Glaucoma Clinical Trial
Official title:
Glaucoma Within Northern Ireland Cohort for the Longitudinal Study of Ageing
Glaucoma is the leading cause of irreversible blindness worldwide. It is caused by damage to
the optic nerve between the back of the eye and the brain leading to progressive blindness.
The cause is poorly understood but ageing, increased intraocular pressure (IOP) and genetics
are all likely to play a role. There is no cure for glaucoma but treatments are available
which slow progression. Because vision cannot be restored once lost, early detection,
monitoring and early treatment are all essential to preserve visual function.
The condition is diagnosed using a combination of the appearance of the optic nerve on
clinical examination or photograph and visual field testing (perimetry). Measurement of IOP
and measurement of the thickness of the retinal layers at the back of the eye complement
diagnostic decisions.
The Northern Ireland Cohort for the Longitudinal Study of Ageing (NICOLA) study does not
include perimetry in the series of tests carried out on all participants but does include
photography of the optic nerve, measurement of IOP and measurement of retinal thickness.
Therefore we propose to invite back participants of the NICOLA study who have abnormal optic
discs and high eye pressure to return for perimetry to confirm a diagnosis of glaucoma.
Calling back participants for perimetry is essential to make the diagnosis not only for
estimating prevalence but also for identifying participant's ill-health.
The primary aim of this study is to quantify the number of participants in the NICOLA study
who have glaucoma and report its risk factors. This will allow an estimate of the number of
people in the whole of NI with glaucoma. We will also perform a series of novel tests using
state-of-the-art technologies to assess if they are better than current tests at diagnosing
glaucoma. This may enable better informed decisions about policy decisions in eyecare.
Purpose and design: This study will answer the following research questions:
1. What is the prevalence of glaucoma within the NICOLA cohort and which systemic and
socioeconomic factors influence its prevalence?
2. What is the diagnostic accuracy (sensitivity and specificity) of Retinal Nerve Fibre
Layer (RNFL) thickness measurements in the diagnosis of glaucoma?
3. What is the diagnostic accuracy (sensitivity and specificity) of macular thickness
analysis in the diagnosis of glaucoma?
4. What is the agreement between intraocular pressure measurement by Ocular Response
Analyser (ORA) and Goldmann tonometry?
5. What is the correlation between structural (circumpapillary RNFL or macular Ganglion
Cell Complex thickness) or functional measurements (retinal oximetry or perimetry) and
Optical Coherence Tomography angiography parameters (% vessel density and vessel
calibre) in the assessment of glaucoma?
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