Senescent CD4+CD28− T Lymphocytes as a Potential Driver of Th17/Treg Imbalance and Alveolar Bone Resorption during Periodontitis

González-Osuna, Luis; Sierra-Cristancho, Alfredo; Cafferata, Emilio A.; Melgar‐Rodríguez, Samanta; Rojas, Carolina; Carvajal, Paola; Cortéz, Cristian; Vernal, Rolando

doi:10.3390/ijms23052543

Cited by 10 publications

(4 citation statements)

References 107 publications

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“…Th17 cells are highly sensitive to autophagy induction which results in a switch of gene expression with lower IL17 expression level and enhanced Foxp3 expression that converts these cells into Tregs. In accordance with that the Treg phenotype is highly dependent on autophagy and inhibition of autophagy in Tregs leads to increased production of IL17A in these cells ( Park et al, 2016 ; González-Osuna et al, 2022 ). These data indicate that the induction of autophagy in Th17 cells might be a trigger to switch the Th17 phenotype to a Treg phenotype thereby promoting anti-inflammatory mechanisms that contribute to the resolution of inflammation.…”

Section: The Impact Of Sphingolipids On T Cells and Their Role In Res...supporting

confidence: 77%

How sphingolipids affect T cells in the resolution of inflammation

2022

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The concept of proper resolution of inflammation rather than counteracting it, gained a lot of attention in the past few years. Re-assembly of tissue and cell homeostasis as well as establishment of adaptive immunity after inflammatory processes are the key events of resolution. Neutrophiles and macrophages are well described as promotors of resolution, but the role of T cells is poorly reviewed. It is also broadly known that sphingolipids and their imbalance influence membrane fluidity and cell signalling pathways resulting in inflammation associated diseases like inflammatory bowel disease (IBD), atherosclerosis or diabetes. In this review we highlight the role of sphingolipids in T cells in the context of resolution of inflammation to create an insight into new possible therapeutical approaches.

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Section: The Impact Of Sphingolipids On T Cells and Their Role In Res...supporting

confidence: 77%

How sphingolipids affect T cells in the resolution of inflammation

2022

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“…3) The senescence of CD4 + T lymphocytes themselves leads to the reduction of Treg cells. As a cellular counterpart, CD4 + T lymphocytes can also undergo cellular senescence, which could also contribute to an immune response biased toward Th17 lymphocytes from Treg lymphocytes ( 88 ). Now, senescent T cells are corroborated to be accumulated in aging, chronic viral infections, and autoimmune disorders, which are also considered as potential targets for disease treatment ( 89 – 91 ).…”

Section: Discussionmentioning

confidence: 99%

Deciphering the endometrial immune landscape of RIF during the window of implantation from cellular senescence by integrated bioinformatics analysis and machine learning

Zhao

Zhao²,

Jiang³

et al. 2022

Front. Immunol.

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Recurrent implantation failure (RIF) is an extremely thorny issue in in-vitro fertilization (IVF)-embryo transfer (ET). However, its intricate etiology and pathological mechanisms are still unclear. Nowadays, there has been extensive interest in cellular senescence in RIF, and its involvement in endometrial immune characteristics during the window of implantation (WOI) has captured scholars’ growing concerns. Therefore, this study aims to probe into the pathological mechanism of RIF from cellular senescence and investigate the correlation between cellular senescence and endometrial immune characteristics during WOI based on bioinformatics combined with machine learning strategy, so as to elucidate the underlying pathological mechanisms of RIF and to explore novel treatment strategies for RIF. Firstly, the gene sets of GSE26787 and GSE111974 from the Gene Expression Omnibus (GEO) database were included for the weighted gene correlation network analysis (WGCNA), from which we concluded that the genes of the core module were closely related to cell fate decision and immune regulation. Subsequently, we identified 25 cellular senescence-associated differentially expressed genes (DEGs) in RIF by intersecting DEGs with cellular senescence-associated genes from the Cell Senescence (CellAge) database. Moreover, functional enrichment analysis was conducted to further reveal the specific molecular mechanisms by which these molecules regulate cellular senescence and immune pathways. Then, eight signature genes were determined by the machine learning method of support vector machine-recursive feature elimination (SVM-RFE), random forest (RF), and artificial neural network (ANN), comprising LATS1, EHF, DUSP16, ADCK5, PATZ1, DEK, MAP2K1, and ETS2, which were also validated in the testing gene set (GSE106602). Furthermore, distinct immune microenvironment abnormalities in the RIF endometrium during WOI were comprehensively explored and validated in GSE106602, including infiltrating immunocytes, immune function, and the expression profiling of human leukocyte antigen (HLA) genes and immune checkpoint genes. Moreover, the correlation between the eight signature genes with the endometrial immune landscape of RIF was also evaluated. After that, two distinct subtypes with significantly distinct immune infiltration characteristics were identified by consensus clustering analysis based on the eight signature genes. Finally, a “KEGG pathway–RIF signature genes–immune landscape” association network was constructed to intuitively uncover their connection. In conclusion, this study demonstrated that cellular senescence might play a pushing role in the pathological mechanism of RIF, which might be closely related to its impact on the immune microenvironment during the WOI phase. The exploration of the molecular mechanism of cellular senescence in RIF is expected to bring new breakthroughs for disease diagnosis and treatment strategies.

