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Can Structural Grading of Foveal Hypoplasia Predict Future Vision in Infantile Nystagmus?
Journal Pre-proof Can structural grading of foveal hypoplasia predict future vision in infantile nystagmus? A longitudinal study Sohaib R. Rufai, BMBS, BMedSc, Mervyn G. Thomas, MBChB, PhD, Ravi Purohit, BSc, MSc), Catey Bunce, MSc, DSc, Helena Lee, PhD, FRCOphth, Frank A. Proudlock, MSc, PhD, Irene Gottlob, MD, FRCOphth PII:
S0161-6420(19)32212-2
DOI:
https://doi.org/10.1016/j.ophtha.2019.10.037
Reference:
OPHTHA 10988
To appear in:
Ophthalmology
Received Date: 23 August 2019 Revised Date:
18 October 2019
Accepted Date: 28 October 2019
Please cite this article as: Rufai SR, Thomas MG, Purohit R, Bunce C, Lee H, Proudlock FA, Gottlob I, Can structural grading of foveal hypoplasia predict future vision in infantile nystagmus? A longitudinal study, Ophthalmology (2019), doi: https://doi.org/10.1016/j.ophtha.2019.10.037. This is a PDF file of an article that has undergone enhancements after acceptance, such as the addition of a cover page and metadata, and formatting for readability, but it is not yet the definitive version of record. This version will undergo additional copyediting, typesetting and review before it is published in its final form, but we are providing this version to give early visibility of the article. Please note that, during the production process, errors may be discovered which could affect the content, and all legal disclaimers that apply to the journal pertain. © 2019 Published by Elsevier Inc. on behalf of the American Academy of Ophthalmology
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Title Page
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Full title
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Can structural grading of foveal hypoplasia predict future vision in infantile nystagmus? A
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longitudinal study
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Authors
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Sohaib R Rufai (BMBS, BMedSc)1, Mervyn G Thomas (MBChB, PhD)1, Ravi Purohit (BSc,
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MSc)1, Catey Bunce (MSc, DSc)3, Helena Lee (PhD, FRCOphth)2, Frank A Proudlock (MSc,
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PhD)1, Irene Gottlob (MD, FRCOphth)1*
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Affiliations
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1. The University of Leicester Ulverscroft Eye Unit, Robert Kilpatrick Clinical Sciences Building, Leicester Royal Infirmary, Leicester, UK. 2. Department of Primary Care & Public Health Sciences, King’s College London, London, UK. 3. Clinical and Experimental Sciences, Faculty of Medicine, University of Southampton, Southampton, UK.
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Corresponding author*
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Professor Irene Gottlob
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E-mail: [email protected]
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Telephone: +44 (0)116 2523268
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Fax: +44 (0)116 2231996
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Meeting Presentations: This study was presented in part at the following international
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meetings: Royal College of Ophthalmologists Annual Congress, May 21-24 2018, Liverpool,
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UK; Association for Research in Vision and Ophthalmology (ARVO) Annual Meeting, April
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29-May 3 2018, Honolulu, Hawaii, USA – Awarded ARVO Members in Training Prize for
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Best Neuro-ophthalmology Poster.
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Financial Support: Medical Research Council, UK (grant numbers: MR/N004566/1 and
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MR/J004189/1); Fight for Sight, UK (grant number: 5009/5010); Ulverscroft Foundation,
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UK; Nystagmus Network, UK. The sponsor or funding organization had no role in the design
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or conduct of this research
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Conflict of Interest: No conflicting relationship exists for any author.
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Running head: Predicting Future Vision in Infantile Nystagmus
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33 34
Abstract
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PURPOSE: To evaluate structural grading and quantitative segmentation of foveal
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hypoplasia using handheld optical coherence tomography (HH-OCT), versus preferential
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looking, as predictors of future vision in preverbal children with infantile nystagmus.
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DESIGN: Longitudinal cohort study
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PARTICIPANTS: 81 eyes from 42 patients with infantile nystagmus (albinism, n=19;
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idiopathic infantile nystagmus (IIN), n=17; achromatopsia, n=6) were examined.
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METHODS: A 10×10mm foveal area was sampled using a 3-dimensional raster scan
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program (500×100, A scans×B scans) with ultra-high resolution spectral-domain HH-OCT
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(Leica Microsystems Envisu C2300, <4 µm axial resolution) in preverbal children aged up to
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36 months. Foveal tomograms were graded using our six-point grading system for foveal
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hypoplasia and segmented for quantitative analysis: photoreceptor (PR) length, outer segment
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(OS) length and foveal developmental index (FDI, a ratio of inner layers versus total foveal
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thickness). Patients were followed up until they could perform chart visual acuity (VA)
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testing. Data was analysed using linear mixed regression models. VA predicted by foveal
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grading was compared to prediction by preferential looking (PL) – the current gold standard
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for visual assessment in infants and young children.
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MAIN OUTCOME MEASURES: Grade of foveal hypoplasia, quantitative parameters (PR
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length, OS length, FDI) and preferential looking VA were obtained in preverbal children for
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comparison with future chart VA outcomes.
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RESULTS: We imaged 81 eyes from 42 patients with infantile nystagmus of mean age 19.8
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months (range: 0.9-33.4; S.D. 9.4) at their first HH-OCT scan. Mean follow-up was 44.1
56
months (range: 18.4-63.2; S.D. 12.0). Structural grading was the strongest predictor of future
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visual acuity (grading: r=0.80, F=67.49, p<0.0001) compared to quantitative measures (FDI:
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r=0.74, F=28.81, p<0.001; OS length: r=0.65; F=7.94, p=0.008; PR length: r=0.65; F=7.94,
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p=0.008). PL was inferior to VA prediction by foveal grading (PL: r=0.42; F=3.12, p<0.03).
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CONCLUSIONS: Infantile nystagmus can be an alarming condition with variable impact on
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vision. HH-OCT can predict future VA in infantile nystagmus. Structural grading is a better
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predictor of future VA than quantitative segmentation and PL testing. Predicting future vision
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could avert parental anxiety and optimise childhood development.
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FINANCIAL DISCLOSURES: The authors have no proprietary or commercial interest in
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any materials discussed in this article.
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Introduction
67 68
Nystagmus is a condition of constant, involuntary to-and-fro movements of the eyes
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occurring in 24 per 10,000 people.1 Onset is usually in early infancy, which can be alarming
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for parents and families especially because the pre-verbal child is unable to communicate
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their level of vision. Parents may initially believe the child is blind or has severely impaired
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vision and their reaction can include fear, anxiety and uncertainty over their child’s future.2
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As there is great variation in visual prognosis, predicting future vision could avert anxiety
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and/or help parents plan adjustments to support the child, particularly to optimise
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development and educational attainment. Targeted interventions may include accessible
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learning materials and toys, as well as support with safe mobility and daily living skills.2
77 78
Optical coherence tomography (OCT) is a non-invasive imaging technique that provides
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ultra-high resolution cross-sectional scans of the retina and optic nerve within seconds.
80
Recently, a handheld spectral-domain OCT (HH-OCT) has been developed for clinical use in
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the paediatric population. It has overcome the limitations of the conventional adult OCT
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system and is demonstrably reliable, including in nystagmus.3-5 The normal retinal6 and optic
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nerve development7 have been recently described in vivo using HH-OCT. Diseases
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investigated with HH-OCT include retinopathy of prematurity and other retinal disorders,
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nystagmus, trauma, optic nerve disease, intraocular tumours and central nervous diseases.3,5,8
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Normal development of the human fovea has been traced from 22 weeks gestation to 45
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months postpartum using ex vivo histological specimens.9 This is characterised by three
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developmental processes occurring at the fovea: i) centrifugal displacement of inner retinal
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layers, ii) cone photoreceptor specialisation, and iii) centripetal migration of cone
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photoreceptors.9 These stages are seen on OCT morphology as the following features of the
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fovea, respectively: i) formation and deepening of foveal pit with outward displacement,
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termed “extrusion”, of the plexiform layers, ii) outer segment (OS) lengthening and iii) outer
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nuclear layer (ONL) widening.10 Failure of any of these processes results in foveal under-
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development called “foveal hypoplasia”, causing reduced visual acuity (VA). Foveal
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hypoplasia is often associated with infantile nystagmus.10 Infantile nystagmus is associated
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with conditions including albinism and aniridia (mutations of the PAX6 gene), or may be
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idiopathic. “Typical” foveal hypoplasia is characterised by an underdeveloped fovea wherein
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the lining of individual retinal layers is intact.10 Early onset degeneration of the outer retina as
100
in achromatopsia also causes abnormal persisting inner retinal layers, but since the
101
underlying photoreceptors are disrupted this has been termed “atypical” foveal
102
hypoplasia.10,11
103 104
Structural grading of OCT morphology can enable classification of foveal hypoplasia based
105
on severity. Thomas et al10 proposed a structural grading scheme for foveal hypoplasia based
106
on OCT data from adults and older children, which has become a widely used scheme with
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Grades 1 to 4 representing the most to least developed fovea, whilst the atypical grade
108
represents disruption of the photoreceptors seen in achromatopsia. Each of the grades
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corresponded to statistically distinct VA levels. A key recommendation was validation of the
110
scheme using an independent dataset. More recently, Wilk et al12 identified two subsets of
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Grade 1 hypoplasia and proposed to subdivide these into Grade 1a, in which nearly normal
112
pit metrics (depth, diameter, and/or volume within 2 S.D. of the normal average) are
113
observed, and Grade 1b, in which the pit is only a shallow indent (see Methods: Figure 1 for
114
structural grading scheme employed by the present study and Figure 2 for accompanying
115
grading algorithm).
