Myopia Outcome Study of Atropine in Children (MOSAIC): an investigator-led, double-masked, placebo-controlled, randomised clinical trial protocol

Management, design and registration

The management team and relevant structures established to oversee the implementation of MOSAIC, including the data safety monitoring committee (DSMC), trial steering committee (TSC) and scientific advisory committee (SAC), are outlined in Figure 1.

Figure 1. MOSAIC support and oversight structures.

MOSAIC is an investigator-led, double-masked, placebo-controlled, randomised clinical trial (RCT) designed to assess the efficacy, safety, acceptability and mechanisms of action of 0.01% atropine for controlling myopia in children. The trial protocol, developed according to Standard Protocol Items Recommendations for Interventional Trials (SPIRIT) guidelines, is registered on the current controlled trials register with the International Standard Randomised Controlled Trials Number 36732601 (ISRCTN36732601) on 4 October 2017 and also on the EudraCTdatabase (2016-003340-37) on the 3 July 2018. The trial is a single centre study conducted at the Centre for Eye Research Ireland (CERI) at Technological University Dublin, Ireland. The progress of participants through the phases of MOSAIC are shown in Figure 2 in the consolidated standards of reporting trials (CONSORT) diagram⁴¹. SPIRIT and CONSORT reporting checklists for MOSAIC are deposited in TU Dublin’s ARROW repository (see Reporting guidelines^42,43).

Figure 2. Flow of participants through the MOSAIC clinical trial.

Patient and public involvement

The MOSAIC protocol and clinical trial documentation were designed to maximise the benefits of patient and public involvement (PPI) throughout the clinical trial⁴⁴. All MOSAIC clinical trial documentation, including consent/assent forms, participant information leaflets and parental questionnaires, were submitted through Fighting Blindness for PPI review. The collated feedback was analysed, and the relevant clinical trial documentation was amended to reflect PPI recommendations.

Research question

To address whether it is clinically justifiable and feasible to offer atropine eye drops to limit the progression of myopia in a European population. This will be achieved by determining the efficacy, safety and acceptability of 0.01% atropine treatment.

Primary outcome measure

Change in spherical equivalent refraction at 24 months measured by cycloplegic auto-refraction.

Secondary outcome measures

Drug manufacture and supply

Unpreserved atropine 0.01% is supplied by the pharmaceutical company Nevakar (Nevakar, Inc. 1019 US Highway 202-206, Building K, NJ Center of Excellence, Bridgewater, NJ 08807, USA) for the duration of the clinical trial. Nevakar’s contracted manufacturer, Excelvision, has a current EU GMPD Certificate and is authorised to manufacture atropine 0.01% and placebo eye drops on behalf of Nevakar, in accordance with the requirements of the EU Guide to Good Manufacturing Practice. The eye drops are manufactured at a site authorised for manufacture of aseptically prepared small volume liquids. Investigational product labelling, packaging and QP release to the trial centre is provided by Xerimis.

Trial intervention

The intervention for the trial is 0.01% w/v atropine eyedrops, an anti-cholinergic agent selective for muscarinic receptors. Unpreserved 0.01% w/v atropine solution is supplied to trial participants as single dose ampoules for daily use. The placebo solution, identical to the atropine eye drop formulation without the active ingredient (atropine), is also supplied to trial participants as single dose ampoules for daily use.

During Phase 1 of MOSAIC, participants instil eye drops (atropine or placebo, per their randomisation status) once nightly into both eyes from the baseline visit to month 24. This is followed by re-randomisation in Phase 2, into continued 0.01% atropine, and washout, at 1:1 ratio for those participants initially randomised to the intervention arm. Participants are monitored in this washout period to examine any potential rebound effects on termination of treatment. All participants initially assigned to the placebo group then crossover to the intervention arm of the study, and for the period from month 24 to 36, instil 0.01% atropine eye drops once nightly. An additional monitoring and re-treatment phase is planned (Phase 3), the design of which will be informed by (i) the outcomes of Phase 1, (ii) consultation with our TSC and SAC, (iii) regulatory approval and (iv) funding availability. To ensure the study population is representative of the Irish population, recruitment is capped by ethnic background in accordance with ethnic classifications in the 2016 Irish Census⁴⁵.

