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Nonspecific increase of αβTCR+ double-negative T cells in pediatric rheumatic diseases

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Abstract

Background

An increased number of double-negative T (DNT) cells expressing the αβ T cell receptor (αβ+DNT cells) is one of the diagnostic criteria for autoimmune lymphoproliferative syndrome (ALPS). Moreover, these cells are expanded in a widely used murine model for lupus. However, the homeostasis of αβ+DNT cells remains inadequately investigated in rheumatic disorders, especially in pediatric patients.

Methods

In this cross-sectional, prospective, and observational study, children with rheumatic disorders and healthy controls were recruited to analyze the quantity and characteristics of circulating DNT cells using flow cytometry.

Results

Overall, the two study groups did not differ in their total DNT cell pool in the bloodstream. However, the number of αβ+DNT cells was significantly higher in rheumatic children than that in the controls, whereas the γδ+DNT cells remained similar. This expansion in the circulating pool of αβ+DNT cells was comparable across different rheumatic diseases, all showing significant differences from the controls in this regard. Moreover, no significant correlation was found between αβ+DNT cell numbers and disease activity.

Conclusions

These preliminary results indicate that circulating αβ+DNT cells are significantly expanded in children with rheumatic disorders; however, this finding appears to be a nonspecific (disease-unrelated) marker of autoimmunity. Further and larger studies are necessary to better investigate and define the role of DNT cells in pediatric rheumatic diseases.

Graphical abstract

Title
Nonspecific increase of αβTCR+ double-negative T cells in pediatric rheumatic diseases
Authors
Kuanysh Dossybayeva
Gulsamal Zhubanova
Assel Mussayeva
Zaure Mukusheva
Aiken Dildabayeva
Galiya Nauryzbayeva
Lyudmila Akhmaltdinova
Ulbolsyn Orumbayeva
Matthew Tanko
Dimitri Poddighe
Publication date
28-11-2024
Publisher
Springer Nature Singapore
Published in
World Journal of Pediatrics / Issue 12/2024
Print ISSN: 1708-8569
Electronic ISSN: 1867-0687
DOI
https://doi.org/10.1007/s12519-024-00854-7
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