Inflammation Clinical Trial
Official title:
Ocular Micro-vascular Research Base on Functional Slip Lamp Biomicroscopy
Dry eye disease (DED), as one of the most common ocular surface diseases that affecting visual acuity, is highly associated with ocular surface inflammation. Until now, there is no accurate quantization index system to evaluate real-time ocular surface inflammation. Besides, an individualized therapy for ocular surface inflammation is also badly needed. As we all know, conjunctival congestion is one of the important clinical appearance of ocular surface inflammation. Hence, we suggest that several specific microvascular indexes could measure the change of ocular surface inflammation. Our program is aiming to investigate the correlation between inflammatory factors and blood flow velocity as well as microvascular distribution detecting from bulbar conjunctiva through our own devices and software.Futhermore, we tend to compare ocular surface microvascular indexes and microvascular distribution in normal people and dry eye patients in order to establish a database for Chinese people. By confirming the relationship between ocular surface microvascular indexes and ocular inflammation, we hope to set up new diagnostic criteria for ocular inflammation and an individualized therapeutic regimen based on ocular surface microvascular indexes. Finally, we want to establish a precision diagnostic and therapeutic pattern for dry eye disease.
Dry eye (DE) is a growing public health concern that affects not only the visual function but
also the quality of life of patients. In 2017, the International DE Study Workshop (DEWSII)
adjusted the definition of DE by particularly emphasizing the inflammation in the ocular
surface, and this adjustment represented a major shift in the understanding of dry eye
disease (DED) pathogenesis and the facilitation of DED treatment.1,2 The recurrence of
chronic and low-grade inflammation plays an important role in long-term disease progression
and gradually deteriorates the ocular surface.3 Previous studies have concluded that the
inflammatory response is involved in the pathological process of DE.4-7 The concentrations of
IL-1α and mature IL-1ß in the tear fluid are increased.4,5 The activity of MMP-9, a suggested
biomarker associated with ocular surface diseases including DE, is significantly elevated in
Meibomian gland dysfunction (MGD), Sjögren's syndrome (SS) and aqueous tear deficiency
(ATD).6 Other studies have indicated that inflammatory mediators such as IL-6, IL-8 and TNFα
are expressed proportionally to the severity of DE symptoms, indicating the involvement of
inflammation.7 The identification of inflammation as a major factor in DE informs the
treatment strategy, including anti-inflammatory medication, which results in improvements to
the ocular surface condition and to ocular comfort in DED patients.8,9 A series of studies
have demonstrated improvements in the subjective and objective signs and symptoms of DE after
anti-inflammatory and immunomodulatory therapies.8-11 To monitor the status of ocular surface
inflammation and the ocular surface condition, traditional assessments, namely, evaluation of
conjunctival hyperemia12 and corneal fluorescein staining using a slit lamp biomicroscope,
are used. However, these methods are subjective and volatile and may not be sensitive
indicators of the disease stage and treatment efficacy.13 A number of new tests have been
used to distinguish inflammation.13-15 These new technologies include corneal confocal
microscopy,15 conjunctival impression cytology16 and inflammatory tear-film cytokine tests in
research and in the clinic.17 These newly implemented techniques have several limitations.
Corneal confocal microscopy is a structure-based instrument with a narrow view of 400 × 400
µm2 that is limited to localization and cell counting. Conjunctival impression cytology16 and
inflammatory tear-film cytokine tests19 are not routinely used, possibly due to the
invasiveness, high cost and discomfort of these techniques.5,18 Therefore, the development of
new methodologies to noninvasively and subjectively evaluate the inflammation status of the
ocular surface is crucial.
The microvascular system of the bulbar conjunctiva can be easily accessed. The release of
inflammatory cytokines on the ocular surface can cause vasodilation, which may result in
alterations to the conjunctival microcirculation.19 Cheung et al. used a computer-assisted
intravital microscope to evaluate vasculopathies of the conjunctival vessels and identified
microvascular abnormalities in patients with diabetes20 and in patients who wore contact
lens.21 Schulze et al. have also performed `evaluations of the redness of the bulbar
conjunctiva using fractal analysis and photometry.22 However, these studies did not directly
measure the microcirculation. The microcirculation is an important aspect of the vascular
system, may directly represent the hemodynamic response to ocular surface inflammation and
may exhibit more sensitivity for monitoring vascular responses to anti-inflammatory
treatment. Recently, Jiang et al. developed a functional slit-lamp biomicroscope that could
be used to measure the conjunctival blood flow velocity (BFV) and vessel diameter.23 The goal
of the present study was to characterize the microvasculature and microcirculation in the
bulbar conjunctiva of DE patients in response to anti-inflammatory treatment.
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