Functional decline in the elderly with MCI: Cultural adaptation of the ADCS-ADL scale

Cintra, Fabiana Carla Matos da Cunha; Cintra, Marco Túlio Gualberto; Nicolato, Rodrigo; Bertola, Laiss; Ávila, Rafaela Teixeira; Malloy-Diniz, Leandro Fernandes; Moraes, Edgar Nunes; Bicalho, Maria Aparecida Camargos

doi:10.1590/1806-9282.63.07.590

Summary

Objective:

Translate, transcultural adaptation and application to Brazilian Portuguese of the Alzheimer’s Disease Cooperative Study - Activities of Daily Living (ADCS-ADL) scale as a cognitive screening instrument.

Method:

We applied the back translation added with pretest and bilingual methods. The sample was composed by 95 elderly individuals and their caregivers. Thirty-two (32) participants were diagnosed as mild cognitive impairment (MCI) patients, 33 as Alzheimer’s disease (AD) patients and 30 were considered as cognitively normal individuals.

Results:

There were only little changes on the scale. The Cronbach alpha coefficient was 0.89. The scores were 72.9 for control group, followed by MCI (65.1) and by AD (55.9), with a p-value < 0.001. The ROC curve value was 0.89. We considered a cut point of 72 and we observed a sensibility of 86.2%, specificity of 70%, positive predictive value of 86.2%, negative predictive value of 70%, positive likelihood ratio of 2.9 and negative likelihood ratio of 0.2.

Conclusion:

ADCS-ADL scale presents satisfactory psychometric properties to discriminate between MCI, AD and normal cognition.

Keywords:
mild cognitive impairment; Alzheimer’s disease; activities of daily living

Resumo

Objetivo:

Tradução, adaptação transcultural para o português brasileiro e aplicação da escala Alzheimer’s Disease Cooperative Study - Activities of Daily Living (ADCS-ADL) como instrumento de triagem cognitiva.

Método:

Retrotradução associada ao método bilíngue e de pré-teste. A amostra foi constituída por 95 idosos e seus respectivos acompanhantes, sendo 30 controles, 32 portadores de comprometimento cognitivo leve (CCL) e 33 portadores de demência de Alzheimer (DA) em fase inicial.

Resultados:

Um pequeno número de modificações ocorreu na escala. O coeficiente alpha de Cronbach foi 0,89. O grupo controle pontuou 72,9, seguido pelo CCL (65,1) e pelo DA (55,9), valor p<0,001. A curva ROC demonstrou valor de 0,89. Com o ponto de corte de 72, observamos sensibilidade de 86,2%, especificidade de 70%, valor preditivo positivo de 86,2%, valor preditivo negativo de 70%, razão de verossimilhança positiva de 2,9 e razão de verossimilhança negativa de 0,2.

Conclusão:

A escala ADCS-ADL apresenta propriedades psicométricas satisfatórias para discriminar entre DA, CCL e cognição normal.

Palavras-chave:
comprometimento cognitivo leve; demência de Alzheimer; atividades cotidianas

Introduction

An accelerated aging process in the population can be observed in both developed and developing countries. In Brazil, from 1940 onwards, the aging process has increased morbidity and mortality due to external causes and chronic-degenerative diseases, such as dementia.¹1 Miranda GMD, Mendes ACG, Silva ALA. O envelhecimento populacional brasileiro: desafios e consequências. Rev Bras Geriatria Gerontol. 2016; 19(3):507-19. The evolution of these diseases is often marked by the progressive decline in functional capacity, with consequent impairment of quality of life.¹1 Miranda GMD, Mendes ACG, Silva ALA. O envelhecimento populacional brasileiro: desafios e consequências. Rev Bras Geriatria Gerontol. 2016; 19(3):507-19.

2 Ramos-Cerqueira AT, Torres AR, Crepaldi AL, Oliveira NI, Scazufca M, Menezes PR, et al. Identification of dementia in the community: a Brazilian experience. J Am Geriatr Soc. 2005; 53(10):1738-42.^-³3 Chaimowicz F. A saúde dos idosos brasileiros às vésperas do século XXI: problemas, projeções e alternativas. Rev Saúde Pública. 1997; 31(2):184-200.

According to the World Alzheimer Report (2011), more than 65 million people worldwide have dementia, 58% of which live in underdeveloped countries. This research also reveals that studies conducted over the last 10 years have shown that only one fifth of dementia cases are routinely recognized and documented in developed countries. In underdeveloped countries, such as Brazil, the situation is even more serious, as up to 90% of the relatives of patients with this clinical condition had not even received guidelines regarding the disease and available treatments.²2 Ramos-Cerqueira AT, Torres AR, Crepaldi AL, Oliveira NI, Scazufca M, Menezes PR, et al. Identification of dementia in the community: a Brazilian experience. J Am Geriatr Soc. 2005; 53(10):1738-42.^,⁴4 Prince M, Bryce R, Ferri C. Alzheimer's Disease International World Alzheimer Report 2011 - The benefits of early diagnosis and intervention. Institute of Psychiatry, King's College London, UK. Published by Alzheimer's Disease International (ADI); 2011 [cited 2015 Sep 15]. Available from: https://www.alz.co.uk/research/WorldAlzheimerReport2011.pdf
https://www.alz.co.uk/research/WorldAlzh...

In recent years, mild cognitive impairment (MCI) has been recognized as an intermediate stage between normal cognition and dementia.⁵5 Albert MS, DeKosky ST, Dickson D, Dubois B, Feldman HH, Fox NC, et al. The diagnosis of mild cognitive impairment due to Alzheimer's disease: recommendations from the National Institute on Aging-Alzheimer's Association workgroups on diagnostic guidelines for Alzheimer's disease. Alzheimers Dement. 2011; 7(3):270-9. MCI indicates that the affected individual presents greater chances of conversion to dementia caused by Alzheimer’s disease (AD) and other degenerative processes than individuals with normal cognition for their educational level.⁵5 Albert MS, DeKosky ST, Dickson D, Dubois B, Feldman HH, Fox NC, et al. The diagnosis of mild cognitive impairment due to Alzheimer's disease: recommendations from the National Institute on Aging-Alzheimer's Association workgroups on diagnostic guidelines for Alzheimer's disease. Alzheimers Dement. 2011; 7(3):270-9.

