Comparative effectiveness of adjunct non-pharmacological interventions on maternal and neonatal outcomes in gestational diabetes mellitus patients: A systematic review and network meta-analysis protocol of randomized controlled trials

Sumanta Saha

doi:10.1371/journal.pone.0263336

. 2022 Jan 27;17(1):e0263336. doi: 10.1371/journal.pone.0263336

Comparative effectiveness of adjunct non-pharmacological interventions on maternal and neonatal outcomes in gestational diabetes mellitus patients: A systematic review and network meta-analysis protocol of randomized controlled trials

Sumanta Saha ^1,^*

Editor: Maria G Grammatikopoulou²

PMCID: PMC8794170 PMID: 35085374

Abstract

Background

Gestational diabetes mellitus (GDM) in pregnancy leads to a range of perinatal complications. Although several randomized controlled trials (RCT) have tested the effect of non-pharmacological standard GDM care adjuncts on these outcomes, there is no agglomerated statistical evidence on how their occurrence risk varies across interventions and with placebo. Therefore, a systematic review and network meta-analysis (NMA) protocol is proposed here to address this evidence gap.

Materials and methods

A search for above RCTs published in the English language will transpire in PubMed, Embase, and Scopus databases irrespective of date and geographic boundary. The RCTs must test nutritional supplementation, digital intervention, structured exercise program, educational program, counseling service, or a combination of these prenatally in GDM patients. These should report ≥1 of the following outcomes- cesarean section, pre-eclampsia, polyhydramnios, preterm birth, macrosomia, prolonged labor, gestational hypertension, premature rupture of membranes, congenital anomaly, Apgar scores, birth weight, birth length, gestational age at birth, neonatal hypoglycemia, neonatal hyperbilirubinemia, and neonatal Corpulence Index. The risk of bias assessment of the recruited trials will transpire using the Revised Cochrane risk-of-bias tool. Determination of the comparative effectiveness between interventions will occur by the frequentist method NMA for respective outcomes. The categorical and continuous outcomes effect size will get calculated in risk ratio and weighted or standardized mean difference, respectively. For each NMA model, network maps and league tables will show the connections between interventions and effect sizes with their 95% confidence intervals for each intervention pair compared, respectively. The publication bias assessment will occur using comparison-adjusted funnel plots. Best intervention prediction for NMA models with statistically significant intervention effect will happen by determining the surface under the cumulative ranking curve values. Statistical analysis will ensue using Stata software (v16). The statistical significance estimation will happen at p<0.05 and 95% confidence interval.

Trial registration

PROSPERO registration no: CRD42021271199; https://clinicaltrials.gov/.

Introduction

Gestational diabetes mellitus (GDM) is glucose intolerance of any degree that occurs or gets detected for the first time during gestation [1]. Its prevalence among pregnant females depends on the criteria used to diagnose GDM [2]. The common perinatal complications of GDM include cesarean section, preeclampsia, macrosomia, neonatal hypoglycemia, new-born hyperbilirubinemia, and birth trauma [3]. Standard GDM care primarily includes medical nutrition therapy, lifestyle modification, and blood glucose monitoring. Insulin therapy is introduced when these conservative approaches are inadequate to achieve glycemic control. Research suggests that the benefits of standard GDM care are not uniform across all its perinatal outcomes. It decreases the risk of outcomes like preeclampsia, shoulder dystocia, and macrosomia [4]. On the other hand, the effects of standard GDM care didn’t vary on certain outcomes like neonatal hypoglycemia and cesarean section from those not treated for GDM [4]. Therefore, it’s crucial to investigate the role of adjunct prenatal non-pharmacological interventions (e.g., nutritional supplementation, digital intervention, exercise therapy, educational intervention) in GDM patients on various perinatal outcomes. Contemporarily several randomized controlled trials (RCTs) have researched it.

