of these cognitive alterations is attributed to a dopamine-dependent dysfunction of the frontostriatal pathways, but there is considerable heterogeneity, as well as the influence of other neurotransmitter systems, including the cholinergic one, which is responsible for the dementia syndrome in PD.⁵5 Papagno C, Trojano L. Cognitive and behavioral disorders in Parkinson’s disease: an update. I: cognitive impairments. Neurol Sci 2018;39(02):215-223. Doi: 10.1007/s10072-017-3154-8
https://doi.org/10.1007/s10072-017-3154-...

In mild cognitive impairment (MCI), the patient may complain of difficulties in complex activities with relative preservation of functionality.⁶6 Portet F, Gabelle A, Touchon J. [Parkinson’s disease dementia and Lewy body dementia]. Psychol Neuropsychiatr Vieil 2006;4(Spec No 1):S35-S50 Despite being referred to as a single and nonamnestic domain, the criteria for this diagnosis are not well established in the literature, with controversies regarding the definition and characteristics of mild cognitive impairment in PD (MCI-PD), due to the methodological diversity among studies.⁶6 Portet F, Gabelle A, Touchon J. [Parkinson’s disease dementia and Lewy body dementia]. Psychol Neuropsychiatr Vieil 2006;4(Spec No 1):S35-S50,⁷7 Tedrus GMAS, Fonseca LC, Letro GH, Bossoni AS, Adriana Bastos S. Dementia and mild cognitive impairment in Parkinson’s disease. Arq Neuropsiquiatr 2009;67(04):1164,⁸8 Tedrus GMAS, Fonseca LC, Letro GH, Bossoni AS, Samara AB. Dementia and mild cognitive impairment in patients with Parkinson’s disease. Arq Neuropsiquiatr. 2009;67(2 B):423-427. Doi: 10.1590/S0004-282X2009000300010
https://doi.org/10.1590/S0004-282X200900...

Dementia in Parkinson’s disease (D-PD) is the most serious manifestation. This condition affects ~ 24 to 31% of patients, increases death risk, and leads to a reduction in the quality of life of patients and caregivers, besides causing an increase in institutionalization and in costs.⁹9 Janvin CC, Larsen JP, Aarsland D, Hugdahl K. Subtypes of mild cognitive impairment in Parkinson’s disease: progression to dementia. Mov Disord 2006;21(09):1343-1349. Doi: 10.1002/mds.20974
https://doi.org/10.1002/mds.20974... ,¹⁰10 Williams-Gray CH, Evans JR, Goris A, et al. The distinct cognitive syndromes of Parkinson’s disease: 5 year follow-up of the CamPaIGN cohort. Brain 2009;132(Pt 11):2958-2969. Doi: 10.1093/brain/awp245
https://doi.org/10.1093/brain/awp245...

Many different instruments can be used to evaluate cognition in PD. The Mini-Mental State Examination (MMSE) was proposed as a screening tool in PD patients¹¹11 Dubois B, Burn D, Goetz C, et al. Diagnostic procedures for Parkinson’s disease dementia: recommendations from the movement disorder society task force. Mov Disord 2007;22(16):2314-2324. Doi: 10.1002/mds.21844
https://doi.org/10.1002/mds.21844... ,¹²12 Folstein MF, Folstein SE, McHugh PR. “Mini-mental state”. A practical method for grading the cognitive state of patients for the clinician. J Psychiatr Res 1975;12(03):189-198. Doi: 10.1016/0022-3956(75)90026-6
https://doi.org/10.1016/0022-3956(75)900... for its simplicity and wide use in dementias. However, early cognitive changes in executive functions are not detected using the MMSE.¹¹11 Dubois B, Burn D, Goetz C, et al. Diagnostic procedures for Parkinson’s disease dementia: recommendations from the movement disorder society task force. Mov Disord 2007;22(16):2314-2324. Doi: 10.1002/mds.21844
https://doi.org/10.1002/mds.21844... ,¹²12 Folstein MF, Folstein SE, McHugh PR. “Mini-mental state”. A practical method for grading the cognitive state of patients for the clinician. J Psychiatr Res 1975;12(03):189-198. Doi: 10.1016/0022-3956(75)90026-6
https://doi.org/10.1016/0022-3956(75)900... The Mattis Dementia Rating Scale (MDRS) assesses various cognitive aspects, but its application is longer and requires specialized professionals. The Montreal Cognitive Assessment (MoCA) is a global and brief battery, but it does not provide subscores by cognitive domains.

Addenbrooke cognitive examination

The ACE is a brief cognitive assessment battery, with high sensitivity and specificity for detecting mild stage dementia, not requiring specialized equipment. It was developed in 2000 by a team conducted by John R. Hodges and Germán E. Berríos at Addenbrooke’s Hospital, Cambridge, UK,¹³13 Mathuranath PS, Nestor PJ, Berrios GE, Rakowicz W, Hodges JR. A brief cognitive test battery to differentiate Alzheimer’s disease and frontotemporal dementia. Neurology 2000;55(11):1613--1620. Doi: 10.1212/01.wnl.0000434309.85312.19
https://doi.org/10.1212/01.wnl.000043430... as a tool to assess early stages and differentiate subtypes of dementia, such as Alzheimer’s Dementia (AD) and Frontal-Temporal Dementia (FTD), Vascular Dementia (VD), Progressive Supranuclear Palsy (PSP), and other parkinsonian syndromes.¹⁴14 Newman JP. Brief assessment of cognitive mental status in Hebrew: Addenbrooke’s Cognitive Examination. Isr Med Assoc J 2005;7(07):451-457,¹⁵15 Mioshi E, Dawson K, Mitchell J, Arnold R, Hodges JR. The Addenbrooke’s Cognitive Examination Revised (ACE-R): a brief cognitive test battery for dementia screening. Int J Geriatr Psychiatry 2006; 21(11):1078–1085. Doi: 10.1002/gps.1610
https://doi.org/10.1002/gps.1610... ,¹⁶16 Stokholm J, Vogel A, Johannsen P, Waldemar G. Validation of the Danish Addenbrooke’s Cognitive Examination as a screening test in a memory clinic. Dement Geriatr Cogn Disord 2009;27(04):361–365. Doi: 10.1159/000209271
https://doi.org/10.1159/000209271... ,¹⁷17 Crawford S, Whitnall L, Robertson J, Evans JJ. A systematic review of the accuracy and clinical utility of the Addenbrooke’s Cognitive Examination and the Addenbrooke’s Cognitive Examination-Revised in the diagnosis of dementia. Int J Geriatr Psychiatry 2012; 27(07):659–669. Doi: 10.1002/gps.2771
https://doi.org/10.1002/gps.2771... It consists of 6 cognitive domains, totaling 100 points: orientation (10 points), attention (8 points), memory (35 points), verbal fluency (14 points), language (28 points), and visual-spatial skills (5 points). The points related to the six domains can be calculated separately. The sum of all of them equals the total score. This total score includes the 30 MMSE points, which can also be calculated separately.