116 117
An alternative method of evaluating foveal hypoplasia is quantitative segmentation. This
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involves measuring the thickness of different foveal layers. Mohammad et al13 demonstrated
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that total photoreceptor thickness and outer segment length are highly correlated with VA in
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adults with albinism. The ratio of inner layer versus total foveal thickness, termed the foveal
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developmental index (FDI), correlated with VA in albinism.14
122 123
The gold standard test for VA assessment in older children is logMAR chart VA testing,
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beginning at four years of age.15 From ages 0-3 years, the gold standard test to assess VA is
125
preferential looking, based on the principle that young children tend to fixate to a pattern
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stimulus in preference to a plain field.16 However, it can be difficult to assess young children
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with nystagmus using preferential looking due to constant eye movements17, hence it would
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be of great value to identify a better tolerated and easier office-based method for VA
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prediction such as using HH-OCT. Visual evoked potentials (VEP) may represent another
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option for estimating VA in infantile nystagmus18, but this is time consuming and difficult to
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perform, requiring specialist diagnostic services.
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In this longitudinal cohort study, we harness the potential of HH-OCT for the diagnosis and
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prognosis of foveal hypoplasia in young children. The primary aim was to validate a
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structural grading system for foveal hypoplasia in infants and young children with infantile
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nystagmus to predict future vision. Secondary aims were: i) to assess whether structural
137
grading is comparable to quantitative segmentation in predicting future vision; ii) to compare
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the predictive power of the grading system with preferential looking VA results taken on first
139
examination; iii) to determine whether the grade remains stable over time.
140 141
Materials and Methods
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Study design and participants
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This was a prospective longitudinal cohort study of patients with infantile nystagmus
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recruited in a quaternary referral centre in Leicester, United Kingdom. Longitudinal data
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were collected between 20th February 2012 and 30th January 2018. This study is reported
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according to the Strengthening the Reporting of Observational Studies in Epidemiology
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(STROBE) statement.
148 149
The study adhered to the tenets of the Declaration of Helsinki and ethics committee approval
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was granted by the East Midlands - Nottingham 2 Research Ethics Committee. Consent was
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obtained by all parents or guardians of study participants.
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Inclusion criteria were: 1) Diagnosis of infantile nystagmus; 2) Age of 36 months or younger
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at first HH-OCT scan; 3) Age of at least 42 months or older and ability to participate in chart
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logMAR visual acuity test on follow up visit. Exclusion criteria included unsuccessful
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acquisition of HH-OCT scan at first visit, loss to follow-up, scans of inadequate quality for
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structural grading and co-existing neurological problems. If the HH-OCT scan was only
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successful in one eye, then the other eye was excluded from analysis. If the HH-OCT scan
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was unsuccessful in both eyes, then the participant was excluded from analysis. Examination
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1 involved HH-OCT and full ophthalmic examination including refraction. Examination 2
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involved full ophthalmic examination and best corrected VA measurement when the
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participant was old enough to participate in chart logMAR vision testing. This age group was
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deemed clinically important as it approaches or coincides with primary school education. In
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addition, longitudinal HH-OCT scans were obtained.
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166
Diagnosis of albinism was made based on abnormal lateralisation on visual evoked potentials
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(VEP), iris transillumination defects, skin hypopigmentation and, if clinical uncertainty
168
existed, genetic testing.19,20 Diagnosis of achromatopsia was made based on typical features
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including light sensitivity, small amplitude nystagmus, inner segment ellipsoid (ISe)
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disruption identified on OCT, as well as confirmatory electrodiagnostic and genetic testing.10
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IIN was diagnosed in children with nystagmus and normal ophthalmic examination, normal
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VEPs and electroretinograms and/or confirmation on genetic testing (i.e. pathogenic FRMD7
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mutation).
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HH-OCT image acquisition, grading and segmentation
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A noncontact, spectral domain HH-OCT scanner (ENVISU C class 2300; <4 µm axial
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resolution; Leica Microsystems, Wetzlar, Germany) was used to image the foveae of all
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participants in an outpatient setting without sedation. Visual fixation devices were employed
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to minimise movement during imaging; these included toys, books and cartoons. The
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acquisition protocol used a 10×10mm scanning window. The 3-dimensional raster scan
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program for both scan sequences comprised 100 B-scans and 500 A-scans per B-scan line.
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The acquisition time was short (1.9 seconds) to facilitate successful image acquisition with
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minimal disruption of quality, thereby avoiding measurement bias.
184 185
The HH-OCT imaging protocol involved scanning the right eye followed by the left eye. The
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en face view was used to identify the optic nerve as a landmark for identification of the fovea.
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The region temporal to the optic nerve was navigated frame by frame until the most central
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foveal B-scan was found. Where a foveal pit was present, the B-scan with the deepest pit was
189
selected for grading and segmentation. Where no pit was present, the B-scan with the highest
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OS peak or, if absent, that with the highest ONL dome was selected. If no foveal landmarks
191
were present (termed fovea plana), a B-scan was selected within the central foveal area. We
192
repeated scans three times per eye, selecting the highest quality scan where the retinal layers
193
were most easily discernible for analysis. If unsuccessful, scans were repeated until an
194
adequate quality image was achieved or until the child ceased to participate. The total
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examination time typically took up to 10 minutes per child. All OCT scans were graded by
196
two graders (SRR and MGT) to assess inter-grader reliability. All OCT scans from
197
Examination 1 were segmented for quantitative analysis. Segmentation was performed using
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ImageJ software (National Institutes of Health, released 2011, Version 1.48, Bethesda,
199
Maryland, U.S.)
200 201
Structural grading was based on the scheme described by Thomas et al10 with Grade 1
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subdivided into 1a and 1b as per Wilk et al.12 The grading scheme is displayed in Figure 1 -
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we refer to this as the Leicester Grading System for Foveal Hypoplasia. The accompanying
204
grading algorithm is displayed in Figure 2. Parameters for segmentation are illustrated in
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Figure 3.
206 207
Visual acuity measurement
208
During Examination 1, preferential looking VA testing using Keeler Acuity Cards (Keeler
209
Ltd, Windsor, UK) was performed where possible; cards were held vertically to more easily
210
determine responses in horizontal nystagmus, thereby avoiding measurement bias.17 During
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Examination 2, the Keeler LogMAR Crowded Acuity Test, which uses crowded letter
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optotypes on charts, was used as the gold standard VA test provided the child could
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cooperate.21 For children who could not cooperate, the Crowded Kay LogMAR Picture test
214
was used.21 This test involves matching easily recognisable pictures (house, car, star, apple,
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boot and duck) and is easier for children who cannot match letters.21 Where possible,
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cycloplegic refraction was performed prior to Examinations 1 and 2. Mean spherical
217
equivalent for this cohort was +2.38 (range: -8.75 to +8.38; S.D. +3.22).
218 219
Statistical analysis
220
Our power calculation demonstrated that 38 patients were required to achieve power (α=0.05,
221
β=0.1, r=0.5), based upon the null hypothesis that the correlation is zero. Data was analysed
222
using linear mixed model regression analysis including grade of foveal hypoplasia and eye
223
recorded (right/left) in the model; the dependent variable was chart tested LogMAR VA
224
recorded at Examination 2. Independent variables recorded at Examination 1 included grade
225
of foveal hypoplasia, quantitative segmentation parameters (OS length, ONL length and FDI)
226
and preferential looking VA in LogMAR. Age in months was also included in the model for
227
preferential looking testing because the VA result is expected to improve with age.16 These
228
analyses were computed using SPSS Statistics (IBM Corp. released 2013, Version 22.0.
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Armonk, NY: IBM Corp.) Agreement between two graders was reported to assess the
230
validity of the grading system. Agreement of grades over time was reported to explore
231
whether grades remain stable over time.22
232
233
Role of the funding source
234
The sponsor or funding organisations had no role in the design or conduct of this research.
235 236
Results
237
Baseline characteristics
238
Out of 47 patients enrolled to this study, data from 42 (89%) were included: two were lost to
239
follow up and three did not cooperate with HH-OCT scanning. During Examination 1, we
240
obtained OCT scans of 81 eyes from 42 patients of mean age 19.8 months (range: 0.9-33.4;
241
S.D. 9.4); 3 right eye tomograms of 3 patients were of inadequate quality for grading and thus
242
excluded. Adequate power was therefore achieved (n=38, α=0.05, β=0.1, r=0.5). Mean
243
follow-up to Examination 2 was 44.1 months (range: 18.4-63.2; S.D. 12.0). 16 patients were
244
female and 26 were male. In Examination 2, LogMAR VA using letter optotypes (Crowded
245
Keeler’s testing) was successfully obtained in 39 patients (93%) with all children being
246
optimally refracted; 3 patients could not read letter optotypes, hence were tested with Kay’s
247
LogMAR Picture Cards. Baseline characteristics of patients are listed in Table 1.
248 249
The cohort included children with albinism (n=19 patients), idiopathic infantile nystagmus
250
(IIN) (n=17) and achromatopsia (n=6).
