Hypertensive disorders of pregnancy and the long-term risk of maternal retinal disease: a systematic review protocol

Review question

Are hypertensive disorders of pregnancy (preeclampsia, gestational hypertension) associated with an increased risk of maternal retinal disease or other ophthalmic disorders in later life?

PECO

Population

Women who have had at least one pregnancy

Exposures

Diagnosis of any HDP, such as preeclampsia (including eclampsia or haemolysis, elevated liver enzymes and low platelets syndrome, HELLP), gestational hypertension, or other. These can be defined either using established clinical criteria, hospital records, diagnostic codes, or self-reporting of a doctor diagnosis.

Comparison

Parous women who never had a corresponding HDP. For example, women who experienced preeclampsia in at least one pregnancy will be compared with parous women who never experienced preeclampsia.

Outcome

Primary outcome: We will include maternal retinal disease (undifferentiated) diagnosed at least six months after a pregnancy complicated by HDP. Subtypes of maternal retinal disease will be explored separately where possible: hypertensive retinopathy, diabetic retinopathy, retinal detachment and/or tears, retinal vein occlusion, retinal artery occlusion, macular oedema and associated maculopathies. We will include any diagnoses based on medical reports, objective clinical codes, and clinical tests or self-reporting.

Secondary outcomes: The secondary outcome will be any maternal ophthalmic disease (undifferentiated). Subtypes of anterior and posterior ophthalmic disease will be explored separately where possible: choroidal disease, macular degeneration, cataract and other causes of visual impairment and/or loss.

Protocol and registration

This study protocol adheres to the guidelines in the Preferred Reporting Items for Systematic Reviews and Meta-Analysis Protocols (PRISMA-P) statement¹². This systematic review protocol was registered with the International Prospective Register of Systematic Reviews (PROSPERO) on 22 September 2024 with registration number CRD42024589508 If any important protocol amendments arise, these will be made promptly to the PROSPERO record.

Search strategy

Two reviewers (PB, CC) will systematically search the literature in the following electronic databases: PubMed, EMBASE, Web of Science, and the Cochrane Library, from inception of the databases until 30 September 2024 (Table 1). A detailed search strategy has been compiled and these terms will be searched according to the principles of Boolean Logic (AND, OR, NOT). Supplementary searches of the grey literature will be conducted using keyword searches in the Bielefeld Academic Search Engine (BASE), Trip Database, and medRxiv. The reference lists of all included studies will be manually searched to find additional potentially eligible research as a supplement to the electronic database searches.

Criteria for considering studies for the review

Inclusion criteria

Exclusion criteria

Selection of studies for inclusion in the review

We will store all titles and abstracts from each database search in EndNote reference manager, and two review authors will independently review them. Full texts will be obtained to screen for eligibility in the systematic review if required. Pre-defined inclusion/exclusion criteria will be applied. Online translation software will be used to screen non-English articles for eligibility (e.g. Google translate) if necessary. If a situation arises whereby consensus on eligibility cannot be achieved, a third review author will be involved in the decision.

Data extraction and management

Data will be extracted from eligible studies using standardised data collection forms by two review authors independently, including the author and year of publication, study design, country and setting, definition of exposure and outcome used, sample size, follow-up time, confounders adjusted for (if any) as well as crude and adjusted effect estimates. Corresponding authors of published studies will be contacted, if required, to obtain further information relating to effect estimates. If any discrepancies arise, these will be resolved by a third reviewer.

Methodological quality appraisal of included studies

Two reviewers will independently assess the methodological quality of all included studies, using an adapted version of the validated Newcastle-Ottawa Quality Assessment Form. An adapted version of each form will be used depending on the study design, with eight distinct topics spanning selection of study groups; comparability of the groups; ascertainment of exposure/outcome of interest (total score ranges from 0 to 9). These topics will be addressed for all cross-sectional, case-control, and cohort studies. We will consider a total score 0 to 3 to be low quality, total score 4 to 6 to be moderate quality, total score 7 to 9 to be high quality. Discrepancies will be discussed between reviewers and where necessary, a third reviewer will be consulted.

