Effects of electroconvulsive therapy on cortical thickness in depression: a systematic review

Tommaso Toffanin; Giulia Cattarinussi; Niccolò Ghiotto; Marialaura Lussignoli; Chiara Pavan; Luca Pieri; Sami Schiff; Francesco Finatti; Francesca Romagnolo; Federica Folesani; Maria Giulia Nanni; Rosangela Caruso; Luigi Zerbinati; Martino Belvederi Murri; Maria Ferrara; Giorgio Pigato; Luigi Grassi; Fabio Sambataro

doi:10.1017/neu.2024.6

Effects of electroconvulsive therapy on cortical thickness in depression: a systematic review

Published online by Cambridge University Press: 12 February 2024

Tommaso Toffanin ,

Giulia Cattarinussi

Niccolò Ghiotto ,

Marialaura Lussignoli ,

Chiara Pavan ,

Luca Pieri ,

Sami Schiff ,

Francesco Finatti ,

Francesca Romagnolo and

Federica Folesani

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Tommaso Toffanin: Affiliation:
Department of Neuroscience and Rehabilitation, Institute of Psychiatry, University of Ferrara, Ferrara, Italy
Giulia Cattarinussi: Affiliation:
Department of Neuroscience (DNS), University of Padova, Padua, Italy Padova Neuroscience Center, University of Padova, Padua, Italy Department of Psychological Medicine, Institute of Psychiatry, Psychology and Neuroscience, Kings College London, London, UK
Niccolò Ghiotto: Affiliation:
Department of Neuroscience (DNS), University of Padova, Padua, Italy
Marialaura Lussignoli: Affiliation:
Department of Neuroscience (DNS), University of Padova, Padua, Italy
Chiara Pavan: Affiliation:
Department of Neuroscience (DNS), University of Padova, Padua, Italy
Luca Pieri: Affiliation:
Department of Medicine, University of Padova, Padua, Italy
Sami Schiff: Affiliation:
Department of Medicine, University of Padova, Padua, Italy
Francesco Finatti: Affiliation:
Department of Neuroscience (DNS), University of Padova, Padua, Italy
Francesca Romagnolo: Affiliation:
Department of Neuroscience and Rehabilitation, Institute of Psychiatry, University of Ferrara, Ferrara, Italy
Federica Folesani: Affiliation:
Department of Neuroscience and Rehabilitation, Institute of Psychiatry, University of Ferrara, Ferrara, Italy
Maria Giulia Nanni: Affiliation:
Department of Neuroscience and Rehabilitation, Institute of Psychiatry, University of Ferrara, Ferrara, Italy
Rosangela Caruso: Affiliation:
Department of Neuroscience and Rehabilitation, Institute of Psychiatry, University of Ferrara, Ferrara, Italy
Luigi Zerbinati: Affiliation:
Department of Neuroscience and Rehabilitation, Institute of Psychiatry, University of Ferrara, Ferrara, Italy
Martino Belvederi Murri: Affiliation:
Department of Neuroscience and Rehabilitation, Institute of Psychiatry, University of Ferrara, Ferrara, Italy
Maria Ferrara: Affiliation:
Department of Neuroscience and Rehabilitation, Institute of Psychiatry, University of Ferrara, Ferrara, Italy
Giorgio Pigato: Affiliation:
Department of Psychiatry, Padova University Hospital, Padua, Italy
Luigi Grassi: Affiliation:
Department of Neuroscience and Rehabilitation, Institute of Psychiatry, University of Ferrara, Ferrara, Italy
Fabio Sambataro*: Affiliation:
Department of Neuroscience (DNS), University of Padova, Padua, Italy Padova Neuroscience Center, University of Padova, Padua, Italy
*: Corresponding author: Fabio Sambataro; Email: fabio.sambataro@unipd.it

Article contents

Abstract
Objective:
Methods:
Results:
Conclusions:
Significant outcomes
Limitations
Introduction
Materials and methods
Results
Discussion
Supplementary material
Financial support
Competing interests
Footnotes
References

Rights & Permissions

Abstract

Objective:

Electroconvulsive therapy (ECT) is one of the most studied and validated available treatments for severe or treatment-resistant depression. However, little is known about the neural mechanisms underlying ECT. This systematic review aims to critically review all structural magnetic resonance imaging studies investigating longitudinal cortical thickness (CT) changes after ECT in patients with unipolar or bipolar depression.

Methods:

We performed a search on PubMed, Medline, and Embase to identify all available studies published before April 20, 2023. A total of 10 studies were included.

Results:

The investigations showed widespread increases in CT after ECT in depressed patients, involving mainly the temporal, insular, and frontal regions. In five studies, CT increases in a non-overlapping set of brain areas correlated with the clinical efficacy of ECT. The small sample size, heterogeneity in terms of populations, comorbidities, and ECT protocols, and the lack of a control group in some investigations limit the generalisability of the results.

Conclusions:

Our findings support the idea that ECT can increase CT in patients with unipolar and bipolar depression. It remains unclear whether these changes are related to the clinical response. Future larger studies with longer follow-up are warranted to thoroughly address the potential role of CT as a biomarker of clinical response after ECT.

Keywords

ECT cortical thickness depression Hamilton rating scale for depression treatment-resistant depression

Type: Review Article
Information: Acta Neuropsychiatrica , First View , pp. 1 - 15

DOI: https://doi.org/10.1017/neu.2024.6 [Opens in a new window]
Creative Commons: This is an Open Access article, distributed under the terms of the Creative Commons Attribution licence (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted re-use, distribution and reproduction, provided the original article is properly cited.
Copyright: © The Author(s), 2024. Published by Cambridge University Press on behalf of Scandinavian College of Neuropsychopharmacology

Significant outcomes

• This review summarises how ECT affects CT in patients with unipolar or bipolar depression.
• The areas that were predominantly affected by ECT were temporo-insular and frontal regions. An association between the antidepressant effect of ECT and CT changes was reported by half of the included studies.
• Identifying the possible cortical changes associated with the clinical efficacy of ECT opens new targets to ameliorate ECT protocols.

Limitations

• The review is based on studies with small numbers of patients and considerable heterogeneity in terms of patients’ characteristics and ECT protocols, thus reducing the strength of evidence supporting a causal link between ECT and CT changes.