The ACE-III was developed in 2013, with different versions validated in several countries.¹⁸18 Bruno D, Slachevsky A, Fiorentino N, et al. Argentinian/Chilean validation of the Spanish-language version of Addenbrooke’s Cognitive Examination III for diagnosing dementia. Neurologia 2020;35(02):82–88. Doi: 10.1016/j.nrl.2017.06.004
https://doi.org/10.1016/j.nrl.2017.06.00... ,¹⁹19 Hsieh S, Schubert S, Hoon C, Mioshi E, Hodges JR. Validation of the Addenbrooke’s Cognitive Examination III in frontotemporal dementia and Alzheimer’s disease. Dement Geriatr Cogn Disord 2013;36(3-4):242–250. Doi: 10.1159/000351671
https://doi.org/10.1159/000351671... ,²⁰20 Kan KC, Subramaniam P, Shahrizaila N, Kamaruzzaman SB, Razali R, Ghazali SE. Validation of the Malay Version of Addenbrooke’s Cognitive Examination III in Detecting Mild Cognitive Impairment and Dementia. Dement Geriatr Cogn Disord Extra 2019;9(01): 66–76. Doi: 10.1159/000495107
https://doi.org/10.1159/000495107... ,²¹21 Matias-Guiu JA, Cortés-Martínez A, Valles-Salgado M, et al. Addenbrooke’s cognitive examination III: diagnostic utility for mild cognitive impairment and dementia and correlation with standardized neuropsychological tests. Int Psychogeriatr 2017;29 (01):105–113. Doi: 10.1017/S1041610216001496
https://doi.org/10.1017/S104161021600149... ,²²22 Peixoto B, Machado M, Rocha P, et al. Validation of the Portuguese version of Addenbrooke’s Cognitive Examination III in mild cognitive impairment and dementia. Adv Clin Exp Med 2018;27 (06):781–786. Doi: 10.17219/acem/68975
https://doi.org/10.17219/acem/68975... ,²³23 Qassem T, Khater MS, Emara T, et al. Validation of the Addenbrooke’s Cognitive Examination-III in Mild Cognitive Impairment in Arabic Speakers in Egypt. Dement Geriatr Cogn Disord 2020;49 (04):418–422,²⁴24 Takenoshita S, Terada S, Yoshida H, et al. Validation of Addenbrooke’s cognitive examination III for detecting mild cognitive impairment and dementia in Japan. BMC Geriatr 2019;19(01):123. Doi: 10.1186/s12877-019-1120-4
https://doi.org/10.1186/s12877-019-1120-... ,²⁵25 Wang BR, Ou Z, Gu XH, Wei CS, Xu J, Shi JQ. Validation of the Chinese version of Addenbrooke’s Cognitive Examination III for diagnosing dementia. Int J Geriatr Psychiatry 2017;32(12):e173–e179. Doi: 10.1002/gps.4680
https://doi.org/10.1002/gps.4680... There is evidence of psychometric property and diagnostic ability to distinguish healthy people from patients with dementia. As in the previous version (ACE-R), ACE-III focuses on five cognitive domains (attention/orientation, memory, verbal fluency, visuospatial ability, and language). The total score is still 100. The runtime is still around 20 to 30 minutes.

In individuals with PD, a study with the first version of ACE²⁶26 Reyes MA, Perez-Lloret S, Roldan Gerschcovich E, Martin ME, Leiguarda R, Merello M. Addenbrooke’s Cognitive Examination validation in Parkinson’s disease. Eur J Neurol 2009;16(01):142–147. Doi: 10.1111/j.1468-1331.2008.02384.x
https://doi.org/10.1111/j.1468-1331.2008... demonstrated 92% sensitivity and 91% specificity with a cutoff score of 83 to detect DPD; however, its sample was small (n = 31, without dementia; n = 13, with dementia). Another study,²⁷27 Kaszás B, Kovács N, Balás I, et al. Sensitivity and specificity of Addenbrooke’s Cognitive Examination, Mattis Dementia Rating Scale, Frontal Assessment Battery and Mini Mental State Examination for diagnosing dementia in Parkinson’s disease. Parkinsonism Relat Disord 2012;18(05):553–556. Doi: 10.1016/j.parkreldis.2012.02.010
https://doi.org/10.1016/j.parkreldis.201... also with a small sample, had a cutoff score of 80, capable of detecting dementia (sensitivity: 74%, specificity: 78.1%). With the same version of the instrument, a cutoff score of 83.5 was shown with better diagnostic accuracy (sensitivity: 87.1%, specificity: 79.7%) in differentiating MCI-PD and 80.5 (sensitivity: 86.9%, specificity: 73.7%) in differentiating D-PD.²⁸28 Lucza T, Karádi K, Kállai J, et al. Screening Mild and Major Neurocognitive Disorders in Parkinson’s Disease. Behav Neurol 2015;2015:983606

Regarding the third version of the ACE, with a sample consisting only of individuals with PD, there is just one study for validation and standardization, conducted by Lucza et al.,²⁹29 Lucza T, Ascherman Z, Kovács M, et al. Comparing Sensitivity and Specificity of Addenbrooke’s Cognitive Examination-I, III and Mini-Addenbrooke’s Cognitive Examination in Parkinson’s Disease. Behav Neurol 2018;2018:5932028 in which the sensitivity and specificity of some versions of ACE (ACE, ACE-III, and mini-ACE) were compared in 552 individuals with PD. For individuals with level of education between 0 and 8 and 9 and 12 years, ACE-III, among the 3 versions, was the one showing the best discrimination skills for MCI-PD (83.5 [level of education: 0–8 years, sensitivity of 93%, and specificity of 64%, area under the curve [AUC] = 0.733]; 85.5 [level of education 9–12 years, sensitivity of 80%, and specificity of 78%, AUC = 0.771]; 88.5 [level of education >12 years, sensitivity of 76%, and specificity of 74%, AUC = 0.838]). To detect dementia, ACE-III showed the best diagnostic accuracy in all educational levels.

