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Treatment-resistant bipolar depression
Introduction
Depressive symptoms are present during almost 70% of the symptomatic period in bipolar disorder patients (BD) ( ). Overall, patients with BD spent more than one-third of the time with subsyndromal or syndromal depression (17.6% and 18.4%, respectively, for BD type I; 17.8% and 19.1%, respectively, for BD type II) ( ). Depression in BD is also highly associated with suicidality. did a systematic review of the relationship between suicide and BD diagnosis and reported rates 20–30 higher than for the general population. Genetic factors, psychiatric comorbidity, and predominant depressive polarity were among the associated factors ( ). These clinical characteristics may contribute to the substantial economic burden associated with BD. Bessonova et al. estimated the economic burden associated with BD in the United States. The results pointed to more than $195 billion per year, with the indirect costs (lost work productivity for both parents and caregivers, and unemployment) accounting for 72%–80% of the total ( ). For many patients, the burden of bipolar depression is compounded by well-known delays in accurately diagnosing bipolar disorders more broadly. For instance, found an association between a longer duration of untreated illness and a depressive polarity of the first episode and more lifetime depressive episodes.
Different treatments are indicated for the management of bipolar depression ( ). However, there are far fewer evidence-supported therapeutic options for treating bipolar depression than for treating manic episodes. Moreover, about one-quarter to one-third of patients with bipolar depression lack response to two or more treatments, a crucial, unmet, clinical challenge in psychiatry ( ; ; ). In this book chapter, we will discuss the concept of treatment-resistant bipolar depression (TRBD), its epidemiology and neurobiology, in addition to promising interventions, pharmacological and nonpharmacological, for its treatment.
Concept
The concept of treatment-resistant depression (TRD) has traditionally been grounded on unipolar depression. In a study published in the 60s, investigated reserpine’s role in treating “imipramine-resistant” patients. The concept of treatment-resistance considered in this study was “endogenous depression” with no improvement after at least 3 weeks of administration of imipramine, with daily doses up to 300 mg. The diagnosis of endogenous depression included: “prolonged pathological depressive emotional disposition, loss of interest and energy, psychomotor inhibition, sleep disturbances, anorexia with loss of weight, feeling of hopelessness, self-reproach, morning depression and an indication of suicidal tendencies.” The outcome was defined according to a clinical scale that included seven symptoms of depression, taking into account how long the improvement was observed, and it was categorized as follows: “good and stable improvement”; “good improvement lasting several days”; “transient of no improvement” ( ). included patients with depression, according to the Feighner criteria, who “had failed to respond to conventional treatment” in a trial with a pharmacological combination compared with electroconvulsive therapy (ECT) ( ; ). Despite the mentioned remission and response and the evaluation through psychometric scales, there is no objective definition of how the outcome was measured ( ). More straightforward inclusion criteria can be found in the study of De Montigny in which lithium was used for patients with depression who did not respond to tricyclic antidepressants after 3 weeks of treatment, meaning a decreased total scored in the Hamilton Depression Rating Scale (HDRS) less than 40% ( ; ). reported patients treated and followed in a Mood Disorder Clinic. The concepts the authors used are more closely aligned with what current studies usually consider, although their remission criteria, if used today, would be classified instead as response (50% decrease in the depression scores from the previous evaluation) ( ) ( Table 26.1 ).