Findings from some of these trials are briefed here. Meta-analyses of trials studying the effect of antenatal vitamin D supplementation in GDM patients suggested a decreased risk of newborn hyperbilirubinemia, newborn hospitalization, macrosomia, and cesarean section [5–7]. A meta-analysis on omega-3 fatty acid supplementation in GDM patients depicted that the risk of preterm delivery, macrosomia, and 5 minute Apgar score, and newborn weight didn’t vary from the placebo recipients [8]. A trial testing the role of face-to-face educational sessions in GDM patients found improvement of 1 and 5 minutes Apgar scores in the neonates [9]. However, it didn’t observe any difference in the newborn birth weights and cesarean section (CS) requirements compared to standard GDM care recipients [9]. A prenatal dietary and exercise counseling testing trial in GDM patients reported a decreased birth weight and reduced risk of large for gestational age in newborns, but CS and preterm delivery risk didn’t vary from the control group [10]. Another trial on GDM patients comparing twice-weekly exercise programs and standard GDM care didn’t find the risk of CS, neonatal hypoglycemia, and newborn hyperbilirubinemia to vary [11]. Regarding a trial testing digital application in GDM patients, a smartphone-based app to inform about GDM didn’t make any difference in the occurrence of chief maternal and neonatal outcomes [12].

Despite these trials, no standard guideline exists on prenatal non-pharmacological adjunct interventions in GDM patients. The plausible reasons are that these trials are underpowered (due to relatively small sample sizes) and/or nongeneralizable (as participant recruitment happened mainly from a particular nation) [5–7,9,11,12]. Moreover, meta-analysis studies (considered to be the highest level of epidemiological evidence) of RCTs in this context are unlikely to be robust. For instance, summary estimates of meta-analysis of nutritional supplementation trials on GDM are based on very few clinical trials (≤5) [5–7]. Furthermore, these meta-analyses have tested a particular intervention (e.g., vitamin D supplementation); therefore, aggregated evidence across various nutritional supplements remains scanty. Meta-analyses are rare beyond nutritional supplementation type prenatal interventions (e.g., digital applications in GDM patients) in GDM patients. Altogether, there is a critical shortage of aggregated evidence comparing perinatal outcomes between non-pharmacological adjuncts themselves and with placebo for an overview of the existing evidence in the context of GDM patients.

Therefore, to address this evidence lacuna, a systematic review and network meta-analysis (NMA) protocol is proposed to study the congregated evidence based on existing clinical trials on how various adjuvant non-pharmacological antenatal interventions might affect the perinatal outcomes in GDM mothers. Due to the incorporation of NMA, this review will allow an indirect comparison between two interventions not compared in any real-life trial. The NMA models will compare the following interventions- nutritional supplementation, digital intervention, structured exercise program, structured educational program, counselling service, and a combination of these. Additionally, the outcomes of interest will get compared between respective nutritional supplements as its secondary aim. The list of perinatal outcomes of interest is available beneath the inclusion criteria below.

Methods

A registered version of the proposed review is available at PROSPERO (Registration no: CRD42021271199) [13]. This report adheres to Preferred Reporting Items for Systematic Review and Meta-Analysis Protocols (PRISMA-P) (2015) reporting system (S1 File) [14].

