nach oben

Erschienen in:

Open Access 01.12.2023 | Research

Clinical characteristics and potential association to Parkinson’s disease and dementia with Lewy bodies in patients with major depressive disorder who received maintenance electroconvulsive therapy: a retrospective chart review study

verfasst von: Shun Kudo, Takahito Uchida, Hana Nishida, Akihiro Takamiya, Toshiaki Kikuchi, Bun Yamagata, Masaru Mimura, Jinichi Hirano

Erschienen in: BMC Psychiatry | Ausgabe 1/2023

Abstract

Background

Maintaining remission after electroconvulsive therapy (ECT) is clinically relevant in patients with depression, and maintenance ECT has been introduced in patients who fail to maintain remission after ECT. However, the clinical characteristics and biological background of patients who receive maintenance ECT are poorly understood. Thus, this study aimed to examine the clinical background of patients who underwent maintenance ECT.

Methods

Patients with major depressive disorder who underwent ECT followed by maintenance ECT (mECT group) and those who did not (acute ECT [aECT] group) were included. Clinical characteristics, including the results of neuroimaging examinations for Parkinson’s disease (PD) and dementia with Levy body (DLB) such as myocardial 123I-metaiodobenzylguanidine (MIBG) scintigraphy and dopamine transporter imaging single-photon emission computerized tomography (DaT-SPECT), were compared between the groups.

Results

In total, 13 and 146 patients were included in the mECT and aECT groups, respectively. Compared to the aECT group, the mECT group showed a significantly higher prevalence of melancholic features (92.3% vs. 27.4%, p < 0.001) and catatonic features (46.2% vs. 9.6%, p = 0.002). Overall, 8 of the 13 patients in the mECT group and 22 of the 146 patients in the aECT group underwent neuroimaging examinations for PD/DLB. The rate of patients examined is significantly higher in the mECT group than in the aECT group (61.5% vs. 11.2%, p < 0.001). Among the groups examined, 7/8 patients in the mECT group and 16/22 patients in the aECT group showed relevant neuroimaging findings for PD/DLB; the positive rate was not significantly different between the two groups (87.5% vs. 72.7%, p = 0.638).

Conclusions

Patients who receive acute and maintenance ECT may have underlying neurodegenerative diseases, including PD/DLB. Investigating the neurobiology of patients who receive maintenance ECT is important for developing appropriate treatments for depression.

Publisher’s Note

Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.

TRD

Treatment-Resistant Depression

ECT

Electroconvulsive Therapy

MDD

Major Depressive Disorder

Parkinson’s disease

DLB

Dementia with Lewy Bodies

DSM

Diagnostic Statistical Manual of Mental Disorders

MIBG

123I-Metaiodobenzylguanidine

DaT-SPECT

Dopamine Transporter Imaging Single-Photon Emission Computerized Tomography

CGI-S

Clinical Global Impression–Severity Scale

c-CGI

Clinical Global Impression Improvement scale

Introduction

Depression is a debilitating mental disorder that requires treatment with different modalities [1, 2] and the response rate is only 43–53% and 42–64% with pharmacotherapy and cognitive behavioral therapy, respectively [3‐5]. Given the evidence for the lower efficacy of pharmacotherapy in older patients with depression [6], it is important to consider interventions beyond pharmacotherapy for this population. Patients with depression who fail to respond to multiple treatments are considered to have treatment-resistant depression (TRD), and electroconvulsive therapy (ECT) has been used for TRD [1]. ECT is regarded as an effective treatment for TRD, with a remission rate of 50–60% [7, 8]. In addition, a meta-analysis indicated that older age is a predictor for good response to ECT [9], implying that ECT may be a reasonable treatment option for this population. However, previous studies have shown that 40–60% of patients relapse after acute ECT, even with continuous treatment with antidepressants [10‐12], and patients do not respond adequately to pharmacotherapy in relapse after ECT [12]. Thus, patients who subsequently relapse after ECT might be regarded as the most severe cases, and maintenance ECT is reported to provide therapeutic benefits for these patients [13].

