Hostname: page-component-78c5997874-v9fdk Total loading time: 0 Render date: 2024-11-05T08:01:59.043Z Has data issue: false hasContentIssue false
  • English
  • Français

Psychological treatments for depression and anxiety in dementia and mild cognitive impairment: Systematic review and meta-analysis

Published online by Cambridge University Press:  02 January 2018

Vasiliki Orgeta ,
Afifa Qazi ,
Aimee Spector  and
Martin Orrell
Vasiliki Orgeta*
Affiliation:
Division of Psychiatry, University College London
Afifa Qazi
Affiliation:
Goodmayes Hospital, North East London Foundation Trust
Aimee Spector
Affiliation:
DClinPsych, Research Department of Clinical, Educational and Health Psychology, University College London
Martin Orrell
Affiliation:
Institute of Mental Health, Nottingham, UK
*
Vasiliki Orgeta, 6th Floor, Maple House, 149 Tottenham Court Road, London W1T 7NF, UK. Email: [email protected]
Rights & Permissions [Opens in a new window]

Abstract

Background

Anxiety and depression are common in people with dementia and mild cognitive impairment (MCI), but there is uncertainty about the effectiveness of both pharmacological and psychological therapies.

Aims

To evaluate the evidence of effectiveness of psychological treatments in treating depression and anxiety in people with dementia and MCI.

Method

We carried out a systematic review and meta-analysis of randomised controlled trials (RCTs) of psychological treatment versus usual care in people with dementia and MCI. Primary outcomes were symptoms of anxiety and depression. Secondary outcomes were quality of life, ability to perform daily activities, neuropsychiatric symptoms, cognition and caregivers' self-rated depressive symptoms.

Results

We included six RCTs, involving 439 participants with dementia, which used cognitive–behavioural therapy, interpersonal therapy, counselling or multimodal interventions including a specific psychological therapy. We found beneficial effects for both depression and anxiety. Overall, the quality of the evidence was moderate for depression and low for anxiety, due to the methodological limitations of the studies we identified and the limited number of trials.

Conclusions

The evidence from six RCTs suggests that psychological treatments are effective in reducing symptoms of depression and anxiety for people with dementia. There is a need for high-quality, multicentre trials including standardised, well-defined interventions.

Declarations of interest

A.Q., A.S. and M.O. are investigators in one of the included studies.

Type
Review article
Information
The British Journal of Psychiatry , Volume 207 , Issue 4 , October 2015 , pp. 293 - 298
Creative Commons
Creative Common License - CCCreative Common License - BY
This is an open access article distributed under the terms of the Creative Commons Attribution (CC BY) licence.
Copyright
Copyright © Royal College of Psychiatrists, 2015

Depression and anxiety are common in people with dementia and mild cognitive impairment (MCI). Estimates of prevalence of depressive symptoms in people with dementia range between 10 and 62%, Reference Enache, Winblad and Aarsland1 with substantially lower rates when employing strict criteria for major depression. Reference Weiner, Doody, Sairam, Foster and Liao2 People with MCI are also susceptible to depression, with rates reported as moderate at 36% Reference Palmer, Berger, Monastero, Winblad, Bäckman and Fratiglioni3 to high at 63%. Reference Solfrizzi, D'Introno, Colacicco, Capurso, Del Parigi and Caselli4 Anxiety symptoms are equally frequent, if not more prevalent, with rates between 8 and 71% Reference Ballard, Neill, O'Brien, McKeith, Ince and Perry5 for people with dementia and between 10 and 74% Reference Lopez, Becker and Sweet6 for people with MCI. Relatively less is known about prevalence of anxiety disorders in dementia and MCI, with rates up to 49% for anxiety-specific disorders Reference Ferreti, McCurry, Logsdon, Gibbons and Teri7 when using the Consortium to Establish a Registry for Alzheimer's Disease Behavioral Rating Scale for Dementia (CERAD-BRSD) criteria. Reference Monastero, Mangialasche, Camarda, Ercolani and Camarda8