Table 26.1
Evolution of the treatment-resistant depression concept in the last decades. a
| Authors and year | Definition of depression | Definition of TRD | Outcome | Outcome measure |
|---|---|---|---|---|
| “Endogenous depression” | No improvement after at least 3 weeks of administration of imipramine | “Good and stable improvement” | According to a clinical scale that included seven symptoms of depression | |
| Feighner criteria | Patients who “had failed to respond to conventional treatment” | Reduction in depression scores | Psychometric scales, including HDRS and BDI | |
| RDC | Decreased total scored in the HDRS less than 40% after treatment with a TCA | Reduction in depression scores | HDRS | |
| DSM-III and RDC criteria | Unsuccessful treatment with at least two different antidepressants or an antidepressant and/or a course of ECT | Full or complete remission | HDRS decreased more than 50% and a CGI score of “very much improved” or “much improved” | |
| DSM-IV | Failure to respond to a SSRI and subsequently failed to respond to nortriptyline | Mean change in the MADRS scores | MADRS | |
| DSM-5 | Failed to respond to at least two adequate antidepressant trials | Change in the MADRS scores from baseline to week 12 | MADRS |
a Concepts related to unipolar depression; BDI , Beck Depression Inventory ( ); CGI , Clinical Global Impressions Scale ( ); ECT , electroconvulsive therapy; HDRS , Hamilton Depression Rating Scale ( ); MADRS , Montgomery-Asberg Depression Rating Scale; RDC , Research Diagnostic Criteria ( ); SSRI , selective serotonin reuptake inhibitors; TCA , tricyclic antidepressants; TRD , treatment-resistant depression; DSM-III , Diagnostic and Statistical Manual of Mental Disorders, 3rd edition ( ).
More recently, the concept of resistance as nonresponse to at least two trials of antidepressants has become more frequent, and also it has been almost the rule for TRBD trials ( Table 26.2 ).
Table 26.2
Characteristics of treatment-resistant bipolar depression definitions according to randomized controlled trial studies.
| Authors and year | Definition of depression | Definition of TRBD | Outcome | Outcome measure |
|---|---|---|---|---|
| DSM-IV criteria and confirmed by the MINI | Failure to achieve remission with ≥ two interventions approved as first, second, or third-line therapies for BD according to CANMAT guidelines | Change in HDRS-17 from baseline to week 4 | HDRS-17 | |
| DSM-IV-TR, BD I or II | Indication for ECT and lack of response to two trials for at least 6 weeks | Longitudinal profile of weekly MADRS scores during the intervention. Remission (MADRS scores ≤ 12) as a secondary outcome | MADRS | |
| DSM-IV | Nonresponsive to at least one AD confirmed by the ATHF | Percent change in MADRS score from baseline | MADRS | |
| SCID-I for DSM-IV, BD I or BD II | Failed to respond to at least one adequate AD | Changes in SHAPS scores from the baseline | SHAPS | |
| SCID-I for DSM-IV, BD I or BD II | Failed of at least one adequate AD trial (assessed by the ATHF), and to have failed a prospective open trial of a mood stabilizer (lithium or valproate) | Changes in MADRS scores | MADRS | |
| M.I.N·I, BD I or BD II | A well-documented failure (e.g., a medical chart was available) to respond to at least two trials of AD or an AD and mood stabilizer regimen or not responded to treatment in first 12 weeks of standard or randomized care pathways for bipolar depression | Recovery as defined by no more than two symptoms meeting DSM-IV threshold criteria for a mood episode and no significant symptoms present for 8 weeks | DSM-IV | |
| DSM-IV-TR, BD I or II | Unsatisfactory response to at least two adequate trials of different classes of AD medication, but not more than six, regardless of AD category | Response, defined as a 50% reduction relative to the mean HRSD score at the baseline | HDRS | |
| SCID-I for DSM-IV | Not responded to at least two adequate trials of standard AD with concomitant mood stabilizers during the current episode | Response, defined as improvement in HDRS score of 50% or more over the baseline score | HDRS |
AD , antidepressant; ATHF , Antidepressant Treatment History Form ( ); BD , bipolar disorders; BD I , bipolar disorders type I; BD II , bipolar disorders type II; BDI , Beck Depression Inventory; CANMAT , The Canadian Network for Mood and Anxiety Treatments ( ); DSM-IV-TR , Diagnostic and Statistical Manual of Mental Disorders, 4th edition, revised ( ); ECT , electroconvulsive therapy; HDRS , Hamilton Depression Rating Scale ( ); MADRS , Montgomery-Asberg Depression Rating Scale ( ); MDD , major depressive episode; MINI , Mini-International Neuropsychiatric Interview ( ); SCID-I , Structured Clinical Interview for DSM Disorders ( ); SHAPS , Snaith-Hamilton Pleasure Scale ( ); TRBD , treatment-resistant bipolar depression.