251 252
Grading of foveal hypoplasia
253
Using the grading scheme alone, the inter-grader correlation coefficient was 0.96 when
254
subdividing Grade 1 into 1a and 1b, suggesting the infant grading system is robust. There was
255
disagreement for 3 eyes from 3 patients during the masked grading by the second grader.
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Each case of disagreement was over what constituted a nearly normal pit as per Grade 1a
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versus a shallow indent as per Grade 1b, however there was total agreement following
258
discussion and training, which involved studying the treatment algorithm and discussing
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examples of 1a versus 1b pits. Agreement between Graders 1 and 2 prior to training is
260
displayed in the Supplemental Table.
261 262
Foveal hypoplasia was identified in 57 eyes according to our structural grading scheme,
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which included Grade 1a (n=17), Grade 1b (n=10), Grade 2 (n=2), Grade 3 (n=10), Grade 4
264
(n=6) and atypical foveal hypoplasia (n=12). Normal tomograms were seen in 24 eyes.
265
266
Figure 4 displays samples of HH-OCT central B-scans per grade. Figure 5 displays a
267
breakdown of diagnoses per grade.
268 269
Prediction of future visual acuity
270
Figure 6 is a box and whisker plot displaying the grade of foveal hypoplasia during
271
Examination 1 versus VA during Examination 2. Median (M) and interquartile range (IQR)
272
per grade were as follows: no foveal hypoplasia: M=0.26, IQR=0.27; Grade 1a: M=0.41,
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IQR=0.32; Grade 1b: M=0.65, IQR=0.16; Grade 2: M=0.60, IQR=0.00; Grade 3: M=0.74,
274
IQR=0.22; Grade 4: M=1.01, IQR=0.23; Atypical: M=0.93; IQR=0.28.
275 276
HH-OCT scans of gradable quality were successfully obtained in 81 out of 90 eyes (90.0%).
277
The Leicester Grading System for Foveal Hypoplasia demonstrated strong predictive power
278
for future VA (r=0.80, F=67.49, p<0.0001). This grading system correctly predicted future
279
VA within 0.3 logMAR in 78 out of 81 eyes (96.3%) and within 0.2 logMAR in 60 out of 81
280
eyes (74.1%).
281 282
Quantitative segmentation analysis
283
All quantitative segmentation parameters demonstrated statistically significant associations
284
with future VA in typical foveal hypoplasia, but none as strongly as structural grading (OS
285
length: r=0.65; F=7.94, p=0.008; PR length: r=0.65, F=6.90, p=0.01; FDI: r=0.74, F=28.81,
286
p<0.001). Scatter plots to show quantitative segmentation analyses for Examination 1 OCT
287
scans versus VA in Examination 2 are shown in eFigure 1.
288 289
Preferential looking
290
Preferential looking testing at Examination 1 was successfully assessed in 49 out of 72 eyes
291
(68.1%). Preferential looking was a poorer predictor of future VA (r=0.42; F=3.12; p=0.03)
292
compared to HH-OCT. Age did not have a statistically significant effect (p=0.09).
293
Preferential looking testing correctly predicted future VA within 0.3 logMAR in 19 out of 49
294
eyes (38.8%) and within 0.2 logMAR in 17 out of 49 eyes (34.7%).
295 296
Longitudinal grading
297
Longitudinal OCT scans were obtained in 80 eyes from 40 patients with mean follow-up 40.5
298
months (range: 10.4-62.3, S.D. 15.7). The longitudinal intra-grade correlation co-efficient
299
was
1.0,
as
all
grades
remained
the
same
over
time.
300 301 302
Discussion
303
To our knowledge, this is the first longitudinal study in infants and young children using HH-
304
OCT to provide a visual prognosis. In foveal hypoplasia the grading scheme10,12 has been
305
validated and demonstrates the strongest prediction of vision compared to quantitative
306
measures and preferential looking in this cohort. The inter-grader reliability testing
307
demonstrates that this scheme is robust. All grades remained stable throughout the study
308
period. In infants and young children, all typical grades achieved VA approximately 2 lines
309
worse than that predicted by grading in adults and older children10: in whom VA per grade
310
was as follows: Grade 1: median 0.20, IQR=0.12; Grade 2: median 0.44, IQR=0.18; Grade 3:
311
median 0.60, IQR=0.0; Grade 4: median=0.78, IQR=0.11; Atypical: median=1.0,
312
IQR=0.08.10 In infants and young children they were as follows: No foveal hypoplasia: 0.26;
313
Grade 1: 0.41; Grade 2: 0.60; Grade 3: 0.74; Grade 4: 1.01; Atypical: 0.93. As only one
314
patient with grade 2 foveal hypoplasia was recruited in this study, results for grade 2 cannot
315
be generalized. These differences could be due to visual acuity still undergoing development
316
and cooperation/ability for VA testing improving with increasing age.23 The slightly better
317
predicted VA in young children with atypical foveal hypoplasia in our study compared to the
318
study in adults and older children is likely because achromatopsia may be a progressive
319
disease.24
320 321
Grading versus quantitative segmentation
322
Our study revealed that grading was a stronger predictor of vision compared to quantitative
323
segmentation. An explanation could be that the grading system incorporates all key elements
324
of foveal development, while measurement of FDI, OS length and PR length only represent
325
individual developmental landmarks. However, quantitative segmentation may give insight
326
into subtle differences within a single grade, which may be particularly useful in
327
achromatopsia, represented solely in one atypical grade. Longitudinal quantitative
328
measurements may also help in the monitoring of patients undergoing emerging therapies.
329
For example, measurements of the ONL in achromatopsia, which changes with increasing
330
age24, are particularly important to determine the degree of cone degeneration in view of gene
331
therapy.
332 333
Grading can be performed rapidly in clinic whereas quantitative segmentation requires
334
special training and takes approximately 20 minutes per patient. Furthermore, grading can
335
help clinicians make appropriate decisions regarding management and investigation. For
336
example, if VA is poorer than expected according to grading, there should be raised suspicion
337
of other pathology limiting the VA. This may include other retinal pathology such as retinal
338
dystrophy, cortical/neurological disorders, amblyopia, conditions affecting the anterior
339
segment or sub-optimally corrected refractive errors. Similarly, if a patient has poor vision
340
consistent with a high degree of foveal hypoplasia, it is likely that the limiting factor for poor
341
VA is accounted at the retinal level.
342 343
Grading versus preferential looking
344
Preferential looking was a poor predictor of future VA, tending to underestimate visual
345
potential in nystagmus. Constant eye movement may increase difficulties of assessing
346
whether the child has correctly identified test cards.17 Suboptimal refraction at Examination 1
347
may have contributed to the poor correlation between preferential looking and chart VA.
348
Mean chart VA predicted by preferential looking in our cohort was 1.0 logMAR, better than a
349
previously published figure in another young cohort with infantile nystagmus of mean age 43
350
months (1.7 logMAR), but still poor.25 Moreover, the success rate in preferential looking was
351
poor (68.1%) compared to HH-OCT (90.0%). Dubowitz et al26 achieved a similar success
352
rate of 70% (n=96) for preferential looking in children with retinopathy of prematurity, also
353
associated with foveal hypoplasia, of a similar age to our study. In our study, preferential
354
looking testing correctly predicted future VA within 3 lines in only 38.8% compared to
355
96.3% for HH-OCT.
356 357
Can the fovea be graded from birth?
358
Our grading system involves identifying the presence or absence of intact ISe, foveal pit, OS
359
lengthening and ONL widening. Histological and OCT studies have demonstrated that all of
360
these landmarks can be identified from birth except OS elongation, which continues up to 5
361
months postnatally.6,27 Hence, it is possible to determine all grades apart from Grade 2 and
362
Grade 3 from birth, as an infant may be inappropriately assigned Grade 3 before OS
363
elongation has occurred. In this study, no patient under 5 months with Grade 2 or 3 foveal
364
hypoplasia was identified. However, we successfully obtained scans from patients aged 1
365
month and 3 months with Grade 4 and atypical foveal hypoplasia, respectively. Longitudinal
366
OCT scans revealed that all grades remained the same until the end of the study period, hence
367
adding age into the regression model would not impact the correlation between grading and
368
future VA.
369 370
Study strengths and limitations
371
To our knowledge, this is the first longitudinal cohort study using HH-OCT to predict future
372
vision in infantile nystagmus. This helps to reassure and/or enable patients and families to
373
optimise the development and educational attainment of the child during this crucial age, as
374
well as helping clinicians in their decision-making process for investigation and management.
375
A powered cohort of infants and young children has been achieved with adequate follow up
376
until the child could participate with chart VA, approaching or coinciding with
377
commencement of primary school education. Our grading system demonstrated an inter-
378
grader coefficient of 0.96, suggesting it is robust. Our grading system shows lower prediction
379
of VA than previously found in older patients.10 This is likely due to less cooperation with
380
logMAR VA testing and an immature visual system.23 Nystagmus characteristics and head
381
posture may influence VA, however, even without taking these factors into account, we
382
found very good correlation between foveal structure and later VA. In the future, a
383
multivariate model including foveal structure and nystagmus could be calculated to
384
investigate whether VA prediction could be refined.