Randomisation

The Mater Misericordiae University Hospital (MMUH) Clinical Research Centre (CRC) will carry out the stratified randomisation procedure. Participants are allocated to one of the two intervention groups according to a 2:1 treatment to control ratio to maximise recruitment success. Allocation is carried out using block randomisation and stratified according to baseline refractive error (<-3D or ≥ -3D). A randomisation list for each strata will be prepared by an independent statistician and will be stored within the CRC.

A key advantage of block randomisation is that treatment groups tend to be uniformly distributed by key outcome-related characteristics and the 2:1 assignment of participants remains similar at all times⁴⁶, even if the full quota of participants are not recruited into the clinical trial. Participants are randomised to a study number unrelated to treatment assignment. Once officially enrolled on the trial, participants receive a unique study identification number at the baseline visit that is pre-randomised to one of the intervention arms.

Masking

Study treatment assignment is double masked during the first 24 months. Atropine and placebo eye drops are packaged identically before delivery of the investigational product to the trial centre, so that the investigator and participants are unable to identify the contents. Labels on the box containing the ampoules have a batch number (that does not indicate to the investigator whether it is atropine or the placebo), study reference number, participant ID, trial sponsor’s name and contact number, investigator name, site address, expiration date of the eye drop, storage instructions, and a statement informing the participant that the drop is for clinical trial use only and is not to be ingested.

No interim analyses are planned. The randomisation code is only broken after all participants have completed the 24-month visit and all data have been subjected to a “Blind Review”. This pre-analysis review, masked to treatment, covers, for example, decisions concerning the exclusion of participants or data from the analysis sets, the checking of possible transformations and definitions of outliers, the addition to the model of important covariates identified in other recent research, and other factors that might be of relevant to the data analysis. Decisions made at this time are described in a report and distinguished from those made after the study statistician has had access to the treatment codes when final decisions can be adequately taken, as masked decisions generally introduce less potential for bias. Only the DSMC has access to the randomisation list to determine allocation to atropine or placebo within the appropriate strata, as well as to facilitate interim trial safety analyses. To reduce performance and ascertainment bias after randomisation, measures are taken as far as is practical to maintain investigator masking.

Storage and disposal of study treatment

The trial intervention drug and placebo eye drops are securely stored at the clinical trial site (CERI). Only the study investigators and the senior research assistant have access to the eye drops. Study medication, monitored constantly with Bluetooth temperature sensors, is stored at room temperature of 20°C to 25°C, with minimal excursions permitted. A room temperature log is maintained at the study site. Subjects and their parent/guardian are also instructed to store the eyedrops at room temperature with no exposure to extreme temperatures (such as refrigeration).

Parents are provided with a study treatment kit set at each visit. Each kit contains a 6-month supply of eye drops consisting of 200-unit dose ampoules. Each 6-month treatment kit consists of two 3-month boxes and each box consists of 20 aluminium foil pouches. Each foil pouch consists of 5-unit dose ampoules. Parents are instructed to open one ampoule per day and administer the eye drop into both eyes of the participant once nightly. After instillation of the eye drop, the open ampoule and the remaining contents should be placed in the provided receptacle that is returned to the study centre for accounting and proper disposal. All returned ampoules are deposited in appropriately labelled hazardous waste containers and disposed of in keeping with chemical waste management policies and procedures. Parents are provided with an information sheet on correct eyedrop use. This includes an instruction to start a new box each month irrespective of how many ampoules remain in the previous box. A contact phone number is also provided in the participant’s study information pack as well as the product label, in case the parent has any queries.

Compliance

The study medication is provided to participants at each study visit during their treatment period. Parents sign to confirm they have received the eye drops once dispensed and are asked to bring trial boxes containing their remaining unused ampoules on all visits after the baseline visit. Parents are provided with a list of suggestions to encourage adherence, and are asked to create a nightly calendar reminder, as well as a calendar log of date and time of eye drop instillation on their phone. Regular phone and text message contact is maintained with parents throughout the study duration. Participants and their parents are questioned regarding adherence at each visit and are constantly reminded about the importance of adhering to the treatment protocol.

Participants are encouraged to attend all study visits. Follow up visits are scheduled at 6, 12, 18, 24, 30 and 36 months after the baseline randomisation visit, +/- 2 weeks. Thus, clinic visits are scheduled from up to 2 weeks before the check-up date is due. If the participant does not attend the visit, a new visit is rescheduled within 4 weeks in the first 12 months of the trial and within 6 weeks thereafter. Participants are informed that they may be removed from the trial if they fail to attend within the defined time period. If a participant is dropped from the trial for this, or any other reason, arrangements are made for collecting used and unused ampoules.