MCI usually affects one or more domains of cognition, and is classified into the amnestic and non-amnestic subtypes, according to the presence or absence of memory impairment. The amnestic type is mainly characterized by memory complaints and may reflect AD in the pre-dementia symptomatic phase. The non-amnestic type is characterized by deficits in any other domain of cognition, for example, executive function, reasoning, attention, and more.⁵5 Albert MS, DeKosky ST, Dickson D, Dubois B, Feldman HH, Fox NC, et al. The diagnosis of mild cognitive impairment due to Alzheimer's disease: recommendations from the National Institute on Aging-Alzheimer's Association workgroups on diagnostic guidelines for Alzheimer's disease. Alzheimers Dement. 2011; 7(3):270-9. The latter, most often progresses to other forms of dementia (not AD).⁶6 Kelley BJ, Petersen RC. Alzheimer's disease and mild cognitive impairment. Neurol Clin. 2007; 25(3):577-609.

7 Petersen RC, Negash S. Mild cognitive impairment: an overview. CNS Spectr. 2008; 13(1):45-53.^-⁸8 Petersen RC. Mild cognitive impairment as a diagnostic entity. J Intern Med. 2004; 256(3):183-94.

According to Bagen et al., elderly people with MCI present difficulties in the performance of activities of daily living (ADL).⁹9 Bangen KJ, Jak AJ, Schiehser DM, Delano-Wood L, Tuminello E, Han SD, et al. Complex activities of daily living vary by mild cognitive impairment subtype. J Int Neuropsychol Soc. 2010; 16(4):630-9. However, there are problems related to the identification and classification of the activities involved. Subtle deficits were identified in advanced and instrumental ADL, which would generally go unnoticed, compromising quality of life and determining the risk of conversion to AD.

Functionality may represent an important marker in the differential diagnosis between individuals with normal cognition and amnestic MCI. However, the existing instruments for functional assessment are heterogeneous, making comparisons difficult. Most tests used are not validated and culturally adapted for use in the Brazilian population with MCI. In addition, doubts remain as to which ADL are compromised and how best to assess them.⁹9 Bangen KJ, Jak AJ, Schiehser DM, Delano-Wood L, Tuminello E, Han SD, et al. Complex activities of daily living vary by mild cognitive impairment subtype. J Int Neuropsychol Soc. 2010; 16(4):630-9.

10 Pereira FS, Yassuda MS, Oliveira AM, Diniz BS, Radanovic M, Talib LL, et al. Profiles of functional deficits in mild cognitive impairment and dementia: benefits from objective measurement. J Int Neuropsychol Soc. 2010; 16(2):297-305.

11 Marshall GA, Olson LE, Frey MT, Maye J, Becker JA, Rentz DM, et al. Instrumental activities of daily living impairment is associated with increase amyloid burden. Dement Geriatr Cogn Disord. 2011; 31(6):443-50.

12 Farias ST, Mungas D, Reed BR, Harvey D, Cahn-Weiner D, Decarli C. MCI is associated with deficits in everyday functioning. Alzheimer Dis Assoc Disord. 2006; 20(4):217-23.^-¹³13 Nitrini R, Caramelli P, Bottino CMC, Damasceno BP, Brucki SMD, Anghinah R. Diagnóstico de doença de Alzheimer no Brasil: avaliação cognitiva e funcional. Recomendações do Departamento Científico de Neurologia Cognitiva e do Envelhecimento da Academia Brasileira de Neurologia. Arq Neuropsiquiatr. 2005; 63(3A):720-7.

In this context, the purpose of this article is to report the results of the process of translation, cross-cultural adaptation and application of the Alzheimer’s Disease Cooperative Study - Activities of Daily Living (ADCS-ADL) scale as an instrument for evaluating the functionality of the Brazilian population for the diagnosis of dementia and its non-dementia clinical phase, also known as MCI.

Method

This is a cross-sectional study in which individuals were recruited from June 2012 to May 2013 by convenience sampling obtained at the Mild Cognitive Impairment outpatient clinic of the Jenny de Andrade Faria Institute for Elderly Care at the Federal University of Minas Gerais (UFMG) Clinics Hospital. All of the participants and/or their companions/caregivers signed the informed consent form (ICF). This study was approved by the UFMG Research Ethics Committee under no. 0318.0.203.000-11.

The ADCS-ADL scale was created in 1997 by Galasko et al.¹⁴14 Galasko D, Bennett D, Sano M, Ernesto C, Thomas R, Grundman M, et al. An inventory to assess activities of daily living for clinical trials in Alzheimer's disease. The Alzheimer's Disease Cooperative Study. Alzheimer Dis Assoc Disord. 1997; 11 (Suppl 2):S33-9. It is a questionnaire with 23 Likert-type questions for functional assessment, in which the subject must express their degree of agreement or disagreement with the questions in the questionnaire (independent, partially independent and totally dependent). It is adapted for elderly people with MCI and it is completed based on the data provided by an informant. The questionnaire describes the performance of patients in the prior month in various activities: Basic (BADL), instrumental (IADL) and advanced (AADL) ADL.¹⁵15 Grundman M, Petersen RC, Ferris SH, Thomas RG, Aisen PS, Bennett DA, et al.; Alzheimer's Disease Cooperative Study. Mild cognitive impairment can be distinguished from Alzheimer disease and normal aging for clinical trials. Arch Neurol. 2004; 61(1):59-66.^,¹⁶16 Pedrosa H, De Sa A, Guerreiro M, Maroco J, Simoes MR, Galasko D, et al. Functional evaluation distinguishes MCI patients from healthy elderly people--the ADCS/MCI/ADL scale. J Nutr Health Aging. 2010; 14(8):703-9.

The procedure for translation and cultural adaptation followed an internationally accepted protocol proposed by Beaton et al.¹⁷17 Beaton DE, Bombardier C, Guillemin F, Ferraz MB. Guidelines for the process of cross-cultural adaptation of self-report measures. Spine. 2000; 25(24):3186-91. The technique used was back-translation associated with the bilingual method, following five stages, namely, two independent translations, synthesis of the Portuguese translations, back translation of the scale into English, and analysis of the questionnaire by a panel of expert judges. The pre-final version was then submitted to pre-testing.

For pre-testing, a sample consisting of 90 Brazilian elderly people living in the community and their respective caregivers or informants was divided into three groups containing 30 individuals each: cognitively normal controls, amnestic MCI patients, and patients with probable early stage AD. The application of the questionnaire was timed.

