Hostname: page-component-78c5997874-lj6df Total loading time: 0 Render date: 2024-11-13T01:21:13.916Z Has data issue: false hasContentIssue false
  • English
  • Français

Bridging early life trauma to difficult-to-treat depression: scoping review

Published online by Cambridge University Press:  08 October 2024

Walter Paganin Open the ORCID record for Walter Paganin [Opens in a new window] ,
Sabrina Signorini  and
Antonio Sciarretta
Walter Paganin*
Affiliation:
University of Tor Vergata, Rome, Italy
Sabrina Signorini
Affiliation:
StudioPsicologiaSignorini, Rome, Italy
Antonio Sciarretta
Affiliation:
IHG, Rome, Italy
*
Correspondence to Walter Paganin (walter.paganin@students.uniroma2.eu)
Rights & Permissions [Opens in a new window]

Abstract

Aims and method

Accumulating evidence suggests that early life trauma (ELT) initiates and perpetuates a cycle of depression, leading to challenges in management and achieving remission. This scoping review aimed to examine the intricate relationship between ELT and difficult-to-treat depression (DTD). An extensive literature search from 1 January 2013 to 21 October 2023 was conducted using the Cochrane Library, PubMed, Scopus, PsycINFO and OpenGrey.

Results

Our review identified scientific literature illustrating the multifaceted link between ELT and DTD, highlighting the dual impact of ELT on therapeutic resistance and clinical complexity.

Clinical implications

This complexity hampers management of patients with DTD, who are characterised by limited pharmacological responsiveness and heightened relapse risk. While exploring the ELT–DTD nexus, the review revealed a paucity of literature on the impact of ELT within DTD. Findings underscore the profound link between ELT and DTD, which is essential for comprehensive understanding and effective management. Tailoring treatments to address ELT could enhance therapeutic outcomes for patients with DTD. Future studies should use larger samples and well-defined diagnostic criteria and explore varied therapeutic approaches.

Keywords

Difficult-to-treat depressionearly life traumatreatment-resistant depressioncomorbidityscoping review
Type
Review Article
Information
BJPsych Bulletin , First View , pp. 1 - 12
Check for updates
Creative Commons
Creative Common License - CCCreative Common License - BY
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
Copyright © The Author(s), 2024. Published by Cambridge University Press on behalf of Royal College of Psychiatrists

Depression: beyond sadness

Depression, in its broadest sense, is a psychological condition marked by feelings of sadness and lack of interest in life's activities.Reference Salik and Marwaha1 Although it is common for individuals to experience transient periods of sadness or ‘feeling down’, these emotions are generally short-lived and can be related to specific events or circumstances. When these feelings become pervasive and persistent and begin to interfere with daily functioning, the progression from a mere emotional state to the clinical condition of depressive disorder occurs. This is a syndrome involving significant disturbances in emotions, neurocognitive functions, physiological functions and behaviour, indicating dysfunctions in psychological, biological or developmental processes, according to the ICD-112 and DSM-5 TR.3 Depressive disorder is associated with considerable disability and dysfunction in the personal, emotional, family, work and social realms, necessitating clinical intervention and treatment when these exceed the normal variations of behaviour from an individual, social or cultural perspective.Reference Ormel, Kessler and Schoevers4 Biological factors such as imbalances in neurotransmitters or hormones and genetic predispositions, as well as external factors such as trauma, loss and prolonged stress, contribute to the transition from simple states of sadness to various depressive disorders.Reference Chand and Arif5 In the ICD-11, developed by the World Health Organization with a global clinical perspective, depressive disorders are grouped into several categories: single-episode depressive disorder, recurrent depressive disorder, dysthymic disorder, mixed depressive and anxiety disorder, premenstrual dysphoric disorder, other specified depressive disorders, and unspecified depressive disorders. In the DSM-5, developed by the American Psychiatric Association and dominated by an Anglophone-American perspective, depressive disorders are classified as follows: disruptive mood dysregulation disorder, premenstrual dysphoric disorder, persistent depressive disorder (dysthymia), major depressive disorder, substance/medication-induced depressive disorder, and depressive disorder due to another medical condition. Research has shown that the origin of depression lies in a complex interplay of genetic and environmental factors. A family history of depression increases the risk of developing the condition,Reference Namkung, Lee and Sawa6,Reference Pham and Gardier7 and factors including neuroinflammation, neurodegenerative diseases, daily stress and traumatic experiences are particularly significant in older adults.Reference Roman and Irwin8Reference Harjono Hadiwiardjo and Damayanti10 Adverse childhood experiences (ACEs), including early traumas, have been recognised in terms of their impact on both post-traumatic stress disorder (PTSD) and depression.Reference Negele, Kaufhold, Kallenbach and Leuzinger-Bohleber11Reference Juul, Hjemdal and Aune13 The interaction between genetic predisposition and environmental factors, particularly early life trauma (ELT), plays a fundamental part in the development of depressive disorders that are difficult to treat, making their management a complex challenge.