385 386
A limitation of our study is that we are currently only able to predict VA in childhood rather
387
than adulthood due to the recent availability HH-OCT. However, it is still of great value to
388
predict an infant’s VA at the time they commence primary education. It is likely that VA will
389
continue to improve based on adult data.10 Another limitation is that only three aetiologies of
390
foveal hypoplasia were represented within this cohort; the grading system was not applied to
391
other conditions associated with foveal hypoplasia such as PAX-6 mutation28, retinopathy of
392
prematurity29, nanophthalmos30 and other photoreceptor dystrophies. There were only two
393
eyes from one patient that fulfilled the criteria for Grade 2, therefore, median VA predicted
394
from this single patient (0.60) cannot be generalized. With respect to image acquisition, if
395
three scans per eye were unsuccessful, patients could not be included. However, most eyes
396
(90%) were successfully scanned.
397 398 399
Author Contributions
400
SRR: Concept, literature search, figures, study design, data collection, data analysis, data
401
interpretation, writing.
402
MGT: Concept, literature search, figures, study design, data analysis, data interpretation,
403
writing, critical revision.
404
RP: Data collection, data interpretation, critical revision.
405
CB: Study design, data analysis, data interpretation, writing, critical revision.
406
HL: Literature search, data collection, data interpretation, writing, critical revision.
407
FAP: Figures, study design, data analysis, data interpretation, writing, critical revision.
408
IG: Concept, study design, data collection, data interpretation, writing, critical revision,
409
overall supervision.
410 411
Acknowledgements
412
The authors would like to thank vision scientists Dr Rebecca McLean and Dr Zhanhan Tu,
413
research orthoptists Helen Kuht and Michael Hisaund, and research optometrist Sonal Shah,
414
for their support in data collection for this study. The authors would like to thank all the
415
patients and families who took part in this study.
416 417
SRR’s post is funded by a National Institute for Health Research (NIHR) Academic Clinical
418
Fellowship. MGT’s and HL’s posts are funded by National Institute for Health Research
419
(NIHR) Academic Clinical Lectureships. CB’s post is part funded/supported by the National
420
Institute for Health Research (NIHR) Biomedical Research Centre based at Guy's and St
421
Thomas' NHS Foundation Trust and King's College London. The views expressed are those
422
of the authors and not necessarily those of the NHS, the NIHR or the Department of Health
423
Figure 3 is reprinted from Ophthalmology, 118(8), Thomas MG, Kumar A, Mohammad S,
424
Proudlock FA, Engle EC, Andrews C, Chan WM, Thomas S, Gottlob I. Structural grading of
425
foveal hypoplasia using spectral-domain optical coherence tomography a predictor of visual
426
acuity? 1653-1660, Copyright (2011), with permission from Elsevier.
427
428
References
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1. Sarvananthan N, Surendran M, Roberts EO, Jain S, Thomas S, Shah N, Proudlock
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FA, Thompson JR, McLean RJ, Degg C, Woodruff G, Gottlob I. The prevalence of
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nystagmus: the Leicestershire nystagmus survey. Invest Ophthalmol Vis Sci. 2009
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Nov;50(11):5201-6.
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2. Nystagmus
Network.
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booklet.
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https://nystagmusnetwork.org/documents/parents-booklet/ Accessed 31 January 2019.
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3. Lee H, Proudlock FA, Gottlob I. Pediatric Optical Coherence Tomography in Clinical
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Practice—Recent Progress. Invest Ophthalmol Vis Sci. July 2016, Vol.57, OCT69-
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OCT79.
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4. Maldonado RS, Izatt JA, Sarin N, et al. Optimizing hand-held spectral domain optical
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coherence tomography imaging for neonates, infants, and children. Invest Ophthalmol
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Vis Sci. 2010; 51: 2678–2685.
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5. Lee H, Proudlock F, Gottlob I. Is handheld optical coherence tomography reliable in
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infants and young children with and without nystagmus? Invest Ophthalmol Vis Sci.
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2013; 54: 8152–8159.
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6. Lee H, Purohit R, Patel A, Papageorgiou E, Sheth V, Maconachie G, Pilat A, McLean
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RJ, Proudlock FA, Gottlob I. In Vivo Foveal Development Using Optical Coherence
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Tomography. Invest Ophthalmol Vis Sci. July 2015, Vol.56, 4537-4545.
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7. Patel A, Purohit R, Lee H, Sheth V, Maconachie G, Papageorgiou E, McLean RJ,
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Gottlob I, Proudlock FA. Optic Nerve Head Development in Healthy Infants and
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Children Using Handheld Spectral-Domain Optical Coherence Tomography.
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Ophthalmology. 2016 Oct; 123(10): 2147–2157.
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8. Papageorgiou E, Pilat A, Proudlock F, Lee H, Purohit R, Sheth V, Vasudevan P,
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Gottlob I. Retinal and optic nerve changes in microcephaly: An optical coherence
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tomography study. Neurology. 2018 Aug 7;91(6):e571-e585.
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9. Hendrickson AE, Yuodelis C. The morphological development of the human fovea. Ophthalmology. 1984;91:603–12.
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10. Thomas MG, Kumar A, Mohammad S, Proudlock FA, Engle EC, Andrews C, Chan
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WM, Thomas S, Gottlob I. Structural Grading of Foveal Hypoplasia. Ophthalmology.
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2011;118(8):1653–1660.
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11. Thomas MG, Kumar A, Kohl S, Proudlock FA, Gottlob I. High-resolution in vivo imaging in achromatopsia. Ophthalmology. 2011 May;118(5):882-7.
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12. Wilk MA, McAllister JT, Cooper RF, Dubis AM, Patitucci TN, Summerfelt P,
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Anderson JL, Stepien KE, Costakos DM, Connor TB, Wirostko WJ, Chiang PW,
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Dubra A, Curcio CA, Brillian MH, Summers CG, Carroll J. Relationship Between
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Foveal Cone Specialization and Pit Morphology in Albinism. Invest Ophthalmol Vis
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Sci. July 2014, Vol.55, 4186-4198. : s.n.
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13. Mohammad S Gottlob I Kumar A. The functional significance of foveal abnormalities
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in albinism measured using spectral-domain optical coherence tomography.
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Ophthalmology. 2011; 118: 1645–1652.
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14. Ather S. Imaging the visual pathway in human albinism. PhD thesis. University of Leicester, June 2016. 15. Huang RZ. Design of visual acuity chart for preschool children. Anhui Medical Journal. 1983;4(3):184–185. 16. Huurneman B, Boonstra, FN. Assessment of near visual acuity in 0–13 year olds with normal and low vision: a systematic review. BMC Ophthalmol. 2016; 16: 215.
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17. Getz LM, Dobson V, Luna B, Mash C. Interobserver Reliability of the Teller Acuity
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Card Procedure in Pediatric Patients. Invest Ophthalmol Vis Sci. 1996;37:180-187.
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18. Yasmin S. Bradfield; Thomas D. France; James Verhoeve; Ronald E. Gangnon.
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Sweep Visual Evoked Potential Testing as a Predictor of Recognition Acuity in
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Albinism. Arch Ophthalmol. 2007;125(5):628-633.
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19. Clinical and oculomotor characteristics of albinism compared to FRMD7 associated
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infantile nystagmus. Invest Ophthalmol Vis Sci. 2011 Apr 8;52(5):2306-13. Kumar A,
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Gottlob I, McLean RJ, Thomas S, Thomas MG, Proudlock FA.
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20. Thomas MG, Maconachie G, Sheth V, McLean RJ, Gottlob I. Development and
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clinical utility of a novel diagnostic nystagmus gene panel using targeted next-
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generation sequencing. Eur J Hum Genet. 2017 Jun;25(6):725-734.
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21. O'Boyle, Chen SI, Little J. Crowded letter and crowded picture logMAR acuity in
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22. Cohen, J. (1960) "A coefficient for agreement for nominal scales" in Education and Psychological Measurement. Vol. 20, pp. 37–46.
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23. Fu VLN, Bilonick RA, Felius J, Hertle RW, Birch EE. Visual Acuity Development of
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Children with Infantile Nystagmus Syndrome. Invest Ophthalmol Vis Sci. 2011 Mar;
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52(3): 1404–1411.
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24. Thomas MG, McLean RJ, Kohl S, Sheth V, Gottlob I. Early signs of longitudinal
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progressive cone photoreceptor degeneration in achromatopsia. Br J Ophthalmol.
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2012 Sep;96(9):1232-6.
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25. Katsumi O, Chedid SG, Kronheim JK, Henry RK, Denno S, Hirose T. Correlating
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preferential looking visual acuity and visual behavior in severely visually
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handicapped children. Acta Ophthalmol Scand. 1995 Oct;73(5):407-13.
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26. Dubowitz LMS, Mishin J, Morante A, Placzek M. The maturation of visual acuity in
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neurologically normal and abnormal newborn infants. Behav Brain Res. 1983; 10: 39-
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45.
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27. Gupta T, Kapoor K, Sahni D, Singh B. Mapping the Time Line of Development in
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Each Layer of Human Foetal Retina. J Clin Diagn Res. 2016 Mar; 10(3): AC04–
505
AC07.
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28. Hingorani M1, Williamson KA, Moore AT, van Heyningen V. Detailed
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ophthalmologic evaluation of 43 individuals with PAX6 mutations. Invest Ophthalmol
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Vis Sci. 2009 Jun;50(6):2581-90.
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29. Hammer DX, Iftimia NV, Ferguson RD, et al. Foveal fine structure in retinopathy of
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prematurity: an adaptive optics Fourier domain optical coherence tomography study.
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Invest Ophthalmol Vis Sci. 2008;49:2061–70.