We included 95 individuals aged 60 years or older with normal cognition, MCI or AD. The diagnosis of probable sporadic AD followed the criteria of Mckhann et al., classified as mild, stage 1 by the Clinical Dementia Rating (CDR).¹⁸18 McKhann GM, Knopman DS, Chertkow H, Hyman BT, Jack CR Jr, Kawas CH, et al. The diagnosis of dementia due to Alzheimer's disease: recommendations from the National Institute on Aging-Alzheimer's Association workgroups on diagnostic guidelines for Alzheimer's disease. Alzheimers Dement. 2011; 7(3):263-9.^,¹⁹19 Morris JC. The Clinical Dementia Rating (CDR): current version and scoring rules. Neurology. 1993; 43(11):2412-4. For MCI, the criteria defined by Albert et al. and Petersen et al. were used.⁵5 Albert MS, DeKosky ST, Dickson D, Dubois B, Feldman HH, Fox NC, et al. The diagnosis of mild cognitive impairment due to Alzheimer's disease: recommendations from the National Institute on Aging-Alzheimer's Association workgroups on diagnostic guidelines for Alzheimer's disease. Alzheimers Dement. 2011; 7(3):270-9.^,²⁰20 Petersen RC, Stevens JC, Ganguli M, Tangalos EG, Cummings JL, DeKosky ST. Practice parameter: early detection of dementia: mild cognitive impairment (an evidence-based review). Report of the Quality Standards Subcommittee of the American Academy of Neurology. Neurology. 2001; 56(9):1133-42. This group only included patients with the amnestic form. The control group consisted of individuals with normal cognition considering the specific cut-off points according to educational level.

Individuals with non-Alzheimer’s dementia, moderate or advanced AD, psychiatric illness, Parkinson’s disease, delirium and MCI secondary to other causes (psychiatric disorders, endocrine-metabolic diseases, autoimmune diseases, traumatic brain injury, drugs, alcohol and drugs) were excluded. We also excluded subjects with impaired mobility, vision or hearing deficits, and those who did not complete all of the assessments. We did not include individuals whose companion and/or caregiver were not present at the assessment interview.

For an adequate assessment of cognition and allocation of individuals to the groups described, all patients underwent evaluation by geriatricians and neuropsychologists trained in cognitive assessment of the elderly. All subjects were submitted to the same study protocol. In order to rule out other causes of cognitive decline and to diagnose concomitant diseases, laboratory and structural and functional neuroimaging examinations (nuclear magnetic resonance or computed tomography of the brain and/or positron emission tomography - PET-CT of the brain) were performed. In all cases, the clinical and neuropsychological diagnoses were concordant.

The following tests were used to assess cognition, mood, functionality and caregiver overload: Mini-Mental State Examination²¹21 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(3):189-98. (MMSE), verbal fluency test - fruit and animal category,²²22 Henry JD, Crawford JR, Phillips LH. Verbal fluency performance in dementia of the Alzheimer's type: a meta-analysis. Neuropsychologia. 2004; 42(9):1212-22. Geriatric Depression Scale - 15-item version,²³23 Almeida OP, Almeida SA. Confiabilidade da versão brasileira da escala de depressão em geriatria (GDS) versão reduzida. Arq Neuropsiquiatr. 1999; 57(2B):421-6. the clock test,²⁴24 Shulman KI. Clock-drawing: is it the ideal cognitive screening test? Int J Geriatr Psychiatry. 2000; 15(6):548-61. word list from the Consortium to Establish a Registry for Alzheimer’s Disease (CERAD),²⁵25 Morris JC, Heyman A, Mohs RC, Hughes JP, van Belle G, Fillenbaum G, et al. The Consortium to Establish a Registry for Alzheimer's Disease (CERAD): Part I. Clinical and neuropsychological assessment of Alzheirmer's disease. Neurology. 1989; 39(9):1159-65. Behavioral Pathology in Alzheimer’s Disease Scale - BEHAVE-AD,²⁶26 Reisberg B, Borenstein J, Salob SP, Ferris SH, Franssen E, Georgotas A. Behavioral symptoms in Alzheimer's disease: phenomenology and treatment. J Clin Psychiatry. 1987; 48 (Suppl):9-15. the Pfeffer Instrumental Activities Questionnaire,²⁷27 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(3):323-9. the List of Figures,²⁸28 Nitrini R, Lefèvre BH, Mathias SC, Caramelli P, Carrilho PEM, Sauaia N, et al. Testes neuropsicológicos de aplicação simples para o diagnóstico de demência. Arq Neuropsiquiatr. 1994; 52(4):457-65. Clinical Dementia Rating (CDR),¹⁹19 Morris JC. The Clinical Dementia Rating (CDR): current version and scoring rules. Neurology. 1993; 43(11):2412-4. the apathy scale,²⁹29 Marin RS, Biedrzycki RC, Firinciogullari S. Reliability and validity of the Apathy Evaluation Scale. Psychiatry Res. 1991; 38(2):143-62 .^,³⁰30 Guimarães HC, Fialho PPA, Carvalho VA, Santos EL, Caramelli P. Brazilian caregiver version of the Apathy Scale. Dement Neuropsychol. 2009; 3(4):321-6. functional stating using the Functional Assessment Staging (FAST),³¹31 Reisberg B. Functional assessment staging (FAST). Psychopharmacol Bull. 1988; 24(4):653-9. the Neuropsychiatric Inventory (NPI),³²32 Cummings JL, Mega M, Gray K, Rosenberg-Thompson S, Carusi DA, Gornbein J. The Neuropsychiatric Inventory: comprehensive assessment of psychopathology in dementia. Neurology. 1994; 44(12): 2308-14. and the DSM-IV Criteria for Depressive Disorder.³³33 American Psychiatric Association, APA. Manual Diagnóstico e Estatístico de Transtornos Mentais. DSM-IV-TR. 4. ed. Porto Alegre: Artmed; 2002.

