The effectiveness and characteristics of pregnancy yoga interventions: a systematic review protocol

Aim

The aim of this systematic review is twofold:

Eligibility criteria

The following criteria will be used to select studies for inclusion in the systematic review:

Information sources

A systematic literature search will be performed using the following databases: (EBSCO)Medline (1946-), CINAHL (1981-), PsycINFO (1990-), (Ovid)Embase (1966-), AMED (1985-), WHOLiS, Web of Science (1864-), ScieLo (2002-) and ASSIA (1970-). Reference lists from included studies and relevant reviews will be screened to ensure coverage of the literature. In addition, Google Scholar results for the last year of publication, will also be visually scanned for any additional material. No restrictions on date of study publication will be included in the search, and all articles available in English will be considered. The review will only include peer-reviewed published studies.

Search strategy

The search strategy was developed by the primary author (LC) and supported by a subject librarian with systematic review expertise (JEC), with input from all authors. Citation and bibliographic searches will be conducted on all included studies to identify additional relevant studies for inclusion. The search will be updated and rerun just before final analysis is conducted and further studies retrieved for inclusion. Extended data: Search Strategy contains sample search terms and a search strategy example. Conference proceedings, editorials, commentaries, and book chapters/book reviews will be excluded.

Study records

Literature search results will be exported to EndNote X9 and duplicate records deleted using the ‘remove duplicates’ function and by manually screening results for accuracy (LC and JEC)¹⁴. Titles and abstracts of identified articles will be imported to Covidence (JEC), a web-based software platform designed to support citation screening and collaboration among multiple authors¹⁵.

Selection process

Two reviewers (LC and DD) will independently screen all titles and abstracts of retrieved studies. Articles clearly not meeting the established inclusion/exclusion criteria will be excluded. If there is disagreement about inclusion, the abstract will be reviewed by a third author (PM) to determine suitability. Following this, two reviewers will independently screen the full text articles of abstracts identified to select the studies to be included (LC and DD). The reference lists of included studies will be scanned to identify any relevant additional studies. Both reviewers will independently screen the full text of these additional articles to determine inclusion/exclusion (LC and DD). Third-party arbitration (PM) will be available to resolve any inconsistencies in the selection of studies for inclusion/exclusion.

If necessary, study authors will be contacted up to three times to resolve questions about eligibility (LC). Reasons will be recorded for excluding studies. Studies will only be included once for evaluation purposes but multiple publications from the same study will be reported. A Preferred Reporting Items for Systematic Review and Meta-Analysis (PRISMA) flow diagram will show the overall process of study selection and summarise the inclusion and exclusion of studies at each stage of the review.

Data collection process

A standardised data extraction tool will be developed specifically for this review based on recommendations provided in the Cochrane Handbook of Systematic Reviews of Interventions (LC)¹⁶. Data will be extracted on study design and methods, sociodemographic characteristics, inclusion and exclusion criteria, study setting, details of experimental intervention and comparison intervention, duration of follow-up and outcomes studied, and extent of effectiveness. Two authors (LC and PM) will independently extract data using the standardised form, piloted in advance to ensure accuracy. Any differences of opinion between the two reviewers will be resolved by a third review author (DD) and consensus achieved. If necessary, study authors will be contacted up to three times to provide further details. Data will be entered into Review Manager Software and checked for accuracy¹⁷.

Outcomes

All outcomes collected at every time point will be included in the review. The primary outcomes of interest will be stress, anxiety, depression and QoL. Secondary outcomes will be birth outcomes including labour duration, pain management in labour and mode of birth. All reported outcome measures will be documented.

Risk of bias

Risk of bias of included studies will be assessed using the Cochrane Risk of Bias Assessment tool that contains several items under 7 categories, such as random sequence generation, allocation concealment, blinding of participants and investigators, the blindness of outcome assessments, incomplete outcome data, selective outcome reporting, and other biases¹⁶. Based on the assessment, the studies will be evaluated as low, unclear, or high bias.