Maintenance ECT is defined as treatment with ECT once every 1–3 months for at least 6 months [14, 15], and approximately 10–15% of patients with affective disorders require maintenance ECT [16]. Accumulating evidence indicates the efficacy of maintenance ECT for the relapse and recurrence of depression. Patients who received maintenance ECT plus pharmacotherapy after acute ECT had a 54% lower risk of recurrence and relapse at 12 months than did those who received pharmacotherapy alone [13]. Moreover, in older patients with psychotic depression, the 2-year relapse rate was only 8% with nortriptyline plus maintenance ECT and 62% with nortriptyline alone [17]. The American Psychiatric Association guideline for the treatment of major depressive disorder (MDD) also recommends maintenance ECT as a treatment for patients with TRD who fail to maintain remission with pharmacotherapy and psychotherapy and have a history of response to acute ECT [18]. Thus, maintenance ECT is the treatment of choice for patients who have experienced the most difficulty in maintaining remission, and it is not uncommon to encounter such patients in clinical settings. However, limited attention has been paid to the clinical background of patients undergoing maintenance ECT.

Several studies have focused on the association of depression with Parkinson’s disease (PD) and with dementia with Lewy bodies (DLB). A Swedish longitudinal follow-up cohort study reported that the risk of PD was three times higher in patients diagnosed with depression over the age of 50 than in the control group [19]. In addition, recent studies have pointed out that potential factors in older adults with MDD might be due to progressive neurodegenerative disorder or vulnerability [20]. A Japanese study reported that 13.8% of patients diagnosed with depression at age ≥ 50 years were diagnosed with DLB after hospitalization [21]. Moreover, 50% of patients with PD have depressive symptoms [22], and antidepressants are less effective for depression associated with PD [23]. Thus, it has been suggested that depression might be associated with PD and DLB, and depression associated with PD may be linked to treatment resistance [23].

This study aimed to examine the clinical background of patients who underwent maintenance ECT, including neuroimaging markers associated with PD and DLB. Towards this goal, we performed a chart review using a dataset of the ECT cohort that included patients who received maintenance ECT and those who did not, and compared the clinical factors between these patients.

Materials and methods

Study design and patients

This study was approved by the ethics committee of Keio University School of Medicine, Tokyo, Japan. The need for written informed consent for this study was waived under the validation of the ethics committee. We further confirm that all methods were employed in accordance with relevant guidelines and regulations. Data were obtained from the Keio Neuropsychiatric ECT database. The database included patients who underwent ECT for treatment of depressive episodes at Keio University Hospital, Tokyo, Japan. In our institution, acute ECT sessions are performed for patients with depression refractory to medications, the need for rapid recovery, and/or according to the patients/relatives’ preference for ECT. Meanwhile, maintenance ECT is provided to patients who fail to maintain remission after acute ECT based on the clinical decision of the psychiatrist in charge.

The current study included patients registered between April 2012 and March 2019. The inclusion criteria were as follows: (1) met the diagnostic criteria for MDD according to the Diagnostic Statistical Manual of Mental Disorders (DSM) IV-TR or DSM-5 [24, 25], as determined by at least two certified psychiatrists and (2) received acute ECT alone or acute ECT followed by maintenance ECT for the treatment of depressive episodes during the study period. The exclusion criteria were those who received acute ECT before the study period and had already been started on maintenance ECT. For patients who received several acute ECTs during the study period, the first acute ECT was selected for our analysis.

Maintenance ECT was defined as treatment with ECT for > 6 months according to the criteria used in the meta-analysis by Elias et al. [13]. The course of ECT other than maintenance ECT was defined as acute ECT. The patients who underwent maintenance ECT were categorized to the mECT group, while the other patients were categorized to the acute ECT (aECT) group.

ECT procedure

All patients were treated with bitemporal stimulation using a half-age method with a brief-pulse (0.5 ms) square-wave ECT device (Thymatron System IV devices; Somatics, Inc., Lake Bliff, IL, USA) for each ECT session. General anesthesia was induced via intravenous administration of sodium thiopental (3–5 mg/kg), propofol (1 mg/kg), or sevoflurane. Succinylcholine (0.5–1.0 mg/kg) was used to induce muscle relaxation. A two-channel electroencephalogram was monitored to ensure adequate seizure duration. The patients were re-stimulated at a higher intensity (i.e., a 50% increase) when the seizure duration was less than 20 s.

Acute ECT was performed two–three times per week until a stable response was obtained or until no response to acute ECT was confirmed. The number of ECT sessions for each acute ECT was decided by the psychiatrist in charge based on clinical judgement. Maintenance ECT was considered for patients who relapsed within a short period after acute ECT even with adequate antidepressants. The psychiatrist in charge made the decision to introduce maintenance ECT to these patients, and the interval between each maintenance ECT session was decided based on clinical observations. If a patient who had received maintenance ECT developed an acute worsening of their depressive symptoms, the patient underwent acute ECT, and maintenance ECT was re-introduced after symptomatic improvement was achieved.