Approaches to difficult-to-treat depression

In the past, the term ‘difficult-to-treat depression’ (DTD) was used interchangeably with ‘treatment-resistant depression’ (TRD). However, a significant paradigm shift occurred in 2020 when an international consensus recommended expanding the TRD model to encompass a more comprehensive perspective.Reference McAllister-Williams, Arango, Blier, Demyttenaere, Falkai and Gorwood14 The TRD model that emerged from studies by Thase and RushReference Thase and Rush15 was limited to individuals who showed resistance only to antidepressant medications or those who could not tolerate the initial drug. Thase and Rush proposed a five-stage model to address resistance to different classes of antidepressant. Over time, this model has been replaced by other classifications and has evolved and been variably defined to describe the failure of antidepressant pharmacological treatment in general. A systematic review identified 155 different definitions of TRD,Reference Brown, Rittenbach, Cheung, McKean, MacMaster and Clement16 whereas Wijeratne and SachdevReference Wijeratne and Sachdev17 noted that there are no formal diagnostic criteria for TRD, and one of its limitations is its exclusive application to acute treatments without considering the possibility of relapse after a transitional period of remission. Subsequently, Rush et alReference Rush, Sackeim, Conway, Bunker, Hollon and Demyttenaere18 listed a series of considerations regarding the concept of TRD. They questioned whether a lack of response or remission could define a treatment as failed, how to consider cases where patients improve but then relapse, whether to include cases where a medication cannot be tolerated in the definition of TRD, and whether previously failed treatments should be considered. Furthermore, they noted that definitions of TRD generally do not include non-pharmacological treatments, such as psychotherapy and psychosocial interventions, stating that ‘TRD has no practical, actionable clinical implications other than to suggest attempting another, primarily pharmacological, treatment trial with a different intervention or combination’.Reference Rush, Sackeim, Conway, Bunker, Hollon and Demyttenaere18 Currently, clinicians and researchers tend to adopt the definition formulated at the turn of the millennium by Souery et alReference Souery, Amsterdam, de Montigny, Lecrubier, Montgomery and Lipp19 and later adopted by the US Food and Drug Administration and the European Medicines Agency which defines TRD as the failure to respond to two or more antidepressant pharmacological regimens despite adequate dose and duration, as well as treatment adherence. In recent years, a significant transition from the TRD model to the DTD model has occurred. The DTD model highlights the importance of a perspective that transcends resistance to pharmacological treatments, favouring a broader and more inclusive approach to treating depression. It underscores the need to consider psychological, social and environmental factors that may influence the response to therapy. DTD is not conceived as a binary condition of therapeutic responses but rather as a continuum that includes full responses, partial responses and non-responses, thus shifting the focus of treatment from a curative model of symptom remission to a disease management model that emphasises functional improvement and quality of life, aiming for optimal symptom control without necessarily achieving complete elimination.Reference Paganin20 Currently, there are no uniform operational criteria used to precisely and measurably define DTD. However, the international consensus statementReference McAllister-Williams, Arango, Blier, Demyttenaere, Falkai and Gorwood14 proposed adopting a list of factors related to treatment, symptomatology and the patient to identify a clinical framework for DTD. A series of interventions were indicated, ranging from self-help methodologies to psychotherapies, pharmacological strategies, neurostimulation techniques and social interventions to support and facilitate access to general and specialised care and job integration. This will require an individualised intervention strategy that emphasises not only symptom remission but also improvement of the patient's psychosocial functionality. Whereas some patients may show a partial response to initial treatments yet remain functionally impaired, others may show no response. The clinical framework of DTD perceives the condition as treatable (albeit challenging) and underscores the need for personalised care and overcoming routine therapeutic paradigms. DTD encompasses a spectrum of severity and functional impairment, often coexisting with psychiatric or somatic comorbidities. Characterising DTD in clinical terms remains challenging and requires a sophisticated and multidimensional understanding.Reference Paganin, Signorini and Sciarretta21 This involves considering various aspects, including clinical manifestations, disease progression, biomedical elements, prognostic markers, neuropsychological aspects and treatment responses. Critical factors include the extent and duration of functional decline, symptom history, relapse patterns and the initial clinical profile, particularly the nature and number of unsuccessful therapeutic interventions, psychiatric and organic pathologies, and a history of childhood trauma. A prevalent observation among patients with TRD is a decline in the effectiveness of previously effective pharmacological treatments, suggesting changes in crucial neurobiological foundations. This observation also raises a concerning possibility: ineffective or partially effective treatments may induce neurobiological changes, reducing treatment responsiveness and exacerbating the intractability of depression.Reference Fava22Reference Paganin, Signorini, Leccese and Sciarretta24 Treatment resistance can worsen, leading to increased chronicity. Unlike a single episode of depression that typically responds to treatment and has no lasting impact on personality, persistent depression, with or without appropriate intervention, can shape the clinical trajectory of DTD. Patients with DTD may develop maladaptive behavioural and cognitive patterns that intensify pessimism and negative self-perception. Essentially, depression perpetuates itself, amplifying self-destructive thought patterns and worsening the condition. In evaluating patients with DTD, it is important to consider the clinical presentation of depressive symptoms, with a specific focus on the incidence of anhedonia and anxiety, as well as psychiatric comorbidities and/or concurrent general medical conditions, including substance use disorders. Furthermore, a meticulous evaluation of pharmacological interventions and the patient's functional deterioration is warranted.Reference Paganin20 The DTD model proposes that in cases where the patient with depression remains unresponsive to treatment, it is important to identify the underlying causes. In the context of medical history, attention should be paid to the number and sequence of previous therapeutic attempts, the types and number of therapeutic failures, as well as family history and treatment adherence. In addition, it is particularly important to identify significant childhood emotional traumas.Reference Negele, Kaufhold, Kallenbach and Leuzinger-Bohleber11,Reference Cohen, McNeil and Menon25 Events that may occur during an episode of major depression and can lead to DTD include: poor acute response to initial pharmacological treatment, risk of relapse despite ongoing treatment, and the use of multiple antidepressants. These factors could be used to help identify affected patients and to recognise subgroups or spectra of patients, potentially together with use of neuroinflammation biomarkers. A specialised taxonomy for DTD could be developed on the basis of assessment of distinctive characteristics that separate DTD cases from non-DTD cases. Such considerations may include comorbid general medical conditions, the nature and severity of anxiety symptoms, the presence of anhedonia, the extent and chronicity of environmental stressors, concurrent substance use or misuse disorders, and a history of early trauma or abuse;Reference McAllister-Williams, Arango, Blier, Demyttenaere, Falkai and Gorwood14,Reference Rush, Aaronson and Demyttenaere26 these factors may interact with other characteristics of DTD, adding complexity to the presentation. Psychosocial determinants of health may act as perpetuating factors and thus warrant attention to improve treatment outcomes. These determinants can include chronic stressors related to occupation, marital status, financial conditions or health problems, as well as lifestyle-related factors such as sedentary behaviour and obesity (see Fig. 1 for a summary of these characteristics).

Fig. 1 Key factors associated with difficult-to-treat depression (DTD), including early life trauma.

Moreover, predisposing elements such as ELT may have persistent effects on DTD by compromising resilience and problem-solving abilities.Reference Negele, Kaufhold, Kallenbach and Leuzinger-Bohleber11 In patients with DTD, ELT events represent important risk factors that can exacerbate the condition or develop into comorbid disorders, further complicating clinical treatment of depression.Reference Rush, Sackeim, Conway, Bunker, Hollon and Demyttenaere18 A history of ELT can also influence the effectiveness of therapeutic approaches, potentially compromising treatment outcomes. A comprehensive assessment focusing on potential ELT and the possibility of medical and psychiatric complications is crucial to devising effective therapeutic strategies for patients with DTD.