Introduction

Electroconvulsive therapy (ECT) was first used in 1938 by Italian scientists Ugo Cerletti and Lucio Bini to induce an epileptic seizure to treat patients with schizophrenia (Gazdag and Ungvari, Reference Gazdag and Ungvari2019). In the following decades, the introduction of general anesthesia and accurate operational protocols greatly improved ECT techniques (Kadiyala and Kadiyala, Reference Kadiyala and Kadiyala2018; Kellner et al., Reference Kellner, Obbels and Sienaert2020), allowing ECT to evolve to become a promising and well-tolerated treatment. Nowadays, it is considered the safest procedure performed under general anesthesia (Tørring et al., Reference Tørring, Sanghani, Petrides, Kellner and Østergaard2017). ECT is an important therapeutic strategy for affective disorders, including severe major depressive disorder (MDD), particularly with psychotic symptoms and a high risk of suicide, treatment-resistant depression (TRD), and depression in bipolar disorder (BD) (Kho et al., Reference Kho, van Vreeswijk, Simpson and Zwinderman2003; Fornaro et al., Reference Fornaro, Carvalho, Fusco, Anastasia, Solmi, Berk, Sim, Vieta and de Bartolomeis2020). Despite the major advances in psychopharmacology and brain stimulation techniques, ECT remains one of the most effective treatments in psychiatry, with response rates in the treatment of unipolar and bipolar depression ranging from 74 to 77 % (Bahji et al., Reference Bahji, Hawken, Sepehry, Cabrera and Vazquez2019).

The exact pathophysiological mechanisms underlying depression have not yet been clarified. Among the putative mechanisms, the “neurotrophin hypothesis of depression” suggests that a stress-induced decrease in the expression of brain-derived neurotrophic factor (BDNF) leads to atrophy of stress-vulnerable neurons in the hippocampus (Duman et al., Reference Duman, Heninger and Nestler1997). Later studies expanded this theory, indicating that changes in BDNF expression and function result in structural brain alterations not only in the hippocampus, but also in the prefrontal cortex (PFC) (Duman and Li, Reference Duman and Li2012). Crucially, magnetic resonance imaging (MRI) investigations have been supporting this theory, demonstrating reductions in grey matter (GM) volumes in MDD in the orbitofrontal cortex (OFC), ventromedial PFC, inferior parietal gyrus, as well as in the hippocampus, parahippocampal gyrus, insula, thalamus, basal ganglia, anterior cingulate cortex (ACC), and posterior cingulate cortex (PCC) (Koolschijn et al., Reference Koolschijn, van Haren, Lensvelt-Mulders, Hulshoff Pol and Kahn2009; Kempton et al., Reference Kempton, Salvador, Munafò, Geddes, Simmons, Frangou and Williams2011; Wise et al., Reference Wise, Radua, Via, Cardoner, Abe, Adams, Amico, Cheng, Cole, de Azevedo Marques Périco, Dickstein, Farrow, Frodl, Wagner, Gotlib, Gruber, Ham, Job, Kempton, Kim, Koolschijn, Malhi, Mataix-Cols, McIntosh, Nugent, O’Brien, Pezzoli, Phillips, Sachdev, Salvadore, Selvaraj, Stanfield, Thomas, van Tol, van der Wee, Veltman, Young, Fu, Cleare and Arnone2017). Similarly, a recent meta-analysis of volumetric studies in MDD identified decreased GM volume in frontal, temporal, and limbic regions. Interestingly, the authors also found an association between drug treatment and larger GM volume in the right striatum and smaller GM volume in the right precuneus (Jiang et al., Reference Jiang, Li, Lin, Hu, Zhao, Sweeney and Gong2023).