Data collection

We extracted clinical information at the time of the first acute ECT for both the mECT and aECT groups, including sex, age at the first ECT, age at MDD onset, number of ECT sessions, number of previous depressive episodes, duration of MDD, duration of the current depressive episode, number of suicidal attempts during the current depressive episode, and family history of MDD. We also extracted the dosage of psychotropics prescribed for included subjects on the day before the first ECT session and converted to a Defined Daily Dose (DDD) [26]. To evaluate cognitive function, we obtained the Mini Mental State Examination (MMSE) score before and after the acute ECT sessions.

Furthermore, the results of neuroimaging markers for PD/DLB, including myocardial 123I-metaiodobenzylguanidine (MIBG) scintigraphy and dopamine transporter imaging single-photon emission computerized tomography (DaT-SPECT), were collected for both the mECT and aECT groups during the study period. These were ordered when psychiatrists or neurologists suspected complications of PD/DLB based on clinical symptoms, including motor symptoms or cognitive symptoms associated with PD or DLB.

Myocardial MIBG scintigraphy and DaT-SPECT have been shown to be helpful in the diagnosis of PD and DLB. DLB Consortium guidelines indicate reduced dopamine transporter uptake in the basal ganglia on SPECT and reduced myocardial MIBG uptake as indicative biomarkers of DLB [27]. In addition, the clinical guideline for PD published by the Movement Disorder Society suggested reduced myocardial MIBG uptake as supportive criteria for PD diagnosis. Further, normal functional neuroimaging of the presynaptic dopaminergic system was indicated as the absolute exclusion criteria for PD [28].

In our institution, myocardial MIBG scintigraphy involves intravenous administration of 111 MBq of 3-iodobenzylguanidine (123I), followed by cardiac scintigraphy using a gamma camera at 15 min and 3–6 h after injection. An early H/M ratio of less than 2.51 or delayed H/M ratio of less than 2.2 is considered positive for myocardial MIBG scintigraphy [29]. In DaT-SPECT, 111–185 MBq of ioflupane (123I) is administered intravenously, and scintigraphy of the head is obtained at 3–6 h intervals. A specific binding ratio of ≤ 4.5 is considered positive for DaT-SPECT [30]. In this study, patients were classified as having a PD/DLB pattern if either the DaT-SPECT or myocardial MIBG scintigraphy results was positive.

Baseline severity of illness was assessed using the Clinical Global Impression–Severity Scale (CGI-S). Briefly, the CGI-S is a 7-point scale, where one means normal or not at all ill, and seven means the most severely ill [31]. In addition, the presence of psychotic, melancholic, and catatonic features, defined based on the criteria of the DSM-IV-TR or DSM-5 at baseline, was also assessed. Treatment response to acute ECT courses was assessed using the clinical Global Impression Improvement scale (c-CGI) [32]. The c-CGI is a 4-point scale where 1 means excellent response and 4 means poor response. This scale has been used in previous retrospective chart reviews of acute ECT. Three board-certified psychiatrists (A.T., T.U., and H.J.) retrospectively assessed CGI-S, presence of psychotic, melancholic, and catatonic features, and c-CGI independently based on the patients’ medical charts, and any disagreements were resolved by discussion.

Statistical analyses

First, clinical characteristics and symptoms were compared between the mECT and aECT groups. Second, because the comparison of all patients with different observation periods may be qualitatively different, we compared patients who had been followed up in our institute for more than 1 year between the aECT group and the mECT group. Third, the mECT group was divided into patients with and without the PD/DLB pattern, and the differences in clinical characteristics between the groups were investigated. Differences in participant characteristics between groups were examined using an independent t-test for continuous variables and χ2 analysis for categorical variables. All statistical analyses were performed using SPSS version 25.0 (IBM corporation, NY, USA). All analyses were two sided, with an α level of 0.05.

Results

In total, 159 patients were included in the analysis; of them, 13 and 146 patients were categorized to the mECT and aECT groups, respectively. The intervals between ECT sessions in the mECT group ranged from 2 to 10 weeks. Table 1 summarizes the clinicodemographic characteristics of the patients. The age at onset and age at first ECT were significantly higher in the mECT group. There was no difference in the number of acute ECT sessions between the two groups. Regarding clinical symptoms, the prevalence of melancholic and catatonic features was significantly higher in the mECT group, although the baseline severity was not significantly different between the groups. The treatment response to acute ECT and DDD of psychotropics just before the first ECT session was also not significantly different between the groups. There were also no differences in cognitive function before and after ECT between the two groups.

