IL-23 Receptor Expression on T Helper 17 Cells and its Implication in Multiple Sclerosis Relapse
Khalifa, R., Abdel Aziz, N., Shalash, A., Nada, M., Abdel Salam, S. (2023). IL-23 Receptor Expression on T Helper 17 Cells and its Implication in Multiple Sclerosis Relapse. EKB Journal Management System, 32(2), 41-47. doi: 10.21608/ejmm.2023.280275
Reham Ali Khalifa; Nesma Abdel Aziz; Ali Shalash; Maha Nada; Shimaa Ahmed Abdel Salam. "IL-23 Receptor Expression on T Helper 17 Cells and its Implication in Multiple Sclerosis Relapse". EKB Journal Management System, 32, 2, 2023, 41-47. doi: 10.21608/ejmm.2023.280275
Khalifa, R., Abdel Aziz, N., Shalash, A., Nada, M., Abdel Salam, S. (2023). 'IL-23 Receptor Expression on T Helper 17 Cells and its Implication in Multiple Sclerosis Relapse', EKB Journal Management System, 32(2), pp. 41-47. doi: 10.21608/ejmm.2023.280275
Khalifa, R., Abdel Aziz, N., Shalash, A., Nada, M., Abdel Salam, S. IL-23 Receptor Expression on T Helper 17 Cells and its Implication in Multiple Sclerosis Relapse. EKB Journal Management System, 2023; 32(2): 41-47. doi: 10.21608/ejmm.2023.280275

IL-23 Receptor Expression on T Helper 17 Cells and its Implication in Multiple Sclerosis Relapse

Egyptian Journal of Medical Microbiology
Volume 32, Issue 2, April 2023, Page 41-47  XML PDF (454.72 K)
Document Type: New and original researches in the field of Microbiology.
DOI: 10.21608/ejmm.2023.280275
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Authors
Reham Ali Khalifa email orcid 1; Nesma Abdel Aziz2; Ali Shalash3; Maha Nada3; Shimaa Ahmed Abdel Salamorcid 4
1Medical Microbiology and Immunology, Faculty of Medicine, Ain Shams University
2Medical Microbiology and Immunology department, Faculty of Medicine, Ain Shams University.
3Neurology department, Faculty of Medicine, Ain Shams University.
4Medical Microbiology and Immunology department, Faculty of Medicine Ain Shams university
Abstract
Background: Multiple Sclerosis (MS) is considered the prototype of neurodegenerative diseases affecting around 2 million people worldwide. MS was marked primarily as an IL-17-mediated autoimmune disease, the hallmark cytokine of T helper (Th) 17 cells. Th 17 cells are considered as one of MS key effectors through the IL-23/IL-17 axis. Objectives: To investigate IL-23 receptor expression on Th17 cells with assessment of serum IL-17 level and their implication in MS relapse. Methodology: Patients included 22 MS patients in remission, 22 MS patients in active relapse and 22 healthy controls. Clinical assessment of the expanded disability severity scale (EDSS) for included patients. All groups were subjected to flow-cytometric analysis to assess expression of IL-23 receptor (IL-23R) on CD4+ T cells and measurement of serum IL-17A level by using ELISA. Results: MS patients during active relapse had a higher IL-17A serum level, and a higher percentage of IL-23R+ CD4+ T cells with increased IL-23R expression density on CD4+ T cells compared to patients in remission and controls. Conclusion:  The results reflected Th 17 key role in MS immune pathogenesis. Thus, the IL-23/IL-17 axis can be a potential target for immunomodulatory therapies ameliorating the Th17 mediated autoimmunity through novel treatments for those patients.
Keywords
Neurodegenerative; cytokines; IL-23; autoreactive; demyelinating
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