Anxiety and depression have a substantial impact on outcomes as they decrease the ability to live independently, Reference Gibbons, Teri, Logsdon, McCurry, Kukull and Bowen9,Reference Rozzini, Chilovi, Peli, Conti, Rozzini and Trabucchi10 increase the risk of institutionalisation Reference Lyketsos, Steele, Baker, Galik, Kopunek and Steinberg11,Reference Stern, Tang, Albert, Brandt, Jacobs and Bell12 and result in higher caregiver burden. Reference González-Salvador, Arango, Lyketsos and Barba13,Reference Schultz, Hoth and Buckwalter14 In people with MCI, early symptoms of depression can often be resistant to antidepressants, Reference Devanand, Pelton, Marston, Camacho, Roose and Stern15 whereas both depression and anxiety have been found to predict higher rates of progression to Alzheimer's disease. Reference Lu, Edland, Teng, Tingus, Petersen and Cummings16

Recent recommendations have stressed that the treatment of anxiety and depressive symptoms should be an essential part of the treatment of Alzheimer's disease and other dementias. Reference Azermai, Petrovic, Elseviers, Bourgeois, Van Bortel and Vander Stichele17 Although pharmacological approaches are commonly used for anxiety and depression in dementia, these can have side-effects and remain largely ineffective. Reference Banerjee, Hellier, Dewey, Romeo, Ballard and Baldwin18 Further limitations include only a small number of trials conducted to date with small sample sizes, Reference Lyketsos, DelCampo, Steinberg, Miles, Steele and Munro19 with most studies investigating classes of antidepressants not used routinely in treating depression in people with dementia in clinical practice. Reference Petracca, Chemerinski and Starkstein20,Reference Reifler, Teri, Raskind, Veith, Barnes and White21 Therefore, psychological treatments adapted for use with people with cognitive impairment may offer an alternative approach. Other reviews have concluded that psychotherapy reduces depression in older adults with depressive symptoms Reference Pinquart and Sörensen22 and that psychological treatments can increase general psychological well-being in late-life depressive disorders. Reference Wilson, Mottram and Vassilas23 There are no reviews of studies, however, evaluating psychological treatments in people with dementia and MCI. In contrast to previous reviews, the present review focuses on psychological interventions for people with dementia or MCI, defined as any psychotherapeutic approach aimed at treating depression and anxiety, according to the World Health Organization criteria, such as cognitive–behavioural therapy (CBT), psychodynamic therapy, interpersonal therapy and supportive counselling. 24

So, in comparison to previous reviews evaluating interventions that target anxiety and depression by incorporating some psychological elements (e.g. reminiscence Reference Woods, Spector, Jones, Orrell and Davies25 ), or focusing on environmental changes Reference Gitlin, Winter, Corcoran, Dennis, Schinfeld and Hauck26 or exercise, Reference Rolland, Pillard, Klapouszczak, Reynish, Thomas and Andrieu27 the primary objective of this review was to determine whether psychological interventions reduce depression and anxiety in people with dementia and MCI. Secondary objectives were to assess whether: (a) psychological interventions improve patient quality of life, cognition, activities of daily living (ADL), and reduce behavioural and psychological symptoms of dementia other than anxiety and depression compared with usual care; and (b) whether psychological treatments improve caregiver quality of life or reduce caregiver burden. This article is based on a Cochrane Review by the same authors, with full details of the review published by the Cochrane Library. Reference Orgeta, Qazi, Spector and Orrell28

Method

We searched the Cochrane Dementia and Cognitive Improvement Group's Specialized Register and major healthcare databases, such as MEDLINE, Embase, CINHAL, PsycINFO, ALIOS and LILACS; our search also included a number of grey literature sources. Database searching was completed in January 2013. We searched for all ‘Treatment MCI’ and ‘Treatment Dementia’ studies with additional relevant terms. To view a list of all sources searched for the ALOIS database, see the ALOIS website (www.medicine.ox.ac.uk/alois/). We searched the identified citations for additional trials and contacted the corresponding authors of the identified trials for additional references and unpublished data. We scanned the reference lists of the identified publications and all review papers that were related to depression and anxiety in dementia and MCI.