In bipolar depression, similar volumetric alterations have been reported, particularly in the frontal and limbic areas. In addition to volumetric changes, alterations in surface measurements have also been reported in depression, such as cortical thickness (CT), which represents the depth of GM as the covering neural sheet of brain foldings and is correlated with the size of neurons, neuroglia, and nerve fibres (Narr et al., Reference Narr, Bilder, Toga, Woods, Rex, Szeszko, Robinson, Sevy, Gunduz-Bruce, Wang, DeLuca and Thompson2005). Importantly, a reduction in CT could indicate a reduction in dendritic arborisation or changes in myelination at the grey/white matter interface (Sowell et al., Reference Sowell, Thompson, Leonard, Welcome, Kan and Toga2004) The Enhancing Neuroimaging Genetics through Meta-Analysis (ENIGMA) Consortium has demonstrated that lower CT in temporal regions is a common feature in various neuropsychiatric disorders (Schmaal et al., Reference Schmaal, Hibar, Sämann, Hall, Baune, Jahanshad, Cheung, van Erp, Bos, Ikram, Vernooij, Niessen, Tiemeier, Hofman, Wittfeld, Grabe, Janowitz, Bülow, Selonke, Völzke, Grotegerd, Dannlowski, Arolt, Opel, Heindel, Kugel, Hoehn, Czisch, Couvy-Duchesne, Rentería, Strike, Wright, Mills, de Zubicaray, McMahon, Medland, Martin, Gillespie, Goya-Maldonado, Gruber, Krämer, Hatton, Lagopoulos, Hickie, Frodl, Carballedo, Frey, van Velzen, Penninx, van Tol, van der Wee, Davey, Harrison, Mwangi, Cao, Soares, Veer, Walter, Schoepf, Zurowski, Konrad, Schramm, Normann and Schnell2017; Boedhoe et al., Reference Boedhoe, Schmaal, Abe, Alonso, Ameis, Anticevic, Arnold, Batistuzzo, Benedetti, Beucke, Bollettini, Bose, Brem, Calvo, Calvo, Cheng, Cho, Ciullo, Dallaspezia, Denys, Feusner, Fitzgerald, Fouche, Fridgeirsson, Gruner, Hanna, Hibar, Hoexter, Hu, Huyser, Jahanshad, James, Kathmann, Kaufmann, Koch, Kwon, Lazaro, Lochner, Marsh, Martínez-Zalacaín, Mataix-Cols, Menchón, Minuzzi, Morer, Nakamae, Nakao, Narayanaswamy, Nishida, Nurmi, O’Neill, Piacentini, Piras, Piras, Reddy, Reess, Sakai and Sato2018; Van Rooij et al., Reference Van Rooij, Anagnostou, Arango, Auzias, Behrmann, Busatto, Calderoni, Daly, Deruelle, Di Martino, Dinstein, Duran, Durston, Ecker, Fair, Fedor, Fitzgerald, Freitag, Gallagher, Gori, Haar, Hoekstra, Jahanshad, Jalbrzikowski, Janssen, Lerch, Luna, Martinho, McGrath, Muratori, Murphy, Murphy, O’Hearn, Oranje, Parellada, Retico, Rosa, Rubia, Shook, Taylor, Thompson, Tosetti, Wallace, Zhou and Buitelaar2018; Hoogman et al., Reference Hoogman, Muetzel, Guimaraes, Shumskaya, Mennes, Zwiers, Jahanshad, Sudre, Wolfers, Earl, Soliva Vila, Vives-Gilabert, Khadka, Novotny, Hartman, Heslenfeld, Schweren, Ambrosino, Oranje, de Zeeuw, Chaim-Avancini, Rosa, Zanetti, Malpas, Kohls, von Polier, Seitz, Biederman, Doyle, Dale, van Erp, Epstein, Jernigan, Baur-Streubel, Ziegler, Zierhut, Schrantee, Høvik, Lundervold, Kelly, McCarthy, Skokauskas, O’Gorman Tuura, Calvo, Lera-Miguel, Nicolau, Chantiluke, Christakou, Vance, Cercignani, Gabel, Asherson, Baumeister, Brandeis, Hohmann, Bramati, Tovar-Moll, Fallgatter, Kardatzki, Schwarz, Anikin, Baranov, Gogberashvili, Kapilushniy, Solovieva, El Marroun, White, Karkashadze, Namazova-Baranova, Ethofer, Mattos, Banaschewski, Coghill, Plessen, Kuntsi, Mehta, Paloyelis, Harrison, Bellgrove, Silk, Cubillo, Rubia, Lazaro, Brem, Walitza, Frodl, Zentis, Castellanos, Yoncheva, Haavik, Reneman, Conzelmann, Lesch, Pauli, Reif, Tamm, Konrad, Oberwelland Weiss, Busatto, Louza, Durston, Hoekstra, Oosterlaan, Stevens, Ramos-Quiroga, Vilarroya, Fair, Nigg, Thompson, Buitelaar, Faraone, Shaw, Tiemeier, Bralten and Franke2019). With regards to MDD, the ENIGMA Major Depressive Disorder Working Group reported thinner cortical GM in MDD compared to controls in the OFC, ACC and PCC, insula, and temporal lobes (Schmaal et al., Reference Schmaal, Hibar, Sämann, Hall, Baune, Jahanshad, Cheung, van Erp, Bos, Ikram, Vernooij, Niessen, Tiemeier, Hofman, Wittfeld, Grabe, Janowitz, Bülow, Selonke, Völzke, Grotegerd, Dannlowski, Arolt, Opel, Heindel, Kugel, Hoehn, Czisch, Couvy-Duchesne, Rentería, Strike, Wright, Mills, de Zubicaray, McMahon, Medland, Martin, Gillespie, Goya-Maldonado, Gruber, Krämer, Hatton, Lagopoulos, Hickie, Frodl, Carballedo, Frey, van Velzen, Penninx, van Tol, van der Wee, Davey, Harrison, Mwangi, Cao, Soares, Veer, Walter, Schoepf, Zurowski, Konrad, Schramm, Normann and Schnell2017). Furthermore, a decrease in CT was also found in elderly patients with MDD (Lim et al., Reference Lim, Jung, Ahn, Won, Hahn, Lee, Kim and Lee2012) and in those with a high risk for suicide (Wagner et al., Reference Wagner, Schultz, Koch, Schachtzabel, Sauer and Schlösser2012) Additionally, a thinner CT in the PCC could indicate a higher risk of non-remission in MDD patients (Järnum et al., Reference Järnum, Eskildsen, Steffensen, Lundbye-Christensen, Simonsen, Thomsen, Fründ, Théberge and Larsson2011). In BD, a recent ENIGMA study highlighted that individuals with BD showed a widespread thinner cortex relative to HC, with the largest effect size in the left fusiform gyrus (Matsumoto et al., Reference Matsumoto, Fukunaga, Miura, Nemoto, Okada, Hashimoto, Morita, Koshiyama, Ohi, Takahashi, Koeda, Yamamori, Fujimoto, Yasuda, Ito, Yamazaki, Hasegawa, Narita, Yokoyama, Mishima, Miyata, Kobayashi, Sasabayashi, Harada, Yamamoto, Hirano, Itahashi, Nakataki, Hashimoto, Tha, Koike, Matsubara, Okada, Yoshimura, Abe, van Erp, Turner, Jahanshad, Thompson, Onitsuka, Watanabe, Matsuo, Yamasue, Okamoto, Suzuki, Ozaki, Kasai and Hashimoto2023).

Although the association between surface measures and the severity of depressive symptoms is unclear, changes in CT after response and remission have been reported after antidepressant treatment. In particular, in a 12-week trial using sertraline in patients with late-life depression, nonremitters presented thinner frontal poles at baseline compared to remitters (Sheline et al., Reference Sheline, Disabato, Hranilovich, Morris, D’Angelo, Pieper, Toffanin, Taylor, MacFall, Wilkins, Barch, Welsh-Bohmer, Steffens, Krishnan and Doraiswamy2012). Another trial showed that sertraline increased CT in the left medial PFC, right medial and lateral PFC, and within the right parietal-temporal lobes in patients with MDD compared to placebo (Nemati and Abdallah, Reference Nemati and Abdallah2020). In addition, CT also predicted the effectiveness of psychotherapy for late-life depression (Mackin et al., Reference Mackin, Tosun, Mueller, Lee, Insel, Schuff, Truran-Sacrey, Arean, Nelson and Weiner2013). Therefore, reduced CT appears to be related to the reduced efficacy of pharmacological interventions in MDD, and successful treatment appears to reverse atrophy in fronto-limbic areas (Motter et al., Reference Motter, Lee, Sneed, Doraiswamy, Pelton, Petrella and Devanand2021). Crucially, reduced CT appears to be associated also with early-life traumas and with other affective disorders, including BD and anxiety (Zhu et al., Reference Zhu, Zhao, Wen, Li, Pan, Fu, Li, Radua, Vieta, Kemp, Biswa and Gong2022; Yang et al., Reference Yang, Jin, Duan, Yu, Ping, Shen, Cheng, Xu and Zhou2023).

The neural mechanisms underlying the effects of ECT in the treatment of depression are still largely unknown, and this further contributes to the scepticism about its use (Bolwig, Reference Bolwig2011). Importantly, recent meta-analytic evidence suggested that ECT is associated with volume increases in the hippocampus and increased integrity of white matter pathways in the frontal and temporal lobes (Gbyl and Videbech, Reference Gbyl and Videbech2018). These findings have also been confirmed by a mega-analysis conducted by the Global ECT-MRI Research Collaboration (GEMRIC), which showed that ECT induced broadly distributed GM volume increases (Ousdal et al., Reference Ousdal, Argyelan, Narr, Abbott, Wade, Vandenbulcke, Urretavizcaya, Tendolkar, Takamiya, Stek, Soriano-Mas, Redlich, Paulson, Oudega, Opel, Nordanskog, Kishimoto, Kampe, Jorgensen, Hanson, Hamilton, Espinoza, Emsell, Eijndhoven, Dols, Dannlowski, Cardoner, Bouckaert, Anand, Bartsch, Kessler, Oedegaard, Dale, Oltedal, Erchinger, Haavik, Sørhaug, Jørgensen, Bolwig, Magnusson, Cano, Pujol, Menchón, Petrides and Sienaert2020). GM volume is determined by CT and surface area; nevertheless, the relationship between GM volume and CT is modest, both globally and locally (Winkler et al., Reference Winkler, Kochunov, Blangero, Almasy, Zilles, Fox, Duggirala and Glahn2010). Conversely, GM volume is highly correlated with surface area. Their limited relationship most probably depends on unrelated genetic factors that are likely tied to different neurobiological processes (Winkler et al., Reference Winkler, Kochunov, Blangero, Almasy, Zilles, Fox, Duggirala and Glahn2010), and is further biased by grey/white matter intensity contrast and curvature differences (Kong et al., Reference Kong, Herold, Zöllner, Salat, Lässer, Schmid, Fellhauer, Thomann, Essig, Schad, Erickson and Schröder2015). For this reason, we wanted to study changes in CT after ECT treatment with the expectation that these results would be complementary to those reported in cortical GM volumetric studies. Given these premises, we aimed to review the available evidence on CT alterations associated with ECT treatment in patients with depression to explore the association between changes in CT and the antidepressant effect of ECT.

