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PubMed Publications| Keyword search (4,163 papers available) |  |
"Little SR" Authored Publications:
| Title | Authors | PubMed ID | |
|---|---|---|---|
| 1 | Correction: Miniaturized scalable arrayed CRISPR screening in primary cells enables discovery at the single donor resolution | Patel MA; Boribong BP; Sinha H; Xiao B; Xie K; Vo PQN; Chin AB; Ellouzi A; Little SR; Shih SCC; Wu H; Muller WJ; Hirukawa A; | 41028230 BIOLOGY |
| 2 | Miniaturized scalable arrayed CRISPR screening in primary cells enables discovery at the single donor resolution | Patel MA; Boribong BP; Sinha H; Xiao B; Xie K; Vo PQN; Chin AB; Ellouzi A; Little SR; Shih S; Wu H; Muller WJ; Hirukawa A; | 40790054 BIOLOGY |
| 3 | Modulatory effects of M3 muscarinic acetylcholine receptor on inflammatory profiles of human memory T helper cells | Gholizadeh F; Hajiaghayi M; Choi JS; Little SR; Rahbari N; Kargar M; Brotto K; Han E; Shih SCC; Darlington PJ; | 40405417 BIOLOGY |
| 4 | A Digital Microfluidic Platform for the Microscale Production of Functional Immune Cell Therapies | Little SR; Rahbari N; Hajiaghayi M; Gholizadeh F; Cloarec-Ung FM; Phillips J; Sinha H; Hirukawa A; Knapp DJHF; Darlington PJ; Shih SCC; | 40390294 BIOLOGY |
| 5 | The β2-adrenergic biased agonist nebivolol inhibits the development of Th17 and the response of memory Th17 cells in an NF-κB-dependent manner | Hajiaghayi M; Gholizadeh F; Han E; Little SR; Rahbari N; Ardila I; Lopez Naranjo C; Tehranimeh K; Shih SCC; Darlington PJ; | 39445009 BIOLOGY |
| 6 | An Automated Single-Cell Droplet-Digital Microfluidic Platform for Monoclonal Antibody Discovery | Ahmadi F; Tran H; Letourneau N; Little SR; Fortin A; Moraitis AN; Shih SCC; | 38441226 BIOLOGY |
| 7 | An electrochemical aptasensor for Δ9-tetrahydrocannabinol detection in saliva on a microfluidic platform | Kékedy-Nagy L; Perry JM; Little SR; Llorens OY; Shih SCC; | 36549107 BIOLOGY |
| 8 | Viral Generation, Packaging, and Transduction on a Digital Microfluidic Platform | Quach ABV; Little SR; Shih SCC; | 35192339 BIOLOGY |
| Title: | The β2-adrenergic biased agonist nebivolol inhibits the development of Th17 and the response of memory Th17 cells in an NF-κB-dependent manner | ||||
| Authors: | Hajiaghayi M, Gholizadeh F, Han E, Little SR, Rahbari N, Ardila I, Lopez Naranjo C, Tehranimeh K, Shih SCC, Darlington PJ | ||||
| Link: | https://pubmed.ncbi.nlm.nih.gov/39445009/ | ||||
| DOI: | 10.3389/fimmu.2024.1446424 | ||||
| Publication: | Frontiers in immunology | ||||
| Keywords: | IL-17A; NF-κ; B activation; Th17 cells; anti-inflammatory response; beta-adrenergic receptor; biased agonist; nebivolol; | ||||
| PMID: | 39445009 | Category: | Date Added: | 2024-10-24 | |
| Dept Affiliation: |
BIOLOGY
1 Department of Biology, Concordia University, Montréal, QC, Canada. 2 Department of Health, Kinesiology and Applied Physiology, Concordia University, Montréal QC, Canada. 3 Department of Electrical and Computer Engineering, Concordia University, Center of Applied Synthetic Biology, Montréal, QC, Canada. |
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Description: |
Introduction: Adrenergic receptors regulate metabolic, cardiovascular, and immunological functions in response to the sympathetic nervous system. The effect of ß2-adrenergic receptor (AR) as a high expression receptor on different subpopulations of T cells is complex and varies depending on the type of ligand and context. While traditional ß2-AR agonists generally suppress T cells, they potentially enhance IL-17A production by Th17 cells. The effects of pharmacological drugs that count as biased agonists of AR like nebivolol are not completely understood. We investigated the impact of nebivolol on human memory CD4+ T (Th1, Th2, Th17) cells and polarized naive Th17 cells, highlighting its potential for IL-17A suppression via a non-canonical ß2-AR cell signaling pathway. Methods: The effects of nebivolol were tested on healthy human peripheral blood mononuclear cells, purified memory Th cells, and polarized naive Th17 cells activated with anti-CD3/anti-CD28/anti-CD2 ImmunoCult reagent. IFN-?, IL-4, and IL-17A, which are primarily derived from Th1, Th2, and Th17 cells, respectively, were quantified by ELISA and flow cytometry. IL-10 was measured by ELISA. Gene expression of RORC, ADRB1, ADRB2, and ADRB3 was evaluated by qPCR. The ADRB2 gene was knocked out in memory Th cells using CRISPR/Cas9. Protein expression of phosphorylated serine133-CREB and phosphorylated NF-?B p65 was assessed by Western blot. Proliferation was assessed by fluorescent dye loading and flow cytometry. Results: Nebivolol treatment decreased IL-17A and IFN-? secretion by activated memory Th cells and elevated IL-4 levels. Nebivolol reduced the proportion of IL-17A+ Th cells and downregulated RORC expression. Unlike the ß2-AR agonist terbutaline, nebivolol inhibited the shift of naive CD4+ T cells toward the Th17 phenotype. IL-10 and the proliferation index remained unchanged. Nebivolol-treated ß2-knockout memory Th cells showed significant inhibition of ß2-AR-mediated signaling, evidenced by the absence of IL-17A suppression compared to controls. Phosphorylation of the NF-?B p65 subunit was inhibited by nebivolol, but CREB phosphorylation was not changed, suggesting a selective transcriptional control. Conclusions: The findings demonstrate that nebivolol acts through a ß2-AR-mediated signaling pathway, as a distinctive anti-inflammatory agent capable of selectively shifting Th17 cells and suppressing the phosphorylation of NF-?B. This highlights nebivolol's potential for therapeutic interventions in chronic autoimmune conditions with elevated IL-17A levels. |