The study is to be conducted using an intention-to-treat basis. The level of compliance with eyedrop use is quantified by questionnaire (self-report), the eyedrop use calendar log and quantification of returned ampoules (extended data⁴⁷). There is no minimum eyedrop insertion compliance criterion that would cause removal from the trial, but compliance is controlled for in statistical analyses and used as a measure of acceptability of the treatment in our secondary objectives.

Any suspected non-compliance or improper eye drop use results in encouragement to parents and children as well as offering an electronic daily reminder system for families who have not instilled the drop as instructed. Evidence of over use is also discussed with participants and they are re-instructed on proper use and compliance with the once-nightly protocol.

Sample size calculation

Based on available atropine trial data from Singapore¹⁷, along with Pirenzepine trials data from the USA⁴⁸, myopia progression in the atropine treatment group is postulated to be -0.25D per annum, with a standard deviation of ±0.3D at two time points (12 months and 24 months). Power analysis of these data resulted in a projected effect difference of 50% between the intervention versus the placebo control group on myopia progression rate. The primary outcome for this study is the progression of myopia over the 2-year trial duration sampled every 6 months. The analyses of progression of myopia will be a 2x5 repeated measures mixed analysis of variance (ANOVA) with the factors of group (placebo and intervention) and time (0 months, 6 months, 12months, 18 months, 24 months). Conducting a power analysis for the repeated measures (RM) ANOVA, anticipating a conservative effect size of 0.3, an alpha of 5%, a power of 95%, with two groups, five repeated measurements and a correlation among the repeated measures of 0.9 resulted in a sample size of 136 with a critical F value of 3.91179. Allowing for a high potential attrition rate (based on the fact that no trial has been conducted to completion in a European population, in whom the acceptability and motivation for long term use remain unknown), a total of 250 children will be recruited. Of these, 167 children will be randomised to the intervention group and 83 to the placebo group.

The study is powered for the primary outcome. However, for secondary measures or subgroup analyses, the MOSAIC team will lead a planned meta-analysis of these data combined with data from ongoing trials in the UK (CHAMP-UK: ISRCTN99883695) and Australia (ATOM-Australia: ACTRN12617000598381). Such a meta-analysis will provide additional statistical power for subgroup and secondary analyses and allow a more definitive exploration of the mechanistic components of atropine’s influence on myopia progression.

Eligibility criteria

Only participants between the ages of six to 16 years inclusive are eligible to participate in the trial. Additional inclusion criteria comprise:

Study recruitment

Participants are recruited into this trial through a variety of channels, each of which were established prior to commencement of the pre-trial phase and are continued throughout the study until recruitment is complete. These avenues included:

Informed consent

In compliance with the National Consent Policy of Ireland (2013 -16 Document reference QPSD-D-026-1), parental consent and child assent (dependent on child age and maturity) is required before any trial-related procedures are undertaken. Study investigators ensure that parents and children understand the trial completely including all information on the participant information leaflet. All study information is available in a child-accessible format. Participants are informed if they are eligible at the baseline visit. All participants are given the opportunity to ask any questions about the study prior to parental consent and child assent being obtained and may withdraw consent at any time. Participant consent is collected in hardcopy and a copy is provided to the participants (extended data⁴⁷).

Study visits

At the baseline visit, each participants’ eligibility is confirmed, the ability of the parent to instil and participants’ ability to tolerate the instillation of an artificial tear eye drop is assessed. The participant or parent/guardian is given the allotted atropine or placebo eye drops to take home and instil one drop every night into both eyes for the trial duration. After the baseline visit, study visits are conducted at 6, 12, 18, 24, 30 and 36 months. Each visit takes approximately 90 minutes. Table 1 summarises the clinical procedures conducted at each visit.

Description of study assessments

Demographics and inclusion/exclusion criteria. At the initial screening visit all parents are required to complete a demographic and health questionnaire on behalf of their child (extended data⁴⁷). Demographic information includes age, sex and race. Iris colour is documented⁵⁰. Medical and ocular history, including the participant’s GP and optometrist name and address, is also collected. To participate in the trial, participants must satisfy all the inclusion and exclusion criteria outlined.