We included all randomised controlled trials (RCTs) that included a control group (usual care) or comparison group receiving no specific psychological intervention. Additional criteria were that the study provided adequate information about study design and results, and separate data on participants with dementia or MCI. Inclusion criteria for participants were older adults diagnosed with dementia, Alzheimer's disease or organic brain syndrome, according to the DSM-IV, ICD-10 or comparable, and participants with a diagnosis of MCI, in any setting (e.g. home, community, institution). Any definition of MCI was acceptable as long as the criteria used were published and included evidence of objective cognitive impairment but no dementia. Reference Petersen, Smith, Waring, Ivnik, Tangalos and Kokmen29Reference Visser, Scheltens and Verhey31

In this review, we considered any psychological therapy designed to reduce depressive and anxiety symptoms in people with dementia, which was defined as any intervention that: (a) was designed to reduce anxiety and depression or improve adaptive functioning; (b) was based on a psychological theory; and (c) involved a structured interaction between a facilitator and a participant, incorporating psychological methods. Eligible interventions included: (a) CBTs (which include CBT, cognitive analytic therapy, behavioural therapy or behaviour management therapy, brief rational insight and problem-solving therapy); (b) relaxation training therapies (e.g. progressive muscle relaxation); (c) psychodynamic therapies (including brief psychotherapy and insight-orientated psychotherapy); (d) interpersonal therapies; and (e) supportive/counselling therapies. We excluded treatments identified as medication, exercise, reminiscence therapy, music therapy, art and drama therapy, befriending or bibliotherapy.

Control conditions included no treatment (usual care) or a comparison group engaging in non-specific psychosocial activity (e.g. attention control, controlling for effects of staff attention or social contact). We did not consider comparisons with other therapeutic interventions in this review. We included studies that used combinations of different psychological treatments or combinations of pharmacological and psychological interventions. Primary outcomes were depression and anxiety, including clinician, caregiver and self-ratings. Secondary outcomes were patient quality of life, cognition, daily activity level (e.g. ADL), frequency of neuropsychiatric symptoms (e.g. Neuropsychiatric Inventory, NPI), and caregivers' quality of life or experience of caregiver burden.

Two reviewers (V.O., A.Q.) worked independently to identify RCTs that met the inclusion criteria, and extracted data independently. They discussed any disagreements with the fourth (M.O.) and third author (A.S.). We contacted the authors of the primary trials if there were doubts regarding missing data or the methodological details of the trial. We employed the approach recommended by the Cochrane Handbook for Systematic Reviews of Interventions (Cochrane Collaboration, Oxford, UK; see http://handbook.cochrane.org/), for assessing risk of bias, addressing the domains of sequence generation, allocation concealment, masking, incomplete outcome data, selective reporting and other issues. We used a fixed-effects model to represent overall estimate effects. We used standardised mean differences in some of the analyses as not all studies used the same outcome scale. We conducted all calculations with RevMan 5.0 for Windows (Cochrane Collaboration, Oxford, UK; see http://tech.cochrane.org/revman/download). We assessed heterogeneity between the included studies with the chi-squared test. Reference Deeks, Altman, Bradburn, Egger, Smih and Altman32 We considered P-values <0.10 to be statistically significant. We quantified heterogeneity by using the I 2 statistic.

Results

We identified a total of 349 references through database searching (January 2013), with three additional references identified (i.e. reference lists of identified studies and reviews of the literature). After removal of duplicates and clearly irrelevant articles, we retrieved 62 full text records. Of these 62 references, we could exclude 22 at this stage as not relevant, leaving 40 full text references to be fully assessed for eligibility. Of these, we excluded a total of 32 studies as they did not meet the review criteria, one study is ongoing and one study is awaiting classification, with further information required to clarify whether it would meet the inclusion criteria of this review. Thus, we found six studies to be eligible for inclusion. See Fig. 1 for details of the search process.

Fig. 1 Review and meta-analysis flow diagram.

Description of studies

The main study characteristics are shown in online Table DS1. We were able to pool data for depression from all six studies. Reference Burgener, Yang, Gilbert and Marsh-Yant33Reference Waldorff, Buss, Eckermann, Rasmussen, Keiding and Rishøj38 When testing the effects of psychological treatment on anxiety only two studies contributed data. We pooled data from three and two studies for self-rated and caregiver-rated quality of life respectively. We pooled data from two studies to test the effects of psychological treatment on ADL and on the effects on neuropsychiatric symptoms. We pooled four studies for analyses on the effects on cognition. No evidence of heterogeneity was detected in the pooled studies, using the chi-squared test. The final analysis included pooled data from three studies on the effects of caregiver depression. In this analysis heterogeneity was evident.

