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Inflammatory Ocular Diseases and Sphingolipid Signaling

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Bioactive Ceramides in Health and Disease

Part of the book series: Advances in Experimental Medicine and Biology ((AEMB,volume 1159))

Abstract

Inflammation is a powerful immune countermeasure to tissue damage and infection. The inflammatory response is complex and requires the involvement of myriad signaling pathways and metabolic processes, all governed by a multitude of regulatory systems. Although inflammation is a vital defense against tissue injury and a necessary step in tissue healing, the mechanisms which modulate the initiation, intensity, and duration of this innate immune response can malfunction and result in inappropriate or out-of-control inflammation, even in the absence of an appropriate stimulus. Though the human eye exists in an immune-privileged microenvironment, it is not spared from this. The eye is neither devoid of immune cells nor is it fully sequestered from systemic immune responses, and is therefore fully capable of ruining itself through localized inflammatory dysfunction and systemic inflammatory disease (Taylor AW, Front Immunol 7:37, 2016; Zhou R, Caspi RR, Biol Rep 2, 2010). In fact, a wide range of ocular inflammatory diseases exist and are major causes of blindness in humans. Advances in the understanding of inflammatory processes have revealed new key pathways and molecular factors involved in the mechanisms of inflammation. Lipids and sphingolipids are increasingly being recognized as having important signaling roles in the pathophysiology of ocular inflammatory diseases. What follows below is a discussion of fundamental inflammatory processes, the place of sphingolipids as mediators of said processes, brief descriptions of major inflammatory ocular diseases, and new findings implicating sphingolipids in their pathogenesis.

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Abbreviations

AMD:

age-related macular degeneration

C1P:

ceramide 1-phosphate

Cer:

ceramide

CLRs:

C-type lectin receptors

COX2:

cyclooxygenase 2

DAMPs:

Damage-Associated Molecular Patterns

DM:

diabetes mellitus

DR:

diabetic retinopathy

GlcCer:

glucosylceramide

ICAM-1:

Intercellular adhesion molecule 1

IOP:

intraocular pressure

IRFs:

Interferon regulatory factors

LacCer:

lactosylceramide

LPS:

lipopolysaccharide

MAPK:

Mitogen-activated protein kinase

MCP1:

monocyte chemoattractant protein 1

MS:

Multiple Sclerosis

NLR:

NOD-like receptors

NPDR:

Nonproliferative diabetic retinopathy

PAMPs:

Pathogen-Associated Molecular Patterns

PDR:

proliferative diabetic retinopathy

PRR:

Pattern Recognition Receptors

PVD:

posterior vitreous detachment

RGC:

retinal glial cell

RIP1:

Receptor interacting protein-1

RLRs:

Retinoic acid-inducible gene (RIG)-I-like receptors

RPE:

retinal pigmented epithelial

S1P:

sphingosine 1-phosphate

S1PR2:

S1P receptor 2

NF-κB:

Nuclear factor-κB

Sph:

Sphingosine

TFLL:

tear film lipid layer

TLRs:

Toll-like receptors

VCAM-1:

Vascular cell adhesion molecule 1

VEGF:

Vascular endothelial growth factor

VLC:

very long chain

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Acknowledgements

The authors acknowledge the support of the National Eye Institute grants [EY022071, EY025256, EY021725], and grants from Foundation Fighting Blindness Inc., USA and Research to Prevent Blindness Inc., USA.

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Correspondence to Nawajes Mandal .

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Grambergs, R., Mondal, K., Mandal, N. (2019). Inflammatory Ocular Diseases and Sphingolipid Signaling. In: Stiban, J. (eds) Bioactive Ceramides in Health and Disease. Advances in Experimental Medicine and Biology, vol 1159. Springer, Cham. https://doi.org/10.1007/978-3-030-21162-2_8

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