Eligibility criteria

Inclusion criteria

Study population: GDM patients of any age irrespective of their history of GDM during previous gestations.
Study design: Placebo-controlled RCTs with any number of intervention arms irrespective of their follow-up duration.
Intervention arm: Along with standard/usual GDM care, trial participants in the intervention arm/s should receive any one or more of the following prenatal interventions:
1. Nutritional supplementation (e.g., vitamin D and probiotics).
2. Digital intervention/s (e.g., smartphone or smart-watch-based applications).
3. Structured supervised exercise program.
4. Structured educational and/or counseling service.
Comparator arm: Participants in the comparator arm should receive standard/usual GDM care with or without a placebo.
Outcomes of interest: The primary outcomes of interest will include the following perinatal outcomes:
- 1
  Cesarean section
- 2
  Pre-eclampsia
- 3
  Polyhydramnios
- 4
  Preterm birth
- 5
  Macrosomia
- 6
  Prolonged labor
- 7
  Gestational hypertension
- 8
  Premature rupture of membranes
- 9
  Neonatal hypoglycemia
- 10
  Neonatal hyperbilirubinemia
- 11
  Congenital anomaly
- 12
  Apgar scores at 1 min
- 13
  Apgar scores at 5 min
- 14
  Birth weight
- 15
  Birth length
- 16
  Gestational age at birth
- 17
  Neonatal Corpulence Index

Outcome no. 12 onwards, the data must be reported in mean and standard deviation. A trial reporting at least one of these outcomes will be eligible for inclusion. Acceptance of the diagnosis of GDM and the definition of the maternal and neonatal outcomes and standard/usual GDM care will happen as per the trialists.

Exclusion criteria

Non-RCT type study designs like observational studies and crossover studies.
Non-GDM type diabetes (e.g., type 1 or 2 diabetes).

Information sources and search strategy

For eligible articles published in the English language, an electronic database search (in PubMed, Embase, and Scopus) will transpire irrespective of the publication date and geographic origin.

A search in the PubMed database will happen using the search strings below. The latter stemmed from key themes of the research question- GDM, clinical trial, and perinatal outcomes.

(("diabetes, gestational"[MeSH Terms] OR "gestational diabetes mellitus"[Title/Abstract] OR "GDM"[Title/Abstract]) AND "randomized controlled trial"[Publication Type]) AND (randomizedcontrolledtrial[Filter])
(("nutrition*"[All Fields] OR ("vitamin s"[All Fields] OR "vitamine"[All Fields] OR "vitamines"[All Fields] OR "vitamins"[Pharmacological Action] OR "vitamins"[MeSH Terms] OR "vitamins"[All Fields] OR "vitamin"[All Fields]) OR "probitic"[All Fields] OR ("synbiotics"[MeSH Terms] OR "synbiotics"[All Fields] OR "synbiotic"[All Fields]) OR ("prebiotically"[All Fields] OR "prebiotics"[MeSH Terms] OR "prebiotics"[All Fields] OR "prebiotic"[All Fields]) OR ("calcification, physiologic"[MeSH Terms] OR ("calcification"[All Fields] AND "physiologic"[All Fields]) OR "physiologic calcification"[All Fields] OR "mineralization"[All Fields] OR "mineral s"[All Fields] OR "mineralisable"[All Fields] OR "mineralisation"[All Fields] OR "mineralisations"[All Fields] OR "mineralise"[All Fields] OR "mineralised"[All Fields] OR "mineralising"[All Fields] OR "mineralizations"[All Fields] OR "mineralize"[All Fields] OR "mineralized"[All Fields] OR "mineralizer"[All Fields] OR "mineralizers"[All Fields] OR "mineralizes"[All Fields] OR "mineralizing"[All Fields] OR "minerals"[MeSH Terms] OR "minerals"[All Fields] OR "mineral"[All Fields]) OR ("digital"[All Fields] OR "digitalisation"[All Fields] OR "digitalised"[All Fields] OR "digitalization"[All Fields] OR "digitalize"[All Fields] OR "digitalized"[All Fields] OR "digitalizer"[All Fields] OR "digitalizing"[All Fields] OR "digitally"[All Fields] OR "digitals"[All Fields] OR "digitization"[All Fields] OR "digitizations"[All Fields] OR "digitize"[All Fields] OR "digitized"[All Fields] OR "digitizer"[All Fields] OR "digitizers"[All Fields] OR "digitizes"[All Fields] OR "digitizing"[All Fields]) OR ("smartphone"[MeSH Terms] OR "smartphone"[All Fields] OR "smartphones"[All Fields] OR "smartphone s"[All Fields]) OR ("exercise"[MeSH Terms] OR "exercise"[All Fields] OR "exercises"[All Fields] OR "exercise therapy"[MeSH Terms] OR ("exercise"[All Fields] AND "therapy"[All Fields]) OR "exercise therapy"[All Fields] OR "exercise s"[All Fields] OR "exercised"[All Fields] OR "exerciser"[All Fields] OR "exercisers"[All Fields] OR "exercising"[All Fields]) OR ("educability"[All Fields] OR "educable"[All Fields] OR "educates"[All Fields] OR "education"[MeSH Subheading] OR "education"[All Fields] OR "educational status"[MeSH Terms] OR ("educational"[All Fields] AND "status"[All Fields]) OR "educational status"[All Fields] OR "education"[MeSH Terms] OR "education s"[All Fields] OR "educational"[All Fields] OR "educative"[All Fields] OR "educator"[All Fields] OR "educator s"[All Fields] OR "educators"[All Fields] OR "teaching"[MeSH Terms] OR "teaching"[All Fields] OR "educate"[All Fields] OR "educated"[All Fields] OR "educating"[All Fields] OR "educations"[All Fields]) OR ("counsel"[All Fields] OR "counseled"[All Fields] OR "counselings"[All Fields] OR "counselled"[All Fields] OR "counselling"[All Fields] OR "counseling"[MeSH Terms] OR "counseling"[All Fields] OR "counsellings"[All Fields] OR "counsels"[All Fields])) AND (("diabetes, gestational"[MeSH Terms] OR "gestational diabetes mellitus"[Title/Abstract] OR "GDM"[Title/Abstract]) AND "randomized controlled trial"[Publication Type] AND "randomized controlled trial"[Publication Type])) AND (randomizedcontrolledtrial[Filter])