Primary outcomes

Depression

The first meta-analysis on the effects of psychological treatment on depression included 439 participants. Results significantly favoured psychological treatment (6 studies, standardised mean difference (SMD) −0.22; 95% CI −0.41 to −0.03) in reducing depressive symptoms for people with dementia (Fig. 2), with little heterogeneity between studies (I 2 = 21%).

Fig. 2 Forest plot of psychological treatment versus treatment as usual. Outcome: 1.1 Depression.

Anxiety

Psychological treatment reduced clinician-rated anxiety measured with the Rating Anxiety in Dementia scale (Fig. 3) (2 studies, 65 participants, mean difference (MD) −4.57; 95% CI −7.81 to −1.32). However, there was no effect on self-rated anxiety (Fig. 4) (2 studies, 65 participants, SMD 0.05; 95% CI −0.44 to 0.54) or caregiver-rated anxiety measured with the NPI-Anxiety (Fig. 5) (1 study, 26 participants, MD −2.40; 95% CI −4.96 to 0.16).

Fig. 3 Forest plot of psychological treatment versus treatment as usual. Outcome: 1.2 Anxiety RAID. RAID, Rating Anxiety in Dementia scale.

Fig. 4 Forest plot of psychological treatment versus treatment as usual. Outcome: 1.3 Anxiety (self-ratings).

Fig. 5 Forest plot of psychological treatment versus treatment as usual. Outcome: 1.4 Anxiety NPI-A. NPI-A, Neuropsychiatric Inventory-Anxiety.

Secondary outcomes

Quality of life

Psychological treatment had no effect on patient self-rated quality of life (online Fig. DS1) (3 studies, 334 participants, MD 0.37; 95% CI −1.01 to 1.75) or on caregiver-rated patient quality of life (online Fig. DS2) (2 studies, 313 participants, MD 0.66; 95% CI −0.77 to 2.09).

Activities of daily living

Psychological treatment had no effect on ADL for people with dementia (online Fig. DS3) (2 studies, 313 participants, SMD −0.13; 95% CI −0.35 to 0.09).

Neuropsychiatric symptoms

Psychological treatment had no effect on neuropsychiatric symptoms (online Fig. DS4) (2 studies, 311 participants, SMD 0.06; 95% CI −0.16 to 0.28).

Cognition

Psychological treatment had no effect on cognition (online Fig. DS5) (4 studies, 381 participants, MD −0.80; 95% CI −1.70 to 0.11).

Caregiver depression

Psychological treatment for people with dementia had no effect on caregivers' depressive symptoms (online Fig. DS6) (3 studies, 337 participants, SMD 0.07; 95% CI −0.14 to 0.29), with moderate heterogeneity between studies in this analysis.

Adverse events

None of the studies reported or described any adverse events.

Discussion

The results of six RCTs with a total of 439 participants (216 receiving psychological treatment, 223 in control groups) showed that psychological treatments reduce depressive symptoms in people with dementia. Data from two studies showed that psychological treatments benefit people with dementia by reducing anxiety symptoms measured with a clinician-rated tool. These results compare favourably with recent studies, which found minimal or no benefits of pharmacological interventions in treating depression in dementia. Reference Bains, Birks and Dening39 Although both anxiety and depression were primary outcomes for this review, only two suitable studies included data for anxiety, and there was no effect of psychological treatment on secondary outcomes, such as ADL, quality of life, neuropsychiatric symptoms and cognition, or on caregiver depression.

The psychological therapies considered in this review stem from various theoretical perspectives, and in all studies individual protocols described the therapies in detail. Moreover, all studies targeted symptoms of anxiety and depression through a structured psychological approach (therapist and patient communication), which included directly teaching people with dementia skills to reduce anxiety and depression. Nevertheless, the trials we have included in this review evaluated a range of different psychological interventions and some used a combination of treatments. The length and duration of intervention also varied in the studies, leading to differences in intensity and frequency of the psychological treatment. A limitation of this review, therefore, is the substantial variation between studies in terms of the nature, duration and intensity of the psychological therapy evaluated, which may contribute to difficulties when interpreting the data.

