Abstract
BackgroundRetinopathy of prematurity (ROP) is a blinding morbidity of preterm infants. Our current screening criteria have remained unchanged since their inception and lack the ability to identify those at greatest risk.ObjectivesWe sought to comprehensively analyze numerous proposed maternal, infant, and environmental ROP risk variables in a robustly phenotyped population using logistic regression to determine the most predictive model for ROP development and severity. We further sought to determine the statistical interaction between significant ROP risk variables, which has not previously been done in the field of ROP. We hypothesize that our comprehensive analysis will allow for better identification of risk variables that independently correlate with ROP disease. Going forward, this may allow for improved infant risk stratification along a time continuum from prenatal to postnatal development, making prevention more feasible.MethodsWe performed a retrospective cohort analysis of preterm infants referred for ROP screening in one neonatal intensive care unit from 2010–2015. The primary outcome measure was presence of ROP. Secondary outcome measures were ROP requiring treatment and severe ROP not clearly meeting current treatment criteria. Univariate, stepwise regression and statistical interaction analyses of 57 proposed ROP risk variables was performed to identify variables which were significantly associated with each outcome measure.ResultsWe identified 457 infants meeting our inclusion criteria. Within this cohort, numerous factors showed a significant individual association with our ROP outcome measures; however, stepwise regression analysis found the most predictive model for overall ROP risk included estimated gestational age, birth weight, the need for any surgery, and maternal magnesium prophylaxis. The corresponding Area Under the Curve (AUC) for this model was 0.8641, while the traditional model of gestational age and birth weight predicted ROP disease less well with an AUC of 0.8489. Development of severe ROP was best predicted by estimated gestational age (week), the need for any surgery and increased probability of death or moderate-severe BPD at 7 days. Finally, the model most predictive for type 1 ROP included estimated gestational age (week) and the presence of severe chronic lung disease. No significant statistical interaction was found between variables.ConclusionsOur work is unique as we report comprehensive analysis of the greatest number of proposed ROP risk variables to date in a robustly phenotyped population. We describe novel risk models for our ROP outcome measures and demonstrate independence of these variables using statistical modeling not previously applied to ROP. This may better allow for individual infant risk stratification and importantly mitigation of future risk.
Highlights
Retinopathy of prematurity (ROP) is a blinding morbidity affecting preterm infants
Development of severe ROP was best predicted by estimated gestational age, the need for any surgery and increased probability of death or moderate-severe BPD at 7 days
Our work is unique as we report comprehensive analysis of the greatest number of proposed ROP risk variables to date in a robustly phenotyped population
Summary
Retinopathy of prematurity (ROP) is a blinding morbidity affecting preterm infants. It is a significant clinical problem and currently represents the leading preventable cause of childhood blindness worldwide. [1], [6], [7] Most data indicate an increasing incidence of ROP disease as industrialized counteries report increased incidence by approximately 10 fold since the 1990’s.[8] ROP pathology is characterized by the presence of avascular retina and subsequent aberrant retinal neovascularization.[9] In the most severe stages of the disease retinal traction and detachment develop leading to permenant blindness.[9], [10] Recent work demonstrates the rates of severe, treatment-worthy, ROP rose from 1.7 to 14.8 per 1000 preterm infants between the years 1990 and 2011. [11] Since that time, we have further clarified epidemiologic risk factors, such as early gestational age and low birth weight, which predispose to the development of ROP. Our current screening criteria have remained unchanged since their inception and lack the ability to identify those at greatest risk
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