Definition of ELT

The term ACE was introduced by Vincent Felitti and Robert Anda between 1995 and 1997 to describe various forms of childhood trauma with significant long-term effects on physical and mental health. Initially, ACEs encompassed seven domains: physical, sexual and emotional abuse; living with individuals experiencing mental illness or substance misuse; and having an incarcerated family member.Reference Felitti, Anda, Nordenberg, Williamson, Spitz and Edwards27 Over time, the definition expanded to include parental separation, neglect and societal factors such as poverty, community violence, homelessness and intra-community violence. The concepts of early life stress (ELS) and ACEs encompass a wide array of stress-inducing and negative events. These events include but are not limited to maltreatment, neglect, parental separation or loss, exposure to extreme poverty, starvation, and various forms of violence within domestic, community or educational environments. Such experiences can occur at any point from infancy and throughout adolescence. ELS and ACE thus serve as umbrella terms, covering a diverse range of stressful or adverse experiences. Conversely, ELT and childhood trauma have been defined with greater specificity, referring to events that inflict significant traumatic impact. These classifications are reserved for events that pose imminent risks of harm or death or significantly compromise the physical safety of the individual or others. Such traumatic events trigger profound responses of horror, fear or helplessness, overwhelming an individual's coping mechanisms. Examples include acts of terrorism, experiences of war, natural and human-made disasters, physical and sexual abuse, medical trauma, motor vehicle accidents, and direct exposure to acts of violence such as homicides or suicides. Traumatic experiences are an important public health concern owing to their high prevalence, with 30–40% of adults reporting significant adverse experiences during their early life according to the literature.Reference Agorastos, Pervanidou, Chrousos and Baker28 The differences between traumatic events and traumatic experiences have been elaborated in the scientific literature and in psychiatric disorder classification systems such as the DSM-5 TR and ICD-11. According to these classifications, traumatic experiences include repeated exposure to physical and/or emotional neglect, maltreatment and sexual abuse. Although these exposures may not match the intensity of singular traumatic events, they nonetheless predispose individuals to syndromes such as complex PTSD (C-PTSD). Recent research indicates a convergence between the concepts of ACEs – representing concrete situations of social, personal, and interpersonal distress that negatively affect a child's emotional development – and ELS and ELT; depending on their operational definitions and contextual factors, these experiences exhibit significant overlap, demonstrating the complex interplay between different forms of early life adversity and their potential to precipitate enduring psychological effects.Reference Desch, Mansuri, Tran, Schwartz and Bakour29,Reference Barton, Ehring, Reinhard, Goerigk, Wüstenberg and Musil30 ELT encompasses a range of experiences potentially harmful to those under 18 years old.Reference Kulkarni, Leyden, Gavrilidis, Thew and Thomas31 Epidemiological research has demonstrated a strong link between ELT and mental health issues throughout life,Reference Moore, Scott, Ferrari, Mills, Dunne and Erskine32 indicating that such traumas cause lasting changes to the hypothalamic–pituitary–adrenal (HPA) axis and affect neurophysiological and inflammatory responses.Reference Westfall and Nemeroff Charles33 Defined as any negative childhood experience with long-term harm potential (Table 1), these events can disrupt crucial developmental stages, affecting a child's emotional regulation and relationship-building.Reference Cruz, Lichten, Berg and George40 Trauma includes abuse, neglect, exposure to violence, and life upheavals such as parental divorce or unstable living situations, which may be further complicated by domestic violence or separation from caregivers.Reference Smith and Pollak39 Early traumas undermine a child's sense of security and can have profound effects on development and health. They also set the stage for stress-related disorders by altering neurodevelopment and mental health. Neurobiologically, trauma can disrupt stress response systems and reducing hippocampal volume, which is essential for stress management and memory.Reference Teicher, Samson, Anderson and Ohashi38 Genetic factors and gene–environment interactions, such as FKBP5 polymorphisms, can increase vulnerability to stress and affect cortisol regulation.Reference Juul, Hjemdal and Aune13 Epigenetic mechanisms such as DNA methylation play an equally important part in modulation of gene expression without altering the DNA sequence.Reference Paganin and Signorini45 DNA methylation is a process in which a methyl group is added to specific DNA bases, often resulting in decreased expression of the corresponding gene. In response to trauma or stress, changes may occur in the methylation of specific genes involved in the stress response, such as the NR3C1 gene that codes for the glucocorticoid receptor.Reference McGowan, Sasaki, D'Alessio, Dymov, Labonté and Szyf46 However, not all individuals who experience childhood trauma develop psychopathological disorders,Reference Jozefiaková, Kaščáková, Adamkovič, Hašto and Tavel42 and the course and outcomes of early traumas can vary enormously from one individual to another, owing to many complex factors including genetics, environment, personal resources, individual resilience; social support can have a protective role, mitigating the negative effects of trauma.Reference Jozefiaková, Kaščáková, Adamkovič, Hašto and Tavel42 Childhood trauma is associated with a wide range of physical health conditions including cardiovascular diseases, immune system dysfunctions, endocrine disorders, gastrointestinal issues, chronic pain and respiratory diseases.Reference Danese, Moffitt, Harrington, Milne, Polanczyk and Pariante44 The likelihood of developing specific mental health disorders, including depression, anxiety disorders, eating disorders, dissociative disorders, sleep disorders, attention-deficit hyperactivity disorder (ADHD), PTSD, C-PTSD, substance use disorders, and personality disorders, is influenced by childhood traumas.Reference Agorastos, Pervanidou, Chrousos and Baker28,Reference Wolff and Shi34,Reference Waldinger, Schulz, Barsky and Ahern47 These disorders can be addressed through a combination of psychological and pharmacological interventions, depending on the individual needs of the patient. Psychological interventions may include cognitive–behavioural therapy (CBT), exposure therapy, mentalisation-based therapy and emotion regulation therapy, whereas pharmacological therapy can be used to treat specific symptoms such as anxiety or depression.Reference Cruz, Lichten, Berg and George40,Reference McKay, Cannon, Chambers, Conroy, Coughlan and Dodd41 Treatment of early trauma always requires an integrated and personalised approach, taking into account the individual needs of the patient and their specific traumatic experiences. ELT is associated with various comorbidities, although there has been a particular focus on the heightened risk of developing PTSD and its severe form, C-PTSD.Reference Wolff and Shi34,Reference Thomaes, Dorrepaal, van Balkom, Veltman, Smit and Hoogendoorn37,Reference Waldinger, Schulz, Barsky and Ahern47,Reference McLaughlin, Koenen, Hill, Petukhova, Sampson and Zaslavsky48 Studies indicate that the prevalence of these disorders varies, with approximately 28% of adults who have experienced childhood abuse meeting the criteria for PTSD and 32% meeting those for C-PTSD.Reference Bernhard, Martinelli, Ackermann, Saure and Freitag35,Reference Haselgruber, Sölva and Lueger-Schuster36 Whereas PTSD typically stems from a single traumatic event and is characterised by symptoms such as flashbacks and hyperarousal, C-PTSD results from prolonged traumas and involves issues with emotional regulation and attachment. In addition, the repercussions of early trauma extend beyond the individual, encompassing intergenerational effects that affect the mental health and well-being of future generations.Reference Reese, Barlow, Dillon, Villalon, Barnes and Crandall43 Neuroendocrine dysregulation, which affects a range of physiological and psychological functions, has been identified as a factor contributing to the co-occurrence of depressive disorders and post-traumatic disorders.Reference Sherin and Nemeroff49,Reference Schiller, Ben-Shaanan and Rolls50

Table 1 Effects of early life trauma, including neurobiological, psychological, cognitive and social impacts, comorbidities and intergenerational transmission

Given the absence of systematic reviews thoroughly exploring the interplay between ELT and DTD, we considered that a scoping review specifically focused on this subject would be timely and relevant. In this review, we aimed to catalogue and analyse the body of existing studies, highlighting both well-established areas of research and those that are emerging or insufficiently explored. Moreover, we endeavoured to provide an updated compendium to outline both current knowledge and information gaps and guide future research. Overall, the goal was to broaden our understanding of the impacts of ELT on DTD and to facilitate the development of targeted and effective therapeutic approaches based on robust and relevant evidence.

Materials and method

Objectives

This scoping review aimed to identify and explore the scientific literature on the role of ELT and its outcomes in DTD. The review was performed in line with the PRISMA Extension for Scoping Review criteria.Reference Tricco, Lillie, Zarin, O'Brien, Colquhoun and Levac51

Method

We conducted a thorough literature search across multiple databases, including the Cochrane Library, PubMed, Scopus and PsycINFO, as well as searching for grey literature in OPEN GREY, using the following keyword string: (‘early life trauma’ OR ‘childhood trauma’ OR ‘early adversity’) AND (‘difficult-to-treat depression’ OR ‘treatment-resistant depression’ OR ‘refractory depression’) AND (‘longitudinal’ OR ‘outcome’ OR ‘follow-up’). The search parameters were tailored to the respective fields of each database. This search yielded 56 research articles from 1 January 2013, to 21 October 2023 (Fig. 2).

Fig. 2 PRISMA flow chart.

Study selection

Initially, the retrieved citations were independently screened by two blinded reviewers (W.P. and S.S.) at the title and/or abstract level, with discrepancies resolved by reaching a consensus. Potentially relevant reports were then fully assessed based on explicit selection criteria. Inclusion criteria included: (a) human studies; (b) studies involving patients with treatment-resistant or difficult-to-treat depressive disorders, particularly those that characterised and explained these conditions in the context of childhood trauma; and (c) studies of interventions intended to treat childhood traumas in the context of DTD. Exclusion criteria were: (a) non-human contexts; (b) report duplications, (c) off-topic research and (d) studies focusing on combat-related traumas.

Data extraction

Data were independently extracted by two blinded reviewers (W.P. and S.S.) using predefined electronic forms, with disagreements resolved by reaching a consensus. The end-points of interest for this scoping review were the relationship between early childhood trauma and treatment-resistant or difficult-to-treat depressive disorders in adults. Given the exploratory yet comprehensive scope of this review, no explicit primary end-point was specified.

Internal validity and quality assessment

The quality of the included studies was independently assessed by two blinded reviewers (W.P. and S.S.). The quality assessment tools used were the Jadad scale for randomised controlled trials, the STROBE checklist for observational studies and the AMSTAR checklist for meta-analyses. For survey studies, letters and reviews, qualitative assessment was performed.

Synthesis of results

The extracted data were thematically synthesised to identify common patterns and key themes across the studies. This involved grouping studies by their primary focus (for instance, intervention studies, epidemiological studies and reviews), identifying key findings and findings related to the impact of early trauma on DTD, and summarising the findings using tables and figures to highlight significant patterns and themes. For details of the assessment criteria and results, see Table 2.

Table 2 Summary of studies

RCT, randomised controlled trial.