512 513
30. Bijlsma WR, van Schooneveld MJ, Van der Lelij A. Optical coherence tomography findings for nanophthalmic eyes. Retina. 2008;28:1002–7.
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Figure Legends
516 517 518 519 520 521 522 523 524 525 526 527 528 529
Figure 1: The Leicester Grading System for Foveal Hypoplasia. Schematic demonstrating the features of a normal fovea detectable using optical coherence tomography (OCT), followed by the features of typical and atypical grades of foveal hypoplasia. The normal fovea features outward displacement, termed “extrusion”, of the plexiform layers. All grades of foveal hypoplasia feature continuation of the plexiform layers. Grade 1a foveal hypoplasia is associated with a nearly normal pit resembling a 'v' shape, OS lengthening and ONL widening relative to the parafoveal OS and ONL lengths, respectively. Grade 1b foveal hypoplasia is associated with a shallow indent, OS lengthening and ONL widening relative to the parafoveal OS and ONL lengths, respectively In Grade 2 foveal hypoplasia, all features of Grade 1 are present except there is no pit. Grade 3 foveal hypoplasia represents all features of Grade 2 except there is no lengthening of the OS segment. Grade 4 foveal hypoplasia represents grade 3 except there is no ONL widening at the fovea (termed fovea plana). Atypical foveal hypoplasia is characterised by a shallow foveal pit and disruption of the inner segment ellipsoid (ISe) band forming a hyporeflective zone. ILM = internal limiting
530 531 532 533 534 535
membrane; RNFL = retinal nerve fibre layer; GCL = ganglion cell layer; IPL = inner plexiform layer; INL = inner nuclear layer; OPL = outer plexiform layer; ONL = outer nuclear layer; ELM = external limiting membrane; ISe = inner segment ellipsoid; OS = outer segment; RPE = retinal pigment epithelium. Reprinted and adapted from Ophthalmology, 118(8), Thomas MG et al, 1653-1660, Copyright (2011), with permission from Elsevier.
536 537
Figure 2: Algorithm for Leicester Grading Scheme for Foveal Hypoplasia. Key: ISe = inner segment ellipsoid; OS = outer segment; ONL = outer nuclear layer.
538 539 540 541 542 543
Figure 3: Parameters for quantitative segmentation analysis. 1A: central foveal B-scan; 1B: En face fundal view. Three metrics were included in the segmentation analysis: (1) outer segment (OS) length: distance between Point I (cone outer segment tips: COST) to Point II (OS); (2) photoreceptor (PR) length: distance between Point I to Point III (outer nuclear layer: ONL) (3) Foveal Developmental Index (FDI): ratio of distance between Point I to Point III divided by distance between point I to point IV (foveal pit).
544
Figure 4: Examples of OCT scans for each grade of foveal hypoplasia.
545
Figure 5: Breakdown of grades by condition
546 547 548
Figure 6: Box and whisker plot to show typical grade of foveal hypoplasia in Examination 1 versus VA in Examination 2. VA = visual acuity, FH = foveal hypoplasia, M = median; IQR = interquartile range.
Variable n Mean (range; S.D.) Number of eyes (patients) 81 (42) Albinism 38 (19) IIN 31 (17) Achromatopsia 12 (6) Males 26 Females 16 Age at Examination 1 in months 19.8 (0.9-33.4; 9.4) Age at Examination 2 in months 63.9 (44.7-88.8; 11.6) Follow-up in months 44.1 (18.4-63.2; 12.0) Table 1: Baseline characteristics of cohort. Key: S.D. = standard deviation; IIN = idiopathic infantile nystagmus.
Handheld optical coherence tomography can predict future vision in infantile nystagmus. The Leicester Grading System for Foveal Hypoplasia provides better prediction of future vision than preferential looking – the current gold standard.
S0161-6420(19)32212-2
DOI:
https://doi.org/10.1016/j.ophtha.2019.10.037
Reference:
OPHTHA 10988
To appear in:
Ophthalmology
Received Date: 23 August 2019 Revised Date:
18 October 2019
Accepted Date: 28 October 2019
Please cite this article as: Rufai SR, Thomas MG, Purohit R, Bunce C, Lee H, Proudlock FA, Gottlob I, Can structural grading of foveal hypoplasia predict future vision in infantile nystagmus? A longitudinal study, Ophthalmology (2019), doi: https://doi.org/10.1016/j.ophtha.2019.10.037. This is a PDF file of an article that has undergone enhancements after acceptance, such as the addition of a cover page and metadata, and formatting for readability, but it is not yet the definitive version of record. This version will undergo additional copyediting, typesetting and review before it is published in its final form, but we are providing this version to give early visibility of the article. Please note that, during the production process, errors may be discovered which could affect the content, and all legal disclaimers that apply to the journal pertain. © 2019 Published by Elsevier Inc. on behalf of the American Academy of Ophthalmology
1
Title Page
2
Full title
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Can structural grading of foveal hypoplasia predict future vision in infantile nystagmus? A
4
longitudinal study
5
Authors
6
Sohaib R Rufai (BMBS, BMedSc)1, Mervyn G Thomas (MBChB, PhD)1, Ravi Purohit (BSc,
7
MSc)1, Catey Bunce (MSc, DSc)3, Helena Lee (PhD, FRCOphth)2, Frank A Proudlock (MSc,
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PhD)1, Irene Gottlob (MD, FRCOphth)1*
9
Affiliations
10 11 12 13 14 15
1. The University of Leicester Ulverscroft Eye Unit, Robert Kilpatrick Clinical Sciences Building, Leicester Royal Infirmary, Leicester, UK. 2. Department of Primary Care & Public Health Sciences, King’s College London, London, UK. 3. Clinical and Experimental Sciences, Faculty of Medicine, University of Southampton, Southampton, UK.
16
Corresponding author*
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Professor Irene Gottlob
18
E-mail: [email protected]
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Telephone: +44 (0)116 2523268
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Fax: +44 (0)116 2231996
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Meeting Presentations: This study was presented in part at the following international
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meetings: Royal College of Ophthalmologists Annual Congress, May 21-24 2018, Liverpool,
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UK; Association for Research in Vision and Ophthalmology (ARVO) Annual Meeting, April
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29-May 3 2018, Honolulu, Hawaii, USA – Awarded ARVO Members in Training Prize for
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Best Neuro-ophthalmology Poster.
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Financial Support: Medical Research Council, UK (grant numbers: MR/N004566/1 and
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MR/J004189/1); Fight for Sight, UK (grant number: 5009/5010); Ulverscroft Foundation,
28
UK; Nystagmus Network, UK. The sponsor or funding organization had no role in the design
29
or conduct of this research
30
Conflict of Interest: No conflicting relationship exists for any author.
31
Running head: Predicting Future Vision in Infantile Nystagmus
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33 34
Abstract
35
PURPOSE: To evaluate structural grading and quantitative segmentation of foveal
36
hypoplasia using handheld optical coherence tomography (HH-OCT), versus preferential
37
looking, as predictors of future vision in preverbal children with infantile nystagmus.
38
DESIGN: Longitudinal cohort study
39
PARTICIPANTS: 81 eyes from 42 patients with infantile nystagmus (albinism, n=19;
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idiopathic infantile nystagmus (IIN), n=17; achromatopsia, n=6) were examined.
41
METHODS: A 10×10mm foveal area was sampled using a 3-dimensional raster scan
42
program (500×100, A scans×B scans) with ultra-high resolution spectral-domain HH-OCT
43
(Leica Microsystems Envisu C2300, <4 µm axial resolution) in preverbal children aged up to
44
36 months. Foveal tomograms were graded using our six-point grading system for foveal
45
hypoplasia and segmented for quantitative analysis: photoreceptor (PR) length, outer segment
46
(OS) length and foveal developmental index (FDI, a ratio of inner layers versus total foveal
47
thickness). Patients were followed up until they could perform chart visual acuity (VA)
48
testing. Data was analysed using linear mixed regression models. VA predicted by foveal
49
grading was compared to prediction by preferential looking (PL) – the current gold standard
50
for visual assessment in infants and young children.
51
MAIN OUTCOME MEASURES: Grade of foveal hypoplasia, quantitative parameters (PR
52
length, OS length, FDI) and preferential looking VA were obtained in preverbal children for
53
comparison with future chart VA outcomes.
54
RESULTS: We imaged 81 eyes from 42 patients with infantile nystagmus of mean age 19.8
55
months (range: 0.9-33.4; S.D. 9.4) at their first HH-OCT scan. Mean follow-up was 44.1
56
months (range: 18.4-63.2; S.D. 12.0). Structural grading was the strongest predictor of future
57
visual acuity (grading: r=0.80, F=67.49, p<0.0001) compared to quantitative measures (FDI:
58
r=0.74, F=28.81, p<0.001; OS length: r=0.65; F=7.94, p=0.008; PR length: r=0.65; F=7.94,
59
p=0.008). PL was inferior to VA prediction by foveal grading (PL: r=0.42; F=3.12, p<0.03).
60
CONCLUSIONS: Infantile nystagmus can be an alarming condition with variable impact on
61
vision. HH-OCT can predict future VA in infantile nystagmus. Structural grading is a better
62
predictor of future VA than quantitative segmentation and PL testing. Predicting future vision
63
could avert parental anxiety and optimise childhood development.
64
FINANCIAL DISCLOSURES: The authors have no proprietary or commercial interest in
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any materials discussed in this article.
