The pathophysiology of depression remains poorly understood, perhaps explaining why half of depressed patients do not adequately respond to available treatments, leading to chronic depression with its associated morbidity, premature mortality, and societal costs. Inflammation in the body is communicated to the brain, leading to depression in some individuals. But the brain also regulates the immune system and yet little is known about how depression-linked neural abnormalities affect systemic immunity. Without more detailed knowledge, intervening therapeutically in the dynamic, homeostatic interplay between the brain and immune system is challenging. We use real-time neurofeedback (NF) to experimentally modulate a key neural node (i.e. amygdala and hippocampus of the medial temporal lobe, MTL) that has been shown to regulate immune function pre-clinically. By comparing depressed subjects who can versus those who cannot regain plasticity or function of the MTL due to NF modulation, we take a step towards identifying immune markers of treatment response and prognosis (aim 1). Conversely, by characterizing the immune changes that occur in subjects who are able to regain MTL plasticity/function, biomarkers of therapeutic brain changes can be identified (aim 2). Moreover, if this NF-induced change in immunity plays a mechanistic role in recovery from depression, then medications can be developed to augment this therapeutic immune response. The NF paradigm used here is focused on the amygdala. In two clinical trials, we showed that training depressed subjects to upregulate their left amygdala activity while recalling positive autobiographical memories significantly reduced symptoms and increased fMRI functional connectivity of the amygdala and hippocampus relative to depressed subjects in the sham group. Here, the main hypotheses are that: (1) baseline levels of inflammatory cytokines and neurotoxic kynurenine metabolites will be higher in subjects who are unable to effectively upregulate their amygdala (non- responders) compared with subjects who effectively upregulate their amygdala (responders). (2) Compared with non-responders, responders to NF will show increases in anti-inflammatory cytokines and neuroprotective kynurenines post-NF training. To test these hypotheses, we will measure depressive symptoms, circuits (amygdala activity and changes in MTL connectivity), and molecules (cytokines and kynurenines) using a within-subjects design. Unmedicated subjects with depression (PHQ-9 score ?10, n=32) will complete two, one hour-long sessions (V1-V2) of NF (no sham). V1 and V2 will be held two weeks apart and will incorporate both training and evaluative components. Serum will be obtained at V1 and V2 and at a third visit without fMRI at week 4 (V3). This research is highly impactful because we need to understand the mechanisms underpinning the bidirectional relationship between inflammation and depression in order to facilitate development of new pharmacological or behavioral therapies, and identify predictive, prognostic, and monitoring biomarkers.

Public Health Relevance

The proposed research is highly relevant to public health because discovering a non-invasive biomarker of depression severity and stage of illness in the context of an experimental modulation of medial temporal lobe function will open-up hitherto closed opportunities for therapeutic monitoring, prognostication, and ultimately, precision medicine. Moreover, the identification of the mechanisms whereby the brain exerts regulatory control over the immune system will highlight a set of molecular targets for the development of novel therapeutics. Thus, the proposed project fits squarely within the NIMH?s strategic research priorities of (1) ?Identifying the molecular mechanisms that control synaptic plasticity and circuit function?; (2) ?Evaluating the utility of modifying network function for therapeutic benefit?; (3) ?Identifying novel targets [including plasticity mechanisms] and further developing emerging therapeutic approaches [including neuromodulation]?; and (4) ?Identifying and validating highly sensitive and specific biomarkers for functional trajectories, particularly for risk, prodrome, onset, progression, recovery, and relapse phases of illness?.

Agency
National Institute of Health (NIH)
Institute
National Institute of Mental Health (NIMH)
Type
Exploratory/Developmental Grants (R21)
Project #
1R21MH113871-01A1
Application #
9599067
Study Section
Biobehavioral Mechanisms of Emotion, Stress and Health Study Section (MESH)
Program Officer
Arango, Victoria
Project Start
2018-08-01
Project End
2020-07-31
Budget Start
2018-08-01
Budget End
2019-07-31
Support Year
1
Fiscal Year
2018
Total Cost
Indirect Cost
Name
Laureate Institute for Brain Research
Department
Type
DUNS #
967230579
City
Tulsa
State
OK
Country
United States
Zip Code
74136