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Multiple brain profiles underlie the same symptoms in depression

by DrMichaelLee

Brain Study Uncovers Depression’s Complex Subtypes

A recent study challenges the conventional understanding of depression, revealing that varied brain profiles can manifest with similar symptoms. This research could pave the way for more personalized and effective treatments for this prevalent mental health disorder.

Unraveling Depression’s Complexity

A new study published in Biological Psychiatry explores the neurological underpinnings of depression. Researchers investigated the relationship between clinical symptoms and neurobiological factors. Their findings suggest both one-to-one and many-to-one heterogeneity within depression.

According to Dr. John Krystal, Editor of Biological Psychiatry, “Depression is a very heterogeneous medical condition. The inability to accurately subtype patients is a major obstacle to matching individual patients to treatments that are more likely to be effective for them. This study makes progress toward this objective. Of note, it unites clinical assessments and brain imaging findings to generate depression subtypes.”

Deeper Dive into the Research

The study’s lead investigator, Dr. Janine D. Bijsterbosch, from Washington University School of Medicine in St. Louis, explained the research’s goal: “Heterogeneity in depression, i.e., differences between patients with the same diagnosis, has been a topic of interest in our field for a long time. For example, patients with depression can differ from one another in clinical characteristics (e.g., what symptoms they experience, what age their depression first started, and how many episodes they have had), and patients can also differ in their neurobiology (e.g., what brain changes are linked to their depressive symptoms). Although prior studies have investigated both these clinical and neurobiological dimensions, we wanted to develop a more thorough understanding of these sources of variation in depression and their relationship.”

The research used data from the UK Biobank to examine the link between clinical and neurobiological variations. The scientists grouped individuals with depression by their clinical presentations. They then compared their neurobiological profiles.

Key Findings and Implications

Dr. Yvette I. Sheline, from the University of Pennsylvania, stated that the research indicated a connection between clinical presentations of depression and brain changes. The study presented the first concrete evidence of many-to-one brain-symptom mapping. One neurobiological profile was associated with worsened cognition. This important outcome has the potential to influence lives.

“Our findings showed that dividing people up into groups based on their clinical presentation of depression led to stronger and more distinct brain changes as compared to a group with a mixed clinical presentation. Our research also showed that more than one brain profile gave rise to the same clinical presentation in patients with acute depression, providing concrete evidence of many-to-one brain-symptom mapping for the first time. Notably, one of the neurobiological profiles we uncovered was associated with worse cognition, which is an important clinical outcome that can substantially impact individuals’ lives; an MRI scan of neurobiology may have the potential to predict clinical outcomes that depression symptom screening alone cannot capture,” said Dr. Sheline.

Depression remains a prevalent issue, impacting around 9.2% of Americans annually. The World Health Organization reports that in 2023, over 280 million individuals globally grapple with depression. (Source: WHO)

Future Directions

Dr. Deanna M. Barch, from Washington University School of Medicine in St. Louis, expressed hope that their findings would motivate future work. They aim to further investigate depression variations, leading to tools that address the connections between clinical and neurobiological heterogeneity. Identifying different depression subtypes could improve future clinical care.

“We hope our findings will motivate future work attempting to disentangle the variations in depression, leading to the development of tools that address the layered and complex relationships between clinical and neurobiological sources of heterogeneity that we revealed. Identifying distinct subtypes of depression that may respond differently to treatment could greatly improve clinical care for patients with depression in the future. However, our findings show that identifying such subtypes of depression will only be achievable by addressing both clinical and neurobiological heterogeneity,” concluded Dr. Barch.

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