Results

This scoping review of the scientific literature found that there have been limited numbers of studies explicitly investigating the role of ELT in DTD. This may be because the DTD paradigm is still in its early stages, and therefore no substantial body of research on its correlation with ELT has yet been generated. However, studies have explored the mechanisms through which ELT may affect depressive conditions that are related to the emerging concept of DTD. The studies reviewed here varied widely in their methodologies, populations and definitions of ELT and DTD, complicating the synthesis of findings and the potential to draw definitive conclusions. We detected potential biases in the studies, including selection bias and recall bias, which could affect the validity of the results. We also noted a paucity of longitudinal studies that could provide insights into the long-term effects of ELT on DTD; such studies will be crucial for understanding the progression and treatment of the condition. One study examined phenotypic data from the 23andMe survey and identified a significant correlation between experience of traumatic life events, especially in childhood, and severity of TRD.Reference Li, Tian, McIntyre, Sun, Hinds and Narayan60 However, the precise mechanisms underlying this relationship require further investigation. In the field of psychotherapy, the cognitive–behavioural analysis system of psychotherapy (CBASP) is a model particularly relevant to treatment of depression due to childhood trauma. CBASP incorporates elements of CBT and psychodynamic psychotherapy and is designed to help patients understand the impact of their behaviour on others and modify dysfunctional behavioural patterns through a process called ‘personal engagement discipline’. However, Brakemeier et alReference Brakemeier, Radtke, Engel, Zimmermann, Tuschen-Caffier and Hautzinger53 found that the integration of CBASP with standard pharmacological therapies could initially exacerbate depression symptoms, particularly when addressing issues of trauma in the initial stages of therapy. Concomitantly, Stevenson et alReference Stevenson, Haliburn and Halovic55 reported substantial improvements in patients with TRD and histories of childhood trauma using the conversational model, despite the presence of comorbid severe personality disorders. Customisation is another key aspect of treatment for patients with TRD. Results of the GEParD and DaCFail studies (research projects exploring various facets of TRD) suggest that personalisation based on variables such as comorbidity, genetic profiles, and history of traumatic life events is a promising approach to developing frameworks to treat DTD.Reference Lichter, Klüpfel, Stonawski, Hommers, Blickle and Burschka73 However, despite extensive research, the precise role to which childhood trauma needs to be taken into account in treatment approaches remains unclear. Taylor et alReference Taylor, Coleman, Lawrence, Strawbridge, Zahn and Cleare68 found that ELT had predictive value for TRD in hospital settings, indicating a need for personalised therapeutic strategies. Strawbridge et alReference Strawbridge, Hodsoll, Powell, Hotopf, Hatch and Breen62 investigated the biological links between traumatic experiences and neuroinflammation in patients with TRD and identified a connection between ELT and elevated IL-12p70 levels. Maruani et alReference Maruani, Molière, Godin, Yrondi, Bennabi and Richieri72 explored the relationships among sleep patterns, depressive symptoms and childhood trauma and found that evening chronotype may exacerbate depression. However, conflicting findings were reported by the Childhood Trauma Meta-Analysis Study Group, which found that MDD patients with ELT responded well to both pharmacological and psychotherapeutic treatments. Benjamin et alReference Benjamin, Hershenberg, Dorrell, Tan, Riva-Posse and McDonald77 found that sexual and gender minority (SGM) patients with TRD often had more severe histories of childhood trauma and increased suicide risk. However, treatment recommendations did not significantly differ between SGM and non-SGM groups, suggesting the need for more tailored approaches. Gruhn et alReference Gruhn, Phan, Klumpp, Ajilore and Gorka65 emphasised the complex responses of ELT patients to pharmacological and CBT and advocated the personalisation of treatment. Tunnard et alReference Tunnard, Rane, Wooderson, Markopoulou, Poon and Fekadu52 reported that childhood trauma may lead to a more severe course of depressive illness and increased suicide risk in patients with TRD. In 2015, Cladder-Micus et alReference Cladder-Micus, Vrijsen, Becker, Donders, Spijker and Speckens54 suggested that mindfulness-based cognitive therapy (MBCT) could be effective for ELT patients; however, their 2023 follow-up did not confirm this finding.Reference Cladder-Micus, Vrijsen, Fest, Spijker, Donders and Becker74 Fischer et alReference Fischer, Simon, Elsner, Dobmeier, Dorr and Blei69 examined the potential correlations of childhood trauma, TRD and levels of high-sensitivity C-reactive protein, raising questions about biomarkers of childhood trauma. Minelli et alReference Minelli, Zampieri, Sacco, Bazzanella, Mezzetti and Tessari58 studied the effects of trauma-focused psychotherapies (eye movement desensitisation and reprocessing (EMDR) and trauma-focused CBT) in TRD patients with trauma histories and found that EMDR showed marginal superiority in reducing depressive symptoms. Fond et alReference Fond, Faugere, Boyer, Peri, Stephan and Moliere76 investigated long-term benzodiazepine use by patients with TRD and reported potential links with childhood trauma. Yrondi et alReference Yrondi, Aouizerate, Bennabi, Richieri, D'Amato and Bellivier64 found that childhood maltreatment was associated with increased TRD severity, indicating a need for more personalised therapies. They subsequently extended this research to a geriatric population,Reference Yrondi, Arbus, Bennabi, D'Amato, Bellivier and Bougerol67 finding an association of childhood physical abuse with depression severity in advanced age. O'Brien et alReference O'Brien, Lijffijt, Wells, Swann and Mathew59,Reference O'Brien, Lijffijt, Lee, Kim, Wells and Murphy66,Reference O'Brien, Lee, Kim, Nandra, Pannu and Swann71 suggested that ketamine may be effective for ELT patients with TRD, particularly those with histories of childhood abuse. Nelson and colleagues, in their 2017 meta-analyses, demonstrated a significantly higher risk of depression, especially severe depression and TRD, in individuals with histories of childhood maltreatment.Reference Nelson, Klumparendt, Doebler and Ehring57 In 2020, Nikkheslat et alReference Nikkheslat, McLaughlin, Hastings, Zajkowska, Nettis and Mariani63 reported decreased antidepressant efficacy in those with childhood traumas, potentially linked to hyperactivation of the HPA axis. Michalak et alReference Michalak, Probst, Heidenreich, Bissantz and Schramm56 and Stevenson et alReference Stevenson, Haliburn and Halovic55 explored the impact of childhood adversities on chronic depression through various therapeutic approaches. Michalak et al found MBCT and CBASP to be more effective for chronic depression, especially in patients with experience of childhood adversities, whereas Stevenson et al emphasised the role of trauma-informed psychodynamic psychotherapy in treating chronic TRD, which is often associated with personality disorders and early trauma. In summary, studies highlight the need for personalised, trauma-informed approaches to treating DTD in individuals with a history of ELT. For details of the reviewed studies, see Supplementary Table 1 available at https://doi.org/10.1192/bjb.2024.75.

Several recurring themes emerged from our review, which can be summarised as follows.

  • Role of ELT: childhood traumas significantly affect the development of depression, its severity and resistance to conventional treatments.

  • Underlying mechanisms: there is growing interest in mechanisms such as chronic inflammation that could underlie the connections between childhood traumas and DTD.

  • Biomarkers: identifying biomarkers associated with childhood traumas could provide tools for more precise diagnosis and treatment.

  • Comorbidities: medical, metabolic and psychiatric comorbidities are often correlated with a history of adversity in childhood and can complicate treatment responses.

  • Complexity of treatment: traumas experienced in childhood can affect the efficacy of therapies, suggesting the need for a personalised therapeutic approach.

  • Overcoming traditional limits: as individuals with ELT may experience reduced effectiveness of antidepressants, there is a need for personalised and innovative treatment approaches such as CBASP and the conversational model, although more research is required to confirm their efficacy in patients with ELT; ketamine is also being explored with respect to its potential use in treatment-resistant cases.

  • Trauma-focused psychotherapies: the efficacy of therapies such as EMDR and trauma-focused CBT in patients with DTD is an emerging area of research.

  • Methodological limitations: further research with larger samples and more rigorous methodologies is needed to confirm the findings of most of the studies.

ELT has a significant impact on the pathogenesis and treatment of DTD is significant, although gaps in knowledge persist. As well as increasing the risk of DTD, early traumas may complicate its management, reducing the effectiveness of standard therapies. Given the enduring effects of ELT, the importance of personalised treatments must be emphasised. A comprehensive evaluation of childhood trauma history is essential for effective management of DTD. An integrated clinical approach, encompassing pharmacological, psychotherapeutic and neurostimulatory therapies tailored to individual cases, is recommended. Further research is warranted to refine therapeutic strategies for this specific patient subgroup.