Table 1

Clinical and demographic characteristics of the mECT and aECT groups

	mECT (n = 13)	aECT		mECT vs all aECT p-value	mECT vs. over 1-year aECT p-value
	mECT (n = 13)	All (n = 146)	Followed up over 1 year (n = 73)	mECT vs all aECT p-value	mECT vs. over 1-year aECT p-value
Male sex	3 (23.1)	64 (43.8)	26 (35.6)	0.146	0.529
Age at the first ECT (years)	76.7 [7.4]	62.0 [14.6]	63.5 [13.6]	< 0.001	0.002
Age at MDD onset (years)	64.0[9.1]	55.3 [7.2]	56.5 [16.0]	0.007	0.009
Number of ECT sessions	9.15 [1.62]	8.99 [2.64]	9.32 [2.50]	0.829	0.824
Number of previous depressive episodes	3.5 [1.9]	2.3 [1.8]	2.4 [1.8]	0.016	0.039
Duration of MDD (months)	75.3 [56.7]	76.4 [88.2]	80.8 [96.9]	0.966	0.239
Duration of the current depressive episode (months)	10.1 [9.5]	18.8 [38.2]	18.0 [41.4]	0.414	0.495
Number of suicide attempts	2 (15.4)	20 (13.7)	9 (12.3)	0.564	0.670
Family history of MDD	1 (7.7)	28 (19.2)	16 (21.9)	0.465	0.449
Melancholic features	12 (92.3)	40 (27.4)	15 (20.5)	< 0.001	< 0.001
Psychotic features	3 (23.1)	48 (32.9)	24 (32.9)	0.350	0.747
Catatonic features	6 (46.2)	14 (9.6)	5 (6.8)	0.002	< 0.001
Baseline CGI-S	5.4 [1.3]	4.8 [1.4]	4.8 [1.4]	0.140	0.187
Post-treatment c-CGI	1.4 [0.7]	1.6 [0.9]	1.4 [0.7]	0.475	0.815
DDD at pre-ECT
Antidepressants	0.96 [0.89]	1.24 [0.95]	1.22 [1.01]	0.298	0.381
Antipsychotics	0.19[0.26]	0.29 [0.58]	0.28 [0.49]	0.525	0.492
Anti-anxiety drugs	0.15 [0.21]	0.14 [0.35]	0.18 [0.44]	0.892	0.818
Hypnotics	0.31 [0.43]	0.74 [0.95]	0.71 [0.76]	0.106	0.065
Anti-epileptic drugs	0	18.8 [38.2]	0	0.498	n/a
Mood stabilizers	0	0.02 [0.20]	0	0.764	n/a
Antidementia drugs	0	0.01 [0.06]	0.01 [0.09]	0.683	0.564
Number of prescriptions at pre-ECT
Antidepressants	9 (69.2)	122 (83.6)	62 (84.9)	0.226	0.215
Antipsychotics	7 (53.8)	71 (48.6)	35 (47.9)	0.772	0.728
Anti-anxiety drugs	5 (38.4)	27 (18.5)	14 (19.2)	0.143	0.154
Hypnotics	5 (38.4)	81 (55.5)	45 (61.6)	0.207	0.105
Anti-epileptic drugs	0	6 (4.1)	0	0.451	0.762
Mood stabilizers	0	1 (0.7)	0	0.762	n/a
Antidementia drugs	0	2 (1.4)	2 (2.7)	0.671	0.546
MMSE at pre-ECT ^a	24.67 [4.51]	27.39 [2.81]	27.21 [3.15]	0.112	0.202
MMSE at post-ECT ^b	24.00 [2.65]	27.11 [3.10]	27.00 [3.49]	0.097	0.168

Data are present as the mean [SD] or n (%)

^amECT, all aECT, and 1 year followed up aECT included 3, 66, and 33 patients, respectively

^bmECT, all aECT, and 1 year followed up aECT included 3, 46, and 22 patients, respectively

aECT Acute electroconvulsive therapy, cCGI Clinical Global Impression Improvement scale, CGI-S Clinical Global Impression–Severity Scale, DDD Defined Daily Dose, mECT Maintenance electroconvulsive therapy, MDD Major depressive disorder, MMSE Mini Mental State Examination

The comparison results between the subgroup of patients in the aECT group who were followed up for more than 1 year after acute ECT (n = 73) and the patients in the mECT group are also shown in Table 1. The results also indicated a higher age of onset, higher age of the first ECT, higher prevalence of melancholic and catatonic features in the mECT group, and no significant difference in baseline severity and treatment response to acute ECT between the groups.

