Identifying a therapeutic option that can modulate the innate immune response without generally suppressing the immune system as a whole has been a key barrier to improving treatment for patients with MS. Using metabolic profiling, we have reported that resolvin D1 (RvD1), a pro-resolving lipid metabolite of omega-3 polyunsaturated fatty acids, is significantly decreased in the plasma of patients with MS. Consistent with this finding, MS patients have lower levels of omega-3 metabolites, which are precursors of resolvins, compared to healthy controls, a finding that has been replicated in animal models of the disease, experimental autoimmune encephalomyelitis (EAE). Notably, we found that daily supplementation with RvD1 significantly attenuated clini- cal symptoms in both chronic and relapsing-remitting EAE. These data are provocative for their translational potential, particularly because the immune system is not depressed by RvD1 treatment as it is with steroids and most other MS therapies. The immunomodulatory effect of RvD1 is mediated through its receptor, formyl peptide receptor 2 (FPR2), leading to modulation of AMP-activated protein kinase (AMPK), an important regulator of cell metabolism. In other human disease models, the RvD1-FPR2 signaling cascade protects by inducing an anti- inflammatory phenotype in macrophages. However, the mechanism affording this protection remains elusive. Granulocyte-macrophage colony-stimulating factor (GM-CSF) is a key player both in the pathology of both MS and EAE, promotes an inflammatory environment and neuronal damage. There is a growing interest in inhibiting the pro-inflammatory effects of GM-CSF signaling as a therapeutic target in MS. In our preliminary work, we found that RvD1 treatment inhibited GM-CSF signaling in macrophages and that this inhibition was AMPK de- pendent. However, how RvD1 affects AMPK activity and GM-CSF signaling to attenuate EAE is unclear. Our long-term goal is to identify natural endogenous signaling mechanisms that can be harnessed to treat autoim- mune diseases, particularly MS. Our overall objective here is to determine the mechanism of action of RvD1 in resolving inflammation and disability in mouse models of MS. Our central hypothesis is that RvD1 attenuates EAE disease progression by abrogating GM-CSF signaling resulting in the polarizing of pro-inflammatory mac- rophages into an anti-inflammatory phenotype. And the underlying mechanisms of macrophage phenotype switch are through FPR2-AMPK-dependent metabolic reprogramming. To test this hypothesis our specific aims are: 1) to identify the effects of RvD1 on the cellular phenotype and function of CNS-infiltrating macro- phages in EAE; and 2) to determine the effects of RvD1 on metabolic reprogramming in macrophages. We will address these aims with a combination of immunological, biochemical and innovative metabolomic ap- proaches that are already well in hand. The proposed studies will form the foundation for the development of innovative therapeutic strategies to resolve inflammation during MS with no side effects and will likely apply to other diseases involving pathogenic activation of the immune system.

Public Health Relevance

People with multiple sclerosis commonly suffer from relapses accompanied by damage-inducing inflammation, and current treatment methods suppress the whole immune system, resulting in unnecessary and ill-tolerated side effects. We have identified an endogenous metabolite that resolves inflammation without altering other components of the immune system. The proposed research will identify the mechanisms by which this endogenous metabolite resolves inflammation, ultimately leading to novel therapeutics for MS and potentially other autoimmune diseases.

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
1R01NS112727-01
Application #
9801758
Study Section
Clinical Neuroimmunology and Brain Tumors Study Section (CNBT)
Program Officer
Utz, Ursula
Project Start
2019-06-15
Project End
2024-03-31
Budget Start
2019-06-15
Budget End
2020-03-31
Support Year
1
Fiscal Year
2019
Total Cost
Indirect Cost
Name
Henry Ford Health System
Department
Type
DUNS #
073134603
City
Detroit
State
MI
Country
United States
Zip Code
48202