MeSH tagging of newly indexed articles in the PubMed database takes some time due to the manual nature of the process. Therefore, to identify such publications, free-text terms and phrases related to GDM were used with MeSH terms.

Relevant filters applied in the above search strings helped narrow the search results to the study design of interest.

These search strings were determined to be appropriate by using the following strategy. The respective search strings successfully retrieved three preidentified publications (testing exercise [11], nutritional [15], and digital [12] intervention in GDM patients) piloted for this purpose within the first 300 citations on relevancy-wise sorting of search results (S1 Table) [16]. An identical search strategy will apply to other databases.

Additional searches will ensue in the bibliography of articles recruited in this review and a preprint server, medRxiv [17].

Study selection

The retrieved citations will get uploaded in the Rayyan systematic reviews software for study selection [18]. After eliminating the duplicate articles, two review authors will independently skim through the titles and abstracts of the remaining and shortlist the seemingly eligible and dubious ones for full-text reading. The review authors will retain the list of excluded full-text-read articles.

Data abstraction

After finalizing the articles to be reviewed, the review authors will independently abstract the subsequent data in pre-piloted forms [19,20] (S2 and S3 Files)-

Study details: Study design, the trial id, the nation/s where the trial got conducted, number of intervention arms, follow up duration of the trial, multi-centre or single centred trial, participant consent, ethical clearance, and funding information.
Study population details: The total number of participants randomized into each intervention arm and their mean age and sex distribution.
Intervention details: Interventions compared along with their administration frequency, duration, and dosages.
Outcome details: Perinatal post-intervention obstetric and neonatal outcomes of interest. When multiple outcomes’ data are reported in an article, it will get captured in the S2 and S3 Files and subsequently reported in the summary table of the proposed review.