Table 26.2 provides a summary of TRBD definition according to different randomized controlled trials. This definition was refined by a consensus of internationally recognized experts in the field, resulting in a proposal for a multitherapy-resistant bipolar depression (MTRBD) concept ( ). These authors pointed out that a clear definition of TRBD could help guide when clinicians could consider novel and nonstandard interventions to treat patients. In summary, TRBD was defined as nonremission for 8 consecutive weeks after two different adequate trials of “at least two recommended monotherapy treatments or at least one monotherapy treatment and another combination treatment” for a patient with a current moderate or severe (bipolar) major depressive episode. MTRBD also requires “the addition of failure of at least one trial with an antidepressant, a psychological treatment and a course of electroconvulsive therapy.” The authors further include a list of the required medications, their adequate therapeutic dose ranges, minimum lithium plasma levels, and the characteristics of therapeutic trials of cognitive-behavioral therapy and the ECT (at least 12 sessions, bilateral) needed to satisfy MTRBD criteria ( ).
Frequency, adherence and guidelines compliance
Mendlewicz et al., for the Group for the Study of Resistant Depression (GSRD), investigated clinical factors associated with TRBD. Of 375 patients with BD type I or II who had received at least 4 weeks of adequate treatment with mood stabilizers and an antidepressant, 99 (26.4%) were classified as treatment-resistant. The criteria for TRBD considered for this study was a failure to reach a score of less than 17 in the Hamilton Depression Rating Scale (HAM-D 17) after at least two adequate consecutive antidepressant trials during the current episode ( ). A similar frequency was found in the study of . The authors investigated clinical predictors of TRBD, defined as lack of response to at least two established treatments for bipolar depression, with an exploratory-hypothesis generating approach. Fifteen of the 53 participants with BD type I or II filled the criteria per TRBD (28.3%) ( ). compared three groups of patients categorized according to the number of medications received regarding several demographic and clinical characteristics. Of the 1034 participants (128 with BD type I and 906 with BD type II), close to one-third of them had received five or more medications, the authors’ criteria as TRBD ( ). Despite no studies have addressed the prevalence of patients with BD and treatment-resistant depression; these findings suggest that about one-quarter to one-third of the patients would lack response to two or more pharmacological treatments.
Variables associated with treatment resistance in bipolar depression
Socio-demographic and clinical variables
investigated predictors of treatment-resistant in patients with bipolar depression. From the 53 individuals with bipolar depression, 15 (28.3%) had a history of lack of response to at least two adequate treatments for depression. The presence of mixed features, including symptoms such as increased energy, psychomotor activity, and irritability, correctly classified more than 70% of patients with TRBD ( ). Parker et al. reported a higher frequency of females among patients with TRBD (64%), early age of depression onset (17.3 years), and a considerable number of medical conditions considering the mean age of the sample (about three medical conditions in a sample with 38.6 years old on average). Psychiatric comorbidity burden was also sizeable: almost half presented generalized anxiety disorder, panic disorder, and obsessive-compulsive disorder: Patients with TRBD also reported a substantial family history of psychiatric disorder (83.1% of depression and more than half of alcohol problems). Functional impairment was also highly-evident, as only 23% of the sample reported being engaged in full-time work ( ). found that patients with TRBD presented an odds ratio around twofold for the severe intensity of the last depressive episode, melancholic features, social phobia, and suicide risk.
Cognitive impairment has been recognized as a hallmark of BD and seems to be present regardless of clinical mood states ( ). Bo et al. reviewed cognitive performance in patients with BD compared to healthy controls (HC) using The Measurement and Treatment Research to Improve Cognition Schizophrenia Consensus Cognitive Battery (MCCB) ( ). Seven studies, including 467 patients with BD and 570 HC, were included in their meta-analyses, with results showing overall lower performance in all seven domains evaluated for the former group. The larger effect size was for processing speed (> 0.8), followed by visual and verbal learning (0.5), and social cognition, reasoning, and problem-solving (0.2) ( ). Kessler et al. evaluated neurocognitive function in patients with TRBD and investigated whether patients with types I and II would present distinct cognitive profiles. The authors found that both groups presented global impairment of clinically significant severity, which was more evident for BD type I, especially processing speed ( ).