Data synthesis, including assessment of heterogeneity

If the data allow, a pooled estimate of the relationship between HDP and retinal disease will be calculated in the meta-analysis. Both crude and adjusted measures of association will be presented, where adjustment is based on the definition outlined in each of the individual studies. Each study's effect estimates will be weighted accordingly by use of the inverse-variance method. Random-effects models will be used to combine the results of different studies.

For the potential cohort studies included in this review, we expect the incidence of maternal retinal or other ophthalmic disease to be relatively low (affecting <5% of participants), and thus we will apply the rare disease assumption that key measures of effect (odds ratios, risk ratios and, by extension, hazard ratios) may be considered as approximations of each other, and thus grouped together for analysis. However, if we identify studies with longer follow-up periods (and higher incidence of maternal retinal disease), this assumption will not be applied, and we will group analyses by effect measure.

A forest plot will be used to present the findings of any meta-analysis. Study heterogeneity will be explored based on χ² statistics and I² values. For the former, heterogeneity will be deemed present if the p-value < 0.1, and the latter will be used to quantify the extent of heterogeneity present.

If a meta-analysis includes a minimum of ten studies, a funnel plot will assess the potential issue of publication bias. Firstly, visual inspection will assess asymmetry (performed on RevMan v5.4). Subsequently, an Egger’s test may be used to test for significance wherein a p-value <0.05 is indicative of publication bias. To quantify the magnitude, and attempt to correct this potential publication bias, Duval and Tweedie’s trim and fill method will be used if necessary.

We will perform the following subgroup analyses where the data allow, using RevMan 5.4:

If other relevant subgroup analyses are identified throughout this review and meta-analysis, they will be clearly assigned to post-hoc analyses.

Presenting and reporting the results

A PRISMA flow diagram will be included to outline the step-by-step study selection process, and a rationale will be provided for excluding studies at full-text screening. The characteristics and quality assessment of all included studies will be presented in tables, and pooled estimates will be presented using forest plots. Where data is unsuitable to conduct meta-analysis, study findings will be narratively synthesized and presented in tabular format, and we will adhere to the Synthesis without meta-analysis (SWiM) reporting guideline¹³

Potential strengths and limitations of this study

This study will summarise and clarify existing knowledge on the associations between HDP and the risk of maternal retinal disease in the long term. Strengths of this study include the use of a comprehensive search strategy and adherence to international reporting guidelines. There will be up to three reviewers involved in screening studies for eligibility, and undertaking data extraction and quality appraisal. These measures will reduce any potential for individual reviewer-based bias in the systematic review.

We acknowledge that there will be some limitations with this review. The use of administrative hospital records may not accurately reflect the true prevalence of HDP or retinal disorders in a population, since some of these issues may be managed in primary care or community settings. Thus, we will include papers that describe HDP and ophthalmic disorders based on self-reported diagnosis, clinical measurement, or diagnostic coding. While this may allow us to provide a more comprehensive summary of the existing literature, it may also introduce heterogeneity to the results. We will consider overall findings in the context of any inherent clinical and methodological diversity between studies, and can do sensitivity analyses if appropriate.

The presence of confounding is a concern in any observational studies and may introduce further heterogeneity between studies. Potential confounders that may be associated with HDP and maternal retinal disease include maternal age, ethnicity, smoking, diabetes and other comorbidities. We will present crude and adjusted pooled odds ratios separately, where adjustment is initially based on the definition outlined in each identified study. Where possible, we will also present adjusted odds ratios which have been controlled for a minimal suite of key confounders (e.g. age, ethnicity, smoking, chronic hypertension, diabetes) to improve comparability of results and to reduce heterogeneity.

For specific exposure-outcome associations, there may not be enough studies to conduct meta-analysis. However, the use of international reporting guidelines will ensure that results are presented in a transparent, accurate, and complete manner. If meta-analysis is feasible, publication bias may remain a limitation. Where possible, funnel plots and statistical tests will be used to evaluate the presence of publication bias.