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Diverse immunological dysregulation, chronic inflammation, and impaired erythropoiesis in long COVID patients with chronic fatigue syndrome. — ME/CFS Atlas

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Diverse immunological dysregulation, chronic inflammation, and impaired erythropoiesis in long COVID patients with chronic fatigue syndrome.

Saito, Suguru, Shahbaz, Shima, Osman, Mohammed et al. · Journal of autoimmunity · 2024 · DOI

Quick Summary

This study compared blood samples from long COVID patients with ME/CFS to those who fully recovered from COVID-19. Researchers found that ME/CFS patients had unusual patterns in their immune cells and higher levels of inflammation-promoting substances in their blood. They also discovered specific immune markers that could reliably distinguish ME/CFS patients from those who recovered, suggesting these markers could potentially be used for diagnosis.

Why It Matters

This research provides objective biological markers that could help clinicians diagnose ME/CFS and distinguish it from other post-COVID conditions. Understanding the specific immune dysfunction patterns opens potential therapeutic targets for treating ME/CFS and may eventually lead to preventive strategies for at-risk COVID-19 patients.

Observed Findings

ME/CFS patients showed elevated neutrophils and monocytes with reduced lymphocytes compared to recovered individuals.
Specific immune cell markers (2B4+CD160+ and TIM3+CD160+ CD8+ T cells) completely separated ME/CFS patients from recovered controls.
Plasma levels of Galectin-9 and artemin were significantly elevated in ME/CFS, with artemin correlating with pain and cognitive impairment.
Expansion of CD71+ immunosuppressive erythroid cells was observed in ME/CFS patients.
Multiple autoantibodies were elevated in long COVID patients, suggesting autoimmune activation.

Inferred Conclusions

ME/CFS represents a distinct immunological state characterized by T cell exhaustion, chronic inflammation, and immune dysregulation distinct from simple viral recovery.
A multi-parameter immunological signature (including terminal effector T cells, artemin, Galectin-9, and reduced regulatory cells) could serve as a diagnostic biomarker for ME/CFS.
CD71+ erythroid cells may play a pathogenic role by suppressing immune regulation while driving artemin production linked to neurological symptoms.
Artemin and Galectin-9 may be mechanistically important in ME/CFS pathogenesis and represent potential therapeutic targets.

Remaining Questions

What This Study Does Not Prove

This study cannot prove that the identified immune abnormalities *cause* ME/CFS symptoms—only that they are associated with the condition. The observational design prevents establishing whether these immune changes preceded ME/CFS onset or resulted from it. Additionally, findings need validation in independent populations and prospective studies to determine if these markers could reliably predict disease development.

Topics

Immune System

Metadata

DOI: 10.1016/j.jaut.2024.103267
PMID: 38797051
Evidence level: Single-study or moderate support from human research
Last updated: 12 April 2026

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About the PEM badge: “PEM required” means post-exertional malaise was an explicit required diagnostic criterion for participant inclusion in this study — not that PEM was studied, observed, or discussed. Studies using criteria that do not require PEM (e.g. Fukuda, Oxford) are tagged “PEM not required”. How the atlas works →

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The first block is for the primary paper and is the citation you should use in research work. The atlas-snapshot line only applies if you are specifically referring to this atlas’s reading of the paper on the date shown.

Primary citation

Saito, Suguru, Shahbaz, Shima, Osman, Mohammed, Redmond, Desiree, Bozorgmehr, Najmeh, Rosychuk, Rhonda J, et al. (2024). Diverse immunological dysregulation, chronic inflammation, and impaired erythropoiesis in long COVID patients with chronic fatigue syndrome.. Journal of autoimmunity. https://doi.org/10.1016/j.jaut.2024.103267

BibTeX

@article{mecfsatlas-saito-2024-diverse-immunological,
  author  = {Saito, Suguru and Shahbaz, Shima and Osman, Mohammed and Redmond, Desiree and Bozorgmehr, Najmeh and Rosychuk, Rhonda J and Lam, Grace and Sligl, Wendy and Cohen Tervaert, Jan Willem and Elahi, Shokrollah},
  title   = {Diverse immunological dysregulation, chronic inflammation, and impaired erythropoiesis in long COVID patients with chronic fatigue syndrome.},
  journal = {Journal of autoimmunity},
  year    = {2024},
  doi     = {10.1016/j.jaut.2024.103267},
  note    = {PubMed: 38797051},
  url     = {https://www.mecfsatlas.com/evidence/saito-2024-diverse-immunological},
}

Atlas snapshot reference

ME/CFS Atlas. Generator v1 / Scanner v1.4 / policy v0.1. Accessed 2026-04-19. https://www.mecfsatlas.com/evidence/saito-2024-diverse-immunological

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