Medical and surgical history. A detailed medical and surgical case history is undertaken in order to ensure that all trial participants are in good general and ocular health and comply with the study inclusion and exclusion criteria, including any history of ocular surgery, amblyopia and patching as well as detailing any allergies to atropine sulphate, hydroxypropyl methylcellulose, proxymetacaine hydrochloride or cyclopentolate hydrochloride.

Heart Rate is measured at baseline and every 6 months thereafter until the final study visit. Heart rate is measured with a heart rate monitor after approximately 3 minutes of rest in the seated position. The participant is excluded if heart rate is persistently (for more than 10 minutes) > 120 beats per minute at any study visit.

Females of childbearing potential are required to provide confirmation of last menstrual period and a negative pregnancy test. Sexually active participants are advised to use an acceptable, effective form of contraception until cessation of treatment.

Pre-cycloplegia measures

Visual acuity. Participants’ corrected visual acuity is measured using a randomised letterset of the MultiQuity (MiQ 720) computerised logMAR chart.

Accommodation and convergence. Amplitude of accommodation (AoA) and near point of convergence (NPC) are measured non-invasively with a RAF (Royal Air Force) rule using the subjective push-up technique. Measurements are taken both monocularly and binocularly for AoA and binocularly for NPC. Lag of accommodation to a 40cm (2.5D) target is measured using the Grand Seiko WAM 5500 open field autorefractor. Accommodative facility is measured using ±2.00D flippers at near.

Binocular Vision Assessment. With subjects best-corrected distance spectacle correction in place, the cover-uncover test and alternating cover test are used to detect the presence of strabismus or phoria. If movement is present, the direction is noted and the extent of the phoria is measured using prisms. Strabismus is an exclusion criterion. The TNO stereoacuity testing chart is used to evaluate stereopsis.

Near VA. Near visual acuity is documented to monitor any changes in visual performance. Near visual acuity is determined as the smallest character size that can be read at 25cms using best-corrected distance spectacle correction.

Infrared pupillometry. The Topcon ALADDIN optical biometer is used to measure scotopic and photopic pupil size and pupil reactivity for each participant at each visit. Atropine causes pupillary dilation, particularly at higher concentrations used in previous trials. This measure is taken pre- and post-cycloplegia and is used to determine the physiological impact of 0.01% atropine on pupillary function as well as to confirm cycloplegia.

Tonometry. An Icare tonometer is used to calculate the intraocular pressure in both eyes at each study visit pre- and post-cycloplegia. This measure is taken at all visits as a safety precaution for participants.

Slit lamp assessment. The slit lamp is used to perform a complete examination of the external eye as a safety precaution throughout the trial in case of sign of allergy or external abnormality. This includes examination of the cornea, conjunctiva, iris, pupil, lids and adnexa, relative to the Brien Holden Vision Institute grading scale where appropiate⁵¹. Results are recorded at each visit study visit, including visits during the washout period. As the study medication contains phosphates, inclusion in the study requires a healthy cornea with no evidence of corneal damage or scarring. Cases of corneal calcification have been reported very rarely in association with the use of phosphate-containing eye drops in some patients with significantly damaged corneas^52,53. The anterior chamber angle of the eye is checked during slit lamp routine before insertion of cycloplegic eye drops. Cycloplegic procedure. One drop of 0.5% topical proxymetacaine hydrochloride is instilled into each eye to achieve topical anaesthesia of the cornea and conjunctiva. This is followed by instillation of one drop of 1.0% cyclopentolate hydrochloride in each eye. A second drop of 1.0% cyclopentolate is instilled in each eye for participants with iris classification green with brown iris ring (v), peripheral green central brown (vi), brown with some peripheral green (vii), brown (viii), and dark brown (ix)³. 15 minutes post cyclopentolate insertion, the subject is examined to ensure both pupils are dilating and amplitude of accommodation is reducing compared to their pre cycloplegia assessment. If the onset of cycloplegia is not apparent at 15 minutes, another drop of cyclopentolate hydrochloride 1% is instilled. Autorefraction is carried out 30 minutes after instillation of the final cycloplegic eye drop.

Post cycloplegia measures

Objective refraction. Refractive error and peripheral refractive error are measured by cycloplegic auto-refraction at the baseline visit using the Grand Seiko WAM 5500 open field autorefractor. Change in spherical equivalent refraction and peripheral refraction (30° nasal and temporal) are measured by cycloplegic auto-refraction at all subsequent visits 30 minutes post cycloplegic drop insertion.

