Table 2.
Neurophysiological and clinical correlates of candidate brain-based depression subtypes.
| Study | Grouping | Symptoms | Treatment response | Brain circuit |
|---|---|---|---|---|
| [88] | Dimension 1 | Mood (feeling sad, suicidality, anhedonia, irritability, persecutory/suspicious, loss sense of self) |
Positively correlated Intra-DMN DMN to frontoparietal Salience-ventral attention and frontoparietal Frontoparietal |
|
| Dimension 2 | Psychosis (auditory perceptions, odd/intrusive thoughts, reality confusion, audible thoughts, superstitions, overly energetic, pressured speech) |
Positively correlated Intra-DMN DMN to executive (frontoparietal and salience) Frontoparietal |
||
| Dimension 3 | Fear (of traveling—agoraphobia, social phobia) |
Negatively correlated Intra-DMN Salience to ventral attention Positively correlated to frontoparietal circuits |
||
| Dimension 4 | Externalizing behavior (trouble following instructions, irritability to unfairness, attention issues, losing temper) |
Negatively correlated Intra-DMN Frontoparietal to dorsal attention Positively correlated Frontoparietal Salience to frontoparietal |
||
| [89] | Dimension 1 |
Externalizing/internalizing Sex Positively correlated with age |
Positively correlated Attentional Networks FPTC Negatively correlated Limbic Intra-subcortical |
|
| Dimension 2 |
Emotional well-being vs. distress Negatively correlated with age |
Negatively correlated Attentional Networks FPTC Positively correlated Limbic Intra-subcortical |
||
| [95] | Subgroup A | 19% of depressed subjects (50% of healthy) | No change in connectivity during positive mood induction task | |
| Subgroup B |
81% of depressed subjects (50% of healthy) Difficulty sustaining positive affect during task Negative bias on reaction time Higher symptom severity |
Hyperconnectivity in ventral affective network during positive mood induction task | ||
| [96] | Subgroup A |
71% patients 65% female |
No change in DMN connectivity | |
| Subgroup B |
Recurrent depression (63%) Comorbid anxiety (42%) 87% female |
Change in the circuit path direction of the dACC (in the DMN) | ||
| [97] | Subgroup 1 |
Comorbid anxiety with severe depression (16% vs. 9% in Subgroup 2) Longer duration (mean 57.5 months) |
||
| Subgroup 2 | Shorter duration (mean 37 months) | |||
| [98] | Subgroup 1 |
Anxiety Insomnia Fatigue |
Strong therapeutic effect for TMS at DMPFC target (82.5% of patients improved significantly) |
Decreased RSFC in the Frontoamygdala ACC Orbitofrontal circuits |
| Subgroup 2 |
Fatigue Lower severity |
No significant effect for TMS at DMPFC target |
Decreased RSFC in the ACC Orbitofrontal circuits |
|
| Subgroup 3 |
Anhedonia Psychomotor retardation |
Mild therapeutic effect for TMS at DMPFC target (61% of patients improved significantly) |
Increased RSFC in the Thalamic Frontostriatal Subcortical circuits |
|
| Subgroup 4 |
Anhedonia Anxiety Insomnia |
No significant effect for TMS at DMPFC target |
Decreased RSFC in the frontoamygdala circuit Increased RSFC in the Thalamic Frontostriatal Subcortical circuits |
|
| [101] | Subgroup 1 |
High CATS High RSFC Low baseline BDI High BDI 6 weeks post-treatment |
Treatment-resistant to SSRI | High Mean FC (angular gyrus in DMN) |
| Subgroup 2 |
Low CATS Moderate RSFC Low baseline BDI Low BDI 6 weeks post-treatment |
Moderate Mean FC (angular gyrus in DMN) | ||
| Subgroup 3 |
High CATS Low RSFC High baseline BDI Low BDI 6 weeks post-treatment |
Treatment-responsive to SSRI | Low Mean FC (angular gyrus in DMN) |
Efforts to identify points of convergence between these studies are complicated by methodological differences in clustering techniques and criteria, data types used for clustering, subject samples, and other technical details. This is especially true for analyses of brain circuit function, which vary widely across studies. Given the very different methods employed by these studies and their varying findings, the available data do not currently support even preliminary conclusions about points of convergence. However, two themes recur in the clinical correlates of the subtypes in multiple studies. First, the presence or absence of comorbid anxiety- and fear-related symptoms is an important feature of the subtyping results in four of six studies [88, 95, 96, 98]. Second, the subtypes differ with respect to overall depression severity in three studies [96, 98, 101] and with respect to recurrence, which often correlates with severity, in a fourth study [95].
dACC dorsal anterior cingulate cortex, BDI Beck Depression Inventory, CATS Child and Adolescent Trauma Screen, DMN default mode network, DMPFC dorsomedial prefrontal cortex, FPTC frontoparietal task control, RSFC resting state functional connectivity, SSRI selective-serotonin reuptake inhibitor, TMS transcranial magnetic stimulation.