Regarding the neuropsychological assessment, cognitive tests were applied considering the low educational level of the study population, based on the service’s protocol, as described below: The Mattis Dementia Rating Scale,³⁴34 Mattis S. Dementia Rating Scale. Professional Manual. Florida: Psychological Assessment Resources; 1988.^,³⁵35 Porto CS, Fichman HC, Caramelli P, Bahia VS, Nitrini R. Brazilian version of the Mattis dementia rating scale diagnosis of mild dementia in Alzheimer's disease. Arq Neuropsiquiatr. 2003; 61(2B):339-45. the Digit Span test,³⁶36 Nascimento E. WAIS-III: manual para administração e avaliação. São Paulo: Casa do Psicólogo; 2004. the Corsi Cubes,³⁷37 Corsi, PM. Human memory and the medial temporal region of the brain [thesis]. Montreal: McGill University; 1972.^,³⁸38 Paula JJ, Schlottfeldt CG, Moreira L, Cotta M, Bicalho MA, Romano-Silva MA, et al. Propriedades psicométricas de um protocolo neuropsicológico breve para uso em populações geriátricas. Rev Psiquiatra Clín. 2010; 37(6):246-50. Token Test,³⁹39 De Renzi E, Faglioni P. Normative data and screening power of a shortened version of the Token Test. Cortex. 1978; 14(1):41-9.^,⁴⁰40 Radanovic M, Mansur LL, Azambuja MJ, Porto CS, Scaff M. Contribution to the evaluation of language disturbances in subcortical lesions: a piloty study. Arq Neuropsiquiatr. 2004; 62(1):51-7. and Rey’s Auditory-Verbal Learning Test - RAVLT.⁴¹41 Rey A. L'examen clinique en psychologie: 2. et. Le psychologue, 1. Paris: Presses Universitaires de France; 1998.

42 Malloy-Diniz LF, Lasmar VA, Gazinelli Lde S, Fuentes D, Salgado JV. The Rey Auditory-Verbal Learning Test: applicability for the Brazilian elderly population. Rev Bras Psiquiatr. 2007; 29(4):324-9.

43 Paula JJ, Malloy-Diniz LF. Executive functions as predictors of functional performance in mild Alzheimer's dementia and mild cognitive impairment elderly. Estud Psicol (Natal). 2013; 18(1):117-24.^-⁴⁴44 de Paula JJ, Bertola L, Ávila RT, Moreira L, Coutinho G, de Moraes EN, et al. Clinical applicability and cutoff values for an unstructured neuropsychological assessment protocol for older adults with low formal education. PLoS ONE. 2013; 8(9):e73167.

The Shapiro-Wilk test was used for normality analysis. The distribution of the sample was considered normal only for the age of the informant variable. Chi-square, Anova and Kruskal-Wallis tests were used as non-parametric tests. To verify correlations between continuous variables, we used Spearman correlation test.

Descriptive and analytical statistics; quality of clinical trials: sensitivity (Se), specificity (Sp), negative (NPV) and positive (PPV) predictive value, positive (PLR) and negative (NLR) accuracy and likelihood ratio; ROC curve (to establish the cut-off point) and Cronbach’s alpha (internal consistency) were performed in order to determine reliability. The data obtained was analyzed using the SPSS statistical software version 19.0, IBM ^®.

Results

Translation and cultural adaptation of the ADCS-ADL Questionnaire

The process of translation and adaptation of the questionnaire showed satisfactory results, indicating semantic equivalence between the two translations and absence of translation difficulties, verified by the small number of modifications carried out by the expert committee. The changes involved: formatting of the questions (47%), cultural expressions (29%) and vocabulary (17%). Other changes totaled 7%. These items were modified or had their format changed in order to facilitate cultural understanding and appropriateness. These changes did not result in significant change to the scale. One subitem to a question (question 24) was added and the score changed from 78 to 79 points.

During the pre-testing application, a statistical difference was observed between the control and AD groups in the subdomain BADL, composed of self-care and feeding activities. This relation was not expected since the decline in BADL only occurs in the more advanced stages of AD. Analyzing the items in this subdomain, we observed that “select/choose clothes” and “eat using forks and knives” were responsible for this difference, since they obtained lower scores when compared to the other items of the BADL subdomain, probably due to the influence of gender in these tasks.

To minimize this bias, we modified the item “eating using forks and knives” to “eating independently” and removed the item “select/choose clothes,” given that even among men in the control group, this activity was performed by a third party, usually the wife or daughter. We observed that for many elderly people the activity of selecting clothes is delegated to the spouse, constituting a pattern of dependence cultivated by personal habits. These modifications to correct the influence of gender did not cause a change in the final score of the questionnaire.

Considering the expert opinions and pre-testing, we constructed the Brazilian version of the ADCS-ADL.

General characteristics of the sample selected for pre-testing

The 95 participants selected were allocated into three groups: 30 controls, 32 MCI and 33 AD. Regarding the MCI group, all of the patients presented the amnestic subtype, with 73% involving multiple domains and 27% a single domain. The sociodemographic data and the comorbidities of the participants are listed in Table 1.

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Table 1
Clinical and sociodemographic characteristics of the sample and their respective caregivers.

Regarding the characterization of the control, MCI and AD groups, we noted a level of statistical significance and difference among groups in the age (p=0.020) and educational level (p=0.037) variables. The AD group, compared to others, was older (78.6±6.6) and presented lower educational level (3.6±3.2). As for comorbidities, 79.3% of the total sample had high blood pressure (HBP), 38.7% dyslipidemia, 21.5% type 2 diabetes mellitus (T2DM) and 20.4% had major depressive disorder. The depression variable showed a statistical difference among groups (p=0.028). Regarding caregiver characterization, the groups were similar in all of the evaluated variables, except age (p=0.015).

The control group achieved higher mean scores in the MMSE tests (control: 26.5; MCI: 24.2 and AD: 19.3) and on the Mattis scale (control: 132.5; MCI: 119.1 and AD: 102.6). In relation to the MMSE variable, there was a significant difference only between the AD-MCI and AD-control groups (p=0.001). As for the Mattis scale, there was a significant difference in all groups (p<0.001).

Functionality, assessed by the Pfeffer and ADCS-ADL scales, presented a similar pattern of results to cognitive ability. Regarding the Pfeffer test, we observed greater independence in the control group (0.4±0.7), greater dependence in the AD group (10.6±7.2) and intermediate result in the MCI group (4.3±4.9), with a statistical difference only detected between AD and MCI (p=0.004).