66
Introduction
67 68
Nystagmus is a condition of constant, involuntary to-and-fro movements of the eyes
69
occurring in 24 per 10,000 people.1 Onset is usually in early infancy, which can be alarming
70
for parents and families especially because the pre-verbal child is unable to communicate
71
their level of vision. Parents may initially believe the child is blind or has severely impaired
72
vision and their reaction can include fear, anxiety and uncertainty over their child’s future.2
73
As there is great variation in visual prognosis, predicting future vision could avert anxiety
74
and/or help parents plan adjustments to support the child, particularly to optimise
75
development and educational attainment. Targeted interventions may include accessible
76
learning materials and toys, as well as support with safe mobility and daily living skills.2
77 78
Optical coherence tomography (OCT) is a non-invasive imaging technique that provides
79
ultra-high resolution cross-sectional scans of the retina and optic nerve within seconds.
80
Recently, a handheld spectral-domain OCT (HH-OCT) has been developed for clinical use in
81
the paediatric population. It has overcome the limitations of the conventional adult OCT
82
system and is demonstrably reliable, including in nystagmus.3-5 The normal retinal6 and optic
83
nerve development7 have been recently described in vivo using HH-OCT. Diseases
84
investigated with HH-OCT include retinopathy of prematurity and other retinal disorders,
85
nystagmus, trauma, optic nerve disease, intraocular tumours and central nervous diseases.3,5,8
86 87
Normal development of the human fovea has been traced from 22 weeks gestation to 45
88
months postpartum using ex vivo histological specimens.9 This is characterised by three
89
developmental processes occurring at the fovea: i) centrifugal displacement of inner retinal
90
layers, ii) cone photoreceptor specialisation, and iii) centripetal migration of cone
91
photoreceptors.9 These stages are seen on OCT morphology as the following features of the
92
fovea, respectively: i) formation and deepening of foveal pit with outward displacement,
93
termed “extrusion”, of the plexiform layers, ii) outer segment (OS) lengthening and iii) outer
94
nuclear layer (ONL) widening.10 Failure of any of these processes results in foveal under-
95
development called “foveal hypoplasia”, causing reduced visual acuity (VA). Foveal
96
hypoplasia is often associated with infantile nystagmus.10 Infantile nystagmus is associated
97
with conditions including albinism and aniridia (mutations of the PAX6 gene), or may be
98
idiopathic. “Typical” foveal hypoplasia is characterised by an underdeveloped fovea wherein
99
the lining of individual retinal layers is intact.10 Early onset degeneration of the outer retina as
100
in achromatopsia also causes abnormal persisting inner retinal layers, but since the
101
underlying photoreceptors are disrupted this has been termed “atypical” foveal
102
hypoplasia.10,11
103 104
Structural grading of OCT morphology can enable classification of foveal hypoplasia based
105
on severity. Thomas et al10 proposed a structural grading scheme for foveal hypoplasia based
106
on OCT data from adults and older children, which has become a widely used scheme with
107
Grades 1 to 4 representing the most to least developed fovea, whilst the atypical grade
108
represents disruption of the photoreceptors seen in achromatopsia. Each of the grades
109
corresponded to statistically distinct VA levels. A key recommendation was validation of the
110
scheme using an independent dataset. More recently, Wilk et al12 identified two subsets of
111
Grade 1 hypoplasia and proposed to subdivide these into Grade 1a, in which nearly normal
112
pit metrics (depth, diameter, and/or volume within 2 S.D. of the normal average) are
113
observed, and Grade 1b, in which the pit is only a shallow indent (see Methods: Figure 1 for
114
structural grading scheme employed by the present study and Figure 2 for accompanying
115
grading algorithm).
116 117
An alternative method of evaluating foveal hypoplasia is quantitative segmentation. This
118
involves measuring the thickness of different foveal layers. Mohammad et al13 demonstrated
119
that total photoreceptor thickness and outer segment length are highly correlated with VA in
120
adults with albinism. The ratio of inner layer versus total foveal thickness, termed the foveal
121
developmental index (FDI), correlated with VA in albinism.14
122 123
The gold standard test for VA assessment in older children is logMAR chart VA testing,
124
beginning at four years of age.15 From ages 0-3 years, the gold standard test to assess VA is
125
preferential looking, based on the principle that young children tend to fixate to a pattern
126
stimulus in preference to a plain field.16 However, it can be difficult to assess young children
127
with nystagmus using preferential looking due to constant eye movements17, hence it would
128
be of great value to identify a better tolerated and easier office-based method for VA
129
prediction such as using HH-OCT. Visual evoked potentials (VEP) may represent another
130
option for estimating VA in infantile nystagmus18, but this is time consuming and difficult to
131
perform, requiring specialist diagnostic services.
132
133
In this longitudinal cohort study, we harness the potential of HH-OCT for the diagnosis and
134
prognosis of foveal hypoplasia in young children. The primary aim was to validate a
135
structural grading system for foveal hypoplasia in infants and young children with infantile
136
nystagmus to predict future vision. Secondary aims were: i) to assess whether structural
137
grading is comparable to quantitative segmentation in predicting future vision; ii) to compare
138
the predictive power of the grading system with preferential looking VA results taken on first
139
examination; iii) to determine whether the grade remains stable over time.
140 141
Materials and Methods
142
Study design and participants
143
This was a prospective longitudinal cohort study of patients with infantile nystagmus
144
recruited in a quaternary referral centre in Leicester, United Kingdom. Longitudinal data
145
were collected between 20th February 2012 and 30th January 2018. This study is reported
146
according to the Strengthening the Reporting of Observational Studies in Epidemiology
147
(STROBE) statement.
148 149
The study adhered to the tenets of the Declaration of Helsinki and ethics committee approval
150
was granted by the East Midlands - Nottingham 2 Research Ethics Committee. Consent was
151
obtained by all parents or guardians of study participants.
152 153
Inclusion criteria were: 1) Diagnosis of infantile nystagmus; 2) Age of 36 months or younger
154
at first HH-OCT scan; 3) Age of at least 42 months or older and ability to participate in chart
155
logMAR visual acuity test on follow up visit. Exclusion criteria included unsuccessful
156
acquisition of HH-OCT scan at first visit, loss to follow-up, scans of inadequate quality for
157
structural grading and co-existing neurological problems. If the HH-OCT scan was only
158
successful in one eye, then the other eye was excluded from analysis. If the HH-OCT scan
159
was unsuccessful in both eyes, then the participant was excluded from analysis. Examination
160
1 involved HH-OCT and full ophthalmic examination including refraction. Examination 2
161
involved full ophthalmic examination and best corrected VA measurement when the
162
participant was old enough to participate in chart logMAR vision testing. This age group was
163
deemed clinically important as it approaches or coincides with primary school education. In
164
addition, longitudinal HH-OCT scans were obtained.
165
166
Diagnosis of albinism was made based on abnormal lateralisation on visual evoked potentials
167
(VEP), iris transillumination defects, skin hypopigmentation and, if clinical uncertainty
168
existed, genetic testing.19,20 Diagnosis of achromatopsia was made based on typical features
169
including light sensitivity, small amplitude nystagmus, inner segment ellipsoid (ISe)
170
disruption identified on OCT, as well as confirmatory electrodiagnostic and genetic testing.10
171
IIN was diagnosed in children with nystagmus and normal ophthalmic examination, normal
172
VEPs and electroretinograms and/or confirmation on genetic testing (i.e. pathogenic FRMD7
173
mutation).
174
HH-OCT image acquisition, grading and segmentation
175 176
A noncontact, spectral domain HH-OCT scanner (ENVISU C class 2300; <4 µm axial
177
resolution; Leica Microsystems, Wetzlar, Germany) was used to image the foveae of all
178
participants in an outpatient setting without sedation. Visual fixation devices were employed
179
to minimise movement during imaging; these included toys, books and cartoons. The
180
acquisition protocol used a 10×10mm scanning window. The 3-dimensional raster scan
181
program for both scan sequences comprised 100 B-scans and 500 A-scans per B-scan line.
182
The acquisition time was short (1.9 seconds) to facilitate successful image acquisition with
183
minimal disruption of quality, thereby avoiding measurement bias.
184 185
The HH-OCT imaging protocol involved scanning the right eye followed by the left eye. The
186
en face view was used to identify the optic nerve as a landmark for identification of the fovea.
187
The region temporal to the optic nerve was navigated frame by frame until the most central
188
foveal B-scan was found. Where a foveal pit was present, the B-scan with the deepest pit was
189
selected for grading and segmentation. Where no pit was present, the B-scan with the highest
190
OS peak or, if absent, that with the highest ONL dome was selected. If no foveal landmarks
191
were present (termed fovea plana), a B-scan was selected within the central foveal area. We
192
repeated scans three times per eye, selecting the highest quality scan where the retinal layers
193
were most easily discernible for analysis. If unsuccessful, scans were repeated until an
194
adequate quality image was achieved or until the child ceased to participate. The total
195
examination time typically took up to 10 minutes per child. All OCT scans were graded by
196
two graders (SRR and MGT) to assess inter-grader reliability. All OCT scans from
197
Examination 1 were segmented for quantitative analysis. Segmentation was performed using
198
ImageJ software (National Institutes of Health, released 2011, Version 1.48, Bethesda,
199
Maryland, U.S.)