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“…Also, the content of NKT cells expressing activation markers CD28 and CD57 was studied in patients with DPP in depending on the outcome of the disease. The CD28 antigen (Tp44) belongs to the immunoglobulin superfamily and is involved in the enhancement of T-cell receptor signals, which determines its role in the regulation of adaptive immunity [13,20]. Blockade of CD28 on the membrane of NKT cells completely suppressed cytokine production [37].…”

Section: Discussionmentioning

confidence: 99%

Disseminated purulent peritonitis outcome affects NKT cell phenotype

Савченко

Борисов

Kudryavtsev

et al. 2022

Russian Journal of Infection and Immunity

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The aim of our study was to investigate the main characteristics of peripheral blood NKT cell phenotype in patients with disseminated purulent peritonitis (DPP) in dynamics of postoperative period, depending on the disease outcome. Fifty-two patients with acute surgical diseases and injuries of the abdominal organs complicated by DPP, and 68 healthy individuals in control group, were examined. Blood sampling was performed before surgery (preoperative period), as well as on the day 7, 14 and 21 of postoperative period. All patients with DPP were divided into two groups depending on disease outcome in postoperative period: patients with favorable disease outcome (n = 34); and patients with unfavorable outcome (n = 18). Study of the phenotype of blood NKT lymphocytes was performed by flow cytometry using direct immunofluorescence of whole peripheral blood samples with monoclonal antibodies. The low relative and absolute level of NKT cells was observed in DPP patients regardless of outcome disease in preoperative period. At the same time, the absolute level of NKT cells returned to normal only in patients with favorable DPP outcome and only by day 21 after surgery. Patients with favorable DPP outcome by the end of examination period had normalized quantity of mature NKT-lymphocytes and significantly decreased level of cytotoxic cells which was apparently associated with migration of such cell subsets to site of inflammation. A reduced level of non-classical (expressing CD8 marker) mature and cytokine-producing NKT cells was detected only in patients with favorable DPP outcome in preoperative period which returned to normal by the end of postoperative period. At the same time, patients with unfavorable disease outcome had reduced quantity of NKT cells of these subsets by day 21 of postoperative treatment. Patients with favorable outcome had high level of mature and cytotoxic CD11b+ NKT cells already in the preoperative period, while patients with unfavorable DPP outcome had increased level of cytotoxic CD11b+ NKT cells only by day 21 after surgery. The proportion of NKT cells expressing activation markers (CD28 and CD57) was reduced in patients in preoperative period that returned to normal immediately after surgery with favorable outcome, while it recovered with unfavorable outcome closer to the end of postoperative examination. The defined features of NKT cell phenotype in patients with unfavorable DPP outcome characterize disturbances in subset ratio and mechanisms of functioning of this cell fraction. This determines a need to develop immunotherapeutic methods aimed at stimulating immunoregulatory activity of NKT cells.

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Senescent CD4+CD28− T Lymphocytes as a Potential Driver of Th17/Treg Imbalance and Alveolar Bone Resorption during Periodontitis

Cited by 10 publications

References 107 publications

How sphingolipids affect T cells in the resolution of inflammation

How sphingolipids affect T cells in the resolution of inflammation

Deciphering the endometrial immune landscape of RIF during the window of implantation from cellular senescence by integrated bioinformatics analysis and machine learning

Disseminated purulent peritonitis outcome affects NKT cell phenotype

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