Risk of bias (RoB) in individual studies

The Revised Cochrane risk-of-bias tool for randomized trials (RoB 2) will be used for the RoB assessment of the respective studies [21]. Utilizing signaling questions, the RoB will get assessed in the following bias domains- randomization process, intended interventions, missing outcome data, outcome data measurement, and reported results. Each of the signaling questions can have any of the following answers based on the review authors’ judgment- yes, probably yes, probably no, no, and no information. For each domain, an assessment of the algorithm-based evaluation of the signaling questions will transpire to incorporate necessary changes. The overall RoB judgment will depend on the evaluations made for respective domains (detailed elsewhere) [21]. Two review authors will independently pursue the RoB assessment.

Role of review authors

Three authors will be conducting the prospective review. The review authors will collate their findings after conducting each of the following independently- database search, study selection, data collection, and RoB assessment. By discoursing, they will try to resolve any conflict in an opinion. However, if this fails to bring resolution, a third-party opinion will be sought.

Data synthesis

NMA

Frequentist method NMA will be performed. The NMA models will contrast the above-stated interventions of interest to determine their relative superiority for respective outcomes (NMA1). The interventions under respective parent intervention categories will get fitted in the NMA1 model as the latter. For instance, interventions falling under the nutritional supplements category like vitamin D, probiotics, and omega-3 fatty acids will get included in NMA1 as nutritional supplements instead of these discrete supplement types. Likewise, a structured exercise program in the NMA1 model will consist of all physical activity-related interventions’ (e.g., brisk walking, aerobics). The same rule will apply to the remaining interventions. Additional network meta-analyses models (NMA2) will compare how respective nutritional supplements (like vitamin D, probiotics, and omega-3 fatty acids) differ for each of the outcomes. Depending on the clinical type of outcome, a decrease or an increase in effect size (ES) will determine the effectiveness. For instance, a risk ratio of <1 will indicate a safer intervention for pre-eclampsia. In all NMA models, standard or usual GDM care recipients (with or without placebo) will form the common comparator. For categorical outcomes, NMA will transpire using the augmentation method, i.e., adding a small amount of data (0.5) to all intervention arms when zero events occur in an intervention arm [22].

Criteria for selecting outcomes for NMA

NMA will be performed for outcomes fulfilling the following conditions:

Low risk of heterogeneity:

By conducting a pairwise meta-analysis (PMA), heterogeneity assessment will happen across trials testing the respective outcomes. The evaluation of the presence or absence of heterogeneity and its quantification will happen using Chi² statistics (statistical significance determined at p<0.1) [23] and I² values (of 25, 50, and 75% will categorize heterogeneity into low, moderate, and high categories, respectively) [24], respectively. This heterogeneity assessment will occur when at least 20 studies are available for PMA and/or the mean sample size is ≥80 for an adequately powered (80%) evaluation [25]. Since the interventions tested across the trials are unlikely to be identical for each outcome, random-effect PMA (inverse variance method) will be used for the heterogeneity assessment. For dichotomous outcomes with zero events in any intervention arm, 0.5 will be added to all cells of the 2x2 table.

Outcome data of trials testing interventions in >1 arm will be combined for PMA. For continuous outcomes, the means and its standard deviation (SD) will be compared by following formulae (Eqs 1 and 2) [23].
$Mean = \frac{(n 1 m 1 + n 2 m 2)}{n 1 + n 2}$ (1)

$SD = \sqrt{(((n 1 - 1) s d 1^{2}) + ((n 2 - 1) s d 2^{2}) + (\frac{n 1 n 2}{n 1 + n 2}) (m 1^{2} + m 2^{2} - 2 m 1 m 2)) / ((n 1 + n 2) - 1)}$ (2)
where n1, n2, m1, m2, sd1 and sd2 are hypothetical sample sizes of intervention arm 1 and 2 of a clinical trial, mean value of arm 1 and 2, and standard deviation of m1 and m2, respectively.
If the SD of the mean is unavailable for two groups of a trial, it will be calculated using the following steps:
1. The t-value estimation will occur using the P-value of a t-test.
2. Then, the SE calculation will transpire using the t value or confidence interval.
3. Finally, the SD calculation will occur using the SE.
The formulae for each of these steps are detailed elsewhere [23]. The calculated SD in this scenario will be assumed to be the same for both groups.