Overall, 8 of the 13 patients (61.5%) in the mECT group underwent examination for neuroimaging markers for PD/DLB for motor symptoms (n = 4), cognitive symptoms (n = 2), and other reasons (n = 2). Meanwhile, 22 of the 146 patients (11.2%) in the aECT group underwent examination for neuroimaging markers for PD/DLB for motor symptoms (n = 13), cognitive symptoms (n = 5), and other reasons (n = 4). The frequency of neuroimaging marker examinations for PD/DLB was significantly higher in the mECT group compared to that in the aECT group (p < 0.001) (Fig. 1a). However, the rate of positive results for neuroimaging markers for PD/DLB was not significantly different between the two groups {7/8 (87.5%) in the mECT group vs. 16/22 (72.7%) in the aECT group, p = 0.638} (Fig. 1b). There were no significant differences in any characteristics between patients with PD/DLB pattern (n = 7) and those without PD/DLB pattern (n = 6) in the mECT group.

Discussion

The clinical characteristics and biological background of patients who receive maintenance ECT are yet to be fully elucidated. The current study showed a higher age of onset, higher age of first ECT, and higher prevalence of melancholic and catatonic features in patients who underwent maintenance ECT than in those who did not. Furthermore, 7 of 13 patients who underwent maintenance ECT showed a PD/DLB pattern, potentially suggesting unique biological characteristics in these patients. However, the positive rate of neuroimaging markers for PD/DLB in the mECT group was not significantly different from that of the aECT group. To the best of our knowledge, this is the first study to focus on the clinical characteristics, including the results of neuroimaging markers for PD/DLB, in patients who underwent maintenance ECT.

The clinical characteristics of the mECT group compared to the aECT group in this study were consistent with the clinical characteristics reported of TRD compared to the non-TRD group [33‐35]. That is, clinical characteristics, including old age of onset and melancholic and catatonic features, may be indicators of treatment resistance at all stages of depression and may provide a rationale for the choice of therapies other than conventional antidepressant therapy for depression patients with these features.

The finding that approximately 40% of patients in the mECT group and 15% of patients in the aECT group showed a positive rate of PD/DLB pattern highlights the potential biological background of these patients. Although the rate of positive PD/DLB patterns was not significantly different between the mECT and aECT groups, a significantly higher proportion of patients in the mECT group underwent examination for neuroimaging markers. These findings suggested that a greater proportion of patients in the mECT group had underlying neurodegeneration. In a prospective cohort study [19], 1.1% of patients with depression had comorbidity with PD, and this rate is much lower than that reported in the present study. The high proportion of PD/DLB patterns in the current study suggest that PD/DLB pathology may be involved in the context of treatment resistance in depression. Indeed, depression associated with PD has been reported to respond inadequately to conventional antidepressants, and dopamine dysfunction may be implicated in treatment resistance [23, 36]. Meanwhile, ECT has been reported to be effective for depression associated with PD [37]. Animal studies show that ECT increases D1 and D3 binding in the striatum [38] and increases D1 receptor binding and vesicular monoamine transporter type 2 binding [39]. Thus, ECT acts on the dopaminergic system and may be an effective treatment for depression in the context of dopaminergic abnormalities.

The biological changes that occur in patients undergoing maintenance ECT is still unclear. Our finding that 40% of the patients in the maintenance ECT group had a PD pattern suggests that the development of PD pathology may be related to treatment resistance. Whether the manifestation of PD is caused by maintenance ECT or whether maintenance ECT is only used in the severely depressed group is a topic beyond the focus of this study; however, the various biological effects of maintenance ECT in severely depressed patients should be continued to be examined.

Our study had the following limitations. First, because we did not systematically assess symptoms associated with PD/DLB for all included subjects, we could not diagnose PD or DLB as a comorbidity, even with positive results for neuroimaging markers for PD/DLB. Second, the mECT group could receive more frequent medical assessments than could the aECT group and therefore had a greater probability of receiving neuroimaging markers for PD/DLB, which may have contributed to the higher rate of examination in the mECT group. Third, due to the small sample size, some factors associated with the mECT group may have been overlooked due to type 2 error. Further studies with a larger sample size and a systematic assessment of PD and DLB are warranted to investigate the pathophysiology of treatment-resistant depression.