No trials of psychological treatment aimed at people with MCI met our inclusion criteria. The three studies identified either did not employ an RCT design, participants had a cognitive impairment that was not specified according to the established criteria of MCI or the intervention that was evaluated was psychologically based but specifically targeted cognitive decline. None of the studies included reported adverse events.

Quality of the evidence

Risk of bias was unclear for multiple domains in a large proportion of the studies, with the information provided by the published reports proving insufficient to determine the risk of bias associated with key methodological indicators. We classified only one of the studies as low risk in all domains of the Cochrane Collaboration's tool for assessing risk of bias. We classified the remaining five studies as being at unclear risk of bias in certain domains, due to limitations such as uncertainties about random sequence generation, allocation concealment, masking of participants and personnel, and outcome assessment. There was also evidence of selective reporting in one trial. Based on the Grades of Recommendation, Assessment, Development and Evaluation (GRADE) system, we have classified the quality of the evidence as ‘moderate’ for depression and ‘low’ for anxiety, due to the methodological limitations and the limited number of trials.

Overall completeness and applicability of evidence

The studies we included in the present review only partially answered the research questions we posed. Few studies provided data on secondary symptoms of anxiety and we could not perform any subgroup analyses. Most studies to date have been conducted in the USA and Europe, limiting generalisability to the rest of the world. In most studies, information on concurrent psychotropic treatments was limited. Most participants had mild dementia, but one trial was conducted with nursing home residents who had more severe dementia.

The review followed guidelines set out by the Cochrane Collaboration. Reference Higgins and Green40 We used a comprehensive and sensitive strategy to identify studies; the first (V.O.) and second author (A.Q.) independently conducted the selection of studies, data extraction and assessments of risk of bias. The present review presents and discusses all outcomes described in the protocol that were available for analysis, regardless of whether or not there was statistical significance. Finally, it is worth noting that there were differences in terms of acceptance into treatment protocols (for example, the requirement of criteria for anxiety in two trials), which is likely to have resulted in some studies that were overly inclusive and others that exercised more conservative guidelines.

Results showed that psychological treatments are superior to usual care in reducing depression and anxiety, although we were not able to investigate whether they are superior to active controls. However, in some studies the control condition was enriched beyond usual care, as opposed to standard care, indicating that the efficacy of psychological therapies may be potentially underestimated.

The current review is distinctive in systematically analysing psychological interventions to reduce anxiety or depression that are conducted primarily with people with dementia, rather than focusing on environmental changes or skills building for family caregivers. Reference Brodaty and Arasaratnam41 Previous reviews have concentrated on the effectiveness of other interventions of a psychosocial nature (including cognitive stimulation, cognitive rehabilitation, reminiscence and activity-based interventions), which are not aimed specifically at anxiety or depression. Reference Livingston, Johnston, Katona, Paton and Lyketsos42,Reference Olazarán, Reisberg, Clare, Cruz, Peña-Casanova and Del Ser43 These reviews do suggest that non-pharmacological interventions can be useful, and potentially cost-effective, in terms of improving psychological outcomes. Reference Livingston, Johnston, Katona, Paton and Lyketsos42,Reference Olazarán, Reisberg, Clare, Cruz, Peña-Casanova and Del Ser43 However, for some studies there was a lack of clear psychiatric diagnosis of depression or anxiety, or a low baseline level of anxiety and depressive symptoms. These factors limit interpretation of the results, so it is uncertain how far these findings may be applicable for people with a specific diagnosis of anxiety or depression, or with higher baseline levels of depression and anxiety.

Implications for practice and research

There is moderate quality evidence that psychological treatments can reduce depressive symptoms in people with dementia, and limited evidence that they can reduce anxiety. Although the effect size for depression was small, the beneficial effects for anxiety suggest that psychological approaches may be associated with potential improvements in both depressive and anxiety symptoms. The findings of this review compare favourably with limited evidence base on pharmacological treatment for anxiety and current evidence of weak support for the use of antidepressants when treating depression in dementia. Reference Bains, Birks and Dening39 Considering that there were no adverse events reported related to the use of psychological treatments, we can conclude that the observed effects are of meaningful clinical benefit to people with dementia.