Choroidal thickness. Swept source optical coherence tomography (OCT) provides a significant improvement over conventional OCT, in particular, there is better penetration of the deeper layers of the eye including the choroid. The 7×7 macula scan on the Topcon DRI OCT Triton, facilitates automated choroidal thickness mapping at each study visit.

Retinal vasculature. The 7×7 macula and angiography scans on the Topcon DRI OCT Triton allows imaging of the central and peripheral retina for detailed analysis of change in retinal vessels in relation to ocular growth and also to examine and monitor retinal health throughout and after the clinical trial.

Ocular biometry. The Topcon ALADDIN optical biometer is used to determine the axial length, anterior chamber depth, pupil size, keratometry, dynamic pupil measurements, white to white and lens thickness at the baseline visit. Changes in dynamic pupil measurements, ocular axial length, anterior chamber depth and/or lens thickness are documented by repeat measurements at all subsequent visits.

Adverse event assessments. A detailed adverse events assessment will be conducted at each visit, which includes specific evaluation as to the experience of known adverse side effects of topical atropine which can include:

The detailed examination carried out at each study visit is used to determine any symptomatic or asymptomatic adverse responses to atropine use. A detailed case history is also used to determine the presence of adverse events attributable to the therapeutic intervention. Occurrence of adverse events are recorded on study-specific adverse report forms. The DSMC review all adverse events and safety data on a quarterly basis, or more frequently if required by any emerging safety concerns during the study.

In the unlikely scenario of a serious adverse event, our team includes a paediatric ophthalmic surgeon, who will make arrangements for ophthalmic service provision with ophthalmology and medical colleagues, as appropriate, to manage ophthalmic adverse events/effects as may be required. Non-ophthalmic adverse events are managed through appropriate public health channels including the family physician, emergency services, accident and emergency unit or other hospital services as may be required. In the event an unexpected and serious adverse side-effect is confirmed to be directly attributable to the investigational product, the DSMC, TSC and Study Sponsor will liaise with the research ethics committee (REC) and Health products Regulatory Authority (HPRA) to determine the appropriate course of action.

Questionnaires

Lifestyle questionnaire. At each study visit parents are asked to complete a lifestyle questionnaire to quantify lifestyle habits including outdoors exposure, sports participation, near work including use of digital technology (see extended data⁴⁷)⁴⁹.

Quality of Life Impact questionnaire. The impact or burden of atropine treatment on the child and the family is assessed using a validated and atropine specific quality of life questionnaire, adapted from the Parent and New Child Amblyopia Treatment Index (ATI) questionnaires used with higher atropine concentrations^49,54.

Statistical analysis

Primary efficacy endpoint. The primary outcome, in line with previous studies^17,55, will be myopia progression amongst study groups, primarily the difference in change in myopic refractive error (in dioptres) from cycloplegic autorefraction from baseline to month 24. The analysis will rely on parametric analysis of variance (ANOVA), to control for the effects of the other continuous variables that are not of primary interest. The treatment difference in response rate and its 95% confidence interval (CI) will be provided.

Secondary efficacy endpoints. Univariate analysis will be performed to evaluate the group effect on mean change in axial length over the 2-year period. Multivariate regression analyses will be used to assess the association between change in axial length and progression of myopia while adjusting for treatment effects. The difference in myopic refractive error from cycloplegic autorefraction and axial length between the treatment groups from baseline to visit 6 will be analysed using RM ANOVA.

The percentage of participants in each treatment group that progress <0.25D, 0.25D≤0.75D and >0.75D from baseline to visit 6 will be displayed in cross tabulations.

A post hoc analysis, with Bonferroni correction to account for any type 1 errors, will be carried out to determine at what time-point over the 24-month treatment period atropine was most effective.

The distribution of scores from the quality of life questionnaire is calculated at each visit for all treatment groups. At the 24-month visit the scores for each visit will be calculated and analysis of variance (ANOVA) and suitable post hoc testing will be used to determine any statistically significant differences between the responses at each visit as well as between groups. Safety and tolerability data will be presented in tables of descriptive statistics and frequency distribution. RM ANOVA will be used to detect changes in anterior chamber depth, crystalline lens thickness, retinal nerve fibre layer thickness and choroidal thickness between treatment groups. A statistical significance level of p < 0.05 is adopted throughout the analysis.