Conclusion

The current study found a higher age at onset, higher age at the first ECT, and higher prevalence of melancholic and catatonic features in patients who underwent maintenance ECT. Furthermore, the results of neuroimaging markers for PD/DLB implied that patients who underwent acute and maintenance ECT have impaired dopamine function or postganglionic cardiac autonomic denervation, which are associated with PD/DLB. Investigating the neurobiology of patients who receive maintenance ECT is important for the development of appropriate treatments for depression.

Acknowledgements

The authors thank Akihiro Hamada, M.D, Makiko Inaoka, M.D, Manato Isobe, M.D, Saori Katayama, M.D, Yuhei Kikuchi, M.D, Shin Kurose, M.D, Narihisa Nitta, M.D, Hiroki Oi, M.D, Mutsuki Sakuma, M.D, Kyousuke Sawada, M.D, Yutarou Shimomura, M.D, Asuka Shiomi, M.D, Shoutarou Takasu, M.D, Masataka Wada, M.D, Michihiko Waki, M.D, Ryo Watanabe, M.D, Mariko Kimura, M.A, and Taisuke Yatomi, M.D, for data collection. The authors also thank Yuki Arita, M.D, Ph.D, for advices on interpretation of the results of neuroimaging markers for PD/DLB. All except Yuki Arita are from the Department of Neuropsychiatry, Keio University School of Medicine, Tokyo, Japan, and Yuki Arita is from the Department of Radiology, Keio University School of Medicine, Tokyo, Japan. All have no conflicts of interest to declare.

Declarations

This study was approved by the ethics committee of Keio University School of Medicine, Tokyo, Japan. The waiver for consent to participate is provided by the ethics committee of Keio University School of Medicine, Tokyo, Japan. We further confirm that all methods were employed in accordance with relevant guidelines and regulations.

Not applicable.

Competing interests

TU has received grants from SENSHIN Medical Research Foundation (Osaka, Japan) within the past two years. BY has received grants from Brain Energy Inc (Tokyo, Japan) within the past two years. MM has received speaker’s honoraria from Biogen Japan, Byer Pharmaceutical, Daiichi Sankyo, Dainippon-Sumitomo Pharma, Demant Japan, Eisai, Eli Lilly, Fuji Film RI Pharma, Hisamitsu Pharmaceutical, H.U. Frontier, Janssen Pharmaceutical, Mochida Pharmaceutical, MSD, Mylan EPD, Nippon Chemipher, Novartis Pharma, Ono Yakuhin, Otsuka Pharmaceutical, Pfizer, Shionogi, Takeda Yakuhin, Teijin Pharma, and Viatris within the past two years. Also, he received grants from Daiichi Sankyo, Eisai, Fronteo, Shionogi, Takeda, Tanabe Mitsubishi and Tsumura within the past two years outside the submitted work. JH has received speaker’s honoraria from Dainippon-Sumitomo Pharma within the past two years.

All other authors declare that they have no competing interests.

Open AccessThis article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons licence, and indicate if changes were made. The images or other third party material in this article are included in the article's Creative Commons licence, unless indicated otherwise in a credit line to the material. If material is not included in the article's Creative Commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this licence, visit http://creativecommons.org/licenses/by/4.0/. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated in a credit line to the data.

Publisher’s Note

Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.

Weiss A, Hussain S, Ng B, Sarma S, Tiller J, Waite S, et al. Royal Australian and New Zealand College of Psychiatrists professional practice guidelines for the administration of electroconvulsive therapy. Aust N Z J Psychiatry. 2019;53:609–23.CrossRefPubMed

Vigo D, Thornicroft G, Atun R. Estimating the true global burden of mental illness. Lancet Psychiatry. 2016;3:171–8.CrossRefPubMed

Cuijpers P, Karyotaki E, Ciharova M, Miguel C, Noma H, Furukawa TA. The effects of psychotherapies for depression on response, remission, reliable change, and deterioration: A meta-analysis. Acta Psychiatr Scand. 2021;144:288–99.CrossRefPubMedPubMedCentral

Keller MB, McCullough JP, Klein DN, Arnow B, Dunner DL, Gelenberg AJ, et al. A comparison of nefazodone, the cognitive behavioral-analysis system of psychotherapy, and their combination for the treatment of chronic depression. N Engl J Med. 2000;342:282–90.CrossRef

Murphy GE, Simons AD, Wetzel RD, Lustman PJ. Cognitive therapy and pharmacotherapy. Singly and together in the treatment of depression. Arch Gen Psychiatry. 1984;41:33–41.CrossRefPubMed