Thus, studies with ACE-III are more focused on neurological conditions, such as AD, FTD, VD, and atypical parkinsonisms, or even on psychiatric conditions such as schizophrenia.³⁰30 Charernboon T, Chompookard P. Detecting cognitive impairment in patients with schizophrenia with the Addenbrooke’s Cognitive Examination. Asian J Psychiatr 2019;40:19-22. Doi: 10.1016/j.ajp.2019.01.006
https://doi.org/10.1016/j.ajp.2019.01.00...

This is the first study performed in Brazil with the third version of the ACE and the first exclusively performed in patients with PD, with the neuropsychological assessment as a reference method, with the use of a comprehensive battery of standardized neuropsychological tests being a strength of the present study. This assessment is the gold standard for the diagnosis of mild cognitive impairment and mild dementia.

The aims of the present study were to investigate the diagnostic accuracy, sensitivity and specificity of the ACE, third version (ACE-III), to detect MCI-PD and D-PD, and its ability to differentiate between subgroups of patients, and to correlate them with demographic, clinical data, and neuropsychological tests.

METHODS

Study design

This is an observational, cross-sectional, case-control study.

Participants and recruitment

A total of 150 idiopathic PD patients, according to the clinical diagnosis criteria of the Parkinson UK Brain Bank, were enrolled in the study. For the diagnosis of MCI-PD, the criteria of the Movement Disorder Society, Level II (2012), were used, based on a broad neuropsychological assessment, with a standard deviation (SD) of 1.5 below the mean of the normative value (depending on the test) for age, and educational level being considered a cognitive deficit. According to MDS Level II criteria, impaired performance in one test in two separate cognitive domains or in two tests in the same cognitive domain means cognitive deficit. Functionality assessment, based on the application of a questionnaire on functional activities and cognitive complaints, was also used to differentiate MCI-PD from D-PD.

These patients were from the neurological rehabilitation program of Rede SARAH de Hospitais de Rehabilitação, from the unit of the city of Salvador, Bahia, Brazil. During their admission, they were evaluated by a neurologist and physiotherapist before being referred for neuropsychological evaluation. Each patient met the clinical diagnostic criteria for PD³¹31 Litvan I, Goldman JG, Tröster AI, et al. Diagnostic criteria for mild cognitive impairment in Parkinson’s disease: Movement Disorder Society Task Force guidelines. Mov Disord 2012;27(03):349-356. Doi: 10.1002/mds.24893
https://doi.org/10.1002/mds.24893... and provided written informed consent according to the approval by the Ethics Committee of the Rede SARAH de Hospitais de Rehabilitação (57521316.8.0000.0022) and the Universidade de São Paulo/Department of Neurology (57521316.8.3001.0065). Participants in the clinical group should be > 40 years old, with ≥ 4 years of formal education, with no major psychiatric disorders or history of substance use and/or abuse, cerebrovascular disease, and/or other known conditions that could impair mental status and interfere with cognitive performance. Demographic details are presented in ►Table 1.

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Table 1
Clinical and sociodemographic characteristics and comparison between clinical subgroups and the healthy control group

Regarding affective aspects, patients with minimum to light intensity scores in the Beck Depression (BDI) and Anxiety (BAI) Inventories (≤ 16 in BDI and ≤ 15 in BAI) were included.

The clinical group was matched for age, sex, and education to the healthy controls. These participants were patients from other rehabilitation programs (orthopedics) or companions for other patients from the same Hospital, who did not participate in the present study, in a rehabilitation program. They were recruited according to the following inclusion criteria: formal education of ≥ 4 years, questionnaire of functional activities³²32 Pfeffer RI, Kurosaki TT, Harrah CH Jr, Chance JM, Filos S. Measurement of functional activities in older adults in the community. J Gerontol 1982;37(03):323-329. Doi: 10.1093/geronj/37.3.323
https://doi.org/10.1093/geronj/37.3.323... of 0 or 1 (minimum score is 0 and maximum is 30, with the presence of functional impairment being considered from a score of > 5 points), with scores above the median values for education,³³33 Brucki SMD, Nitrini R, Caramelli P, Bertolucci PHF, Okamoto IH. Suggestions for utilization of the mini-mental state examination in Brazil. Arq Neuropsiquiatr 2003;61(3B):777-781 delayed Recall of the Figure Memory Test from the Brief Cognitive Screening Battery (BCSB) ≥ 7 of gross scoring.³⁴34 Nitrini R, Caramelli P, Herrera Júnior E, et al. Performance of illiterate and literate nondemented elderly subjects in two tests of long-term memory. J Int Neuropsychol Soc 2004;10(04): 634-638. Doi: 10.1017/S1355617704104062
https://doi.org/10.1017/S135561770410406... ,³⁵35 Nitrini R, Lefèvre BH, Mathias SC, et al. Neuropsychological tests of simple application for diagnosing dementia. Arq Neuropsiquiatr 1994;52(04):457-465. Doi: 10.1590/S0004-282 × 1994000400001
https://doi.org/10.1590/S0004-282 × 1994... Individuals with neurological or psychiatric disorders, cerebrovascular disease, and substance use/abuse were excluded.

ACE-III

As there is little difference between the revised version and the third version of ACE, except for the design belonging to the visuospatial part, the test was performed in Portuguese, with complementation of this part belonging to ACE-III, since it is different from the revised version. The correction remained as in ACE-R.