Adjustment for baseline characteristics will be performed by analysis of covariance (ANCOVA). Several comparisons will ensue based on further stratification by a) sex; b) age; c) ethnicity; d) baseline refractive error and e) baseline axial length, using data pooled from both eyes, assuming the sample size is sufficient. The primary statistical analysis will be based on the intention-to-treat principle, but supported by additional per-protocol analyses.

Trial steering and oversight

Three committees have been established to provide independent oversight and steer the strategic direction of the trial.

Data Safety Monitoring Committee

A three-member independent DSMC has been established to oversee the safety of trial participants. The establishment of the DSMC is justified given the paediatric population under investigation and the need to detect any potential harm to participants as early as possible, even though the anticipated potential for harm in this trial is very low. Safety monitoring will be the major task for the appointed DSMC. All members of the DSMC are completely independent of the trial and have no possible financial or other potential conflict of interest in the study. The DSMC is composed of a statistician with expertise in biomedical research, a paediatric ophthalmologist and an ophthalmologist with medical and surgical retina expertise (chairperson).

Trial Steering and Scientific Advisory Committees

In addition to the DSMC, a TSC and SAC has been appointed to contribute to the design and conduct of the trial. The TSC includes individuals with expertise and involvement in other atropine trials for myopia control. The SAC includes international scientists with expertise in the exploration of efficacy, safety and mechanistic aspects of myopia and its control. The trial investigators are represented on the Steering Committee by JL and IF. Together the co-PIs maintain responsibility for all study design, implementation and oversight across all facets of the study. The TSC hold teleconference meetings as required. Meetings address trial strategy, trial protocol and matters arising from the various work packages including staff and other resource concerns, data collection and all operational issues as they arise. The scientific and clinical members of the steering committee have the responsibility of informing the clinical protocol required to effectively and safely implement the trial, including determination of patient eligibility, examination protocol, data capture and recording protocol, inter-professional communication protocol, and decision review protocol. Members of the TSC and SAC are identified in Figure 1.

Regulatory approval

Regulatory approval for MOSAIC was granted by the Health Products Regulatory Authority (HPRA), reference CT0900/622/001. Clinical trials in Ireland are currently governed by the European Communities (Clinical Trials on Medicinal Products for Human Use) Regulations, 2004, SI No 190 of 2004, transposed into Irish law the provisions of Council Directive 2001/20/EC.

Ethics

Ethical approval for the study was granted by the Research Ethics Committee (REC) at the MMUH, Dublin, Ireland (reference 1/478/81), and by the REC at TU Dublin, Ireland (reference 16-45). MOSAIC adheres to the tenets of the Declaration of Helsinki and follows the full code of ethics with respect to participant recruitment, participant testing and General Data Protection Regulations (GDPR, effective May 2018).

As required under the EU Directive on Clinical Trials (European Union - Directive 2001/20/EC), parental or guardian consent is obtained as required for clinical trials involving minors, who are defined in this case as persons under the age of 16 years. MOSAIC is carried out within the framework of Children First: National Guidance for the Protection and Welfare of Children (DCYA, 2011). Child assent is also obtained in recognition of the importance of the voice of the child in this type of research⁵⁶.

Dissemination of findings

Findings and underlying data from MOSAIC will be disseminated at appropriate conferences, through scientific publications and published in open access format on the TU Dublin ARROW repository. Findings will also be shared online through social media channels, blogs, and publications, as well as through print, broadcast and at stakeholder events.

Study status

Recruiting will being June 2019 and continue through to March 2020.

Underlying data

No data is associated with this article.

Extended data

ARROW @ TU Dublin: Myopia Outcome Study of Atropine in Children (MOSAIC): Design and Methodology. https://doi.org/10.21427/xyq9-ck53⁴⁷

Reporting guidelines

ARROW@TU Dublin: CONSORT checklist for ‘Myopia Outcome Study of Atropine in Children (MOSAIC): an investigator-led, double-masked, placebo-controlled, randomised clinical trial protocol’. https://doi.org/10.21427/3neg-gr77³⁵

ARROW@TU Dublin: SPIRIT checklist for ‘Myopia Outcome Study of Atropine in Children (MOSAIC): an investigator-led, double-masked, placebo-controlled, randomised clinical trial protocol’. https://doi.org/10.21427/2dbf-t103³⁶