Neurobiological characteristics
The neurobiological characterization of BD could help identify novel targets for intervention, optimizing the efficacy, safety, and broadening the array of options for its treatment. Moreover, it would facilitate the characterization of illness biotypes contributing to precise and personalized therapeutic strategies ( ). However, its etiology and pathophysiology are complex, involving several biological mechanisms, including dysfunctions in serotoninergic, noradrenergic, and glutamatergic systems, neurotrophic factors, inflammation, and external stressors, which challenges identifying critical pathways for intervention. Scaini et al. reviewed biological findings associated with BD, including genetic, biochemical, and neuroimaging ( ). According to this study, BD is highly heritable (70%–80%), and patients exhibit DNA methylation, alterations in the levels of micro-RNAs, and long noncoding RNAs, all potentially contributing to the phenotypic clinical presentation of the disease. Some studies also showed changes in brain-derived neurotrophic factor (BDNF), nerve growth factor (NGF), neurotrophin-3 (NT-3), and NT-4, which are associated with synaptic formation, neuronal growth, and regulation of neuronal survival processes ( ). Dysfunctions in the immune system and alterations on the inflammatory marker are also extensively found among patients with BD. Fernandes et al. reported increased C-reactive protein levels (CPR) in individuals with BD during all mood states, which were not associated with symptoms severity ( ). Postmortem studies showed inflammation in several brain regions, like the dorsolateral prefrontal cortex, anterior cingulate cortex, amygdala, and hippocampus ( ). Among the alterations, the authors reported those related to glial density and cytoarchitecture, and inflammatory gene and protein expression ( ). Excessive oxidative stress and mitochondrial dysfunction have also been found in patients with BD, as changes in mitochondrial morphology, high-energy phosphates and pH, and downregulation of proteins related to mitochondrial respiration ( ). Finally, neuroimaging studies have shown several structural and connectivity alterations in patients with BD compared with HC, as increased putamen volume, decreased volume of the amygdala, gray matter reductions in the insula, dorsolateral and orbitofrontal regions, and decreased connectivity in fronto-limbic tracts, cingulum, corpus callosum, and uncinate fasciculus ( ).
Although numerous studies have examined BD’s neurobiology, the majority of this work focused on patients with treatment-resistant depression has done so in the context of unipolar depression—not bipolar depression ( ). That being said, some of the studies that investigated interventions for TRBD (discussed in detail below) targeted a number of the biological mechanisms discussed above. Next, we will discuss important clinical issues concerning the management of TRBD more broadly. We will then summarize intervention studies for patients with TRBD, specifically, focusing on the results of randomized controlled trials that enrolled patients with rigorously-defined treatment-resistant illness.
Management of treatment-resistant bipolar depression
Initial assessment
When a clinician is treating a patient with bipolar depression who has not had an adequate response to sequential trials, it is imperative to carefully reevaluate the diagnosis to, first, confirm the existing diagnosis of BD and, second, to investigate missed or inadequately-treated psychiatric and nonpsychiatric comorbidities, assess treatment adherence, investigate whether past treatments for BD have been delivered at proper doses and for sufficient periods of time, and to evaluate the quality of (and adherence to) psychosocial interventions ( ).