Discussion

The results of our scoping review indicate a complex relationship between ELT and DTD, in which ELT is a significant risk factor that not only contributes to the development and persistence of depressive disorders but also complicates their clinical management. The impact of ELT on various parameters of DTD (Fig. 3) indicates how early adversities affect multiple dimensions of an individual's life, including overall resilience, treatment response and functional outcomes, and have a crucial role in shaping the parameters that contribute to the manifestation of DTD.

Fig. 3 The relationship between early life trauma (ELT) and difficult-to-treat depression (DTD), in which ELT is a significant risk factor, not only contributes to the development and persistence of depressive disorders but also complicates their clinical management.

ELT is associated with elevated rates of treatment failure, with individuals often experiencing multiple failed attempts owing to the complex interaction between trauma-induced neurobiological changes and psychological adaptations. These factors reduce the effectiveness of standard pharmacological and psychotherapeutic interventions. The chronicity and severity of depressive symptoms in patients with ELT mean that they may receive various forms of therapy, not all of which are effective, resulting in a sequence of failed treatments. Thus, there is a need for personalised therapeutic strategies. ELT significantly contributes to the development of both psychiatric and medical comorbidities, including PTSD, anxiety disorders, personality disorders, substance use disorders and chronic pain syndromes, further complicating the clinical picture of DTD and making remission difficult to achieve.

Patients with DTD often have significant functional impairments in various areas of life, including interpersonal relationships, occupational functioning and overall quality of life. The variability in symptom presentation further complicates the course and treatment of their depression. The presence of ELT interacts with genetic predispositions, influencing familial patterns of depressive disorders and suggesting that individuals with a family history of depression and ELT are at higher risk of developing more severe and treatment-resistant forms of depression. Neurobiological alterations resulting from ELT, such as changes in the HPA axis and increased levels of inflammatory markers, contribute to the pathophysiology of DTD, affecting the brain's stress response systems and reducing the efficacy of antidepressants and other therapeutic interventions. ELT is closely linked to specific symptomatic features such as anhedonia and anxiety, which are difficult to treat. The course of depression in these patients is often severe and chronic, with frequent relapses and incomplete remissions.Reference Tunnard, Rane, Wooderson, Markopoulou, Poon and Fekadu52,Reference Nelson, Klumparendt, Doebler and Ehring57,Reference Nikkheslat, McLaughlin, Hastings, Zajkowska, Nettis and Mariani63,Reference Yrondi, Aouizerate, Bennabi, Richieri, D'Amato and Bellivier64

Trauma-related factors can also influence treatment adherence, as individuals with ELT may have trust issues and difficulty establishing therapeutic alliances. In addition, concomitant medications for comorbid conditions can further complicate the management of DTD. When DTD is suspected, clinical re-evaluations are strongly recommended to detect possible ELT as an underlying cause of DTD. The presence of such disorders can lead to treatment resistance, facilitated by the negative mutual interference of the two disorders and the individual's poor coping and problem-solving skills, as well as a lack of general resilience.Reference Giampetruzzi, Tan, LoPilato, Kitay, Riva Posse and McDonald75

The presence of ELT in the anamnesis is associated with an increased risk of relapse in depressive disorders, often triggering a persistent and recurrent course of the illness, and there is evidence of more psychopathological manifestations such as anxiety, anhedonia and apathy in such cases.Reference Cladder-Micus, Vrijsen, Fest, Spijker, Donders and Becker74 The emotional consequences of trauma can also translate into increased suicidal ideation and profound emotional distress, culminating in a pervasive sense of despair.Reference Levy, El-Hage, Bennabi, Allauze, Bouvard and Camus70 This in turn affects emotional, cognitive and somatic domains, leading to complex interactions between ELT and depressive symptoms in adulthood.Reference Robakis, Watson-Lin, Wroolie, Myoraku, Nasca and Bigio61 The difficulty of treatment is further exacerbated by neurobiological alterations resulting from childhood trauma, which can lead to impulsivity and high-risk behaviours that impede adherence to care.Reference Nikkheslat, McLaughlin, Hastings, Zajkowska, Nettis and Mariani63,Reference Fischer, Simon, Elsner, Dobmeier, Dorr and Blei69 Hyperarousal states resulting from severe traumas, which are characterised by hypervigilance and impaired concentration, can disrupt attentional processes, generating symptoms similar to those of ADHD;Reference Cuffe, McCullough and Pumariega79 indeed, these states can be mistaken for ADHD. In the therapeutic context, those who do not respond or only partially respond to treatments often have more severe trauma histories compared with those who show a favourable response, indicating a negative impact of childhood adversity on treatment outcomes. Over time, the cumulative effects of childhood trauma can lead to marked functional decline and increased symptom variability. Therefore, early identification of childhood trauma is crucial for the effective management of DTD, as is the use of a targeted and personalised therapeutic approach.

Integration of evidence-based therapies such as EMDR and trauma-focused CBT is fundamental to directly addressing the role of ELT in DTD. EMDR, in which eye movements are used to help patients process and overcome the emotional effects of traumatic memories, is particularly effective in treating PTSD. Similarly, trauma-focused CBT helps patients to restructure negative thoughts related to trauma, providing effective strategies for managing emotions and reactions. Integrating these therapies into the treatment plan for TRD could offer more effective care pathways, overcoming the barriers to healing imposed by trauma.Reference Michalak, Probst, Heidenreich, Bissantz and Schramm56,Reference Minelli, Zampieri, Sacco, Bazzanella, Mezzetti and Tessari58,Reference Cladder-Micus, Vrijsen, Fest, Spijker, Donders and Becker74

Overall, approaches based on the use of psychotherapies in conjunction with pharmacological therapy have proven particularly effective for patients with DTD.Reference Cladder-Micus, Vrijsen, Becker, Donders, Spijker and Speckens54,Reference Stevenson, Haliburn and Halovic55,Reference Gruhn, Phan, Klumpp, Ajilore and Gorka65,Reference Kuzminskaite, Gathier, Cuijpers, Penninx, Ammerman and Brakemeier78 ELT not only increases the risk of developing DTD but is also closely linked to the severity of symptoms and less favourable treatment outcomes.Reference Tunnard, Rane, Wooderson, Markopoulou, Poon and Fekadu52,Reference Nelson, Klumparendt, Doebler and Ehring57,Reference Yrondi, Aouizerate, Bennabi, Richieri, D'Amato and Bellivier64,Reference Yrondi, Arbus, Bennabi, D'Amato, Bellivier and Bougerol67 This results in more severe symptoms, resistance to standard therapies and ‘masked’ disorders that can be misinterpreted as other conditions. The comorbidity between PTSD and DTD adds a further layer of complexity, negatively influencing the patient's social interactions and coping strategies. Directly addressing the role of childhood trauma can be decisive in improving the treatment response of patients with depression. A comprehensive assessment of the presence of ELT is necessary, both to identify the full clinical expression of the patient's psychiatric disorder and evaluate their prognosis, and to develop an effective and exhaustive care pathway that considers the relative importance of all aspects of the disorder (psychopathological, cognitive, global functioning, psycho-affective).

Our review, despite intrinsic limitations owing to the scarcity of scientific literature on the topic, unequivocally confirms the close connection between childhood trauma in relation to TRD. This indicates that psychotherapeutic interventions should be considered to be an integral part of the treatment of DTD.

Conclusions

This review underscores several pivotal point, which can be summarised as follows.

  • The established correlation between ELT and DTD is fundamental to both our understanding of DTD and its therapeutic management. Recognising this relationship will be vital in tailoring treatment approaches that directly address the underlying trauma, potentially leading to improved clinical outcomes.

  • Management of DTD requires integrated and tailored therapies specifically targeting the repercussions of ELT. Personalised treatment plans are key; these should aim not only to improve DTD symptoms but also to provide patients with the means to overcome the multiple psychological and health challenges resulting from early childhood adversity. Recognising and addressing childhood trauma is central to improving therapeutic outcomes for patients with DTD, and there is a need to adopt psychotherapies specifically directed at these intertwined conditions.