Mallery L, MacLeod T, Allen M, McLean-Veysey P, Rodney-Cail N, Bezanson E, et al. Systematic review and meta-analysis of second-generation antidepressants for the treatment of older adults with depression: questionable benefit and considerations for frailty. BMC Geriatr. 2019;19:306.CrossRefPubMedPubMedCentral

Dierckx B, Heijnen WT, van den Broek WW, Birkenhäger TK. Efficacy of electroconvulsive therapy in bipolar versus unipolar major depression: a meta-analysis. Bipolar Disord. 2012;14:146–50.CrossRefPubMed

Geddes J, Carney S, Cowen P, Goodwin G, Rogers R, Dearness K, et al. Efficacy and safety of electroconvulsive therapy in depressive disorders: a systematic review and meta-analysis. Lancet. 2003;361:799–808.CrossRef

Yao Z, McCall WV, Essali N, Wohl E, Parker C, Rosenquist PB, et al. Precision ECT for major depressive disorder: A review of clinical factors, laboratory, and physiologic biomarkers as predictors of response and remission. Pers Med Psychiatry. 2019;17–18:23–31.

10.

Jelovac A, Kolshus E, McLoughlin DM. Relapse following successful electroconvulsive therapy for major depression: A meta-analysis. Neuropsychopharmacology. 2013;38:2467–74.CrossRefPubMedPubMedCentral

11.

Rasmussen KG, Mueller M, Rummans TA, Husain MM, Petrides G, Knapp RG, et al. Is baseline medication resistance associated with potential for relapse after successful remission of a depressive episode with ECT? Data from the Consortium for Research on Electroconvulsive Therapy (CORE). J Clin Psychiatry. 2009;70:232–7.CrossRefPubMed

12.

Sackeim HA, Haskett RF, Mulsant BH, Thase ME, Mann JJ, Pettinati HM, et al. Continuation pharmacotherapy in the prevention of relapse following electroconvulsive therapy: A randomized controlled trial. J Am Med Assoc. 2001;285:1299–307.CrossRef

13.

Elias A, Phutane VH, Clarke S, Prudic J. Electroconvulsive therapy in the continuation and maintenance treatment of depression: Systematic review and meta-analyses. Aust N Z J Psychiatry. 2018;52:415–24.CrossRefPubMed

14.

Elias A, Chathanchirayil SJ, Bhat R, Prudic J. Maintenance electroconvulsive therapy up to 12 years. J Affect Disord. 2014;156:228–31.CrossRefPubMed

15.

American Psychiatric Association. The practice of electroconvulsive therapy : recommendations for treatment, training, and privileging : a task force report of the American Psychiatric Association. 2001.

16.

Abrams R. Electroconvulsive therapy. 2002.

17.

Gill SP, Kellner CH. Clinical Practice Recommendations for Continuation and Maintenance Electroconvulsive Therapy for Depression: Outcomes from a Review of the Evidence and a Consensus Workshop Held in Australia in May 2017. J ECT. 2019;35:14–20.CrossRefPubMed

18.

American Psychiatric Association. Practice Guideline For The Treatment of Patients With Major Depressive Disorder 3rd edition. 2010.

19.

Gustafsson H, Nordström A, Nordström P. Depression and subsequent risk of Parkinson disease A nationwide cohort study. Neurology. 2015;84:2422–9.CrossRefPubMedPubMedCentral

20.

Kawakami I, Iga J ichi, Takahashi S, Lin YT, Fujishiro H. Towards an understanding of the pathological basis of senile depression and incident dementia: Implications for treatment. Psychiatry Clin Neurosci. 2022;76:620–32.CrossRefPubMed

21.

Takahashi S, Mizukami K, Yasuno F, Asada T. Depression associated with dementia with Lewy bodies (DLB) and the effect of somatotherapy. Psychogeriatrics. 2009;9:56–61.CrossRefPubMed

22.

Baquero M. Depressive symptoms in neurodegenerative diseases. World J Clin Cases. 2015;3:682.CrossRefPubMedPubMedCentral

23.

Rocha FL, Murad MGR, Stumpf BP, Hara C, Fuzikawa C. Antidepressants for depression in Parkinson’s disease: Systematic review and meta-analysis. J Psychopharmacol. 2013;27:417–23.CrossRefPubMed

24.

American Psychiatric Association. Diagnostic and Statistical Manual of Mental Disorders 5th edition (DSM-5). 2013.CrossRef

25.

American Psychiatric Association. Diagnostic and Statistical Manual of Mental Disorders 4th edition, Text Revision (DSM-IV-TR). 2000.CrossRef

26.

