Long COVID Brain Inflammation Decreases Over Time

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Summary: A precision neuroimaging study challenged the widely held hypothesis that widespread, persistent brain inflammation is the primary driver of Long COVID. The research used advanced PET and MRI scans to compare Long COVID patients against both healthy controls and multiple sclerosis (MS) patients.

The data revealed no significant differences in long-term neuroinflammation or neurodegeneration between Long COVID subjects and healthy controls. Instead, the findings expose a time-dependent disease profile where brain inflammation peaks early post-infection and naturally diminishes over time, shifting the therapeutic focus toward emotional and stress regulation networks.

Key Facts

  • Challenging the Widespread Myth: While persistent brain inflammation has long been suspected to cause Long COVID symptoms like fatigue and brain fog, direct, localized evidence has remained scarce. This study refines that narrative by proving widespread neuroinflammation is not the sustained driver of the condition.
  • The Clinical Baseline Audit: Researchers utilized highly sensitive positron emission tomography (PET) imaging to track neuroinflammation alongside structural MRI scans and blood biomarker evaluations for glial and neuronal damage.
  • No Elevated Long-Term Baseline: When compared to MS patients, Long COVID individuals showed significantly lower inflammatory activity in the brain’s white matter. Crucially, no statistical differences in neuroinflammation or neurodegeneration were found between Long COVID patients and healthy controls.
  • The 16-Month Inflammation Window: The study uncovered a clear temporal link: patients scanned within 16 months of their initial SARS-CoV-2 infection exhibited higher white matter inflammatory activity than those with longer disease durations, proving inflammation fades over time.
  • Localized Emotional Activation: Higher levels of depression, anxiety, and lowered quality of life correlated directly with elevated cellular activity in the hippocampus and amygdala, the precise brain regions governing memory, stress, and emotional regulation.
  • Re-Calibrating Future Therapies: Because the underlying inflammatory changes weaken over time, the research team suggests that long-term sufferers would benefit significantly more from targeted stress and emotional regulation interventions rather than anti-inflammatory drugs.

Source: University of Turku

Long COVID has been suspected to involve persistent brain inflammation following SARS-CoV-2 infection, potentially explaining symptoms such as fatigue, cognitive impairment, anxiety, and depression. While previous studies have suggested this possibility, direct evidence has been limited.

Researchers at the University of Turku, Finland, used advanced brain imaging techniques to investigate whether long COVID patients with persistent symptoms show signs of brain inflammation.

This shows a brain.
While widespread white matter brain inflammation is present in the first 16 months following a SARS-CoV-2 infection, it naturally decreases over time, leaving long-term symptoms tied to localized cellular activity in the hippocampus and amygdala. Credit: Neuroscience News

โ€œWe did not observe evidence of widespread brain inflammation in patients with long COVID when compared to healthy controls,โ€ says Professor of Neuroimmunology and InFLAMES Research Flagship group leader Laura Airas, who led the study.

The study included 14 individuals with long COVID, 11 healthy controls, and 13 patients with multiple sclerosis (MS), a neurological disease known to involve brain inflammation.

All participants underwent PET imaging sensitive to neuroinflammation, along with magnetic resonance imaging (MRI) to assess brain structure and white matter changes. Blood samples were analysed for biomarkers reflecting neuronal and glial damage.

Compared to MS patients, individuals with long COVID showed significantly lower inflammatory activity in the brainโ€™s white matter. No differences in markers of brain inflammation or neurodegeneration were observed between long COVID patients and healthy controls.

Brain inflammation may be present early after infection

Clear signs of brain inflammation have previously been observed in neuropathological studies of severe acute COVID-19. In the current study, individuals scanned within 16 months of infection showed higher white matter inflammatory activity compared to those with longer disease duration.

According to Airas, this suggests that inflammation may be more prominent during the early phase of the disease and decrease over time.

An important finding of the study was that higher levels of depression and anxiety, as well as lower quality of life, were associated with increased cellular activity in the hippocampus and amygdala. They are brain regions involved in memory, emotional regulation, and stress responses.

These findings suggest that altered cellular activation in emotion-regulating brain regions may be linked to symptom severity in some patients with long COVID.