200 201
Structural grading was based on the scheme described by Thomas et al10 with Grade 1
202
subdivided into 1a and 1b as per Wilk et al.12 The grading scheme is displayed in Figure 1 -
203
we refer to this as the Leicester Grading System for Foveal Hypoplasia. The accompanying
204
grading algorithm is displayed in Figure 2. Parameters for segmentation are illustrated in
205
Figure 3.
206 207
Visual acuity measurement
208
During Examination 1, preferential looking VA testing using Keeler Acuity Cards (Keeler
209
Ltd, Windsor, UK) was performed where possible; cards were held vertically to more easily
210
determine responses in horizontal nystagmus, thereby avoiding measurement bias.17 During
211
Examination 2, the Keeler LogMAR Crowded Acuity Test, which uses crowded letter
212
optotypes on charts, was used as the gold standard VA test provided the child could
213
cooperate.21 For children who could not cooperate, the Crowded Kay LogMAR Picture test
214
was used.21 This test involves matching easily recognisable pictures (house, car, star, apple,
215
boot and duck) and is easier for children who cannot match letters.21 Where possible,
216
cycloplegic refraction was performed prior to Examinations 1 and 2. Mean spherical
217
equivalent for this cohort was +2.38 (range: -8.75 to +8.38; S.D. +3.22).
218 219
Statistical analysis
220
Our power calculation demonstrated that 38 patients were required to achieve power (α=0.05,
221
β=0.1, r=0.5), based upon the null hypothesis that the correlation is zero. Data was analysed
222
using linear mixed model regression analysis including grade of foveal hypoplasia and eye
223
recorded (right/left) in the model; the dependent variable was chart tested LogMAR VA
224
recorded at Examination 2. Independent variables recorded at Examination 1 included grade
225
of foveal hypoplasia, quantitative segmentation parameters (OS length, ONL length and FDI)
226
and preferential looking VA in LogMAR. Age in months was also included in the model for
227
preferential looking testing because the VA result is expected to improve with age.16 These
228
analyses were computed using SPSS Statistics (IBM Corp. released 2013, Version 22.0.
229
Armonk, NY: IBM Corp.) Agreement between two graders was reported to assess the
230
validity of the grading system. Agreement of grades over time was reported to explore
231
whether grades remain stable over time.22
232
233
Role of the funding source
234
The sponsor or funding organisations had no role in the design or conduct of this research.
235 236
Results
237
Baseline characteristics
238
Out of 47 patients enrolled to this study, data from 42 (89%) were included: two were lost to
239
follow up and three did not cooperate with HH-OCT scanning. During Examination 1, we
240
obtained OCT scans of 81 eyes from 42 patients of mean age 19.8 months (range: 0.9-33.4;
241
S.D. 9.4); 3 right eye tomograms of 3 patients were of inadequate quality for grading and thus
242
excluded. Adequate power was therefore achieved (n=38, α=0.05, β=0.1, r=0.5). Mean
243
follow-up to Examination 2 was 44.1 months (range: 18.4-63.2; S.D. 12.0). 16 patients were
244
female and 26 were male. In Examination 2, LogMAR VA using letter optotypes (Crowded
245
Keeler’s testing) was successfully obtained in 39 patients (93%) with all children being
246
optimally refracted; 3 patients could not read letter optotypes, hence were tested with Kay’s
247
LogMAR Picture Cards. Baseline characteristics of patients are listed in Table 1.
248 249
The cohort included children with albinism (n=19 patients), idiopathic infantile nystagmus
250
(IIN) (n=17) and achromatopsia (n=6).
251 252
Grading of foveal hypoplasia
253
Using the grading scheme alone, the inter-grader correlation coefficient was 0.96 when
254
subdividing Grade 1 into 1a and 1b, suggesting the infant grading system is robust. There was
255
disagreement for 3 eyes from 3 patients during the masked grading by the second grader.
256
Each case of disagreement was over what constituted a nearly normal pit as per Grade 1a
257
versus a shallow indent as per Grade 1b, however there was total agreement following
258
discussion and training, which involved studying the treatment algorithm and discussing
259
examples of 1a versus 1b pits. Agreement between Graders 1 and 2 prior to training is
260
displayed in the Supplemental Table.
261 262
Foveal hypoplasia was identified in 57 eyes according to our structural grading scheme,
263
which included Grade 1a (n=17), Grade 1b (n=10), Grade 2 (n=2), Grade 3 (n=10), Grade 4
264
(n=6) and atypical foveal hypoplasia (n=12). Normal tomograms were seen in 24 eyes.
265
266
Figure 4 displays samples of HH-OCT central B-scans per grade. Figure 5 displays a
267
breakdown of diagnoses per grade.
268 269
Prediction of future visual acuity
270
Figure 6 is a box and whisker plot displaying the grade of foveal hypoplasia during
271
Examination 1 versus VA during Examination 2. Median (M) and interquartile range (IQR)
272
per grade were as follows: no foveal hypoplasia: M=0.26, IQR=0.27; Grade 1a: M=0.41,
273
IQR=0.32; Grade 1b: M=0.65, IQR=0.16; Grade 2: M=0.60, IQR=0.00; Grade 3: M=0.74,
274
IQR=0.22; Grade 4: M=1.01, IQR=0.23; Atypical: M=0.93; IQR=0.28.
275 276
HH-OCT scans of gradable quality were successfully obtained in 81 out of 90 eyes (90.0%).
277
The Leicester Grading System for Foveal Hypoplasia demonstrated strong predictive power
278
for future VA (r=0.80, F=67.49, p<0.0001). This grading system correctly predicted future
279
VA within 0.3 logMAR in 78 out of 81 eyes (96.3%) and within 0.2 logMAR in 60 out of 81
280
eyes (74.1%).
281 282
Quantitative segmentation analysis
283
All quantitative segmentation parameters demonstrated statistically significant associations
284
with future VA in typical foveal hypoplasia, but none as strongly as structural grading (OS
285
length: r=0.65; F=7.94, p=0.008; PR length: r=0.65, F=6.90, p=0.01; FDI: r=0.74, F=28.81,
286
p<0.001). Scatter plots to show quantitative segmentation analyses for Examination 1 OCT
287
scans versus VA in Examination 2 are shown in eFigure 1.
288 289
Preferential looking
290
Preferential looking testing at Examination 1 was successfully assessed in 49 out of 72 eyes
291
(68.1%). Preferential looking was a poorer predictor of future VA (r=0.42; F=3.12; p=0.03)
292
compared to HH-OCT. Age did not have a statistically significant effect (p=0.09).
293
Preferential looking testing correctly predicted future VA within 0.3 logMAR in 19 out of 49
294
eyes (38.8%) and within 0.2 logMAR in 17 out of 49 eyes (34.7%).
295 296
Longitudinal grading
297
Longitudinal OCT scans were obtained in 80 eyes from 40 patients with mean follow-up 40.5
298
months (range: 10.4-62.3, S.D. 15.7). The longitudinal intra-grade correlation co-efficient
299
was
1.0,
as
all
grades
remained
the
same
over
time.
300 301 302
Discussion
303
To our knowledge, this is the first longitudinal study in infants and young children using HH-
304
OCT to provide a visual prognosis. In foveal hypoplasia the grading scheme10,12 has been
305
validated and demonstrates the strongest prediction of vision compared to quantitative
306
measures and preferential looking in this cohort. The inter-grader reliability testing
307
demonstrates that this scheme is robust. All grades remained stable throughout the study
308
period. In infants and young children, all typical grades achieved VA approximately 2 lines
309
worse than that predicted by grading in adults and older children10: in whom VA per grade
310
was as follows: Grade 1: median 0.20, IQR=0.12; Grade 2: median 0.44, IQR=0.18; Grade 3:
311
median 0.60, IQR=0.0; Grade 4: median=0.78, IQR=0.11; Atypical: median=1.0,
312
IQR=0.08.10 In infants and young children they were as follows: No foveal hypoplasia: 0.26;
313
Grade 1: 0.41; Grade 2: 0.60; Grade 3: 0.74; Grade 4: 1.01; Atypical: 0.93. As only one
314
patient with grade 2 foveal hypoplasia was recruited in this study, results for grade 2 cannot
315
be generalized. These differences could be due to visual acuity still undergoing development
316
and cooperation/ability for VA testing improving with increasing age.23 The slightly better
317
predicted VA in young children with atypical foveal hypoplasia in our study compared to the
318
study in adults and older children is likely because achromatopsia may be a progressive
319
disease.24
320 321
Grading versus quantitative segmentation
322
Our study revealed that grading was a stronger predictor of vision compared to quantitative
323
segmentation. An explanation could be that the grading system incorporates all key elements
324
of foveal development, while measurement of FDI, OS length and PR length only represent
325
individual developmental landmarks. However, quantitative segmentation may give insight
326
into subtle differences within a single grade, which may be particularly useful in
327
achromatopsia, represented solely in one atypical grade. Longitudinal quantitative
328
measurements may also help in the monitoring of patients undergoing emerging therapies.
329
For example, measurements of the ONL in achromatopsia, which changes with increasing
330
age24, are particularly important to determine the degree of cone degeneration in view of gene
331
therapy.
332 333
Grading can be performed rapidly in clinic whereas quantitative segmentation requires
334
special training and takes approximately 20 minutes per patient. Furthermore, grading can
335
help clinicians make appropriate decisions regarding management and investigation. For
336
example, if VA is poorer than expected according to grading, there should be raised suspicion
337
of other pathology limiting the VA. This may include other retinal pathology such as retinal
338
dystrophy, cortical/neurological disorders, amblyopia, conditions affecting the anterior
339
segment or sub-optimally corrected refractive errors. Similarly, if a patient has poor vision
340
consistent with a high degree of foveal hypoplasia, it is likely that the limiting factor for poor
341
VA is accounted at the retinal level.