The mean application time of the ADCS-ADL scale was 12 minutes. The control group showed a better score on the scale (72.9), followed by the MCI group, with intermediate performance (65.1). The AD group had the worst performance (55.9) (p<0.001). As for the subitems in the ADCS-ADL scale, AADL and IADL presented a p-value <0.001, while BADL resulted in p=0.004. This difference is shown in Figure 1, which enables the detection of different functional profiles among the control, MCI and AD groups, showing mainly functional decline from the AD group to the MCI group, and from this group to the control group, especially regarding the IADL and AADL subitems.

FIGURE 1
Characterization of the functional profile of the groups based on the mean points obtained by subdomain of the ADCS-ADL scale.

As for the BADL subitem, despite the statistical difference observed, this was not clinically important due to very close values among the groups, especially considering the standard deviation. The AD group’s result was 19.9±2.3, MCI’s 20.8±1.5 and the control group’s was 21.5±0.7.

Reliability

The reliability of the Brazilian ADCS-ADL scale was obtained by analyzing the internal consistency coefficient of its 23 questions distributed in three subdomains: BADL (6 questions), IADL (10 questions) and AADL (7 questions). This analysis was verified by Cronbach’s alpha coefficient, yielding 0.89. This value suggests a good correlation among domains. The Cronbach’s coefficient was applied question to question rather than by domains (AADL, IADL and BADL), and in all cases the values found were higher than 0.80.

Criterion validity

Our study’s hypothesis that the constructs measured by the ADCS-ADL scale and the clinical and neuropsychological diagnoses would be associated and that this could be used as a diagnostic tool for MCI and AD was established and tested.

The results showed a significant association between the total ADCS-ADL scale and the clinical and neuropsychological diagnosis (p<0.001) with ROC_c=0.89. The AADL subdomain of the total ADCS-ADL scale presented a greater area under the curve (ROC_c=0.92) in relation to the reference line (clinical and neuropsychological diagnosis). The results of these variables are close to those in the curve delimited by the Mattis scale (ROC_c=0.918), whose study demonstrated greater diagnostic accuracy among study subjects, namely the control, MCI and AD.⁴⁴44 de Paula JJ, Bertola L, Ávila RT, Moreira L, Coutinho G, de Moraes EN, et al. Clinical applicability and cutoff values for an unstructured neuropsychological assessment protocol for older adults with low formal education. PLoS ONE. 2013; 8(9):e73167. On the other hand, the Pfeffer IADL scale showed an area under the curve of 0.89.

We established the cut-off point as 71 for the ADCS-ADL scale, to distinguish MCI and AD patients from controls, based on the sensitivity (Se) of 86.2%, specificity (Sp) of 70.0%, PPV of 86.2%, NPV of 70.0% and accuracy of 81.1%. The PLR was 2.9 and the NLR was 0.2.

In order to differentiate the MCI subjects from the controls, the ADCS-ADL scale with a cut-off value of 71 points presents sensitivity of 75% and specificity of 70%. To distinguish individuals with AD from the controls, we observed a sensitivity of 97.0% and specificity of 70%. Finally, to discriminate between AD and MCI, we found a sensitivity of 97.0% and specificity of 25%. The other quality tests of the scale carried out with the subitems IADL and BADL are described in Table 2.

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Table 2
Analysis of the quality measure of the ADCS-ADL scale.

We demonstrated that the AADL subitem of the ADCS-ADL scale shows good accuracy to discriminate subjects from the control, MDI and AD groups, and is superior even to the full results of the scale. We established a cut-off of 18 points, and found the following results: Se: 90.8%; Sp: 73.3%; PPV: 88.1%; NPV: 78.6%; accuracy: 85.3%. PLR was 3.4 and NLR was 0.1.

The subitem AADL with a cut-off point of 18 points presents 84.4% sensitivity and 73.3% specificity to differentiate MCI subjects from controls. To distinguish individuals with AD from the controls, we detected a sensitivity of 97.0% and specificity of 73.3%. To discriminate between AD and MCI, we obtained a sensitivity of 97.0% and specificity of 15.6%. The data relating to IADL and BADL are described in Table 2.

Discussion

Despite the great amount of knowledge regarding the description and monitoring of functional decline in the population with dementia, there is a gap in the literature with regard to the analysis of impairment of ADL in elderly people with MCI, characterized as a pre-dementia symptomatic stage of AD.⁴⁵45 Belchior P, Korner-Bitensky N, Holmes M, Robert A. Identification and assessment of functional performance in mild cognitive impairment: a survey of occupational therapy practices. Aust Occup Ther J. 2015; 62(3):187-96.

Several studies have aimed to characterize the nature of functional decline in this heterogeneous population, since the inclusion of the criterion “preservation of daily activities with slight impairment in complex activities” as a diagnostic for MCI in 2004. However, the unsystematic use and variability of the functional assessments employed have impaired more accurate results.⁴⁶46 Perneczky R, Pohl C, Sorg C, Hartmann J, Tosic N, Grimmer T, et al. Impairment of activities of daily living requiring memory or complex reasoning as part of the MCI syndrome. Int J Geriatr Psychiatry. 2006; 21(2):158-62.

47 Brown PJ, Devanand DP, Liu X, Caccappolo E; Alzheimer's Disease Neuroimaging Initiative. Functional impairment in elderly patients with mild cognitive impairment and mild Alzheimer disease. Arch Gen Psychiatry. 2011; 68(6):617-26.

48 Marshall GA, Amariglio RE, Sperling RA, Rentz DM. Activities of daily living: where do they fit in the diagnosis of Alzheimer's disease? Neurodegener Dis Manag. 2012; 2(5):483-91.^-⁴⁹49 Yeh YC, Lin KN, Chen WT, Lin CY, Chen TB, Wang PN. Functional disability profiles in amnestic mild cognitive impairment. Dement Geriatr Cogn Disord. 2011; 31(3):225-32.

We know that there are many scales for the assessment of ADL in the elderly. However, they were created with the objective of assessing the functional decline in elderly people with dementia, whose deficit proves to be more significant when compared to elderly people with MCI.⁴⁸48 Marshall GA, Amariglio RE, Sperling RA, Rentz DM. Activities of daily living: where do they fit in the diagnosis of Alzheimer's disease? Neurodegener Dis Manag. 2012; 2(5):483-91. This may create a “ceiling effect” in the instrument, masking the functional decline presented by individuals with MCI.⁵⁰50 Maher CG, Latimer J, Costa LOP. A importância da adaptação transcultural e clinimétrica para instrumentos de fisioterapia. Rev Bras Fisioter. 2007; 11(4):245-52.