  • There is an urgent need to advance our understanding of DTD and develop innovative diagnostic and therapeutic strategies that acknowledge the impact of childhood trauma. This will require methodologically robust studies with ample sample sizes to validate and extend existing knowledge. Such research endeavours should investigate the neurobiological and psychosocial mechanisms linking ELT to DTD, with the aim of guiding the development of more effective treatments for this complex condition.

Addressing the nuanced interplay between ELT and DTD is of paramount importance. A multidisciplinary approach based on comprehensive research and innovative treatments will be essential to overcoming the challenges of DTD and offering hope and improved care for those affected.

About the authors

Walter Paganin is a psychiatrist-psychotherapist and PhD candidate in neuroscience at the University of Tor Vergata, Rome, Italy. Sabrina Signorini is a psychologist and psychotherapist at the StudioPsicologiaSignorini, Guidonia, Rome, Italy. Antonio Sciarretta is a psychiatrist at IHG, Guidonia, Rome, Italy.

Supplementary material

Supplementary material is available online at https://doi.org/10.1192/bjb.2024.75.

Data availability

The data that support the findings of this study are available from the corresponding author, W.P., upon reasonable request.

Author contributions

W.P. was the principal investigator and was responsible for the majority of the research and the writing and revision of the manuscript. S.S. contributed to the data analysis and literature review. A.S. assisted with the data analysis. All authors reviewed and approved the final version of the manuscript.

Funding

None.

Declaration of interest

None.