The small number of studies in this review and the variations in the type and duration of treatment make it difficult to draw conclusions about the best way to provide psychological treatment. There is a need for well-designed, multicentre RCTs that adhere to the high standards of methodology and reporting, following the Consolidated Standards of Reporting Trials (CONSORT) statement. These trials should focus on standardised theory-based psychological therapies, rather than multimodal approaches which combine a variety of approaches. The lack of follow-up data makes it difficult to use this research to inform evidence-based policy about how best to deliver psychological therapy services, and this is compounded by the lack of data about cost-effectiveness. Future studies should also examine the longer-term effects of psychological treatment for people with dementia.

Acknowledgements

We would like to thank all of the authors that provided data and further information for this review, the Editorial Team and the Review Coordinator of the Cochrane Dementia and Cognitive Improvement Group.

Footnotes

See editorial, pp. 286–287 this issue.

References

1 Enache, D, Winblad, B, Aarsland, D. Depression in dementia: epidemiology, mechanisms, and treatment. Curr Opin Psychiatry 2011; 24: 461–72.CrossRefGoogle ScholarPubMed
2 Weiner, MF, Doody, RS, Sairam, R, Foster, B, Liao, TY. Prevalence and incidence of major depressive disorder in Alzheimer's disease: findings from two databases. Dement Geriatr Cogn Disord 2002; 13: 812.Google Scholar
3 Palmer, K, Berger, AK, Monastero, R, Winblad, B, Bäckman, L, Fratiglioni, L. Predictors of progression from mild cognitive impairment to Alzheimer disease. Neurology 2007; 68: 1596–602.Google Scholar
4 Solfrizzi, V, D'Introno, A, Colacicco, AM, Capurso, C, Del Parigi, A, Caselli, RJ, et al. Incident occurrence of depressive symptoms among patients with mild cognitive impairment: the Italian longitudinal study on aging. Dement Geriatr Cogn Disord 2007; 24: 5564.CrossRefGoogle ScholarPubMed
5 Ballard, C, Neill, D, O'Brien, J, McKeith, IG, Ince, P, Perry, R. Anxiety, depression and psychosis in vascular dementia: prevalence and associations. J Affect Disord 2000; 59: 97106.Google Scholar
6 Lopez, OL, Becker, JT, Sweet, RA. Non-cognitive symptoms in mild cognitive impairment subjects. Neurocase 2005; 11: 6571.Google Scholar
7 Ferreti, L, McCurry, SM, Logsdon, R, Gibbons, L, Teri, L. Anxiety and Alzheimer's disease. J Geriatr Psychiatry Neurol 2001; 14: 52–8.Google Scholar
8 Monastero, R, Mangialasche, F, Camarda, C, Ercolani, S, Camarda, R. A systematic review of neuropsychiatric symptoms in mild cognitive impairment. J Alzheimers Dis 2009; 18: 1130.Google Scholar
9 Gibbons, LE, Teri, L, Logsdon, R, McCurry, SM, Kukull, W, Bowen, J, et al. Anxiety symptoms as predictors of nursing home placement in patients with Alzheimer's disease. J Clin Geropsychol 2002; 8: 335–42.Google Scholar
10 Rozzini, L, Chilovi, BV, Peli, M, Conti, M, Rozzini, R, Trabucchi, M, et al. Anxiety symptoms in mild cognitive impairment. Int J Geriatr Psychiatry 2009; 24: 300–5.Google Scholar
11 Lyketsos, CG, Steele, C, Baker, L, Galik, E, Kopunek, S, Steinberg, M, et al. Major and minor depression in Alzheimer's disease: prevalence and impact. J Neuropsychiatry Clin Neurosci 1997; 9: 556–61.Google Scholar
12 Stern, Y, Tang, MX, Albert, MS, Brandt, J, Jacobs, DM, Bell, K, et al. Predicting time to nursing home care and death in individuals with Alzheimer disease. JAMA 1997; 277: 806–12.Google Scholar