The ACE-R version contains items from the MMSE and, therefore, the authors themselves decided to create the ACE-III. It was used in the present study to assess its accuracy in the evaluation of patients with Parkinson’s disease.

Neuropsychological, functional, and mood evaluations

Disease severity was assessed using the Hoehn and Yahr - H&Y scale by the same examiner (assessed in the on-phase of medication and collected from the electronic medical records).

Cognitive functions were assessed by a neuropsychologist using a comprehensive tests battery: Digit Span (WMS-R),³⁶36 Wechsler D. Manual for Wechsler Memory Scale-Revised. The Psychological Corporation; 1987 Corsi Block-Tapping Test,³⁷37 Lezak MD, Loring DW, Hannay HJ, Fischer JS. Neuropsychological Assessment. 4th ed. Oxford University Press; 2004 Mental Control (WMS-R),³⁶36 Wechsler D. Manual for Wechsler Memory Scale-Revised. The Psychological Corporation; 1987 Rey’s Auditory-Verbal Learning Test (RAVLT),³⁸38 Malloy-Diniz LF, Lasmar VAP, Gazinelli Lde SR, Fuentes D, Salgado JV. The Rey Auditory-Verbal Learning Test: applicability for the Brazilian elderly population. Rev Bras Psiquiatr (São Paulo). 2007; 29(04):324-329. Doi: 10.1590/S1516-44462006005000053
https://doi.org/10.1590/S1516-4446200600... Rey Complex Figure (RCF),³⁷37 Lezak MD, Loring DW, Hannay HJ, Fischer JS. Neuropsychological Assessment. 4th ed. Oxford University Press; 2004 Trail Making Test, parts A and B (TMT-A and TMT-B),³⁹39 Straus E, Sherman EMS, Spreen O. A Compendium of Neuropsychological Tests: Administration, Norms, and Commentary. 3rd ed. Oxford University Press; 2006 and Phonemic Verbal Fluency (PVF).³⁹39 Straus E, Sherman EMS, Spreen O. A Compendium of Neuropsychological Tests: Administration, Norms, and Commentary. 3rd ed. Oxford University Press; 2006

These tests were conducted in patients in on-medication phase. To avoid fatigue in the PD, the neuropsychological assessment was conducted over 2 sessions, each lasting ~ 90 minutes.

The patients were classified as 3 subgroups: (1) normal cognition in Parkinson disease (NC-PD), n = 24; (2) mild cognitive impairment due to Parkinson disease (MCI-PD), n = 104; (3) dementia due to Parkinson disease (D-PD), n = 22, according to the guidelines of the Movement Disorder Society (MDS).³¹31 Litvan I, Goldman JG, Tröster AI, et al. Diagnostic criteria for mild cognitive impairment in Parkinson’s disease: Movement Disorder Society Task Force guidelines. Mov Disord 2012;27(03):349-356. Doi: 10.1002/mds.24893
https://doi.org/10.1002/mds.24893... ,⁴⁰40 Emre M. Dementia associated with Parkinson’s disease. Lancet Neurol 2003;2(04):229-237. Doi: 10.1016/S1474-4422(03)00351-X
https://doi.org/10.1016/S1474-4422(03)00... Gross data were converted to Z-score and those with a score of 1.5 SDs below the average, for their age and education, in 1 test in 2 separate cognitive domains or in 2 tests in the same cognitive domain, and preserved functionality, were diagnosed as MCI-PD. For the diagnosis of dementia, loss of functionality and decline were considered (Pfeffer Functional Activity Questionnaire [FAQ] > 5 and/or IQCODE > 3.41). The individuals were classified by a professional with experience in cognitive neurology, and who was blinded for the information of the patient.

Statistical analysis

Data were analyzed using a statistical technique with the aid of the IBM SPSS Statistics for Windows, version 22.0 (IBM Corp., Armonk, NY, USA). The variables were analyzed using the chi-squared test, the Student t-test, the Bonferroni test, ROC analysis, the Pearson correlation coefficient, and the Spearman rho coefficient, according to the type of data (categorical or continuous) and its distribution.

Demographic data, scores on cognitive evaluations, and other quantitative measures were compared through oneway analysis of variance (ANOVA) with Bonferroni post hoc comparisons.

Pearson correlation coefficients were used among the continuous variables, such as performance on ACE-III with other cognitive tests, as well as between ACE-III scores and clinical (disease progression and severity) and functional data (FAQ and IQCODE scales scores). The Spearman correlation coefficient, nonparametric correlation, was used for ordinal variables, such as the H&Y scale.

The battery’s diagnostic accuracy was investigated through the analysis of the ROC, 95% confidence interval (CI), curves to check the sensitivity and specificity of the cutoff points (total and domains cutoff scores of the ACE-III), to distinguish between groups of participants (healthy controls versus MCI-PD and healthy controls versus D-PD). A cutoff score was identified based on high sensitivity and specificity. The best cutoff point was chosen to balance sensitivity and specificity, identifying the point on the curve closest to point (0.1). In the ROC curve analysis, the groups were combined to estimate the area under the curve (AUC) used to discriminate nonpathological from pathological groups. An AUC between 0.9 and 1.0 was considered ”excellent” accuracy; 0.8 to 0.9, ”good”; 0.7 to 0.89, ”not good”; and 0.6 to 0.79, ”worthless”⁴¹41 Zhu K, van Hilten JJ, Marinus J. Predictors of dementia in Parkinson’s disease; findings from a 5-year prospective study using the SCOPA-COG. Parkinsonism Relat Disord 2014;20(09):980-985. Doi: 10.1016/j.parkreldis.2014.06.006
https://doi.org/10.1016/j.parkreldis.201... . Diagnostic accuracy was also evaluated through the levels of education (4-9,10-12 and ≥ 13 years).

|Significance was set at p ≤ 0.05.

RESULTS

Demographic and clinical profile

A total of 150 patients and 60 healthy controls were recruited for the present study.