References

Salik, I, Marwaha, R. Electroconvulsive therapy. StatPearls 2023. Availabe from: https://www.ncbi.nlm.nih.gov/books/NBK538266/.Google Scholar
World Health Organization (WHO). International Classification of Diseases (11th revision). WHO, 2022.Google Scholar
American Psychiatric Association (APA). Diagnostic and Statistical Manual of Mental Disorders (5th edn, text revision). APA, 2022.Google Scholar
Ormel, J, Kessler, RC, Schoevers, R. Depression: more treatment but no drop in prevalence: how effective is treatment? And can we do better? Curr Opin Psychiatry 2019; 32(4): 348–54.CrossRefGoogle ScholarPubMed
Chand, SP, Arif, H. Depression. StatPearls 2023. Available from: https://www.ncbi.nlm.nih.gov/books/NBK430847/.Google ScholarPubMed
Namkung, H, Lee, BJ, Sawa, A. Causal inference on pathophysiological mediators in psychiatry. Cold Spring Harb Symp Quant Biol 2018; 83: 1723.10.1101/sqb.2018.83.037655CrossRefGoogle ScholarPubMed
Pham, TH, Gardier, AM. Fast-acting antidepressant activity of ketamine: highlights on brain serotonin, glutamate, and GABA neurotransmission in preclinical studies. Pharmacol Ther 2019; 199: 5890.CrossRefGoogle ScholarPubMed
Roman, M, Irwin, MR. Novel neuroimmunologic therapeutics in depression: a clinical perspective on what we know so far. Brain Behav Immun 2020; 83: 721.CrossRefGoogle ScholarPubMed
Autry, AE. Function of brain-derived neurotrophic factor in the hypothalamus: implications for depression pathology. Front Mol Neurosci 2022; 15: 1028223.CrossRefGoogle ScholarPubMed
Harjono Hadiwiardjo, Y, Damayanti, R. Biopsychosocial factors associated with depression in the elderly: a systematic literature review. F1000Res 2022; 11: 1068.CrossRefGoogle Scholar
Negele, A, Kaufhold, J, Kallenbach, L, Leuzinger-Bohleber, M. Childhood trauma and its relation to chronic depression in adulthood. Depress Res Treat 2015; 2015: 650804.Google ScholarPubMed
Remes, O, Mendes, JF, Templeton, P. Biological, psychological, and social determinants of depression: a review of recent literature. Brain Sci 2021; 11(12): 1633.CrossRefGoogle ScholarPubMed
Juul, EML, Hjemdal, O, Aune, T. Prevalence of depressive symptoms among older children and young adolescents: a longitudinal population-based study. Scand J Child Adolesc Psychiatry Psychol 2021; 9(1): 6472.Google Scholar
McAllister-Williams, RH, Arango, C, Blier, P, Demyttenaere, K, Falkai, P, Gorwood, P, et al. The identification, assessment and management of difficult-to-treat depression: an international consensus statement. J Affect Disord 2020; 267: 264–82.10.1016/j.jad.2020.02.023CrossRefGoogle ScholarPubMed
Thase, ME, Rush, AJ. When at first you don't succeed: sequential strategies for antidepressant nonresponders. J Clin Psychiatry 1997; 58(13): 23–9.Google ScholarPubMed
Brown, S, Rittenbach, K, Cheung, S, McKean, G, MacMaster, FP, Clement, F. Current and common definitions of treatment-resistant depression: findings from a systematic review and qualitative interviews. Can J Psychiatry 2019; 64(6): 380–7.CrossRefGoogle ScholarPubMed
Wijeratne, C, Sachdev, P. Treatment-resistant depression: critique of current approaches. Aust N Z J Psychiatry 2008; 42(9): 751–62.10.1080/00048670802277206CrossRefGoogle ScholarPubMed
Rush, AJ, Sackeim, HA, Conway, CR, Bunker, MT, Hollon, SD, Demyttenaere, K, et al. Clinical research challenges posed by difficult-to-treat depression. Psychol Med 2022; 52(3): 419–32.CrossRefGoogle ScholarPubMed
Souery, D, Amsterdam, J, de Montigny, C, Lecrubier, Y, Montgomery, S, Lipp, O, et al. Treatment resistant depression: methodological overview and operational criteria. Eur Neuropsychopharmacol 1999; 9(1–2): 8391.CrossRefGoogle Scholar
Paganin, W. Viewpoint: difficult-to-treat depression versus treatment-resistant depression: a new integrative perspective for managing depression. Eur Psychiatry 2023; 66(1): e73.10.1192/j.eurpsy.2023.2448CrossRefGoogle ScholarPubMed
Paganin, W, Signorini, S, Sciarretta, A. Difficult-to-treat depression. Scoping review. Clin Neuropsychiatry 2023; 20(3): 173–82.Google ScholarPubMed
Fava, GA. Can long-term treatment with antidepressant drugs worsen the course of depression? J Clin Psychiatry 2003; 64(2): 123–33.10.4088/JCP.v64n0204CrossRefGoogle ScholarPubMed
Andrews, P, Amsterdam, J. A hormetic approach to understanding antidepressant effectiveness and the development of antidepressant tolerance – a conceptual view. Psychiatr Pol 2020; 54(6): 1067–90.CrossRefGoogle ScholarPubMed
Paganin, W, Signorini, S, Leccese, V, Sciarretta, A. Depressione resistente a trattamento. Dalla classificazione alle nuove terapie. Riv Psichiatr 2022; 57(6): 258–72.Google Scholar
Cohen, JR, McNeil, S, Menon, SV. Childhood maltreatment and anhedonic symptoms: test of a dual-risk model in emerging adults. J Interpers Violence 2022; 37(9–10): NP744769.CrossRefGoogle Scholar
Rush, AJ, Aaronson, ST, Demyttenaere, K. Difficult-to-treat depression: a clinical and research roadmap for when remission is elusive. Aust N Z J Psychiatry 2019; 53(2): 109–18.CrossRefGoogle ScholarPubMed
Felitti, VJ, Anda, RF, Nordenberg, D, Williamson, DF, Spitz, AM, Edwards, V, et al. Relationship of childhood abuse and household dysfunction to many of the leading causes of death in adults. American J Prev Med 1998; 14(4): 245–58.CrossRefGoogle ScholarPubMed
Agorastos, A, Pervanidou, P, Chrousos, GP, Baker, DG. Developmental trajectories of early life stress and trauma: a narrative review on neurobiological aspects beyond stress system dysregulation. Front Psychiatry 2019; 10: 118.10.3389/fpsyt.2019.00118CrossRefGoogle ScholarPubMed
Desch, J, Mansuri, F, Tran, D, Schwartz, SW, Bakour, C. The association between adverse childhood experiences and depression trajectories in the Add Health study. Child Abuse Neglect 2023; 137: 106034.CrossRefGoogle ScholarPubMed
Barton, BB, Ehring, T, Reinhard, MA, Goerigk, S, Wüstenberg, T, Musil, R, et al. Effects of resilience and timing of adverse and adaptive experiences on interpersonal behavior: a transdiagnostic study in a clinical sample. Sci Rep 2023; 13(1): 18131.10.1038/s41598-023-44555-zCrossRefGoogle ScholarPubMed
Kulkarni, J, Leyden, O, Gavrilidis, E, Thew, C, Thomas, EHX. The prevalence of early life trauma in premenstrual dysphoric disorder (PMDD). Psychiatry Res 2022; 308: 114381.CrossRefGoogle ScholarPubMed
Moore, SE, Scott, JG, Ferrari, AJ, Mills, R, Dunne, MP, Erskine, HE, et al. Burden attributable to child maltreatment in Australia. Child Abuse Negl 2015; 48: 208–20.CrossRefGoogle Scholar
Westfall, NC, Nemeroff Charles, B. The preeminence of early life trauma as a risk factor for worsened long-term health outcomes in women. Curr Psychiatry Rep 2015; 17(11): 90.CrossRefGoogle ScholarPubMed
Wolff, N, Shi, J. Childhood and adult trauma experiences of incarcerated persons and their relationship to adult behavioral health problems and treatment. IJERPH 2012; 9(5): 1908–26.CrossRefGoogle Scholar
Bernhard, A, Martinelli, A, Ackermann, K, Saure, D, Freitag, CM. Association of trauma, posttraumatic stress disorder and conduct disorder: a systematic review and meta-analysis. Neurosci Biobehav Rev 2018; 91: 153–69.10.1016/j.neubiorev.2016.12.019CrossRefGoogle ScholarPubMed
Haselgruber, A, Sölva, K, Lueger-Schuster, B. Validation of ICD -11 PTSD and complex PTSD in foster children using the international trauma questionnaire. Acta Psychiatr Scand 2020; 141(1): 6073.CrossRefGoogle ScholarPubMed
Thomaes, K, Dorrepaal, E, van Balkom, AJLM, Veltman, DJ, Smit, JH, Hoogendoorn, AW, et al. [Complex PTSD following early-childhood trauma: emotion-regulation training as addition to the PTSD guideline]. Tijdschr Psychiatr 2015; 57(3): 171–82.Google Scholar
Teicher, MH, Samson, JA, Anderson, CM, Ohashi, K. The effects of childhood maltreatment on brain structure, function and connectivity. Nat Rev Neurosci 2016; 17(10): 652–66.CrossRefGoogle ScholarPubMed
Smith, KE, Pollak, SD. Early life stress and development: potential mechanisms for adverse outcomes. J Neurodevelop Disord 2020; 12(1): 34.10.1186/s11689-020-09337-yCrossRefGoogle ScholarPubMed
Cruz, D, Lichten, M, Berg, K, George, P. Developmental trauma: conceptual framework, associated risks and comorbidities, and evaluation and treatment. Front Psychiatry 2022; 13: 800687.CrossRefGoogle Scholar
McKay, MT, Cannon, M, Chambers, D, Conroy, RM, Coughlan, H, Dodd, P, et al. Childhood trauma and adult mental disorder: a systematic review and meta-analysis of longitudinal cohort studies. Acta Psychiatr Scand 2021; 143(3): 189205.CrossRefGoogle ScholarPubMed
Jozefiaková, B, Kaščáková, N, Adamkovič, M, Hašto, J, Tavel, P. Posttraumatic growth and its measurement: a closer look at the PTGI's psychometric properties and structure. Front Psychol 2022; 13: 801812.10.3389/fpsyg.2022.801812CrossRefGoogle Scholar
Reese, EM, Barlow, MJ, Dillon, M, Villalon, S, Barnes, MD, Crandall, A. Intergenerational transmission of trauma: the mediating effects of family health. IJERPH 2022; 19(10): 5944.CrossRefGoogle ScholarPubMed
Danese, A, Moffitt, TE, Harrington, H, Milne, BJ, Polanczyk, G, Pariante, CM, et al. Adverse childhood experiences and adult risk factors for age-related disease: depression, inflammation, and clustering of metabolic risk markers. Arch Pediatr Adolesc Med 2009; 163(12): 1135–43.CrossRefGoogle ScholarPubMed
Paganin, W, Signorini, S. Biomarkers of post-traumatic stress disorder from emotional trauma: a systematic review. Eur J Trauma Dissoc 2023; 7(2): 100328.CrossRefGoogle Scholar
