Abstract

Monocytes/macrophages play a central role in immune response by secreting inflammatory cytokines upon activation. Two of the major cytokines secreted by the activated monocytes are Interleukin-6 (IL-6) and tumor necrosis factor alpha (TNF-alpha). Cytokines stimulate immune cells by autocrine and paracrine mechanisms. Treatment with morphine seems to affect the functioning of the immune system by selective inhibiting the secretion of cytokines. At the present time the mechanism by which morphine inhibit cytokine gene expression is not completely understood. Based on our preliminary studies, we hypothesize that morphine inhibit the activation of an important transcription factor necessary for cytokine gene expression. In order to determine the molecular mechanisms involved, we will use a model system (Bac 1.25 cell line) representing monocyte activation by bacterial lipopolysaccharides (LPS). Morphine treatment of Bac 1.25 cells has been shown to inhibit LPS induced expression IL-6 and TNF-alpha. Expression of both of these cytokine genes is dependent on the activation of a transcription factor, NFkappaB. Interestingly, morphine treatment also inhibited the activation of NFkappaB by LPS. In the current proposal, we will investigate the molecular mechanism by which morphine selectively inhibit NFkappaB activation by LPS. Initially, we will study whether morphine inhibit NFkappaB synthesis or its translocation into the nucleus. NFkappaB is normally retained in the cytoplasm as an inactive complex with an inhibitory protein, IkappaB. Phosphorylation of specific serine and threonine residues induces a conformational change in IkappaB and dissociation in the complex. Phosphorylated IkappaB is a signal for its eventual ubiquitinylation and proteolytic degradation. We will systematically investigate how morphine treatment influences of IkappaB phosphorylation associated events. Finally, we will determine which of the upstream intracellular signaling pathways leading to NFkappaB activation is affected by morphine. These studies will help in understanding he molecular mechanism of morphine mediated immunosuppression and help in the development of novel therapeutic regimens to overcome opportunistic infections.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Drug Abuse (NIDA)
Type
Specialized Center (P50)
Project #
5P50DA011806-05
Application #
6606509
Study Section
Project Start
2002-07-01
Project End
2003-06-30
Budget Start
Budget End
Support Year
5
Fiscal Year
2002
Total Cost
Indirect Cost

  Institution

Name
University of Minnesota Twin Cities
Department
Type
DUNS #
168559177
City
Minneapolis
State
MN
Country
United States
Zip Code
55455

  Publications

Hwang, Cheol Kyu; Wagley, Yadav; Law, Ping-Yee et al. (2017) Phosphorylation of poly(rC) binding protein 1 (PCBP1) contributes to stabilization of mu opioid receptor (MOR) mRNA via interaction with AU-rich element RNA-binding protein 1 (AUF1) and poly A binding protein (PABP). Gene 598:113-130
Kibaly, Cherkaouia; Lin, Hong-Yiou; Loh, Horace H et al. (2017) Spinal or supraspinal phosphorylation deficiency at the MOR C-terminus does not affect morphine tolerance in vivo. Pharmacol Res 119:153-168
Kibaly, Cherkaouia; Kam, Angel Y F; Loh, Horace H et al. (2016) Naltrexone Facilitates Learning and Delays Extinction by Increasing AMPA Receptor Phosphorylation and Membrane Insertion. Biol Psychiatry 79:906-16
Meng, Jingjing; Roy, Sabita (2016) Study of Epithelium Barrier Functions by Real-time TER Measurement. Bio Protoc 6:
Banerjee, S; Sindberg, G; Wang, F et al. (2016) Opioid-induced gut microbial disruption and bile dysregulation leads to gut barrier compromise and sustained systemic inflammation. Mucosal Immunol 9:1418-1428
Banerjee, Santanu; Ninkovic, Jana; Meng, Jingjing et al. (2015) Morphine compromises bronchial epithelial TLR2/IL17R signaling crosstalk, necessary for lung IL17 homeostasis. Sci Rep 5:11384
Wang, Yan; Wang, Yan-Xia; Liu, Ting et al. (2015) ?-Opioid receptor attenuates A? oligomers-induced neurotoxicity through mTOR signaling. CNS Neurosci Ther 21:8-14
Meng, Jingjing; Banerjee, Santanu; Li, Dan et al. (2015) Opioid Exacerbation of Gram-positive sepsis, induced by Gut Microbial Modulation, is Rescued by IL-17A Neutralization. Sci Rep 5:10918
Kotecki, Lydia; Hearing, Matthew; McCall, Nora M et al. (2015) GIRK Channels Modulate Opioid-Induced Motor Activity in a Cell Type- and Subunit-Dependent Manner. J Neurosci 35:7131-42
Hwang, Cheol Kyu; Wagley, Yadav; Law, Ping-Yee et al. (2015) Analysis of epigenetic mechanisms regulating opioid receptor gene transcription. Methods Mol Biol 1230:39-51

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