In a survey of individuals with BD, 48% of the respondents did not receive the diagnosis of BD until they had consulted with three or more professionals, and 10% received the diagnosis only after visiting with seven or more professionals ( ). These findings highlight the challenging nature of diagnosing BD, even in mental health specialty settings; therefore, the chance of misdiagnosis should always be considered when dealing with treatment-resistant patients. Efforts at clarifying the BP diagnosis may be enhanced by obtaining additional histories from family members and other collateral informants and by using structured or semistructured interviews ( ). BD is often confused with borderline personality disorder, given a number of shared clinical features such as impulsivity and emotional dysregulation ( ). In the study of , among 145 patients who had reported a diagnosis of BD, the diagnosis could not be confirmed in 56.5% of the sample after using a gold-standard structured interview. Both conditions are also highly comorbid, conferring an additional challenge in the management of the patients. A systematic review found that 21.6% of people with BD may also meet diagnostic criteria for borderline personality disorder and 18.5% of individuals with borderline personality disorder may beet diagnostic criteria for BD ( ). A high frequency of cooccurring substance abuse or dependence and anxiety disorders has also been reported in BD patients ( ). Regarding nonpsychiatric comorbidities in patients with BD, Forty et al. found a self-reported frequency of asthma, diabetes, dyslipidemia, and hypertension in patients with BD of 19.2%, 6%, 19.2%, and 15%, respectively. The degree of burden from comorbid general medical conditions have been associated with longer illness duration, a greater number of psychiatric admissions, worse functioning, and ECT treatment in patients with BD ( ).
BD is a chronic illness that usually requires a complex treatment approach, including distinct pharmacological interventions—each with different dosage, adverse effect, and efficacy profiles—and adjunctive psychological interventions. About one-third of BD patients in the United States are receiving polytherapy, with almost three psychotropic medications per person on average ( ). Thus, patients who present a lack of response to several treatments for bipolar depression need careful evaluation of current and past treatments, with an eye toward nonadherence, inadequately conducted therapeutic trials (due to inadequate treatment duration and suboptimal dose/blood levels where applicable), and the use of interventions not supported by the best scientific evidence available before classifying patients as having TRBD. reviewed adherence and pharmacological treatment profiles among patients with BD in the United States. The authors reported that only 30% of the patients remained on the prescribed mood stabilizer after 1 year of treatment. The results also showed an association between common comorbidities, such as a history of alcohol or drug abuse, and higher illness complexity (including moderate to severe BD, an indication of self-harm, or comorbidity other than substance abuse) with lower treatment adherence ( ). Low conformity with guidelines for treatment could also prevent patients from responding to evidence-based interventions, although some studies have shown no significant association between good compliance with guideline-based practices and clinical outcomes in young patients with BD ( ; ). On the other hand, showed that both suboptimal medication adherence and clinical management were among the main drivers of the direct economic costs of BD, which were estimated at around $50 billion in the United States.
Psychosocial interventions
Psychosocial interventions have a crucial role in the management of patients with BD. In a systematic review, Miklowitz et al. found that cognitive behavioral therapy (CBT), family or conjoint therapy, and interpersonal therapy were associated with stabilizing depressive symptoms. Also, the findings showed the benefits of psychoeducation with guided practice of illness management skills in a family or group format in preventing recurrences and a better retention profile of brief psychoeducation and family therapy ( ). Other advantages of psychosocial interventions to treat patients with BD include educating patients about their illness, addressing comorbid psychiatric disorders, promoting self-monitoring, managing stress, addressing problems with relationships and work, and developing a plan to cope with an acute crisis ( ). reviewed published studies that focused on the clinical effects of evidence-based, bipolar-specific psychotherapies including psychoeducation, CBT, functional remediation, family-focused psychotherapy, interpersonal and social rhythm therapy, and integrated care management. However, as the authors point out, most randomized controlled trials that compared two psychosocial interventions did not find considerable differences. This suggests that the psychosocial intervention of choice may depend on treatment availability and a continuous reassessment of psychosocial needs in consultation with the patient and their family members (if appropriate) ( ). Guideline-based recommendations for various psychosocial interventions as adjuncts to pharmacotherapy for acute bipolar depression and bipolar maintenance treatment were summarized by . The information provided highlighted the role of psychoeducation as a first line recommendation (Canadian Network for Mood and Anxiety Treatments (CANMAT)/International Society for Bipolar Disorders (ISBD) and British Association for Psychopharmacology) and level 1 evidence (Royal Australian and New Zealand College of Psychiatrists (RANZCP)) for bipolar maintenance and CBT as a second line (CANMAT/ISBD) and level 1 evidence (RANZCP) for acute bipolar depression ( ).
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