Azithromycin Differentially Alters TCR-Activated Helper T Cell Subset Phenotype and Effector Function

6533b862fe1ef96bd12c7725

RESEARCH PRODUCT

Azithromycin Differentially Alters TCR-Activated Helper T Cell Subset Phenotype and Effector Function

Abdul Wahid Ansari Fatemeh Saheb Sharif-askari Manju Nidagodu Jayakumar Abdul Khader Mohammed Narjes Saheb Sharif-askari Thenmozhi Venkatachalam Bassam Mahboub Reinhold E. Schmidt Rifat Akram Hamoudi Rifat Akram Hamoudi Rifat Akram Hamoudi Rabih Halwani Rabih Halwani Qutayba Hamid Qutayba Hamid

subject

lcsh:Immunologic diseases. Allergy 0301 basic medicine Receptors CCR4 Receptors CXCR3 Receptor expression Immunology Receptors Antigen T-Cell Biology CXCR3 03 medical and health sciences Chemokine receptor Interferon-gamma 0302 clinical medicine Downregulation and upregulation Cell Movement T-Lymphocyte Subsets Immunology and Allergy Humans IFN-γ Interleukin 4 Cells Cultured Original Research anti-inflammatory azithromycin CD4+ helper T cells CXCR3 Effector Cell growth T-cell receptor IL-4 apoptosis Cell Differentiation Bacterial Infections Th1 Cells Healthy Volunteers Cell biology Anti-Bacterial Agents 030104 developmental biology CCR4 Interleukin-4 lcsh:RC581-607 030215 immunology

description

In addition to their antibiotic activities, azithromycin (AZM) exhibits anti-inflammatory effects in various respiratory diseases. One of the potent anti-inflammatory mechanisms is through inhibition of CD4+ helper T (Th) cell effector function. However, their impact on specific Th subset is obscure. Herein, we demonstrate the cellular basis of phenotypic and functional alterations associated with Th subsets following AZM treatment in vitro. Using well-characterized Th subset specific chemokine receptors, we report significant suppression of T cell receptor (TCR)-stimulated hyperactivated CCR4+CXCR3+ (Th0) expansion compared to CCR4-CXCR3+ (Th1-like) and CCR4+CXCR3- (Th2-like) cells. Interestingly, this effect was associated with diminished cell proliferation. Furthermore, AZM significantly inhibited the inflammatory cytokines IFN-γ and IL-4 production, CCR4 and CXCR3 receptor expression, and viability of Th0, Th1-like, and Th2-like subsets. Our findings suggest that AZM differentially affects TCR-activated Th subsets phenotype and function, and CCR4 and CXCR3 downregulation and suppressed Th0 subset expansion could potentially influence their trafficking and differentiation into cytokine-producing effector cells.

year	journal	country	edition	language
2020-09-01	Frontiers in Immunology

10.3389/fimmu.2020.556579 http://europepmc.org/articles/PMC7575909