Nosè M, Tansella M, Thornicroft G, Schene A, Becker T, Veronese A, et al. Is the Defined Daily Dose system a reliable tool for standardizing antipsychotic dosages? Int Clin Psychopharmacol. 2008;23:287–90.CrossRefPubMed

27.

McKeith IG, Boeve BF, DIckson DW, Halliday G, Taylor JP, Weintraub D, et al. Diagnosis and management of dementia with Lewy bodies: Fourth consensus report of the DLB Consortium. Neurology. 2017;89:88–100.CrossRefPubMedPubMedCentral

28.

Postuma RB, Berg D, Stern M, Poewe W, Olanow CW, Oertel W, et al. MDS clinical diagnostic criteria for Parkinson’s disease. Mov Disord. 2015;30:1591–601.CrossRefPubMed

29.

Komatsu J, Samuraki M, Nakajima K, Arai H, Arai H, Arai T, et al. 123I-MIBG myocardial scintigraphy for the diagnosis of DLB: a multicentre 3-year follow-up study. J Neurol Neurosurg Psychiatry. 2018;89:1167–73.CrossRefPubMed

30.

Tossici-Bolt L, Hoffmann SMA, Kemp PM, Mehta RL, Fleming JS. Quantification of [123I]FP-CIT SPECT brain images: An accurate technique for measurement of the specific binding ratio. Eur J Nucl Med Mol Imaging. 2006;33:1491–9.CrossRefPubMed

31.

Guy W. ECDEU assessment manual for psychopharmacology. 1976.

32.

Kaster TS, Goldbloom DS, Daskalakis ZJ, Mulsant BH, Blumberger DM. Electroconvulsive therapy for depression with comorbid borderline personality disorder or post-traumatic stress disorder: A matched retrospective cohort study. Brain Stimul. 2018;11:204–12.CrossRefPubMed

33.

Cepeda MS, Reps J, Ryan P. Finding factors that predict treatment-resistant depression: Results of a cohort study. Depress Anxiety. 2018;35:668–73.CrossRefPubMedPubMedCentral

34.

De Carlo V, Calati R, Serretti A. Socio-demographic and clinical predictors of non-response/non-remission in treatment resistant depressed patients: A systematic review. Psychiatry Res. 2016;240:421–30.CrossRefPubMed

35.

Suija K, Aluoja A, Kalda R, Maaroos HI. Factors associated with recurrent depression: A prospective study in family practice. Fam Pract. 2011;28:22–8.CrossRefPubMed

36.

Galts CPC, Bettio LEB, Jewett DC, Yang CC, Brocardo PS, Rodrigues ALS, et al. Depression in neurodegenerative diseases: Common mechanisms and current treatment options. Neurosci Biobehav Rev. 2018;2019(102):56–84.

37.

Takamiya A, Seki M, Kudo S, Yoshizaki T, Nakahara J, Mimura M, et al. Electroconvulsive Therapy for Parkinson’s Disease: A Systematic Review and Meta-Analysis. Mov Disord. 2021;36:50–8.CrossRefPubMed

38.

Strome EM, Zis AP, Doudet DJ. Electroconvulsive shock enhances striatal dopamine D1 and D3 receptor binding and improves motor performance in 6-OHDA-lesioned rats. J Psychiatry Neurosci. 2007;32:193.PubMedPubMedCentral

39.

Landau AM, Clark C, Jivan S, Doudet DJ. Antiparkinsonian mechanism of electroconvulsive therapy in MPTP-lesioned non-human primates. Neurodegener Dis. 2012;9:128–38.CrossRefPubMed

Titel: Clinical characteristics and potential association to Parkinson’s disease and dementia with Lewy bodies in patients with major depressive disorder who received maintenance electroconvulsive therapy: a retrospective chart review study
verfasst von: Shun Kudo
Takahito Uchida
Hana Nishida
Akihiro Takamiya
Toshiaki Kikuchi
Bun Yamagata
Masaru Mimura
Jinichi Hirano
Publikationsdatum: 01.12.2023
Verlag: BioMed Central
Erschienen in: BMC Psychiatry / Ausgabe 1/2023
Elektronische ISSN: 1471-244X
DOI: https://doi.org/10.1186/s12888-023-04743-7

Live-Webinar "Urologie und Sexualmedizin in der Praxis"

Springer Medizin

Clinical characteristics and potential association to Parkinson’s disease and dementia with Lewy bodies in patients with major depressive disorder who received maintenance electroconvulsive therapy: a retrospective chart review study