Materials and methods

Literature search and screening

The study inclusion criteria were the following: a) participants with a diagnosis of MDD or BD according to the Diagnostic and Statistical Manual of Mental Disorders (DSM) or International Classification of Disease (ICD) criteria or TRD (any definition); b) participants underwent MRI pre- and post-ECT; c) changes of CT were assessed longitudinally, that is, before and after the ECT treatments; c) CT changes were longitudinally evaluated, that is, before and after the ECT sessions (no restrictions in terms of the number of sessions or temporal distance between ECT and MRI).

A comprehensive search of the literature was performed on PubMed, Medline, and Embase using the following keywords: (ECT [Title/Abstract] OR Electroconvulsive Therapy [Title/Abstract] OR Electroconvulsive Treatment [Title/Abstract]) AND ((Major Depressive Disorder [Title/Abstract] OR Depression [Title/Abstract] OR Bipolar Disorder [Title/Abstract]) OR Bipolar Depression [Title/Abstract]) AND Cortical thickness [Title/Abstract]). No language restrictions were applied to identify peer-reviewed articles published up to April 2023.

We screened titles and abstracts of all potentially eligible studies, retrieving the full-text articles. References cited by each study were also manually screened to ensure that no relevant studies were left out. This procedure was carried out according to the Preferred Reporting Items for Systematic Reviews and Meta-Analysis (PRISMA) guidelines (Liberati et al., Reference Liberati, Altman, Tetzlaff, Mulrow, Gøtzsche, Ioannidis, Clarke, Devereaux, Kleijnen and Moher2009). Of the 35 initial studies, 25 remained after removing duplicates, and 11 citations met the title/abstract screening eligibility criteria and were included. After full-text screening, 1 article was excluded because it did not report longitudinal changes after ECT (Wade et al., Reference Wade, Sui, Hellemann, Leaver, Espinoza, Woods, Abbott, Joshi and Narr2017), resulting in 10 eligible studies (Fig. 1). Since only two studies reported quantitative measures of the effects of ECT on CT, we could not perform a meta-analysis.

Figure 1. PRISMA flow chart of selection of publications for inclusion in the review.

Assessment of methodological quality

The methodological quality of the included studies was assessed using a point system derived from Gbly and Videbech (Gbyl and Videbech, Reference Gbyl and Videbech2018). Briefly, the quality score consisted of the following items: a) number of subjects; b) presence of a control group; c) number of MRI scans the control group underwent; d) MRI scanner field strength; e) voxel size of the MRI scan; f) medication status; g) consecutively collected sample; h) duration of follow-up. A higher score indicated better methodological quality (see Supplementary Material).

Results

Demographic, clinical, and ECT characteristics of included studies

Table 1. Studies investigating the effect of ECT on CT in depressed patients

AVLT: Auditory Verbal Learning Test; BD: bipolar disorder; BDI-II: Beck Depression Inventory-II; CT: cortical thickness; ECT: electroconvulsive therapy; HAM-D: Hamilton Rating Scale for Depression; HC: healthy controls; MADRAS: Montgomery-Åsberg Depression Rating Scales; MDD: major depressive disorder; NA: not applicable; NR: not reported; ST: seizure threshold TAU: treatment as usual; TRD: treatment-resistant depression.

Total quality score was calculated using a point system derived from Gbly and Videbech (Reference Gbyl and Videbech2018) (see Supplementary Material).

Figure 2. Magnetic resonance imaging (MRI) scan timeline of the studies of the effect of ECT on cortical thickness in patients with depression. For each study, we have reported the timing of the structural magnetic resonance images relative to the entire ECT treatment (in orange), including the baseline scan (solid black line, T1), the second scan (hatched line, T2), and the third scan (cross-hatched line, T3). The time is measured relative to the beginning (T1), during (T2) and after (T2, T3) the ECT treatment.