Two reviewers will independently assess each article for risk of bias (LC and PM). Discrepancies will be resolved by discussion or if required referral to a third reviewer (DD). Where reported information is unclear or where data are missing all attempts will be made to contact the primary authors for clarification.

Assessment of the body of evidence – the GRADE approach

Quality of the evidence will be evaluated using the Grades of Recommendation, Assessment, Development and Evaluation (GRADE) approach¹⁸. This will assess the quality of evidence for specific outcomes. The evidence can be downgraded from ‘high quality’ by one level for serious or two levels for very serious limitations, depending on assessments of risk of bias, indirectness of evidence, serious inconsistency, imprecision of effect estimates or publication bias. Two reviewers will independently assess each article for quality (LC and PM). Discrepancies will be resolved by discussion or if required referral to a third reviewer (DD). Where reported information is unclear or where data are missing all attempts will be made to contact the primary authors for clarification.

GRADE profiler will be used to import data from Review Manager Software version 5.3 (RevMan 5.3) in order to create the summary of findings table (LC)^17,19. A summary of intervention effect and a measure of quality according to the GRADE approach will be presented for the following outcomes of interest:

Data synthesis

Two review authors (LC and PM) will extract the following study characteristics from included studies:

Heterogeneity between studies will be assessed using RevMan 5.3 by comparing study settings, populations and study design, using the I² statistic¹⁶. Results from included studies will be presented as summary risk ratios with 95% confidence intervals for dichotomous outcomes. The mean difference will be used for continuous data where outcomes are measured in the same way between trials. Where trials measure the same outcome using different methods the standardised mean difference will be used. We will combine the outcome measures from the individual trials through meta-analysis where possible (clinical comparability of populations, interventions, outcomes and time of assessment between trials) using a random-effects model, because we expect some between-study variation. Should the data be considered not sufficiently similar to be combined in a meta-analysis, the results from clinically comparable trials will be described qualitatively in the text. Statistical heterogeneity will be assessed in each meta-analysis using the T², I² and chi square statistics¹⁶. For included studies, levels of attrition will be recorded and the impact of including studies with high levels of missing data on assessment of treatment effect will be explored further using sensitivity analysis.

The information will be presented in narrative and tabular format to summarise the characteristics and results of the included studies and explain the average treatment effect and outcomes within and between studies.

Sensitivity analysis

For the primary and secondary outcomes, we will compare analyses including and excluding trials at high risk of bias (as defined in assessment of risk of bias in included studies) in order to explore the impact of risk of bias on estimates of treatment effects.

Analysis of subgroups or subsets

Subgroup analysis will be conducted where appropriate to stratify results by:

Separate comparisons and analyses for primary and secondary outcomes will be performed where possible and when appropriate.

Dissemination of results

The systematic review will be disseminated in peer-reviewed journals. The dataset generated and/or analysed during the study shall be available from the corresponding author on reasonable request.

Amendments

Any amendments to this protocol will be described in a table including the date of each amendment as well as a description of and rationale for this. The PROSPERO register will remain updated with the protocol and any amendments made.

Ethics approval and consent to participate

Ethical approval is not required for this study as it will not involve conducting experimental research, nor include identifying personal data.

Underlying data

No data is associated with this article.

Extended data

Open Science Framework: The effectiveness and characteristics of pregnancy yoga interventions: a systematic review protocol, https://doi.org/10.17605/OSF.IO/J3X4M²¹

This project contains the following extended data:

Reporting guidelines

Open Science Framework: PRISMA-P checklist for ‘The effectiveness and characteristics of pregnancy yoga interventions: a systematic review protocol’, https://doi.org/10.17605/OSF.IO/J3X4M²¹

Data are available under the terms of the Creative Commons Zero “No rights reserved” data waiver (CC0 1.0 Public domain dedication).