In this context, the concern for early diagnosis is added to the need for instruments adapted and validated for the Brazilian population that assess the risk of dementia and MCI quickly, accurately and at a low cost. Our study aimed to perform a cultural adaptation, initial validation and analysis of the psychometric properties of the ADCS-ADL in view of its applicability and the satisfactory results observed in other studies.¹⁵15 Grundman M, Petersen RC, Ferris SH, Thomas RG, Aisen PS, Bennett DA, et al.; Alzheimer's Disease Cooperative Study. Mild cognitive impairment can be distinguished from Alzheimer disease and normal aging for clinical trials. Arch Neurol. 2004; 61(1):59-66.^,¹⁶16 Pedrosa H, De Sa A, Guerreiro M, Maroco J, Simoes MR, Galasko D, et al. Functional evaluation distinguishes MCI patients from healthy elderly people--the ADCS/MCI/ADL scale. J Nutr Health Aging. 2010; 14(8):703-9.^,⁴⁶46 Perneczky R, Pohl C, Sorg C, Hartmann J, Tosic N, Grimmer T, et al. Impairment of activities of daily living requiring memory or complex reasoning as part of the MCI syndrome. Int J Geriatr Psychiatry. 2006; 21(2):158-62.^,⁵¹51 Li M, Ng TP, Kua EH, Ko SM. Brief informant screening test for mild cognitive impairment and early Alzheimer's disease. Dement Geriatr Cogn Disord. 2006; 21(5-6):392-402. To our knowledge, this is one of the few Brazilian studies that describe the functional profile of elderly people with MCI, compared to that of elderly people with normal cognition and initial AD.¹⁶16 Pedrosa H, De Sa A, Guerreiro M, Maroco J, Simoes MR, Galasko D, et al. Functional evaluation distinguishes MCI patients from healthy elderly people--the ADCS/MCI/ADL scale. J Nutr Health Aging. 2010; 14(8):703-9.^,⁴⁶46 Perneczky R, Pohl C, Sorg C, Hartmann J, Tosic N, Grimmer T, et al. Impairment of activities of daily living requiring memory or complex reasoning as part of the MCI syndrome. Int J Geriatr Psychiatry. 2006; 21(2):158-62.^,⁵²52 Galasko D, Bennett DA, Sano M, Marson D, Kaye J, Edland SD; Alzheimer's Disease Cooperative Study. ADCS Prevention Instrument Project: assessment of instrumental activities of daily living for community-dwelling elderly individuals in dementia prevention clinical trials. Alzheimer Dis Assoc Disord. 2006; 20(4 Suppl 3):S152-69.

The use of a scale based on information from third parties (caregivers or informants) seems to be the most suitable for assessing the functionality of elderly people with MCI, given that these elderly people often present anosognosia and do not recognize the extent of their difficulties.⁵³53 Almeida OP, Crocco EI. Percepção dos déficits cognitivos e alterações do comportamento em pacientes com doença de Alzheimer. Arq Neuropsiquiatr. 2000; 58(2A):292-9.

54 Carr DB, Gray S, Baty J, Morris JC. The value of informant versus individual's complaints of memory impairment in early dementia. Neurology. 2000; 55(11):1724-6.^-⁵⁵55 Spalletta G, Girardi P, Caltagirone C, Orfei MD. Anosognosia and neuropsychiatric symptoms and disorders in mild Alzheimer disease and mild cognitive impairment. J Alzheimers Dis. 2012; 29(4):761-72.

In our study, we were able to verify that there are different functional profiles among subjects with MCI, AD and controls, with MCI assuming an intermediate pattern between the control group and the elderly with AD. We also noted that elderly people with MCI presented deficits in AADL and IADL when compared to controls with normal cognition for age and educational level. Elderly people with AD also present deficits in these specific areas but functional decline is greater.

Our results resemble those of Perneczky et al. and Pereira et al.⁴⁶46 Perneczky R, Pohl C, Sorg C, Hartmann J, Tosic N, Grimmer T, et al. Impairment of activities of daily living requiring memory or complex reasoning as part of the MCI syndrome. Int J Geriatr Psychiatry. 2006; 21(2):158-62.^,⁵⁶56 Pereira FS, Yassuda MS, Oliveira AM, Forlenza OV. Executive dysfunction correlates with impaired functional status in older adults with varying degrees of cognitive impairment. Int Psychogeriatr. 2008; 20(6):1104-15. They found that elderly individuals with MCI presented a functional decline in complex ADL compared to control subjects. The literature on the subject reveals that despite variability in the use of ADL assessment scales, several studies have identified a decline in AADL (exercise of roles and social activities typical of adult life) and IADL (management of domestic and community practical life) in elderly people with MCI.⁴⁷47 Brown PJ, Devanand DP, Liu X, Caccappolo E; Alzheimer's Disease Neuroimaging Initiative. Functional impairment in elderly patients with mild cognitive impairment and mild Alzheimer disease. Arch Gen Psychiatry. 2011; 68(6):617-26.

48 Marshall GA, Amariglio RE, Sperling RA, Rentz DM. Activities of daily living: where do they fit in the diagnosis of Alzheimer's disease? Neurodegener Dis Manag. 2012; 2(5):483-91.^-⁴⁹49 Yeh YC, Lin KN, Chen WT, Lin CY, Chen TB, Wang PN. Functional disability profiles in amnestic mild cognitive impairment. Dement Geriatr Cogn Disord. 2011; 31(3):225-32.^,⁵⁷57 De Vriendt P, Gorus E, Cornelis E, Velghe A, Petrovic M, Mets T. The process of decline in advanced activities of daily living: a qualitative explorative study in mild cognitive impairment. Int Psychogeriatr. 2012; 24(6):974-86.

It is important to emphasize that this type of instrument can be influenced by factors such as the level of caregiver overload, degree of proximity and the emotional state of the informant.⁵⁸58 Paixão CM Jr, Reichenheim ME. [A review of functional status evaluation instruments in the elderly]. Cad Saúde Pública. 2005; 21(1):7-19. To reduce the chance of error, the ADCS-ADL scale also has a manual with clear and objective explanations for all items. Another positive point is that it assesses the individual’s actual performance in a month, and therefore excludes the caregiver’s opinion about what the individual could do if they presented conditions to do so, as well as what the caregiver subjectively thinks with respect to the subject assessed.