As it can be seen in ►Table 1, there was no statistically significant difference between the groups (total clinical and control) in relation to age (t = 0.1942, p = 0.84), years of formal education (t = 1. 1003, p = 0.2725), and sex (χ² = 0.7046, p = 0.401). In clinical measures of mood and anxiety, as well as in the functional measures, a higher score was observed, that is, a worse result, in the clinical group. Regarding the severity of motor symptoms, there was a higher proportion of patients in stages I and II of the H&Y scale, that is, with less severe disease. This table also illustrates the comparison of ACE-III scores and subscores between these two groups (total clinical and control). There were statistically significant differences in the mean scores of the total ACE-III score (t= -3.1861, p = 0.0017), and in its attention/orientation (t = -3.1886, p = 0.0017), memory (t = -2.9926, p = 0.0031), and visuospatial component (t = -2.5188, p = 0.0125) domains.

Cognitive assessment

►Table 2 shows that, after the stratification of the clinical group, due to cognitive impairment, a difference was observed in relation to age between the subgroups NC-PD and D-PD, severity of the disease between the subgroups D-PD and MCI-PD, NC-PD and MCI-PD, as well as for the NC-PD and DPD subgroups. Regarding the severity of the disease, assessed using the H&Y scale, a difference was observed between the subgroups, mainly between the NC-PD and D-PD (χ² = 12.5645, p = <0.0001) subgroups. The post hoc analysis (Bonferroni test) revealed that the DPD group had significantly lower mean scores for the total ACE-III score and in all five domains when compared with the NC-PD, MCI-PD, and healthy control groups. The comparison between the MCI-PD and healthy control groups showed that the MCI-PD group had only significantly lower mean scores in the total ACE-III and memory domain. The comparison between D-PD and MCI-PD, D-PD and healthy controls, D-PD and NC-PD showed statistically significant differences in all measures (total score of ACE-III and its five cognitive domains).

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Table 2
ACE-III scores and neuropsychological tests and comparison between the four groups

As for the cognitive tests of the neuropsychological battery (MDS level II assessment), there was a statistically significant difference between the total clinical and control groups regarding mental control measures, ROCF (copy, immediate recall, delayed recall), RAVLT (learning, list A; list B; A after interference, delayed recall, and recognition), phonemic verbal fluency (F-A-S), digit span (reverse order),

Corsi block test (forward and reverse order), and trail test (time of execution, parts A and B).

Correlation between ACE-III, demographic, clinical data, and neuropsychological tests

Age was inversely associated with the total ACE-III scores and all of its cognitive domains, that is, score performance decreased when age increased; however, only the verbal fluency, language, and visual-spatial domains showed significant correlation. On the other hand, the performance of cognitive scores was positively associated with years of formal education in all ACE-III scores. The higher the level of education, the better the performance on cognitive scores (►Table 3).

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Table 3
Correlation coefficients and determination of scores by age and education (total ACE-III and its domains)

ACE-III: discriminant ability between subgroups/diagnostic accuracy/diagnostic interpretation

►Table 4 reveals the cut-off scores, sensitivity, and specificity of ACE-III, through analyses of the ROC curve. The ideal cut-off point for ACE-III to discriminate healthy controls was 85/100 (sensitivity = 58.65%, specificity = 60%). The AUC for ACE-III was 0.6400. To discriminate between healthy controls and the DPD subgroup, the ideal cutoff point for ACE-III observed was 81/100 (sensitivity = 77.27%, specificity = 78.33%). The AUC for ACE-III was 0.8848.

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Table 4
Cutoff, sensitivity and specificity notes to identify MCI-PD and D-PD, using the total ACE-III score

When ROC analysis was performed by different levels of education years, the optimal ACE-III cut-off to discriminate D-PD from healthy controls, with 10 to 12 years of education, was 78 points, 100% sensitivity and 100% specificity, AUC = 1 (95% CI: 1-1); followed by ≥ 13 years (83 points, 75.00%: sensitivity and 100%: specificity; AUC = 0.9167; 95%CI: 0.73-1]) and 4-9 years (78, points, 81.82%: sensitivity and 62.50%: specificity; AUC = 0.8504; 95%CI: 0.69-1). The optimal ACE-III cut-off to discriminate MCI-PD from healthy controls, with ≥ 13 years, was 91 points (73.08% sensitivity and 77.78% specificity; AUC = 0.8312; 95%CI: 0.67-0.98), followed by 10 to 12 years with 85 points (57% sensitivity and 74.07% specificity; AUC = 0.7089; 95%CI: 0.60–0.83]) and 4 to 9 years with 81 points (60% sensitivity and 50% specificity; AUC = 0.6110; 95%CI: 0.46–0.75) (►Supplementary Material Tables S1-S3).

DISCUSSION

The need for brief instruments, with good psychometric properties and accuracy to detect mild cognitive changes and dementia in DP, is important in clinical practice. The frequency of MCI-PD and D-PD can be of 30% depending on age, disease duration, and comorbidities.²⁹29 Lucza T, Ascherman Z, Kovács M, et al. Comparing Sensitivity and Specificity of Addenbrooke’s Cognitive Examination-I, III and Mini-Addenbrooke’s Cognitive Examination in Parkinson’s Disease. Behav Neurol 2018;2018:5932028

The third version (ACE-III) was only applied in the PD population by Lucza et al.,²⁹29 Lucza T, Ascherman Z, Kovács M, et al. Comparing Sensitivity and Specificity of Addenbrooke’s Cognitive Examination-I, III and Mini-Addenbrooke’s Cognitive Examination in Parkinson’s Disease. Behav Neurol 2018;2018:5932028 who aimed to compare the sensitivity and specificity of the different versions of the ACE available in Hungary (ACE-I, ACE-III, and Mini-ACE), to detect major and minor neurocognitive disorders, according to the DSM-5 criteria. The ACE-III had the best diagnostic accuracy at all levels of education (cut-off points: 70.5, 77.5, and 78.5 points for individuals with educational level from 0 to 8, from 9 to 12 and >12 years, respectively). Therefore, the present study demonstrated that the ACE-III and its abbreviated version, M-ACE, had the best diagnostic accuracy to detect MCI-PD and D-PD.