Toward a clearer understanding of long COVID and targeted treatments

The researchers note that the findings refine our understanding of long COVID and challenge the idea that persistent brain inflammation is the primary driver of prolonged symptoms in all patients. Instead, the results point to a more complex disease profile, where inflammatory changes may be strongest right after infection and diminish over time.

Long COVID is a recognised condition affecting millions of people worldwide, with symptoms that can persist for months or even years after the initial infection.

The researchers suggest that patients with prolonged symptoms may benefit more from treatments targeting stress and emotional regulation rather than therapies aimed solely at reducing inflammation.

โ€œThis study highlights the need to continue investigating the complex biological mechanisms underlying long COVID. Understanding these processes is essential for developing targeted treatments,โ€ notes Airas.

The study by Airas and colleagues has been published in the Journal of Neurology.

Key Questions Answered:

Q: If Long COVID isn’t causing chronic brain inflammation, why do I still feel so depressed, anxious, and exhausted?

A: The study reveals that your symptoms are completely real, but the biological engine behind them changes over time. While widespread inflammation appears to peak during the early months after infection, long-term symptoms are tied to altered cellular activity in specific emotion and stress-processing hubs, the hippocampus and the amygdala.

Q: How did comparing Long COVID patients to multiple sclerosis patients help solve this mystery?

A: Multiple sclerosis is a neurological disease known for definitive, aggressive brain inflammation. By scanning Long COVID patients alongside MS patients and healthy individuals, the team created a clear benchmark. The scans revealed that the white matter in Long COVID brains had significantly less inflammation than MS brains, matching the baseline of healthy controls.

Q: Does this mean taking anti-inflammatory medications for long-term Long COVID is a waste of time?

A: The data suggests that anti-inflammatory treatments might only be highly effective during the initial phase of the disease, particularly within the first 16 months post-infection. For patients dealing with prolonged, multi-year symptoms, the brain’s inflammatory response has already quieted down, meaning therapies targeting stress paths and emotional regulation will offer much better relief.

Editorial Notes:

  • This article was edited by a Neuroscience News editor.
  • Journal paper reviewed in full.
  • Additional context added by our staff.

About this Long-COVID and neurology research news

Author:ย Tuomas Koivula
Source:ย University of Turku
Contact:ย Tuomas Koivula โ€“ University of Turku
Image:ย The image is credited to Neuroscience News

Original Research:ย Open access.
โ€œAssociation between post-COVID-19 neuropsychiatric symptoms and persistent glial activation in the limbic system: a TSPO PET studyโ€ by Joel Tuomaala, Maija Saraste, Emma Smith, Matilda Kuusi, Elisabet Westerberg, Eveliina Honkonen, Rahim Kargar, Sini Laaksonen, Jussi Lehto, Amelie Luoma, Markus Matilainen, Olavi Misin, Janne Atosuo, Mari Kanerva, Helena Liira, Sini Laakso, Tatiana Posharina, Virva Saunavaara, Saara Wahlroos, Johan Rajander & Laura Airas.ย Journal of Neurology
DOI:10.1007/s00415-026-13842-w

Abstract

Association between post-COVID-19 neuropsychiatric symptoms and persistent glial activation in the limbic system: a TSPO PET study

Background

A subset of individuals experience prolonged neurological and psychiatric symptoms following SARS-CoV-2 infection, a condition referred to as long COVID (LC). Limited evidence implicates ongoing neuroinflammatory processes as a driver of LC. This study investigates neuroinflammation in LC using translocator protein positron emission tomography (TSPO PET).

Methods

14 LC, 11 healthy control (HC) and 13 multiple sclerosis (MS) participants were included in the study. They underwent [11C]PK11195 TSPO PET and 3T magnetic resonance imaging (MRI) to evaluate glial activation, white matter (WM) pathology and brain volumetrics.

Serum neurofilament light chain (NfL) and glial fibrillary acidic protein (GFAP) were measured as markers of neuronal and glial damage. LC participants completed neurological examinations and mental health assessments.

Results

TSPO availability, measured as distribution volume ratio (DVR), was not elevated in LC compared to HCs but was significantly lower in LC compared to MS (WM DVR 1.03 vs. 1.06;ย pโ€‰=โ€‰0.007). Individuals imaged within 16ย months of SARS-CoV-2 infection showed higher WM DVR compared to those with a longer disease duration (1.05 vs. 1.02;ย pโ€‰=โ€‰0.04).