It was verified that few items were left unanswered (8.7%), which contributes to the high internal validity of the test. Most caregivers were close relatives. However, a small percentage (17.4%) were comprised of other relatives, which may have contributed to the unanswered items.

It is important to emphasize that some items in the IADL and BADL subdomains of the ADCS-ADL scale may be influenced by the gender variable, such as cooking, using cutlery and washing and ironing. Culturally, these activities are carried out by Brazilian women.⁵⁹59 Duarte YA, Lebrão ML, Lima FD. Contribuição dos arranjos domiciliares para o suprimento de demandas assistenciais dos idosos com comprometimento funcional em São Paulo, Brasil. Rev Panam Salud Publica. 2005; 17(5-6):370-8. As previously described, the necessary adaptations were performed after pre-testing applications, adjusting the test to the cultural demands by gender.

Regarding the analysis of the psychometric properties, the ADCS-ADL scale provided good reliability, also verified in the study by Pedrosa et al.¹⁶16 Pedrosa H, De Sa A, Guerreiro M, Maroco J, Simoes MR, Galasko D, et al. Functional evaluation distinguishes MCI patients from healthy elderly people--the ADCS/MCI/ADL scale. J Nutr Health Aging. 2010; 14(8):703-9. In addition, the study presented a moderate Se value in the control-MCI differentiation (75%) and high Se value to differentiate AD-control (97%). However, there were moderate Sp values in both cases (70%).

According to the analyses regarding the differentiation of the MCI-AD group, the scale showed a high Se value (97%) and low Sp value (25%), which indicates that it is effective in the discrimination of this group. It should be noted that our specificity values are lower than those presented in the study by Pedrosa et al.¹⁶16 Pedrosa H, De Sa A, Guerreiro M, Maroco J, Simoes MR, Galasko D, et al. Functional evaluation distinguishes MCI patients from healthy elderly people--the ADCS/MCI/ADL scale. J Nutr Health Aging. 2010; 14(8):703-9.

We can infer from these results that the ADCS-ADL scale constitutes a test with high Se and moderate Sp, presenting greater power to detect people with cognitive impairment, although susceptible to false positives, especially in the differentiation between AD-control and MCI-AD. The scale was reasonable in the distinction between control-MCI. It can be used as a screening instrument for identifying individuals at risk of MCI or AD, requiring further evaluation in order to define the diagnosis.⁶⁰60 Pagano M, Gauvreau K. Princípios de Bioestatística. São Paulo: Cengage Learning; 2010.

We believe the ADCS-ADL scale to be a viable instrument as it is easy to apply, and external materials or resources are not required for its completion. Furthermore, it is quick to apply, especially compared to other diagnostic assessment instruments.

When analyzing the psychometric properties of the subitems in the ADCS-ADL scale, we are faced with the fact that AADL, composed of seven questions, presents results superior to the full scale in discriminating between control, MCI and AD patients, especially for differentiating the subjects with MCI from the controls more effectively than the full version of the ADCS-ADL scale. In addition, this subitem presents results only slightly below those obtained using the Mattis scale and above those in the Pfeffer ADL scale, when evaluated using the ROC curve. However, this subitem needs to be evaluated in the future as a reduced version of the ADCS-ADL scale with the same psychometric properties as the full scale.

It should be noted that the AADL subitem presents high sensitivity and a PLR value close to 0.1. These properties point to the potential of using the questionnaire as a screening tool, which reinforces the possibility of it being applied in primary care. This fact is of extreme importance in view of the difficulty in identifying these patients in primary health care, which has an impact on the diagnosis and management of cognitive and functional disorders, especially when considering early diagnosis. It should be noted that the data relating to the AADL subdomain are not comparable, given that no other study with the full scale has adopted this division.

In primary care, initial AD and MCI are often not diagnosed. Data from the literature show that in developed countries only 20 to 50% of patients with dementia are diagnosed, whereas in some underdeveloped countries the rate is less than 10%.⁴4 Prince M, Bryce R, Ferri C. Alzheimer's Disease International World Alzheimer Report 2011 - The benefits of early diagnosis and intervention. Institute of Psychiatry, King's College London, UK. Published by Alzheimer's Disease International (ADI); 2011 [cited 2015 Sep 15]. Available from: https://www.alz.co.uk/research/WorldAlzheimerReport2011.pdf
https://www.alz.co.uk/research/WorldAlzh... These data reinforce the importance of the results found in the AADL subitem. Given the above, we suggest validation studies in primary care, especially those involving community health agents or nurses at health centers.

The Pfeffer Instrumental Activities Questionnaire presented ROC = 0.89, close to the values shown by the ADCS-ADL scale. It is worth noting that the scale was originally described for functional assessment, and was mainly used to evaluate initial AD with Se: 85% and Sp: 81%.²⁷27 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(3):323-9. There is no cut-off point defined for MCI in the analysis of all the existing versions of the test in Brazil, with a cut-off point of 3 and 5 points described for functional impairment and functional incapacity, respectively.⁶¹61 Assis LO, Assis MG, de Paula JJ, Malloy-Diniz LF. O questionário de atividades funcionais de Pfeffer: revisão integrativa da literatura brasileira. Estud Interdiscipl Envelhec. 2015; 20(1):297-324. Studies for screening cognitive impairment in elderly populations with low levels of education, such as in Brazil, indicate that the use of Pfeffer’s instrumental activities questionnaire is not sufficient for adequate screening of cognitive decline, and other cognitive tests must be combined to obtain suitable sensitivity and specificity values.⁶²62 Jacinto AF, Brucki SM, Porto CS, Martins MA, Citero VA, Nitrini R. Suggested instruments for General Practitioners in countries with low schooling to screen for cognitive impairment in the elderly. Int Psychogeriatr. 2014; 26(7):1121-5.