The present study showed that ACE-III is a brief cognition assessment tool and is able to differentiate individuals with MCI-PD and D-PD from healthy controls, with cut-off scores of 85/100 and 81/100, to detect MCI-PD and D-PD, respectively.

Most studies used cognitive or brief screening batteries, such as MMSE, MoCA and MADRS, as a comparison method, with few studies including comprehensive neuropsychological batteries. The current study showed correlation of ACE-III domains with standardized neuropsychological tests for this population.

The cut-off scores of the present study were lower than those of studies with ACE²⁶26 Reyes MA, Perez-Lloret S, Roldan Gerschcovich E, Martin ME, Leiguarda R, Merello M. Addenbrooke’s Cognitive Examination validation in Parkinson’s disease. Eur J Neurol 2009;16(01):142–147. Doi: 10.1111/j.1468-1331.2008.02384.x
https://doi.org/10.1111/j.1468-1331.2008... and ACE-R.⁴²42 Berankova D, Janousova E, Mrackova M, et al. Addenbrooke’s Cognitive Examination and Individual Domain Cut-Off Scores for Discriminating between Different Cognitive Subtypes of Parkinson’s Disease. Parkinsons Dis 2015;2015:579417 In the present study, the instrument was used to distinguish the cognitive subtypes in PD (CN-PD, CCL-PD, D-PD = 69), with a cut-off score of 88.5 being identified as capable of differentiating CN-PD from MCI-PD (with 0.68 sensitivity and 0.91 specificity) and 82.5 points (with 0.70 sensitivity and 0.73 specificity) to differentiate MCI-PD from D-PD, with an AUC of 0.78 (95%CI: 0.63–0.93).⁴²42 Berankova D, Janousova E, Mrackova M, et al. Addenbrooke’s Cognitive Examination and Individual Domain Cut-Off Scores for Discriminating between Different Cognitive Subtypes of Parkinson’s Disease. Parkinsons Dis 2015;2015:579417 This result was similar to the previous study by Biundo et al.,⁴³43 Biundo R, Calabrese M, Weis L, et al. Anatomical Correlates of Cognitive Functions in Early Parkinson’s Disease Patients. Draganski B, editor. PLoS One. 2013 May 22;8(05):e64222 with a lower cut-off score of 80 points, but higher than the studies with the ACE-R in Brazil.⁴⁴44 Rocha MSG, Bassetti EM, Oliveira MO, Kuark RGB, Estevam NM, Brucki SMD. Addenbrooke’s Cognitive Examination-Revised is accurate for detecting dementia in Parkinson’s disease patients with low educational level. Dement Neuropsychol 2014;8(01):20-25,⁴⁵45 Sobreira E, Pena-Pereira MA, Eckeli AL, et al. Screening of cognitive impairment in patients with Parkinson’s disease: diagnostic validity of the Brazilian versions of the Montreal Cognitive Assessment and the Addenbrooke’s Cognitive Examination-Revised. Arq Neuropsiquiatr 2015;73(11):929-933. Doi: 10.1590/0004-282X20150156
https://doi.org/10.1590/0004-282X2015015...

Thus, the studies were different from the present one regarding education. The present study also has the highest average. The age and years of disease progression were similar, with minimal difference. Education influenced the total ACE-III score, regardless of the stratification of the clinical sample.

When analyzed by educational level, the results showed greater sensitivity and specificity to differentiate healthy controls from patients with D-PD. This is probably related to the fact that among patients with low education, low cognitive scores may signal disease and poor schooling simultaneously, and patients with low education may perform poorly without having cognitive impairment.

These aspects should be considered when interpreting the cut-off scores to improve the accuracy of cognitive performance and the cognitive diagnosis.

Therefore, the present study suggests that ACE-III was able to detect the presence of cognitive impairment in patients with PD. Thus, this battery can be used as a quick and efficient tool in the assessment of cognitive deficits associated with PD, that is, it can be widely useful in clinical practice, even more so in hospital contexts, where the application of sensitive and brief instruments is required. A combination with neuropsychological instruments is required, especially in those individuals with higher level of education and/or milder/initial deficits, to avoid false negatives. Although the application time of ACE-III is longer than that of other batteries, such as the MoCA, it has better accuracy in this population for the diagnosis of cognitive impairment.

This study had the following strengths: (1) the analysis of the clinical utility and psychometric properties of ACE-III among PD subgroups. (2) the use of comprehensive and standardized neuropsychological instruments for this clinical condition as a method of comparison. (3) Matching the clinical group with the healthy control group in terms of age, education, and sex contributed to the results of the present study, strengthening the statistical analyses.

There are some limitations to the present study: (1) the participants were recruited from a rehabilitation hospital; therefore, the result is subject to reference bias and may not be applicable to community populations. (2) nonmotor aspects (fatigue, insomnia, for example) may have influenced cognitive and functional results, as scales were not used for this purpose; however, when any interference of these aspects was observed, the evaluation was interrupted and continued later. The sample size of the subgroups was relatively small, mainly in relation to the CN-PD and D-PD. This aspect may have reduced the magnitude of the difference between the clinical group and the control group. Future studies with larger samples are required to add to these results.

Acknowledgments

The authors would like to thank Eneida Mioshi for having given permission to use the instrument, and all the participants involved in the present study.

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Publication Dates

Publication in this collection
15 May 2023
Date of issue
2023

History

Received
22 Mar 2022
Reviewed
20 June 2022
Accepted
04 July 2022

This is an Open Access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

[1] ¹
Lees AJ, Hardy J, Revesz T. Parkinson’s disease. Lancet 2009;373 (9680):2055-2066. Doi: 10.1016/S0140-6736(09)60492-X
» https://doi.org/10.1016/S0140-6736(09)60492-X

[2] ²
Emre M, Aarsland D, Brown R, et al. Clinical diagnostic criteria for dementia associated with Parkinson’s disease. Mov Disord 2007; 22(12):1689-1707, quiz 1837. Doi: 10.1002/mds.21507
» https://doi.org/10.1002/mds.21507

[3] ³
Cerasa A, Gioia MC, Salsone M, et al. Neurofunctional correlates of attention rehabilitation in Parkinson’s disease: an explorative study. Neurol Sci 2014;35(08):1173-1180. Doi: 10.1007/s10072-014-1666-z
» https://doi.org/10.1007/s10072-014-1666-z