13 González-Salvador, MT, Arango, C, Lyketsos, CG, Barba, AC. The stress and psychological morbidity of the Alzheimer patient caregiver. Int J Geriatr Psychiatry 1999; 14: 701–10.Google Scholar
14 Schultz, SK, Hoth, A, Buckwalter, K. Anxiety and impaired social function in the elderly. Ann Clin Psychiatry 2004; 16: 4751.Google Scholar
15 Devanand, DP, Pelton, GH, Marston, K, Camacho, Y, Roose, SP, Stern, Y. Sertraline treatment of elderly patients with depression and cognitive impairment. Int J Geriatr Psychiatry 2003; 18: 123–30.Google Scholar
16 Lu, PH, Edland, SD, Teng, E, Tingus, K, Petersen, RC, Cummings, JL, et al. Donepezil delays progression to AD in MCI subjects with depressive symptoms. Neurology 2009; 72: 2115–21.Google Scholar
17 Azermai, M, Petrovic, M, Elseviers, MM, Bourgeois, J, Van Bortel, LM, Vander Stichele, RH. Systematic appraisal of dementia guidelines for the management of behavioural and psychological symptoms. Ageing Res Rev 2012; 11: 7886.Google Scholar
18 Banerjee, S, Hellier, J, Dewey, M, Romeo, R, Ballard, C, Baldwin, R, et al. Sertraline or mirtazapine for depression in dementia (HTA-SADD): a randomised, multicentre, double-blind, placebo-controlled trial. Lancet 2011; 378: 403–11.Google Scholar
19 Lyketsos, CG, DelCampo, L, Steinberg, M, Miles, Q, Steele, CD, Munro, C, et al. Treating depression in Alzheimer disease: efficacy and safety of sertraline therapy, and the benefits of depression reduction: the DIADS. Arch Gen Psychiatry 2003; 60: 737–46.Google Scholar
20 Petracca, GM, Chemerinski, E, Starkstein, SE. A double-blind, placebo-controlled study of fluoxetine in depressed patients with Alzheimer's disease. Int Psychogeriatr 2001; 13: 233–40.Google Scholar
21 Reifler, BV, Teri, L, Raskind, M, Veith, R, Barnes, R, White, E, et al. Double-blind trial of imipramine in Alzheimer's disease patients with and without depression. Am J Psychiatry 1989; 146: 45–9.Google Scholar
22 Pinquart, M, Sörensen, S. How effective are psychotherapeutic and other psychosocial interventions with older adults? A meta-analysis. J Ment Health Aging 2001; 7: 207–43.Google Scholar
23 Wilson, KC, Mottram, PG, Vassilas, CA. Psychotherapeutic treatments for older depressed people. Cochrane Database Syst Rev 2008; 23: CD004853.Google Scholar
24 World Health Organization, Regional Office for Europe. Health Evidence Network, 2007 (http://www.euro.who.int/en/data-and-evidence/evidence-informed-policy-making/health-evidence-network-hen).Google Scholar
25 Woods, RT, Spector, AE, Jones, CA, Orrell, M, Davies, SP. Reminiscence therapy for dementia. Cochrane Database Systematic Rev 2009; 2: CD001120.Google Scholar
26 Gitlin, LN, Winter, L, Corcoran, M, Dennis, MP, Schinfeld, S, Hauck, WW. Effects of the home environmental skill-building program on the caregiver-care recipient dyad: 6-month outcomes from the Philadelphia REACH Initiative. Gerontologist 2003; 43: 532–46.Google Scholar
27 Rolland, Y, Pillard, F, Klapouszczak, A, Reynish, E, Thomas, D, Andrieu, S, et al. Exercise program for nursing home residents with Alzheimer's disease: a 1-year randomized, controlled trial. J Am Geriatr Soc 2007; 55: 158–65.CrossRefGoogle ScholarPubMed
28 Orgeta, V, Qazi, A, Spector, AE, Orrell, M. Psychological treatments for depression and anxiety in dementia and mild cognitive impairment. Cochrane Database Syst Rev 2014; 1: CD009125.Google Scholar
29 Petersen, RC, Smith, GE, Waring, SC, Ivnik, RJ, Tangalos, EG, Kokmen, E. Mild cognitive impairment: clinical characterization and outcome. Arch Neurol 1999; 56: 303–8.Google Scholar
30 Petersen, RC. Conceptual Overview. In Mild Cognitive Impairment: Aging to Alzheimer's Disease (ed. Petersen, RC): 114. Oxford University Press, 2003.Google Scholar