Our study has limitations given that the scale is not yet validated due to the absence of the peer evaluation phase. The validation process for the Brazilian Portuguese version must be completed, despite the existence of a validated version in Portuguese from Portugal.⁶³63 Pedrosa HMD. Avaliação Funcional em doentes com Defeito Cognitivo Ligeiro: a escala ADCS MCI ADL [dissertation]. Lisboa: Faculdade de Medicina de Lisboa, Universidade de Lisboa; 2007. Brazil and Portugal, although adopting the same official language, hold profound cultural and linguistic differences, which justify the need for a separate validation for each country.⁶⁴64 Reichenheim ME, Moraes CL. Operacionalização de adaptação transcultural de instrumentos de aferição usados em epidemiologia. Rev Saúde Pública. 2007; 41(4):665-73. Furthermore, it is important to highlight the differences resulting from the influence of different levels of education among the elderly population of the two countries.⁶⁵65 Dias EG, Andrade FB, Duarte YA, Santos JL, Lebrão ML. [Advanced activities of daily living and incidence of cognitive decline in the elderly: the SABE Study]. Cad Saúde Pública. 2015; 31(8):1623-35. The authors of the original scale have given their authorization for cross-cultural adaptation in Brazil, which did not extend to disclosure in the original format and in the adapted version, therefore the ADCS-ADL scale is not attached to this article.

We conclude that the translated version of the ADCS-ADL adapted to Brazilian Portuguese has satisfactory psychometric properties to differentiate patients with cognitive incapacity from those with MCI. In view of the psychometric properties described for the AADL subitem of the ADCS-ADL scale, we suggest validation of this reduced version as a possible functional screening tool in primary care.

Study conducted at Faculdade de Medicina da Universidade Federal de Minas Gerais (FM-UFMG), Belo Horizonte, MG, Brazil

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Pereira FS, Yassuda MS, Oliveira AM, Forlenza OV. Executive dysfunction correlates with impaired functional status in older adults with varying degrees of cognitive impairment. Int Psychogeriatr. 2008; 20(6):1104-15.
⁵⁷
De Vriendt P, Gorus E, Cornelis E, Velghe A, Petrovic M, Mets T. The process of decline in advanced activities of daily living: a qualitative explorative study in mild cognitive impairment. Int Psychogeriatr. 2012; 24(6):974-86.
⁵⁸
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⁵⁹
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⁶²
Jacinto AF, Brucki SM, Porto CS, Martins MA, Citero VA, Nitrini R. Suggested instruments for General Practitioners in countries with low schooling to screen for cognitive impairment in the elderly. Int Psychogeriatr. 2014; 26(7):1121-5.
⁶³
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⁶⁴
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⁶⁵
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Publication Dates

Publication in this collection
July 2017

History

Received
13 Dec 2016
Accepted
02 Jan 2017

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[1] Study conducted at Faculdade de Medicina da Universidade Federal de Minas Gerais (FM-UFMG), Belo Horizonte, MG, Brazil

Variables	Control group n=30	Group MCI n=32	Group AD n=33	Total n=95	p-value
Sample data
Sex
Female (%)	63.3%	65.6%	51.5%	60.0%	0.461
Male (%)	36.7%	34.4%	48.5%	40.0%
Education
(Mean±SD in years)	5.7±4.4	5.2±3.9	3.6±3.3	4.8±3.9	0.037^* * significant difference.
Age
(Mean±SD in years)	73.4±7.9	75.3±7.6	78.6±6.6	75.9±7.6	0.020^* * significant difference.
HBP (%)	79.3%	65.6%	84.4%	76.3%	0.190
T2DM (%)	20.7%	18.8%	25%	21.5%	0.824
Dyslipidemia (%)	41.4%	43.8%	31.3%	38.7%	0.554
Depression (%)	6.9%	18.8%	34.4%	20.4%	0.028^* * significant difference.
Caregivers' data
Sex
Female (%)	74.3%	75.0%	90.0%	80.0%	0.147
Male (%)	25.7%	25.0%	10.0%	20.0%
Education
(Mean±SD in years)	9.9±3.8	8.7±3.1	9.2±4.1	9.2±2.6	0.276
Age
(Mean±SD in years)	52.2±17.1	55.0±13.0	52.1±14.9	53.1±14.9	0.015^* * significant difference.
Degree of family relations
Close relatives (%)^ Close relatives: wife, husband, children or siblings.	85.7%	75.0%	87.5%	82.6%	0.285
Other	14.3%	25.0%	12.5%	17.4%

Analysis of the total ADCS-ADL scale with cut-off value set at 71 points
	Se	Sp	PPV	NPV	Accuracy	PLR	NLR
Cognitive decline (MCI and AD) versus controls	86.2%	70%	86.2%	70%	81.1%	2.9	0.2
MCI versus control	75%	70%	72.7%	72.4%	72.6%	2.5	0.4
AD versus control	97%	70%	78%	95.4%	84.1%	3.2	0.04
AD versus MCI	97%	25%	42.9%	88.9%	61.5%	1.3	0.1
Analysis of the AADL subitem of the ADCS scale with cut-off value set at 18 points
	Se	Sp	PPV	NPV	Accuracy	PLR	NLR
Cognitive decline (MCI and AD) versus controls	90.8%	73.3%	88.1%	78.6%	85.3%	3.4	0.1
MCI versus control	84.4%	73.3%	77.1%	81.5%	79%	3.2	0.2
AD versus control	97%	73.3%	80%	95.7%	85.7%	3.6	0.04
AD versus MCI	97%	15.6%	54.2%	83.3%	56.9%	1.1	0.2
Analysis of the IADL subitem of the ADCS-ADL scale with cut-off value set at 32 points
	Se	Sp	PPV	NPV	Accuracy	PLR	NLR
Cognitive decline (MCI and AD) versus controls	81.5%	76.7%	88.3%	65.7%	80%	3.5	0.2
MCI versus control	68.8%	76.7%	75.9%	69.7%	72.6%	3.0	0.4
AD versus control	93.9%	76.7%	81.6%	92%	85.7%	4.0	0.08
AD versus MCI	93.9%	31.3%	41.5%	83.3%	63.1%	1.4	0.2
Analysis of the BADL subitem of the ADCS-ADL scale with cut-off value set at 21 points
	Se	Sp	PPV	NPV	Accuracy	PLR	NLR
Cognitive decline (MCI and AD) versus controls	66.2%	63.3%	79.6%	46.3%	65.3%	1.8	0.9
MCI versus control	68.8%	63.3%	66.7%	65.5%	66.1%	1.9	0.5
AD versus control	63.6%	63.3%	65.6%	61.3%	63.5%	1.7	0.6
AD versus MCI	63.6%	31.3%	48.8%	45.5%	47.7%	0.9	1.2

Brasil