[4] ⁴
Kulisevsky J, Pagonabarraga J. Cognitive impairment in Parkinson’s disease: tools for diagnosis and assessment. Mov Disord 2009;24(08):1103-1110. Doi: 10.1002/mds.22506
» https://doi.org/10.1002/mds.22506

[5] ⁵
Papagno C, Trojano L. Cognitive and behavioral disorders in Parkinson’s disease: an update. I: cognitive impairments. Neurol Sci 2018;39(02):215-223. Doi: 10.1007/s10072-017-3154-8
» https://doi.org/10.1007/s10072-017-3154-8

[6] ⁶
Portet F, Gabelle A, Touchon J. [Parkinson’s disease dementia and Lewy body dementia]. Psychol Neuropsychiatr Vieil 2006;4(Spec No 1):S35-S50

[7] ⁷
Tedrus GMAS, Fonseca LC, Letro GH, Bossoni AS, Adriana Bastos S. Dementia and mild cognitive impairment in Parkinson’s disease. Arq Neuropsiquiatr 2009;67(04):1164

[8] ⁸
Tedrus GMAS, Fonseca LC, Letro GH, Bossoni AS, Samara AB. Dementia and mild cognitive impairment in patients with Parkinson’s disease. Arq Neuropsiquiatr. 2009;67(2 B):423-427. Doi: 10.1590/S0004-282X2009000300010
» https://doi.org/10.1590/S0004-282X2009000300010

[9] ⁹
Janvin CC, Larsen JP, Aarsland D, Hugdahl K. Subtypes of mild cognitive impairment in Parkinson’s disease: progression to dementia. Mov Disord 2006;21(09):1343-1349. Doi: 10.1002/mds.20974
» https://doi.org/10.1002/mds.20974

[10] ¹⁰
Williams-Gray CH, Evans JR, Goris A, et al. The distinct cognitive syndromes of Parkinson’s disease: 5 year follow-up of the CamPaIGN cohort. Brain 2009;132(Pt 11):2958-2969. Doi: 10.1093/brain/awp245
» https://doi.org/10.1093/brain/awp245

[11] ¹¹
Dubois B, Burn D, Goetz C, et al. Diagnostic procedures for Parkinson’s disease dementia: recommendations from the movement disorder society task force. Mov Disord 2007;22(16):2314-2324. Doi: 10.1002/mds.21844
» https://doi.org/10.1002/mds.21844

[12] ¹²
Folstein MF, Folstein SE, McHugh PR. “Mini-mental state”. A practical method for grading the cognitive state of patients for the clinician. J Psychiatr Res 1975;12(03):189-198. Doi: 10.1016/0022-3956(75)90026-6
» https://doi.org/10.1016/0022-3956(75)90026-6

[13] ¹³
Mathuranath PS, Nestor PJ, Berrios GE, Rakowicz W, Hodges JR. A brief cognitive test battery to differentiate Alzheimer’s disease and frontotemporal dementia. Neurology 2000;55(11):1613--1620. Doi: 10.1212/01.wnl.0000434309.85312.19
» https://doi.org/10.1212/01.wnl.0000434309.85312.19

[14] ¹⁴
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n = 210	NC-PD (n = 24)	MCI-PD (n = 104)	D-PD (n = 22)	Control Group (n = 60)	p-value
n = 210	NC-PD (n = 24)	MCI-PD (n = 104)	D-PD (n = 22)	Control Group (n = 60)	D-PD vs MCI-PD	D-PD vs Control	MCI-PD vs Control	NC-PD vs MCI-PD	NC-PD vs Control	NC-PD vs D-PD
Sex n (%)- Male	15 (62.50%)	78 (75%)	11 (50%)	38 (63.33%)	0.019*	2.75	0.114	0.216	0.943	0.393^b
Age, years old	59.50 (8.94)	63.90 (8.44)	66.50 (9.24)	63.32 (9.04)	1.000	0.877	1.000	0.165	0.436	0.044*^a
Education, years	12.21 (4.11)	11.05 (3.83)	9.68 (4.44)	10.38 (3.51)	0.786	1.000	1.000	1.000	0.303	1.000^a
Disease duration, years	5.58 (4.00)	6.69 (4.79)	7.32 (4.92)	-	1.000	-	-	0.895	-	0.637^a
Hoehn & Yahr Scale (%)				-	0.005**	-	-	0.023*	-	<0.0001***^a
I-II	20 (13.33%)	59 (39.33%)	7 (4.66%)	-	0.034*	-	-	0.016*	-	<0.0001***^b
III-IV	4 (2.66%)	45 (30%)	15 (10%)	-	-	-	-	-	-	-
BDI	4.63 (3.88)	5.75 (4.37)	8.14 (4.23)	0.68 (1.63)	0.041*	0.000***	0.000***	1.000	0.000***	0.010*^a
BAI	2.29 (1.68)	3.02 (3.06)	4.59 (3.67)	0.20 (0.51)	0.054	0.000***	0.000***	1.000	0.005**	0.015*^a
FAQ	0.83 (1.31)	2.02 (1.88)	7.23 (4.68)	0.27 (0.48)	0.000***	0.000***	0.000***	0.072	1.000	<0.0001***^a
IQCODE	3.08 (0.17)	3.32 (0.43)	4.35 (0.87)	3.13 (0.23)	0.000***	0.000***	0.034*	0.077	1.000	<0.0001***^a
n = 210	Clinical Group (n = 150)			Control Group (n = 60)	*p-value*
Sex (%) - Male	104			38 (63.33%)	0.401^b
Age, years old	63.58 (8.81)			63.32 (9.04)	0.8462^a
Level of education, years	11.03 (4.00)			10.38 (3.51)	0.2725^a
Length of disease (years)	6.61 (4.69)			-	-
Hoehn & Yahr scale (%) I-II	86 (57.33%)			-	-
Hoehn & Yahr scale (%) III	64 (42.67%)			-	-
BDI	5.92 (4.37)			0.68 (1.63)	< 0.0001 ***^a
BAI	3.13 (3.04)			0.20 (0.51)	< 0.0001 ***^a
FAQ	2.59 (3.12)			0.27 (0.48)	< 0.0001 ***^a
IQCODE	3.44 (0.63)			3.13 (0.23)	< 0.0003***^a