McGowan, PO, Sasaki, A, D'Alessio, AC, Dymov, S, Labonté, B, Szyf, M, et al. Epigenetic regulation of the glucocorticoid receptor in human brain associates with childhood abuse. Nat Neurosci 2009; 12(3): 342–8.CrossRefGoogle ScholarPubMed
Waldinger, RJ, Schulz, MS, Barsky, AJ, Ahern, DK. Mapping the road from childhood trauma to adult somatization: the role of attachment. Psychosom Med 2006; 68(1): 129–35.CrossRefGoogle Scholar
McLaughlin, KA, Koenen, KC, Hill, ED, Petukhova, M, Sampson, NA, Zaslavsky, AM, et al. Trauma exposure and posttraumatic stress disorder in a national sample of adolescents. J Am Acad Child Adolesc Psychiatry 2013; 52(8): 81530.e14.CrossRefGoogle Scholar
Sherin, JE, Nemeroff, CB. Post-traumatic stress disorder: the neurobiological impact of psychological trauma. Dialogues Clin Neurosci 2011; 13(3): 263–78.CrossRefGoogle ScholarPubMed
Schiller, M, Ben-Shaanan, TL, Rolls, A. Neuronal regulation of immunity: why, how and where? Nat Rev Immunol 2021; 21(1): 2036.10.1038/s41577-020-0387-1CrossRefGoogle ScholarPubMed
Tricco, AC, Lillie, E, Zarin, W, O'Brien, KK, Colquhoun, H, Levac, D, et al. PRISMA extension for scoping reviews (PRISMA-ScR): checklist and explanation. Ann Intern Med 2018; 169(7): 467–73.CrossRefGoogle ScholarPubMed
Tunnard, C, Rane, LJ, Wooderson, SC, Markopoulou, K, Poon, L, Fekadu, A, et al. The impact of childhood adversity on suicidality and clinical course in treatment-resistant depression. J Affect Disord 2014; 152–4: 122–30.CrossRefGoogle Scholar
Brakemeier, EL, Radtke, M, Engel, V, Zimmermann, J, Tuschen-Caffier, B, Hautzinger, M, et al. Overcoming treatment resistance in chronic depression: a pilot study on outcome and feasibility of the cognitive behavioral analysis system of psychotherapy as an inpatient treatment program. Psychother Psychos 2015; 84(1): 51–6.CrossRefGoogle Scholar
Cladder-Micus, MB, Vrijsen, JN, Becker, ES, Donders, R, Spijker, J, Speckens, AEM. A randomized controlled trial of mindfulness-based cognitive therapy (MBCT) versus treatment-as-usual (TAU) for chronic, treatment-resistant depression: study protocol. BMC Psychiatry 2015; 15: 275.CrossRefGoogle Scholar
Stevenson, J, Haliburn, J, Halovic, S. Trauma, personality disorders and chronic depression – the role of the conversational model of psychodynamic psychotherapy in treatment resistant depression. Psychoanalytic Psychother 2016; 30(1): 2341.CrossRefGoogle Scholar
Michalak, J, Probst, T, Heidenreich, T, Bissantz, N, Schramm, E. Mindfulness-based cognitive therapy and a group version of the cognitive behavioral analysis system of psychotherapy for chronic depression: follow-up data of a randomized controlled trial and the moderating role of childhood adversities. Psychother Psychosom 2016; 85(6): 378–80.CrossRefGoogle Scholar
Nelson, J, Klumparendt, A, Doebler, P, Ehring, T. Childhood maltreatment and characteristics of adult depression: meta-analysis. Br J Psychiatry 2017; 210(2): 96104.CrossRefGoogle ScholarPubMed
Minelli, A, Zampieri, E, Sacco, C, Bazzanella, R, Mezzetti, N, Tessari, E, et al. Clinical efficacy of trauma-focused psychotherapies in treatment-resistant depression (TRD) in-patients: a randomized, controlled pilot-study. Psychiatry Res 2019; 273: 567–74.CrossRefGoogle ScholarPubMed
O'Brien, B, Lijffijt, M, Wells, A, Swann, AC, Mathew, SJ. The impact of childhood maltreatment on intravenous ketamine outcomes for adult patients with treatment-resistant depression. Pharmaceuticals 2019; 12(3): 133.Google ScholarPubMed
Li, QS, Tian, C, McIntyre, MH, Sun, Y, Hinds, DA, Narayan, VA. Phenotypic analysis of 23andMe survey data: treatment-resistant depression from participants’ perspective. Psychiatry Res 2019; 278: 173–9.CrossRefGoogle Scholar
Robakis, TK, Watson-Lin, K, Wroolie, TE, Myoraku, A, Nasca, C, Bigio, B, et al. Early life adversity blunts responses to pioglitazone in depressed, overweight adults. Eur Psychiatry 2019; 55: 49.CrossRefGoogle Scholar
Strawbridge, R, Hodsoll, J, Powell, TR, Hotopf, M, Hatch, SL, Breen, G, et al. Inflammatory profiles of severe treatment-resistant depression. J Affect Disord 2019; 246: 4251.10.1016/j.jad.2018.12.037CrossRefGoogle ScholarPubMed
Nikkheslat, N, McLaughlin, AP, Hastings, C, Zajkowska, Z, Nettis, MA, Mariani, N, et al. Childhood trauma, HPA axis activity and antidepressant response in patients with depression. Brain Behav Immun 2020; 87: 229–37.CrossRefGoogle ScholarPubMed
Yrondi, A, Aouizerate, B, Bennabi, D, Richieri, R, D'Amato, T, Bellivier, F, et al. Childhood maltreatment and clinical severity of treatment-resistant depression in a French cohort of outpatients (FACE-DR): one-year follow-up. Depress Anxiety 2020; 37(4): 365–74.CrossRefGoogle Scholar
Gruhn, M, Phan, K, Klumpp, H, Ajilore, O, Gorka, S. Early life adversity as a moderator of symptom change following selective serotonin reuptake inhibitors and cognitive behavioral therapy. Cogn ther Res 2021; 45(2): 343–54.CrossRefGoogle Scholar
O'Brien, B, Lijffijt, M, Lee, J, Kim, YS, Wells, A, Murphy, N, et al. Distinct trajectories of antidepressant response to intravenous ketamine. J Affect Disord 2021; 286: 320–9.CrossRefGoogle ScholarPubMed
Yrondi, A, Arbus, C, Bennabi, D, D'Amato, T, Bellivier, F, Bougerol, T, et al. Relationship between childhood physical abuse and clinical severity of treatment-resistant depression in a geriatric population. PLoS One 2021; 16(4): e0250148.CrossRefGoogle Scholar
Taylor, RW, Coleman, JRI, Lawrence, AJ, Strawbridge, R, Zahn, R, Cleare, AJ. Predicting clinical outcome to specialist multimodal inpatient treatment in patients with treatment resistant depression. J Affect Disord 2021; 291: 188–97.CrossRefGoogle Scholar
Fischer, KF, Simon, MS, Elsner, J, Dobmeier, J, Dorr, J, Blei, L, et al. Assessing the links between childhood trauma, C-reactive protein and response to antidepressant treatment in patients with affective disorders. Eur Arch Psychiatry Clin Neurosci 2021; 271(7): 1331–41.CrossRefGoogle ScholarPubMed
Levy, A, El-Hage, W, Bennabi, D, Allauze, E, Bouvard, A, Camus, V, et al. Occurrence of Side effects in treatment-resistant depression: role of clinical, socio-demographic and environmental characteristics. Front Psychiatry 2021; 12: 795666.10.3389/fpsyt.2021.795666CrossRefGoogle ScholarPubMed
O'Brien, B, Lee, J, Kim, S, Nandra, GS, Pannu, P, Swann, AC, et al. Replication of distinct trajectories of antidepressant response to intravenous ketamine. J Affect Disord 2023; 321: 140–6.CrossRefGoogle ScholarPubMed
Maruani, J, Molière, F, Godin, O, Yrondi, A, Bennabi, D, Richieri, R, et al. Diurnal symptoms of sleepiness and dysfunction predict future suicidal ideation in a French cohort of outpatients (FACE-DR) with treatment resistant depression: a 1-year prospective study about sleep markers. J Affect Disord 2023; 329: 369–78.CrossRefGoogle Scholar
Lichter, K, Klüpfel, C, Stonawski, S, Hommers, L, Blickle, M, Burschka, C, et al. Deep phenotyping as a contribution to personalized depression therapy: the GEParD and DaCFail protocols. J Neural Trans 2023; 130(5): 707–22.10.1007/s00702-023-02615-8CrossRefGoogle ScholarPubMed
Cladder-Micus, MB, Vrijsen, JN, Fest, A, Spijker, J, Donders, ART, Becker, ES, et al. Follow-up outcomes of mindfulness-based cognitive therapy (MBCT) for patients with chronic, treatment-resistant depression. J Affect Disord 2023; 335: 410–7.CrossRefGoogle ScholarPubMed
Giampetruzzi, E, Tan, AC, LoPilato, A, Kitay, B, Riva Posse, P, McDonald, WM, et al. The impact of adverse childhood experiences on adult depression severity and treatment outcomes. J Affect Disord 2023; 333: 233–9.CrossRefGoogle ScholarPubMed
Fond, G, Faugere, M, Boyer, L, Peri, P, Stephan, F, Moliere, F, et al. Long-term benzodiazepine prescription in treatment-resistant depression: a national FACE-TRD prospective study. Prog Neuropsychopharmacol Biol Psychiatry 2023; 126: 110779.CrossRefGoogle ScholarPubMed
Benjamin, I, Hershenberg, R, Dorrell, KD, Tan, AC, Riva-Posse, P, McDonald, WM, et al. Differences in clinical presentations of patients seeking care for treatment-resistant depression across sexual orientations and gender identities. Ann Clin Psychiatry 2023; 35(3): 199208.CrossRefGoogle ScholarPubMed
Kuzminskaite, E, Gathier, AW, Cuijpers, P, Penninx, BWJH, Ammerman, RT, Brakemeier, EL, et al. Treatment efficacy and effectiveness in adults with major depressive disorder and childhood trauma history: a systematic review and meta-analysis. Lancet Psychiatry 2022; 9(11): 860–73.CrossRefGoogle Scholar
Cuffe, SP, McCullough, EL, Pumariega, AJ. Comorbidity of attention deficit hyperactivity disorder and post-traumatic stress disorder. J Child Fam Stud 1994; 3(3): 327–36.CrossRefGoogle Scholar
Figure 0

Fig. 1 Key factors associated with difficult-to-treat depression (DTD), including early life trauma.

Figure 1

Table 1 Effects of early life trauma, including neurobiological, psychological, cognitive and social impacts, comorbidities and intergenerational transmission

Figure 2

Fig. 2 PRISMA flow chart.

Figure 3

Table 2 Summary of studies

Figure 4

Fig. 3 The relationship between early life trauma (ELT) and difficult-to-treat depression (DTD), in which ELT is a significant risk factor, not only contributes to the development and persistence of depressive disorders but also complicates their clinical management.

Supplementary material: File

Paganin et al. supplementary material

Paganin et al. supplementary material
Download Paganin et al. supplementary material(File)
File 51.6 KB
Submit a response

eLetters

No eLetters have been published for this article.