Moreover, lower quality of life was associated with higher DVRs in the hippocampus, amygdala and thalamus (ฯโ€‰= โˆ’โ€‰0.83-โ€‰โˆ’โ€‰0.70), and depression and anxiety correlated positively with DVRs in the hippocampus and amygdala (ฯโ€‰=โ€‰0.75โ€“0.97).

Conclusions

LC TSPO availability did not differ from HCs in any studied brain area. However, lower WM TSPO availability in individuals with longer LC duration suggests COVID-19-associated neuroinflammation may subside with time, while the association between limbic TSPO availability and LC severity may imply a role for limbic activity in LC symptomology.

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2 Comments

  1. This article suggests “that patients with prolonged symptoms may benefit more from treatments targeting stress and emotional regulation rather than therapies aimed solely at reducing inflammation,” which is misleading, since not all LC patients would benefit from this approach. The article’s conclusion should be rewritten. The background section mentions, “A SUBSET of individuals experience prolonged neurological and psychiatric symptoms,” and the article should make it clear that THESE SUBSET of LC patients “with higher levels of depression and anxiety, as well as lower quality of life, were associated with increased cellular activity in the hippocampus and amygdala” may benefit from treatments targeting stress and emotional regulation.

    There are many subsets of long covid patients that would not benefit from this approach. To the contrary, there are subsets of LC patients that experience at least neurological symptoms if not psychiatric as well that would rather benefit from immunomodulatory treatments, anti-inflammatory treatments and even steroids in some cases over stress reduction and emotional regulation approaches, e.g. those LC patients with primary autonomic dysfunction, autoimmune and MECFS components, which can ignite brain and systemic inflammation constantly or periodically and when in PEM states, especially if not properly treated.

    The way the conclusion currently reads, it makes it seem as though all LC patients that are a few years out should be straying away from anti-inflammatory treatments and immunomodulation treatments intended to regulate ongoing inflammatory signaling, simply because the author of the study concluded that brain inflammation is not an underlying cause of symptoms, which may very well be true. Given the small size of the study, the article also fails to account for those dealing with endothelial dysfunction, autonomic dysfunction and immune dysregulation as a potential driver of symptoms and whether there are any discrepancies found in these patients regarding brain inflammation.

    I do not disagree with the findings. The focus on stress management may be helpful for some LC patients. I disagree with the overbroad conclusion that should be clarified to mean that the LC patients that may benefit from stress management over other treatments applies to a specific subset of LC patients screened particularly for this study, or as the study states, screened “participants with well-defined symptom subtypes.” Thank you.

    Reply

  2. I am a doctor and from 2019 to 2023 I experienced nine episodes of COVID-19, the first two requiring hospitalization in intensive care, interstitial pneumonia, very low oxygen levels, and the need for systemic therapy with high doses of corticosteroids and antibiotics. Especially after the last episode, which was managed with home therapy for 15 days, I experienced the worst symptoms in some disabling circumstances (such as during the summer season), with asthenia and the inability to perform my daily sports activities, migratory joint pain, insomnia, depression, dizziness, tinnitus, and, fortunately, only minimal difficulty concentrating. Therefore, despite enormous sacrifices, I was able to continue my freelance work, without any support from insurance companies that do not recognize, at least in Italy, the condition defined as Long Covid. My IL-6 levels were consistently elevated over the years, along with stress and increased cortisol levels, resulting in my inability to lose weight following steroid therapy and fatigue. FINALLY, after years of silent suffering, I can say I’ve regained my energy and my physical and mental health. I want to emphasize that, despite having suggested to highly renowned specialists that my condition could be caused by LONG COVID, I underwent a TSPO-PET, 3TMRI, and neurological tests, which led to a diagnosis that I found completely incorrect… fortunately. I was prescribed a treatment that I immediately stopped, and I studied everything in the scientific literature on LC. MY EXPERIENCE IS INTENDED TO BE A TESTIMONY OF HOW THIS COMPLEX PATHOLOGICAL AND CLINICAL CONDITION CAN TOO OFTEN BE MISSED, EVEN BY AUTHORITATIVE PROFESSIONALS. THANK YOU FOR YOUR WONDERFUL WORK.

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