n = 210	Controls (n = 60)	NC-PD (n = 24)	MCI-PD (n = 104)	D-PD (n = 22)	p-value
ACE-III (total score)	87.02 (7.70)	92.42 (4.92)	82.05 (9.83)	69.27 (12.74)	< 0.0001***
Attention/Orientation	16.88 (1.52)	16.92 (1.53)	16.13 (1.82)	14.18 (2.20)	< 0.0001***
Memory	20.37 (3.89)	22.50 (3.02)	18.21 (4.26)	14.00 (5.01)	< 0.0001***
Verbal Fluency	9.93 (2.68)	11.42 (1.64)	9.37 (2.73)	6.64 (2.87)	< 0.0001***
Language	25.13 (1.29)	25.92 (0.28)	24.63 (2.11)	22.59 (3.32)	< 0.0001***
Visuospatial	14.70 (1.57)	15.67 (0.48)	13.70 (2.67)	11.86 (3.27)	< 0.0001***
Mental Control	5.7 ± 0.6	5.6 ± 0.6	5.2 ± 1.0	4.2 ± 1.6	< 0.0001***
ROCFT (copy)	30.6 ± 6.5	34.7 ± 2.0	26.6 ± 8.7	20.6 ± 10.8	< 0.0001***
ROCFT (sec)	307.1 ± 144.4	286.0 ± 157.8	377.0 ± 251.3	401.2 ± 243.3	< 0.0640
ROCFT (immediate memory)	16.5 ± 8.4	22.4 ± 6.9	1 2.8 ± 6.6	8.9 ± 5.3	< 0.0001***
ROCFT (delayed memory)	16.2 ± 7.8	22.9 ± 5.4	1 2.0 ± 6.3	8.4 ± 5.2	< 0.0001***
RAVLT - Total A	42.3 ± 8.2	46.5 ± 6.5	34.7 ± 8.5	28.6 ± 10.9	< 0.0001***
RAVLT - B	5.3 ± 2.2	5.4 ± 1.7	4.3 ± 1.6	3.1 ± 1.3	< 0.0001***
RAVLT - A (after interference)	8.1 ± 2.8	10.2 ± 1.9	6.4 ± 2.6	5.7 ± 2.5	< 0.0001***
RAVLT - delayed memory	7.9 ± 2.7	9.8 ± 2.2	6.6 ± 2.8	5.4 ± 2.7	< 0.0001***
RAVLT - recognition	13.8 ± 1.3	14.2 ± 1.3	11.9 ± 2.6	11.4 ± 2.3	< 0.0001***
Verbal Fluency (F, A, S)	33.6 ± 11.6	37.0 ± 11.3	26.09 ± 9.9	19.2 ± 8.6	< 0.0001***
Verbal Fluency (animals)	15.5 ± 4.3	18.4 ± 4.9	14.8 ± 4.9	10.7 ± 4.3	< 0.0001***
Digit Span (forward)	5.3 ± 1.0	5.5 ± 0.6	5.0 ± 0.9	4.4 ± 0.8	0.0001 **
Digit Span (backward)	3.9 ± 1.0	4.4 ± 1.0	3.5 ± 0.7	3.1 ± 0.8	< 0.0001***
Corsi Blocks (forward)	5.1 ± 0.9	5.5 ± 0.9	4.7 ± 0.9	3.9 ± 1.1	< 0.0001***
Corsi Blocks (backward)	4.3s ± 0.8	5.1 ± 0.9	3.9 ± 0.9	3.2 ± 0.7	< 0.0001***
TMT-A (sec)	67.4 ± 31.1	56.3 ± 26.3	88.3 ± 61.7	111.4 ± 64.4	< 0.0004**
TMT-B (sec)	197.9 ± 111.8	131.5 ± 65.3	233.5 ± 115.5	250.9 ± 84.0	< 0.0001***
TMT (B – A)	132.3 ± 98.8	75.2 ± 50.5	145.8 ± 96.5	129.7 ± 84.6	0.0106*

	Age (years old)		Schooling (years)
	r	r²	r	r²
ACE-III (total)	- 0.1296	0.0167	0.4373***	0.0191
Attention/Orientation	- 0.0336	0.0011	0.2685***	0.0720
Memory	- 0.0339	0.0011	0.4257***	0.1812
Verbal Fluency	- 0.1373*	0.0188	0.3368***	0.1134
Language	- 0.1428*	0.0203	0.2693***	0.0725
Visuospatial	- 0.1970**	0.0388	0.2925***	0.0855

ACE-III	MCI-PD
Cutoff scores	Sensivity	Specificity
83	50.96%	71.67%
84	54.81%	66.67%
85	58.65%	60.00%
86	60.58%	55.00%
87	61.54%	51.67%
	D-PD
78	72.73%	85.00%
79	72.73%	81.67%
80	77.27%	78.33%
81	81.82%	75.00%
82	81.82%	71.67%

Brasil

Brasil

Addenbrooke’s cognitive examination III: diagnostic utility for detecting mild cognitive impairment and dementia in Parkinson’s disease

Exame cognitivo de Addenbrooke III: utilidade diagnóstica para detectar comprometimento cognitivo leve e demência na doença de Parkinson

Abstract

Background

Objective

Methods

Results

Conclusions

Resumo

Antecedentes

Objetivo

Métodos

Resultados

Conclusões

INTRODUCTION

Addenbrooke cognitive examination

METHODS

Study design

Participants and recruitment

ACE-III

Neuropsychological, functional, and mood evaluations

Statistical analysis

RESULTS

Demographic and clinical profile

Cognitive assessment

Correlation between ACE-III, demographic, clinical data, and neuropsychological tests

ACE-III: discriminant ability between subgroups/diagnostic accuracy/diagnostic interpretation

DISCUSSION

Acknowledgments

References

Publication Dates

History