CT changes after ECT

Most studies identified CT alterations in the temporal, insular, and frontal areas, mainly proximally to the electrode (Fig. 3). Gryglewski et al. (Reference Gryglewski, Baldinger-Melich, Seiger, Godbersen, Michenthaler, Klöbl, Spurny, Kautzky, Vanicek, Kasper, Frey and Lanzenberger2019) and Sartorius et al. (Reference Sartorius, Demirakca, Böhringer, Clemm von Hohenberg, Aksay, Bumb, Kranaster and Ende2016) combined voxel-based morphometry and CT analysis (Sartorius et al., Reference Sartorius, Demirakca, Böhringer, Clemm von Hohenberg, Aksay, Bumb, Kranaster and Ende2016; Gryglewski et al., Reference Gryglewski, Baldinger-Melich, Seiger, Godbersen, Michenthaler, Klöbl, Spurny, Kautzky, Vanicek, Kasper, Frey and Lanzenberger2019). The first investigation reported a widespread increase in CT of the right hemisphere, including the insula, supramarginal gyrus, inferior parietal gyrus, superior temporal gyrus, inferior temporal gyrus, superior temporal sulcus, temporal pole, postcentral gyrus, and fusiform gyrus (Gryglewski et al., Reference Gryglewski, Baldinger-Melich, Seiger, Godbersen, Michenthaler, Klöbl, Spurny, Kautzky, Vanicek, Kasper, Frey and Lanzenberger2019). Similarly, Sartorius et al. (Reference Sartorius, Demirakca, Böhringer, Clemm von Hohenberg, Aksay, Bumb, Kranaster and Ende2016) found an increase in CT in the right temporal pole and the bilateral insula gyrus in MDD compared to HC (Sartorius et al., Reference Sartorius, Demirakca, Böhringer, Clemm von Hohenberg, Aksay, Bumb, Kranaster and Ende2016). Van Eijndhoven et al. (Reference van Eijndhoven, Mulders, Kwekkeboom, van Oostrom, van Beek, Janzing, Schene and Tendolkar2016) revealed large bilateral clusters of increased CT in TRD after ECT treatment extending from the temporal pole, middle and superior temporal gyrus to the insula, and inferior temporal gyrus in the left hemisphere. Post-hoc analyses demonstrated that the increase in CT of the insular cortex was greater in responders compared to non-responders to ECT. Notably, a higher number of ECT sessions correlated with greater mean CT of the left temporal pole and the left middle and inferior temporal cortex (van Eijndhoven et al., Reference van Eijndhoven, Mulders, Kwekkeboom, van Oostrom, van Beek, Janzing, Schene and Tendolkar2016). Xu et al. (Reference Xu, Wang, Bai, Zhang, Li, Hu, Li, Zhang, Wei, Tian and Wang2019) calculated vertex-wise and regional CT within each of the 68 anatomically defined regions from the Desikan–Killiany Atlas in MDD (Xu et al., Reference Xu, Wang, Bai, Zhang, Li, Hu, Li, Zhang, Wei, Tian and Wang2019). The authors reported a higher vertex-wise CT in the left temporal pole, left fusiform gyrus, left inferior parietal gyrus, left insula, as well as in the right lateral occipital gyrus, right supramarginal gyrus, right superior temporal gyrus, right insula and right precentral gyrus in patients with MDD after ECT. Furthermore, a greater regional CT was observed in the bilateral fusiform gyrus, bilateral parahippocampus, inferior temporal gyrus, left superior temporal gyrus, left inferior parietal gyrus, left insula, left superior temporal sulcus, right superior frontal gyrus, and the right anterior rostral cingulate, as well as increased vertex-wise and regional CT in the left temporal pole, fusiform gyrus, and bilateral insula in MDD patients after ECT (Xu et al., Reference Xu, Wang, Bai, Zhang, Li, Hu, Li, Zhang, Wei, Tian and Wang2019). Pirnia et al. (Reference Pirnia, Joshi, Leaver, Vasavada, Njau, Woods, Espinoza and Narr2016) and Yrondi et al. (Reference Yrondi, Nemmi, Billoux, Giron, Sporer, Taib, Salles, Pierre, Thalamas, Rigal, Danet, Pariente, Schmitt, Arbus and Péran2019) to better delineate the course of CT changes during the entire ECT treatment, acquired an initial scan (T1), an intermediate scan between the first and the last ECT session (T2), and a scan within one week of the last ECT (T3) (Pirnia et al., Reference Pirnia, Joshi, Leaver, Vasavada, Njau, Woods, Espinoza and Narr2016; Yrondi et al., Reference Yrondi, Nemmi, Billoux, Giron, Sporer, Taib, Salles, Pierre, Thalamas, Rigal, Danet, Pariente, Schmitt, Arbus and Péran2019). In the study of Yrondi et al (Reference Yrondi, Nemmi, Billoux, Giron, Sporer, Taib, Salles, Pierre, Thalamas, Rigal, Danet, Pariente, Schmitt, Arbus and Péran2019), the second MRI was performed immediately after the first ECT was considered effective. The researchers detected a significant increase in CT in the superior temporal gyrus in the patient group between baseline and time T3, between T2 and T3, but not between T1 and T2, suggesting that CT changes occur only after multiple ECT sessions. A post-hoc analysis revealed that, at baseline, MDD had thinner CT in the frontal lobe, in the fusiform gyrus, inferior, middle, and superior temporal gyri, parahippocampal gyrus, and the transverse temporal gyrus compared to HC. These differences were no longer significant after ECT (Yrondi et al., Reference Yrondi, Nemmi, Billoux, Giron, Sporer, Taib, Salles, Pierre, Thalamas, Rigal, Danet, Pariente, Schmitt, Arbus and Péran2019). In Pirnia et al. (Reference Pirnia, Joshi, Leaver, Vasavada, Njau, Woods, Espinoza and Narr2016), the second scan was performed within 48 hours after the second ECT treatment; CT became significantly thicker in the bilateral ACC, right parahippocampal gyrus, superior temporal gyrus, and temporal pole between T1 and T3 in patients with unipolar and bipolar depression. An additional region of interest (ROI) analysis showed significant effects of ECT in the ACC, parahippocampal, entorhinal, superior temporal, inferior temporal, and fusiform cortex. To determine whether ECT was associated with a normalisation towards control values, differences in CT between patients and HC were examined at baseline in the entire cortex and in ROIs that showed significant effects of ECT. Within the cortical ROIs, at baseline, patients showed reduced CT in the fusiform and superior temporal cortex compared to HC, which was not present at the two subsequent time points. Importantly, this study presented a high methodological quality (Pirnia et al., Reference Pirnia, Joshi, Leaver, Vasavada, Njau, Woods, Espinoza and Narr2016). Gbyl et al. (Reference Gbyl, Rostrup, Raghava, Carlsen, Schmidt, Lindberg, Ashraf, Jørgensen, Larsson, Rosenberg and Videbech2019) explored CT changes in 18 patients with MDD from baseline to six months after the last ECT, with an intermediate scan after the first ECT. They reported an increase in CT in 26 cortical regions, mainly within the frontal, temporal, and insular cortex immediately after the first series of ECT, which returned to baseline at six months of follow-up (Gbyl et al., Reference Gbyl, Rostrup, Raghava, Carlsen, Schmidt, Lindberg, Ashraf, Jørgensen, Larsson, Rosenberg and Videbech2019). A recent study by Bracht et al. (Reference Bracht, Walther, Breit, Mertse, Federspiel, Meyer, Soravia, Wiest and Denier2023) with high methodological quality compared longitudinal changes in CT between the ECT-treated group, treatment-as-usual (TAU) responders, and HC. Patients with unipolar and bipolar TRD were scanned twice, at the beginning and at the end of the ECT series, while patients with TAU were scanned at baseline and after achieving remission of depressive symptoms or within 12 weeks after the first MRI scan. The global mean CT was increased in the right hemisphere in the ECT group and bilaterally in the TAU responders. Exploratory analyses revealed that CT changes common to the ECT group and TAU-responders included the right insula and the right lateral OFC (Bracht et al., Reference Bracht, Walther, Breit, Mertse, Federspiel, Meyer, Soravia, Wiest and Denier2023). Another recent longitudinal study with high methodological quality explored CT in 96 patients with MDD before and after ECT and reported CT increases in bilateral medial areas of the superior temporal gyrus and bilateral insula compared to baseline (Ji et al., Reference Ji, Li, Liao, Wang, Zhang, Bai, Zhang, Xie, He, Zhu, Dukart, Baeken, Tian and Wang2022). Lastly, Schmitgen et al. (Reference Schmitgen, Kubera, Depping, Nolte, Hirjak, Hofer, Hasenkamp, Seidl, Stieltjes, Maier-Hein, Sambataro, Sartorius, Thomann and Wolf2020) investigated several surface-based measures in 12 patients with TRD and found no differences in CT relative to 12 HC and no longitudinal changes of this parameter in the group of patients before and after ECT (Schmitgen et al., Reference Schmitgen, Kubera, Depping, Nolte, Hirjak, Hofer, Hasenkamp, Seidl, Stieltjes, Maier-Hein, Sambataro, Sartorius, Thomann and Wolf2020).