31 Visser, PJ, Scheltens, P, Verhey, FR. Do MCI criteria in drug trials accurately identify subjects with predementia Alzheimer's disease? J Neurol Neurosurg Psychiatry 2005; 76: 1348–54.CrossRefGoogle ScholarPubMed
32 Deeks, JJ, Altman, DG, Bradburn, MJ. Statistical methods for examining heterogeneity and combining results from several studies in meta-analysis. In Systematic Reviews in Health Care: Meta-analysis in Context (eds Egger, M, Smih, GD, Altman, DG): 285312. BMJ Books, 2001.Google Scholar
33 Burgener, SC, Yang, Y, Gilbert, R, Marsh-Yant, S. The effects of a multimodal intervention on outcomes of persons with early-stage dementia. Am J Alzheimers Dis Other Demen 2008; 23: 382–94.Google Scholar
34 Burns, A, Guthrie, E, Marino-Francis, F, Busby, C, Morris, J, Russell, E, et al. Brief psychotherapy in Alzheimer's disease. Randomised controlled trial. Br J Psychiatry 2005; 187: 143–7.Google Scholar
35 Spector, A, Orrell, M, Lattimer, M, Hoe, J, King, M, Harwood, K, et al. Cognitive behavioural therapy (CBT) for anxiety in people with dementia: study protocol for a randomised controlled trial. Trials 2012; 13: 197.Google Scholar
36 Stanley, MA, Calleo, J, Bush, AL, Wilson, N, Snow, AL, Kraus-Schuman, C, et al. The peaceful mind program: a pilot test of a cognitive-behavioral therapy-based intervention for anxious patients with dementia. Am J Geriatr Psychiatry 2012; 21: 696708.Google Scholar
37 Tappen, RM, Williams, CL. Therapeutic conversation to improve mood in nursing home residents with Alzheimer's disease. Res Gerontol Nurs 2009; 2: 267–75.Google Scholar
38 Waldorff, FB, Buss, DV, Eckermann, A, Rasmussen, ML, Keiding, N, Rishøj, S, et al. Efficacy of psychosocial intervention in patients with mild Alzheimer's disease: the multicentre, rater blinded, randomised Danish Alzheimer Intervention Study (DAISY). BMJ 2012; 345: e4693.Google Scholar
39 Bains, J, Birks, J, Dening, T. Antidepressants for treating depression in dementia. Cochrane Database Syst Rev 2002; 4: CD003944.Google Scholar
40 Higgins, J, Green, S. Cochrane Handbook for Systematic Reviews of Interventions Version 5.1.0. The Cochrane Collaboration, 2011 (http://handbook.cochrane.org/).Google Scholar
41 Brodaty, H, Arasaratnam, C. Meta-analysis of nonpharmacological interventions for neuropsychiatric symptoms of dementia. Am J Psychiatry 2012; 169: 946–53.Google Scholar
42 Livingston, G, Johnston, K, Katona, C, Paton, J, Lyketsos, CG. Systematic review of psychological approaches to the management of neuropsychiatric symptoms of dementia. Am J Psychiatry 2005; 162: 19962021.Google Scholar
43 Olazarán, J, Reisberg, B, Clare, L, Cruz, I, Peña-Casanova, J, Del Ser, T, et al. Nonpharmacological therapies in Alzheimer's disease: a systematic review of efficacy. Dement Geriatr Cogn Disord 2010; 30: 161–78.Google Scholar
Figure 0

Fig. 1 Review and meta-analysis flow diagram.

Figure 1

Fig. 2 Forest plot of psychological treatment versus treatment as usual. Outcome: 1.1 Depression.

Figure 2

Fig. 3 Forest plot of psychological treatment versus treatment as usual. Outcome: 1.2 Anxiety RAID. RAID, Rating Anxiety in Dementia scale.

Figure 3

Fig. 4 Forest plot of psychological treatment versus treatment as usual. Outcome: 1.3 Anxiety (self-ratings).

Figure 4

Fig. 5 Forest plot of psychological treatment versus treatment as usual. Outcome: 1.4 Anxiety NPI-A. NPI-A, Neuropsychiatric Inventory-Anxiety.

Supplementary material: PDF

Orgeta et al. supplementary material

Supplementary Material

Download Orgeta et al. supplementary material(PDF)
PDF 59.7 KB
Submit a response

eLetters

No eLetters have been published for this article.