Corneal epithelial dendritic cells, tear neuropeptides and corneal nerves continue to be affected more than 12 months after LASIK

Chao, Cecilia; Tajbakhsh, Zahra; Stapleton, Fiona; Mobeen, Rabia; Madigan, Michele C.; Jalbert, Isabelle; Briggs, Nancy; Golebiowski, Blanka

doi:10.1111/aos.15270

Cited by 11 publications

(42 citation statements)

References 52 publications

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“…(54)(55)(56) The presence of thick dendrites is an indicator of migratory capacity of DC. (9,15,57) DC with migratory potential were evident mostly at the limbus. This may be due to their close proximity to limbal vessels which facilitate DC migration.…”

Section: Discussionmentioning

confidence: 98%

“…Bright/ hyperreflective cells at least 10 µm in size, with a linear/ curvilinear cell body, with or without dendrites (both short and long), located at the subbasal corneal epithelium and distributed among nerve fibres that do or do not cross them or conjunctival epithelium were considered as DC. (15) To minimise bias, DC density and morphology were assessed by an experienced investigator who was masked to the participants' identity and measurement timepoint.…”

Section: Image Analysismentioning

confidence: 99%

“…DC body size and presence of dendrites at all locations were assessed using a grading system developed by our group. (15) Cell body size refers to the cell soma and does not include the dendrites and was graded as small (10-25 µm), medium (26-40 µm), or large (>40 µm), based on the largest cell body size observed in any of the 5 images (or in the single inferior whorl image). The measurement was based on an estimation of cell body size by using a pictorial reference as described previously by our group without further analysis by software to make it easy to use and accessible.…”

Section: Image Analysismentioning

confidence: 99%

“…The measurement was based on an estimation of cell body size by using a pictorial reference as described previously by our group without further analysis by software to make it easy to use and accessible. (15) The presence of any dendrites, the presence of long dendrites and the presence of thick dendrites in any of the 5 images (or in the single inferior whorl image) were recorded. Images devoid of DC were not included in the DC morphology analysis.…”

Section: Image Analysismentioning

confidence: 99%

“…(5) Changes in DC morphology can also be a marker of immune response activation, indicating the antigen capture and migratory capacity of these cells as summarised and reviewed. (2,(6)(7)(8)(9)(10)(11)(12)(13)(14)(15)(16)(17)(18)(19) Ocular surface DC present in a steady state in ocular tissues that are in contact with the external environment and, in the event of an injury or insult, they undergo significant alteration to activate the immune response. (2) Upon activation, DC undergo morphological changes induced by the expression of surface markers such as major histocompatibility complex.…”

Section: Introductionmentioning

confidence: 99%

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Diurnal changes and topographical distribution of ocular surface epithelial dendritic cells in humans, and repeatability of density and morphology assessment

Tajbakhsh

Jalbert

Stapleton

et al. 2022

Preprint

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Purpose: Dendritic cells (DC) play a crucial role in ocular surface defence. DC can be visualised in vivo by confocal microscopy but have not yet been fully characterised in humans. This study investigated the diurnal variation, topographical distribution, and repeatability of DC density and morphology measurement. Methods: In vivo confocal microscopy was conducted on 20 healthy participants (mean age 32.7±6.4 years, 50% F) at baseline and repeated after 30 minutes, 2, 6, and 24 hours. Images were captured at the corneal centre, inferior whorl, corneal periphery, limbus, and bulbar conjunctiva. DC density was counted manually, and morphology of DC was assessed for the largest cell body size, presence of dendrites, presence of long dendrites, and presence of thick dendrites. Mixed model analysis, non-parametric analyses, Bland & Altman plots, the Coefficient of Repeatability (CoR), and kappa were used. Results: There were no significant changes in DC density (p≥0.74) or morphology (p>0.07) at any location over the 24-hour period. Highest DC density was observed at the corneal limbus followed by the peripheral cornea (p<0.001), with lowest density at the corneal centre, inferior whorl, and bulbar conjunctiva. Most DC at the corneal periphery, limbus, and bulbar conjunctiva had larger cell bodies compared to the corneal centre (p≤0.01), and presence of long dendrites was observed mostly at non-central locations. DC with thick dendrites were mostly observed at the limbus. Day-to-day CoR for DC density ranged from ±28.1 cells/mm2 at the corneal centre to ±56.4 cells/mm2 at the limbus. Day-to-day agreement of DC morphology determined by kappa ranged from 0.5 to 0.95 for cell body size, 0.60 to 0.95 for presence of dendrites, and 0.55 to 0.80 for presence of long dendrites, at various locations. Conclusions: No diurnal changes are apparent in corneal or conjunctival DC. Substantial topographical differences exist in DC density and morphology. In vivo confocal microscopy provides good repeatability of DC density and acceptable agreement of DC morphology. Keywords: cornea, conjunctiva, dendritic cell, diurnal variation, antigen capture capacity, migratory capacity.

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Section: Discussionmentioning

confidence: 98%

Section: Image Analysismentioning

confidence: 99%

Section: Image Analysismentioning

confidence: 99%

Section: Image Analysismentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Diurnal changes and topographical distribution of ocular surface epithelial dendritic cells in humans, and repeatability of density and morphology assessment

Tajbakhsh

Jalbert

Stapleton

et al. 2022

Preprint

Self Cite

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Neurophysiology of corneal neuropathic pain and emerging pharmacotherapeutics

Asiedu

2023

J of Neuroscience Research

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The altered activity generated by corneal neuronal injury can result in morphological and physiological changes in the architecture of synaptic connections in the nervous system. These changes can alter the sensitivity of neurons (both second‐order and higher‐order projection) projecting pain signals. A complex process involving different cell types, molecules, nerves, dendritic cells, neurokines, neuropeptides, and axon guidance molecules causes a high level of sensory rearrangement, which is germane to all the phases in the pathomechanism of corneal neuropathic pain. Immune cells migrating to the region of nerve injury assist in pain generation by secreting neurokines that ensure nerve depolarization. Furthermore, excitability in the central pain pathway is perpetuated by local activation of microglia in the trigeminal ganglion and alterations of the descending inhibitory modulation for corneal pain arriving from central nervous system. Corneal neuropathic pain may be facilitated by dysfunctional structures in the central somatosensory nervous system due to a lesion, altered synaptogenesis, or genetic abnormality. Understanding these important pathways will provide novel therapeutic insight.

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Analysis of Clinical Characteristics and Neuropeptides in Patients with Dry Eye with and without Chronic Ocular Pain after FS-LASIK

Zhao,

Zhou,

Duan

et al. 2024

Ophthalmol Ther

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Corneal epithelial dendritic cells, tear neuropeptides and corneal nerves continue to be affected more than 12 months after LASIK

Cited by 11 publications

References 52 publications

Diurnal changes and topographical distribution of ocular surface epithelial dendritic cells in humans, and repeatability of density and morphology assessment

Diurnal changes and topographical distribution of ocular surface epithelial dendritic cells in humans, and repeatability of density and morphology assessment

Neurophysiology of corneal neuropathic pain and emerging pharmacotherapeutics

Analysis of Clinical Characteristics and Neuropeptides in Patients with Dry Eye with and without Chronic Ocular Pain after FS-LASIK

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