Figure 3. Changes in cortical thickness in patients with depression after ECT. Results from morphometric studies are displayed on the Desikan-Killiany atlas. The medial and lateral cortical surfaces are displayed for each hemisphere on the leftmost part, the subcortical regions in the center, and the colorbar on the rightmost part of each panel, respectively. The color bar code indicates the total number of subjects who showed an increase in cortical thickness. L, left hemisphere; R, right hemisphere. The renderings were created using the R-package ggseg.

Correlations between CT changes and clinical improvements

Ten studies explored the correlations between CT changes and clinical improvements in depression measured with HAM-D between baseline and follow-up, and five reported a significant association. Gbyl et al. (Reference Gbyl, Rostrup, Raghava, Carlsen, Schmidt, Lindberg, Ashraf, Jørgensen, Larsson, Rosenberg and Videbech2019) found a positive correlation between CT increases in the right lateral orbitofrontal gyrus and clinical improvement of depression (Gbyl et al., Reference Gbyl, Rostrup, Raghava, Carlsen, Schmidt, Lindberg, Ashraf, Jørgensen, Larsson, Rosenberg and Videbech2019). Similarly, positive correlations were observed between changes in CT in the fusiform, superior, and inferior temporal gyrus and clinical improvement in depression (Pirnia et al., Reference Pirnia, Joshi, Leaver, Vasavada, Njau, Woods, Espinoza and Narr2016); in particular, CT of the ACC increased shortly (T1 and T2) after the initiation of ECT treatment and was predictive of the general clinical response (>50% improvement in HAM-D scores) to ECT. In van Eijndhoven et al. (Reference van Eijndhoven, Mulders, Kwekkeboom, van Oostrom, van Beek, Janzing, Schene and Tendolkar2016), increased mean CT of the right insula was associated with clinical improvement in depressive symptoms (van Eijndhoven et al., Reference van Eijndhoven, Mulders, Kwekkeboom, van Oostrom, van Beek, Janzing, Schene and Tendolkar2016). Schmitgen et al. (Reference Schmitgen, Kubera, Depping, Nolte, Hirjak, Hofer, Hasenkamp, Seidl, Stieltjes, Maier-Hein, Sambataro, Sartorius, Thomann and Wolf2020) observed that pre- and post-ECT CT of the left rostral anterior cingulate gyrus predicted a greater improvement in depression. Furthermore, the authors also found a correlation between clinical improvement and increased CT of the left medial orbitofrontal gyrus after but not before ECT treatment, suggesting a mediator role of cortical changes in this region (Schmitgen et al., Reference Schmitgen, Kubera, Depping, Nolte, Hirjak, Hofer, Hasenkamp, Seidl, Stieltjes, Maier-Hein, Sambataro, Sartorius, Thomann and Wolf2020). Lastly, Xu et al. (Reference Xu, Wang, Bai, Zhang, Li, Hu, Li, Zhang, Wei, Tian and Wang2019) reported a correlation between vertex-wise CT increases in the left occipital gyrus and the improvement of depression. Furthermore, to test the brain mechanisms of tolerability of ECT, the authors explored the association between cognitive functions and CT changes. In particular, ECT-dependent memory impairments measured by Auditory Verbal Learning Test (ALVT) delayed recall scores were negatively correlated with CT increase in the left inferior parietal gyrus and marginally in the right precentral gyrus after ECT treatment (Xu et al., Reference Xu, Wang, Bai, Zhang, Li, Hu, Li, Zhang, Wei, Tian and Wang2019).

Discussion

This review summarised the evidence on CT changes associated with ECT among patients with depression. We found that ECT was associated with a widespread increase in CT in patients with depression, located primarily in the temporal lobe and insula cortex and, to a lesser extent, in the frontal areas. This pattern of increased CT was consistent across studies with lower and higher methodological quality scores. Some investigations showed a correlation between increases in CT and clinical improvement, but this was only confirmed by a few studies with higher methodological quality.

