Pathogenesis of Acute and Delayed Corneal Lesions after Ocular Exposure to Sulfur Mustard Vapor

Pathogenesis of Acute and Delayed Corneal Lesions after Ocular Exposure to Sulfur Mustard Vapor

A subset of victims of ocular sulfur mustard (SM) exposure develops an irreversible, idiotypic keratitis with associated secondary pathologies, collectively referred to as mustard gas keratopathy (MGK). MGK involves a progressive corneal degeneration resulting in chronic ocular discomfort and impair...

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Bibliographische Detailangaben
Hauptverfasser: McNutt, Patrick, Lyman, Megan, Swartz, Adam, Tuznik, Kaylie, Kniffin, Denise, Whitten, Kim, Milhorn, Denise, Hamilton, Tracey
Format: Report
Sprache:eng
Schlagworte:
ACCUMULATION
Anatomy and Physiology
BIOCHEMISTRY
CASUALTIES
CHEMICAL WARFARE AGENTS
Chemical, Biological and Radiological Warfare
CLINICAL MEDICINE
CORNEA
DYSFUNCTION
EDEMA
EPITHELIUM
EROSION
EXPOSURE(GENERAL)
EYE
GASES
HUMANS
LESIONS
Medicine and Medical Research
MEMBRANES(BIOLOGY)
MUSTARD AGENTS
MUSTARD GAS KERATOPATHY
OCULAR TOXICITY
PATHOGENESIS
REPRINTS
SULFUR
SURFACES
THERAPY
TISSUES(BIOLOGY)
TOXICITY
VAPORS
VISION
WOUNDS AND INJURIES
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Zusammenfassung:A subset of victims of ocular sulfur mustard (SM) exposure develops an irreversible, idiotypic keratitis with associated secondary pathologies, collectively referred to as mustard gas keratopathy (MGK). MGK involves a progressive corneal degeneration resulting in chronic ocular discomfort and impaired vision for which clinical interventions have typically had poor outcomes. Using a rabbit corneal vapor exposure model, we previously demonstrated a clinical progression with acute and chronic sequelae similar to that observed in human casualties. However, a better understanding of the temporal changes that occur during the biphasic SM injury is crucial to mechanistic understanding and therapeutic development. Here we evaluate the histopathologic, biochemical and ultrastructural expressions of pathogenesis of the chronic SM injury over eight weeks. We confirm that MGK onset exhibits a biphasic trajectory involving corneal surface regeneration over the first two weeks, followed by the rapid development and progressive degeneration of corneal structure. Preclinical markers of corneal dysfunction were identified, including destabilization of the basal corneal epithelium, basement membrane zone abnormalities and stromal deformation. Clinical sequelae of MGK appeared abruptly three weeks after exposure, and included profound anterior edema, recurring corneal erosions, basement membrane disorganization, basal cell necrosis and stromal degeneration. Unlike resolved corneas, MGK corneas exhibited frustrated corneal wound repair, with significantly elevated histopathology scores. Increased lacrimation, disruption of the basement membrane and accumulation of proinflammatory mediators in the aqueous humor provide several mechanisms for corneal degeneration. These data suggest that the chronic injury is fundamentally distinct from the acute lesion, involving injury mechanisms that operate on different time scales and in different corneal tissues. The original document contains color images. Published in PLOS ONE, v7 n8 e42837 p1-10 Aug 2012.