Severity of traumatic brain injury governs alterations in type 17 T helper cell subset composition

A. O. Norka; Норка А. О.; S. V. Vorobyev; Воробьев С. В.; R. N. Kuznetsova; Кузнецова Р. Н.; M. K. Serebriakova; Серебрякова М. К.; I. V. Kudryavtsev; Кудрявцев И. В.; S. N. Kovalenko; Коваленко С. Н.; D. N. Monashenko; Монашенко Д. Н.

doi:10.46235/1028-7221-16629-SOT

Severity of traumatic brain injury governs alterations in type 17 T helper cell subset composition

作者: Norka A.O.¹^,2, Vorobyev S.V.³, Kuznetsova R.N.¹^,2, Serebriakova M.K.⁴, Kudryavtsev I.V.²^,4, Kovalenko S.N.⁵, Monashenko D.N.⁶
隶属关系:
1. Saint Petersburg Pasteur Institute
2. First St. Petersburg State I. Pavlov Medical University
3. Almazov National Medical Research Centre
4. Institute of Experimental Medicine
5. S. Kirov Military Medical Academy
6. Russian Research Institute of Traumatology and Orthopedics
期: 卷 27, 编号 3 (2024)
页面: 613-620
栏目: SHORT COMMUNICATIONS
URL: https://ogarev-online.ru/1028-7221/article/view/267531
DOI: https://doi.org/10.46235/1028-7221-16629-SOT
ID: 267531

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Immune cell hyperactivation along with cytokines they overproduce plays an important role in traumatic brain injury (TBI). A central place in the immunopathogenesis of TBI is held by diverse cell-mediated reactions governed by T helper (Th) cell populations including Th17 subset. We studied peripheral blood plasma samples of the patients with sarcoidosis (n = 123): group 1 – patients with concussion; group 2 – mild TBI; group 3 – moderate TBI; and group 4 – severe TBI. The control group was samples from healthy volunteers (n = 48). T cell subset composition was assessed by flow cytometry. Within Th central memory cells (Th CM): the level of “double-negative” Th17 (DN Th17) was significantly increased in patients with mild TBI (p = 0.014) and moderate TBI (p = 0.003); the level of “classical” Th17 (p = 0.010) also was significantly increased, but only with severe TBI; the level of “non-classical” Th 17 (Th17.1) were shown to have significantly reduced level only patients with severe TBI (p = 0.008); the level of “double-positive” Th17 (DP Th17) was significantly increased in patients with mild TBI (p = 0.006) and moderate TBI (p = 0.012). Within Th effector memory cells, an increased level of DN Th17 turned out to be significantly increased in all groups (p < 0.05) and “classical” Th17 in patients with mild TBI and moderate TBI (р < 0,05); the level of Th17.1 was significantly reduced in patients with severe TBI (p = 0.015). The results indicate the active generation of a subpopulation of Th17 cells of both central (Th CM) and effector memory (ThEM), which indicates directed migration of cells in response to TBI. This probably occurs due to the high plasticity of Th17 (changes in phenotype) and functional properties that change depending on the microenvironment into which a particular cell finds itself, which causes the occurrence of reciprocal changes as a response to damage in nervous tissue of different severity.

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traumatic brain injury, CD4+T cells, Th cell differentiation, Th17 cell subsets, flow cytometry

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作者简介

A. Norka

Saint Petersburg Pasteur Institute; First St. Petersburg State I. Pavlov Medical University

编辑信件的主要联系方式.
Email: norka-anna@mail.ru

PhD (Medicine), Senior Laboratory Assistant, Department of Immunology, Neurologist, Medical Centre

俄罗斯联邦, St. Petersburg; St. Petersburg

S. Vorobyev

Almazov National Medical Research Centre

Email: norka-anna@mail.ru

PhD, MD (Medicine), Chief Research Associate, Research Laboratory of Neurology and Neurorehabilitation

俄罗斯联邦, St. Petersburg

R. Kuznetsova

Saint Petersburg Pasteur Institute; First St. Petersburg State I. Pavlov Medical University

Email: norka-anna@mail.ru

PhD (Medicine), Associate Professor, Department of Immunology, Allergist-Immunologist, Medical Centre

俄罗斯联邦, St. Petersburg; St. Petersburg

M. Serebriakova

Institute of Experimental Medicine

Email: norka-anna@mail.ru

Postraduate Student, Research Associate, Department of Immunology

俄罗斯联邦, St. Petersburg

I. Kudryavtsev

First St. Petersburg State I. Pavlov Medical University; Institute of Experimental Medicine

Email: norka-anna@mail.ru

PhD (Biology), Senior Research Associate, Department of Immunology, Associate Professor, Department of Immunology

俄罗斯联邦, St. Petersburg; St. Petersburg

S. Kovalenko

S. Kirov Military Medical Academy

Email: norka-anna@mail.ru

Lecturer, Department of Neurosurgery

俄罗斯联邦, St. Petersburg

D. Monashenko

Russian Research Institute of Traumatology and Orthopedics

Email: norka-anna@mail.ru

PhD (Medicine), Neurosurgeon

俄罗斯联邦, St. Petersburg

参考

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2. Figure 1. Distribution of Th17 across cell subpopulations within the total pool of CCR6+Th central memory (Th CM) with phenotype CD45RA-CD62L+ patients with TBI of varying severity Note. Results are presented as median and interquartile range (Me (Q0.25-Q0.75)); Group 1, concussion; Group 2, mild TBI; Group 3, moderate TBI; Group 4, severe bruise; Group 5, control group.

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3. Figure 2. Distribution of Th17 by main subpopulations of cells within the general pool of CCR6+ Th effector memorv (Th EM) with the CD45RA-CD62L+ phenotype in patients with TBI of varying severity Note. As for Figure 1.

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