Temporal lobe

Most of the reviewed studies found that ECT was followed by increased CT in the temporal lobe, including the superior, middle, and inferior temporal gyri and temporal pole (Pirnia et al., Reference Pirnia, Joshi, Leaver, Vasavada, Njau, Woods, Espinoza and Narr2016; Sartorius et al., Reference Sartorius, Demirakca, Böhringer, Clemm von Hohenberg, Aksay, Bumb, Kranaster and Ende2016; van Eijndhoven et al., Reference van Eijndhoven, Mulders, Kwekkeboom, van Oostrom, van Beek, Janzing, Schene and Tendolkar2016; Gbyl et al., Reference Gbyl, Rostrup, Raghava, Carlsen, Schmidt, Lindberg, Ashraf, Jørgensen, Larsson, Rosenberg and Videbech2019; Gryglewski et al., Reference Gryglewski, Baldinger-Melich, Seiger, Godbersen, Michenthaler, Klöbl, Spurny, Kautzky, Vanicek, Kasper, Frey and Lanzenberger2019; Xu et al., Reference Xu, Wang, Bai, Zhang, Li, Hu, Li, Zhang, Wei, Tian and Wang2019; Yrondi et al., Reference Yrondi, Nemmi, Billoux, Giron, Sporer, Taib, Salles, Pierre, Thalamas, Rigal, Danet, Pariente, Schmitt, Arbus and Péran2019; Ji et al., Reference Ji, Li, Liao, Wang, Zhang, Bai, Zhang, Xie, He, Zhu, Dukart, Baeken, Tian and Wang2022). Although most increases were observed near the placement of the electrodes, temporal changes were also observed when the electrodes were located in the frontal lobe (Xu et al., Reference Xu, Wang, Bai, Zhang, Li, Hu, Li, Zhang, Wei, Tian and Wang2019; Ji et al., Reference Ji, Li, Liao, Wang, Zhang, Bai, Zhang, Xie, He, Zhu, Dukart, Baeken, Tian and Wang2022). Despite decades of use, the precise mechanisms by which ECT exerts its therapeutic effects remain poorly understood (Fridgeirsson et al., Reference Fridgeirsson, Deng, Denys, van Waarde and van Wingen2021; Deng et al., Reference Deng, Robins, Regenold, Rohde, Dannhauer and Lisanby2023). Among the hypotheses of ECT action, three main theories have been proposed: the generalised seizure theory, the neuroendocrine–diencephalic theory, and a combined anatomical–ictal theory (Bolwig, Reference Bolwig2011). According to the generalised seizure theory, the therapeutic effects of ECT depend on the elicitation of generalised seizures. Indeed, as first demonstrated by Ottosson in 1960, generalised seizures are essential for the efficacy of ECT, and subconvulsive stimuli have weaker or no antidepressant effect (Ottosson, Reference Ottosson1960). This theory is supported by evidence showing that bilateral electrode placement, which induces a more pronounced seizure generalisation, presents a higher therapeutic efficacy compared to unilateral electrode placement (Bolwig, Reference Bolwig2011). In addition, seizure-inducing drugs, such as flurothyl and pentylendetetrazol, show similar clinical effects to ECT (Karliner and Padula, Reference Karliner and Padula1960; Cooper and Fink, Reference Cooper and Fink2014). However, recent research has challenged the notion that widespread seizure activity is the main responsible for ECT efficacy in depression, given the evidence that increasing the strength of the electric field can affect the clinical effectiveness of ECT, without affecting the characteristics of the seizure (Argyelan et al., Reference Argyelan, Oltedal, Deng, Wade, Bikson, Joanlanne, Sanghani, Bartsch, Cano, Dale, Dannlowski, Dols, Enneking, Espinoza, Kessler, Narr, Oedegaard, Oudega, Redlich, Stek, Takamiya, Emsell, Bouckaert, Sienaert, Pujol, Tendolkar, van Eijndhoven, Petrides, Malhotra and Abbott2019). Notably, current literature suggests a higher intensity of the electric field may be associated with greater neuronal plasticity after treatment (Argyelan et al., Reference Argyelan, Oltedal, Deng, Wade, Bikson, Joanlanne, Sanghani, Bartsch, Cano, Dale, Dannlowski, Dols, Enneking, Espinoza, Kessler, Narr, Oedegaard, Oudega, Redlich, Stek, Takamiya, Emsell, Bouckaert, Sienaert, Pujol, Tendolkar, van Eijndhoven, Petrides, Malhotra and Abbott2019). In this regard, animal studies have shown that electroconvulsive seizures stimulate dendritic arborisation, synaptic density, and glial proliferation (Ongür et al., Reference Ongür, Pohlman, Dow, Eisch, Edwin, Heckers, Cohen, Patel and Carlezon2007; Maynard et al., Reference Maynard, Hobbs, Rajpurohit and Martinowich2018). Furthermore, a recent quantitative MRI study that explored brain’s myelin, iron, and tissue water content at multiple time-points before, during and after ECT treatment, suggested that myelin changes rather than oedema are associated with the longitudinal effects of ECT (Gyger et al., Reference Gyger, Ramponi, Mall, Swierkocz-Lenart, Stoyanov, Lutti, von Gunten, Kherif and Draganski2021). This may be a consequence of the increased expression and release of BDNF induced by ECT (Polyakova et al., Reference Polyakova, Schroeter, Elzinga, Holiga, Schoenknecht, de Kloet and Molendijk2015), which could ultimately be the basis for the therapeutic efficacy of ECT. Taken together, this evidence seems to support the hypothesis that seizure activity synergistically with an electric field is involved in the clinical efficacy of ECT and has a profound effect on the biology of the human brain. Unfortunately, only two of the included studies reported information about seizure duration (Gryglewski et al., Reference Gryglewski, Baldinger-Melich, Seiger, Godbersen, Michenthaler, Klöbl, Spurny, Kautzky, Vanicek, Kasper, Frey and Lanzenberger2019; Van Eijndhoven et al., Reference van Eijndhoven, Mulders, Kwekkeboom, van Oostrom, van Beek, Janzing, Schene and Tendolkar2016) and no studies described the electric field strength, so we cannot draw any conclusion on the association between ECT-induced seizure activity or ECT-induced electric field, CT changes, and antidepressant effect.

Increased CT in the superior and inferior temporal gyrus was associated with an improvement in depressive symptoms only in one study (Pirnia et al., Reference Pirnia, Joshi, Leaver, Vasavada, Njau, Woods, Espinoza and Narr2016). Furthermore, Gbyl et al. (Reference Gbyl, Rostrup, Raghava, Carlsen, Schmidt, Lindberg, Ashraf, Jørgensen, Larsson, Rosenberg and Videbech2019) observed that, although CT in the temporal lobe increased after the first ECT, it returned to baseline after six months, even if the antidepressant effect persisted (Bolwig, Reference Bolwig2011).

Taken together, this evidence suggests that temporal CT is primarily affected by ECT, regardless of electrode placement. Less clear is the role of temporal CT changes in clinical improvements. Although most investigations showed that changes in CT did not correlate with clinical symptoms, this was not replicated in all included studies. Therefore, more evidence is needed to clarify the role of temporal CT in changes in depressive symptoms.

Insula

Frontal lobe

The frontal lobe, in particular the OFC, the superior, middle, and inferior frontal gyrus, have been consistently implicated in the pathophysiology of unipolar and bipolar depression (Drevets, Reference Drevets2007; Altshuler et al., Reference Altshuler, Bookheimer, Townsend, Proenza, Sabb, Mintz and Cohen2008; Fitzgerald et al., Reference Fitzgerald, Laird, Maller and Daskalakis2008). Three of the ten studies included in the present review showed cortical thickening in these areas (Gbyl et al., Reference Gbyl, Rostrup, Raghava, Carlsen, Schmidt, Lindberg, Ashraf, Jørgensen, Larsson, Rosenberg and Videbech2019; Xu et al., Reference Xu, Wang, Bai, Zhang, Li, Hu, Li, Zhang, Wei, Tian and Wang2019; Bracht et al., Reference Bracht, Walther, Breit, Mertse, Federspiel, Meyer, Soravia, Wiest and Denier2023) and, interestingly, only in the study by Xu et al. (Reference Xu, Wang, Bai, Zhang, Li, Hu, Li, Zhang, Wei, Tian and Wang2019) the electrodes were localised in the frontal lobe. Remarkably, Gbyl et al. (Reference Gbyl, Rostrup, Raghava, Carlsen, Schmidt, Lindberg, Ashraf, Jørgensen, Larsson, Rosenberg and Videbech2019) reported a strong association between cortical thickening of the right lateral OFC and the antidepressant effect of ECT (Gbyl et al., Reference Gbyl, Rostrup, Raghava, Carlsen, Schmidt, Lindberg, Ashraf, Jørgensen, Larsson, Rosenberg and Videbech2019). In depression, a reduced volume along with altered activity in OFC has previously been reported (Drevets, Reference Drevets2007). A recent study showed that direct stimulation of this region produced an acute improvement in depressive symptoms in epileptic subjects with moderate to severe depression (Rao et al., Reference Rao, Sellers, Wallace, Lee, Bijanzadeh, Sani, Yang, Shanechi, Dawes and Chang2018). Noticeably, OFC CT increased immediately after the ECT series but returned to baseline levels at six months of follow-up, despite the continued antidepressant effect, suggesting that the persistence of the clinical efficacy of ECT was not related to orbitofrontal CT. Interestingly, a recent GEMRIC consortium study identified a multivariate discriminative pattern of volume alterations in the cortical midline, striatal, and lateral prefrontal areas that differentiated responders from non-responders, suggesting that structural changes in prefrontal areas might play a role in the clinical response to ECT (Mulders et al., Reference Mulders, Llera, Beckmann, Vandenbulcke, Stek, Sienaert, Redlich, Petrides, Oudega, Oltedal, Oedegaard, Narr, Magnusson, Kessler, Jorgensen, Espinoza, Enneking, Emsell, Dols, Dannlowski, Bolwig, Bartsch, Argyelan, Anand, Abbott, van Eijndhoven and Tendolkar2020).