342 343
Grading versus preferential looking
344
Preferential looking was a poor predictor of future VA, tending to underestimate visual
345
potential in nystagmus. Constant eye movement may increase difficulties of assessing
346
whether the child has correctly identified test cards.17 Suboptimal refraction at Examination 1
347
may have contributed to the poor correlation between preferential looking and chart VA.
348
Mean chart VA predicted by preferential looking in our cohort was 1.0 logMAR, better than a
349
previously published figure in another young cohort with infantile nystagmus of mean age 43
350
months (1.7 logMAR), but still poor.25 Moreover, the success rate in preferential looking was
351
poor (68.1%) compared to HH-OCT (90.0%). Dubowitz et al26 achieved a similar success
352
rate of 70% (n=96) for preferential looking in children with retinopathy of prematurity, also
353
associated with foveal hypoplasia, of a similar age to our study. In our study, preferential
354
looking testing correctly predicted future VA within 3 lines in only 38.8% compared to
355
96.3% for HH-OCT.
356 357
Can the fovea be graded from birth?
358
Our grading system involves identifying the presence or absence of intact ISe, foveal pit, OS
359
lengthening and ONL widening. Histological and OCT studies have demonstrated that all of
360
these landmarks can be identified from birth except OS elongation, which continues up to 5
361
months postnatally.6,27 Hence, it is possible to determine all grades apart from Grade 2 and
362
Grade 3 from birth, as an infant may be inappropriately assigned Grade 3 before OS
363
elongation has occurred. In this study, no patient under 5 months with Grade 2 or 3 foveal
364
hypoplasia was identified. However, we successfully obtained scans from patients aged 1
365
month and 3 months with Grade 4 and atypical foveal hypoplasia, respectively. Longitudinal
366
OCT scans revealed that all grades remained the same until the end of the study period, hence
367
adding age into the regression model would not impact the correlation between grading and
368
future VA.
369 370
Study strengths and limitations
371
To our knowledge, this is the first longitudinal cohort study using HH-OCT to predict future
372
vision in infantile nystagmus. This helps to reassure and/or enable patients and families to
373
optimise the development and educational attainment of the child during this crucial age, as
374
well as helping clinicians in their decision-making process for investigation and management.
375
A powered cohort of infants and young children has been achieved with adequate follow up
376
until the child could participate with chart VA, approaching or coinciding with
377
commencement of primary school education. Our grading system demonstrated an inter-
378
grader coefficient of 0.96, suggesting it is robust. Our grading system shows lower prediction
379
of VA than previously found in older patients.10 This is likely due to less cooperation with
380
logMAR VA testing and an immature visual system.23 Nystagmus characteristics and head
381
posture may influence VA, however, even without taking these factors into account, we
382
found very good correlation between foveal structure and later VA. In the future, a
383
multivariate model including foveal structure and nystagmus could be calculated to
384
investigate whether VA prediction could be refined.
385 386
A limitation of our study is that we are currently only able to predict VA in childhood rather
387
than adulthood due to the recent availability HH-OCT. However, it is still of great value to
388
predict an infant’s VA at the time they commence primary education. It is likely that VA will
389
continue to improve based on adult data.10 Another limitation is that only three aetiologies of
390
foveal hypoplasia were represented within this cohort; the grading system was not applied to
391
other conditions associated with foveal hypoplasia such as PAX-6 mutation28, retinopathy of
392
prematurity29, nanophthalmos30 and other photoreceptor dystrophies. There were only two
393
eyes from one patient that fulfilled the criteria for Grade 2, therefore, median VA predicted
394
from this single patient (0.60) cannot be generalized. With respect to image acquisition, if
395
three scans per eye were unsuccessful, patients could not be included. However, most eyes
396
(90%) were successfully scanned.
397 398 399
Author Contributions
400
SRR: Concept, literature search, figures, study design, data collection, data analysis, data
401
interpretation, writing.
402
MGT: Concept, literature search, figures, study design, data analysis, data interpretation,
403
writing, critical revision.
404
RP: Data collection, data interpretation, critical revision.
405
CB: Study design, data analysis, data interpretation, writing, critical revision.
406
HL: Literature search, data collection, data interpretation, writing, critical revision.
407
FAP: Figures, study design, data analysis, data interpretation, writing, critical revision.
408
IG: Concept, study design, data collection, data interpretation, writing, critical revision,
409
overall supervision.
410 411
Acknowledgements
412
The authors would like to thank vision scientists Dr Rebecca McLean and Dr Zhanhan Tu,
413
research orthoptists Helen Kuht and Michael Hisaund, and research optometrist Sonal Shah,
414
for their support in data collection for this study. The authors would like to thank all the
415
patients and families who took part in this study.
416 417
SRR’s post is funded by a National Institute for Health Research (NIHR) Academic Clinical
418
Fellowship. MGT’s and HL’s posts are funded by National Institute for Health Research
419
(NIHR) Academic Clinical Lectureships. CB’s post is part funded/supported by the National
420
Institute for Health Research (NIHR) Biomedical Research Centre based at Guy's and St
421
Thomas' NHS Foundation Trust and King's College London. The views expressed are those
422
of the authors and not necessarily those of the NHS, the NIHR or the Department of Health
423
Figure 3 is reprinted from Ophthalmology, 118(8), Thomas MG, Kumar A, Mohammad S,
424
Proudlock FA, Engle EC, Andrews C, Chan WM, Thomas S, Gottlob I. Structural grading of
425
foveal hypoplasia using spectral-domain optical coherence tomography a predictor of visual
426
acuity? 1653-1660, Copyright (2011), with permission from Elsevier.
427
428
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Figure Legends
516 517 518 519 520 521 522 523 524 525 526 527 528 529
Figure 1: The Leicester Grading System for Foveal Hypoplasia. Schematic demonstrating the features of a normal fovea detectable using optical coherence tomography (OCT), followed by the features of typical and atypical grades of foveal hypoplasia. The normal fovea features outward displacement, termed “extrusion”, of the plexiform layers. All grades of foveal hypoplasia feature continuation of the plexiform layers. Grade 1a foveal hypoplasia is associated with a nearly normal pit resembling a 'v' shape, OS lengthening and ONL widening relative to the parafoveal OS and ONL lengths, respectively. Grade 1b foveal hypoplasia is associated with a shallow indent, OS lengthening and ONL widening relative to the parafoveal OS and ONL lengths, respectively In Grade 2 foveal hypoplasia, all features of Grade 1 are present except there is no pit. Grade 3 foveal hypoplasia represents all features of Grade 2 except there is no lengthening of the OS segment. Grade 4 foveal hypoplasia represents grade 3 except there is no ONL widening at the fovea (termed fovea plana). Atypical foveal hypoplasia is characterised by a shallow foveal pit and disruption of the inner segment ellipsoid (ISe) band forming a hyporeflective zone. ILM = internal limiting
530 531 532 533 534 535
membrane; RNFL = retinal nerve fibre layer; GCL = ganglion cell layer; IPL = inner plexiform layer; INL = inner nuclear layer; OPL = outer plexiform layer; ONL = outer nuclear layer; ELM = external limiting membrane; ISe = inner segment ellipsoid; OS = outer segment; RPE = retinal pigment epithelium. Reprinted and adapted from Ophthalmology, 118(8), Thomas MG et al, 1653-1660, Copyright (2011), with permission from Elsevier.
536 537
Figure 2: Algorithm for Leicester Grading Scheme for Foveal Hypoplasia. Key: ISe = inner segment ellipsoid; OS = outer segment; ONL = outer nuclear layer.
538 539 540 541 542 543
Figure 3: Parameters for quantitative segmentation analysis. 1A: central foveal B-scan; 1B: En face fundal view. Three metrics were included in the segmentation analysis: (1) outer segment (OS) length: distance between Point I (cone outer segment tips: COST) to Point II (OS); (2) photoreceptor (PR) length: distance between Point I to Point III (outer nuclear layer: ONL) (3) Foveal Developmental Index (FDI): ratio of distance between Point I to Point III divided by distance between point I to point IV (foveal pit).
544
Figure 4: Examples of OCT scans for each grade of foveal hypoplasia.
545
Figure 5: Breakdown of grades by condition
546 547 548
Figure 6: Box and whisker plot to show typical grade of foveal hypoplasia in Examination 1 versus VA in Examination 2. VA = visual acuity, FH = foveal hypoplasia, M = median; IQR = interquartile range.
Variable n Mean (range; S.D.) Number of eyes (patients) 81 (42) Albinism 38 (19) IIN 31 (17) Achromatopsia 12 (6) Males 26 Females 16 Age at Examination 1 in months 19.8 (0.9-33.4; 9.4) Age at Examination 2 in months 63.9 (44.7-88.8; 11.6) Follow-up in months 44.1 (18.4-63.2; 12.0) Table 1: Baseline characteristics of cohort. Key: S.D. = standard deviation; IIN = idiopathic infantile nystagmus.
Handheld optical coherence tomography can predict future vision in infantile nystagmus. The Leicester Grading System for Foveal Hypoplasia provides better prediction of future vision than preferential looking – the current gold standard.