Other brain areas

ECT was associated with cortical thickening in several other areas, including the ACC, the parahippocampal gyrus, the entorhinal cortex, the fusiform gyrus, the superior and inferior parietal gyrus, the pre- and postcentral gyrus, and the lateral occipital gyrus. Although all these areas have been consistently implicated in the pathogenesis of unipolar and bipolar depression and appear to be influenced by antidepressant treatments (Bartlett et al., Reference Bartlett, DeLorenzo, Sharma, Yang, Zhang, Petkova, Weissman, McGrath, Fava, Ogden, Kurian, Malchow, Cooper, Trombello, McInnis, Adams, Oquendo, Pizzagalli, Trivedi and Parsey2018; Klimes-Dougan et al., Reference Klimes-Dougan, Westlund Schreiner, Thai, Gunlicks-Stoessel, Reigstad and Cullen2018; Yi et al., Reference Yi, Wang, Yang, Huang, Liu, Chen, Zhang, Zhao, Li, Fang and Liu2022), only increased CT in the right lateral occipital gyrus, an area involved in the perception of the face and emotion (Nagy et al., Reference Nagy, Greenlee and Kovács2012), was associated with clinical improvement (Xu et al., Reference Xu, Wang, Bai, Zhang, Li, Hu, Li, Zhang, Wei, Tian and Wang2019). Future studies with larger sample sizes are needed to clarify the effect of ECT on CT in these areas and the potential association with clinical improvements.

Biological significance of CT findings

Limitations and conclusions

The findings of this review should be interpreted in light of the limitations of primary studies. First, the small sample size of the included studies could have skewed the results and decreased the power of the studies, leading to a type II error. Thus, the abnormalities described in this review might be limited to some brain areas that presented changes with large effect sizes, neglecting changes with smaller effect sizes. This could, at least partially, explain why the mega-analysis by Ousdal et al. (Reference Ousdal, Argyelan, Narr, Abbott, Wade, Vandenbulcke, Urretavizcaya, Tendolkar, Takamiya, Stek, Soriano-Mas, Redlich, Paulson, Oudega, Opel, Nordanskog, Kishimoto, Kampe, Jorgensen, Hanson, Hamilton, Espinoza, Emsell, Eijndhoven, Dols, Dannlowski, Cardoner, Bouckaert, Anand, Bartsch, Kessler, Oedegaard, Dale, Oltedal, Erchinger, Haavik, Sørhaug, Jørgensen, Bolwig, Magnusson, Cano, Pujol, Menchón, Petrides and Sienaert2020) showed more widespread ECT-related brain changes (Ousdal et al., Reference Ousdal, Argyelan, Narr, Abbott, Wade, Vandenbulcke, Urretavizcaya, Tendolkar, Takamiya, Stek, Soriano-Mas, Redlich, Paulson, Oudega, Opel, Nordanskog, Kishimoto, Kampe, Jorgensen, Hanson, Hamilton, Espinoza, Emsell, Eijndhoven, Dols, Dannlowski, Cardoner, Bouckaert, Anand, Bartsch, Kessler, Oedegaard, Dale, Oltedal, Erchinger, Haavik, Sørhaug, Jørgensen, Bolwig, Magnusson, Cano, Pujol, Menchón, Petrides and Sienaert2020). Furthermore, only six studies had a control group, and not all studies reported baseline differences in CT between patients and HC. Second, the different clinical phenotypes of the participants (e.g., comorbidities, illness phase, duration of the illness) may have contributed to the heterogeneity of the results. In addition, two studies included individuals with bipolar depression, which may have affected their results. Third, the studies did not report effect size but only significance levels. The significance of a result depends on both effect and sample size, so that with a small effect and few individuals, a low number of regions can be detected. Fourth, the heterogeneity in the positioning of the electrodes during the administration of the ECT may have also influenced CT results. Similarly, the timing of the second MRI scan was not clearly defined in all studies, leading to the speculation that some studies conducted the second MRI immediately after ECT and others completed it some days after ECT, which could have affected the CT findings. Lastly, in this literature, the sex-related difference in CT changes after ECT was not investigated, and this could be due to the lack of evidence of sex differences in CT in depression.

In conclusion, available studies lend support to the hypothesis that ECT in depression is associated with cortical thickening of the temporal lobe, insula, and, to a lesser extent, frontal lobe, and several other areas of the brain involved in the pathophysiology of depression. These findings are consistent with evidence of increased CT after pharmacological and neuromodulation treatments, suggesting that cortical changes may not be specific to ECT, but rather reflect mechanisms of therapeutic response. Future studies with higher methodological quality, longer follow-up periods, and multiple methods of evaluating morphological changes are warranted to increase knowledge of the effects of ECT on CT in MDD. Such studies may also clarify the potential role of CT and other cortical measures, including surface area, gyrification, and cortical complexity, as biomarkers of the clinical response in depression.

Supplementary material

The supplementary material for this article can be found at https://doi.org/10.1017/neu.2024.6.

Acknowledgements

None.

Financial support

GC was supported by a grant from Cassa di Risparmio di Padova e Rovigo (CARIPARO).

Competing interests

None.

Footnotes

Tommaso Toffanin and Giulia Cattarinussi contributed equally.

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Figure 1. PRISMA flow chart of selection of publications for inclusion in the review.

Table 1. Studies investigating the effect of ECT on CT in depressed patients

Toffanin et al. supplementary material

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Article contents

Effects of electroconvulsive therapy on cortical thickness in depression: a systematic review

Abstract

Keywords

Significant outcomes

Limitations

Introduction

Materials and methods

Literature search and screening

Assessment of methodological quality

Results

Demographic, clinical, and ECT characteristics of included studies

CT changes after ECT

Correlations between CT changes and clinical improvements

Discussion

Temporal lobe

Insula

Frontal lobe

Other brain areas

Biological significance of CT findings

Limitations and conclusions

Supplementary material

Acknowledgements

Financial support

Competing interests

Footnotes

References

Toffanin et al. supplementary material

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