PMA of outcomes with adequately powered heterogeneity assessment depicting I²≤25% and p-value of Chi² statistics <0.1 will get included in the NMA models.
The NMA model produces a connected network.
There is a degree of freedom for heterogeneity in a network to ensure a random-effect consistency model fitting.
There is a degree of freedom for inconsistency in a network to ensure an inconsistency model fitting.

ES

The ES estimation of categorical and continuous outcomes will ensue in the risk ratio and weighted or standardized mean difference, respectively, for both NMA and PMA.

Network map

The construction of network maps will transpire for a visual depiction of NMA models. It will help to understand the direct and indirect relationships among interventions. Each of the nodes and their thicknesses in the network map will denote a non-pharmacologic intervention and the number of participants receiving it, respectively. The line connecting two nodes will depict the trials that tested these interventions, and it will thicken with the number of trials testing it. Using an iterative method that swaps intervention pairs, excessive overlapping of lines caused complex network maps will be simplified [22].

Transitivity and consistency

A rationalized transitivity evaluation will ensue to identify potential effect modifiers. To ensure clinical homogeneity among participants across all trials, the proposed review’s study population will not include patients with diabetes other than GDM.

Transitivity evaluation will also happen statistically by local (node-splitting method testing inconsistency in respective treatment pairs) and overall inconsistency assessment [26]. If both indicate an absence of inconsistency, a network consistency assumption will be accepted.

League tables and ranking probabilities

The calculated ES and its 95% confidence interval from respective NMA models will be presented in league tables. The diagonal cells across these tables will denote the contrasting interventions. When the same set of interventions is included in NMA models of two outcomes, for simplicity of presentation, their ESs will be placed in the same league table along with the upper and lower triangle of the league table (i.e., on either side of the diagonal cells).

NMA models of outcomes with at least one statistically significant efficacious finding will be subjected to best intervention prediction by successive estimation of the surface under the cumulative ranking curve values [27]. These values can range from 0–100%, where a higher value denotes a better-ranked intervention. Besides, cumulative ranking plots will be used for a visual presentation of estimated and predictive ranking [26].

RoB across studies

The assessment of the RoB across studies will include an evaluation of selective reporting by comparing the reported results with the pre-stated notion of the trialists. Additionally, a small study effect evaluation will ensue for each NMA model by constructing comparison-adjusted funnel plots. Asymmetric funnel plots will suggest the presence of variation in ESs between large and small studies.

Sensitivity analysis

A sensitivity analysis will repeat NMA1 and 2 by eliminating any trial with a high RoB component.

Analytic tools

The ‘meta’ and ‘network’ packages of Stata statistical software version 16.0 (StataCorp, College Station, Texas, USA) will be used for PMA and NMA, respectively. The statistical significance estimation of all ESs will happen at p<0.05 and 95% confidence interval.

Reporting of the review

The proposed review report will follow PRISMA for Network Meta-Analyses statement guideline [28].

Confidence in cumulative evidence

To assess the evidence quality of statistically significantly beneficial ESs in the NMA models, the Grading of Recommendations Assessment, Development and Evaluation (GRADE) approach proposed by GRADE Working Group (2004) will be used. This grading will label evidence into any of the following quality categories- high, moderate, low, and very low.

Ethics and dissemination

As the proposed article will be a systematic review and network meta-analysis not requiring any direct human participation, an ethical clearance requirement will not apply. Once the review is complete, dissemination will happen by publishing it in an international journal and/or conference presentation.

Limitation

As review authors of the proposed review are adept in the English language only, articles published in any other language will not get included in this review.

Supporting information

S1 Table. PubMed search strategy.

Proposed search strategy in PubMed and its relevance.

(DOCX)

Click here for additional data file.^{(19.1KB, docx)}

S1 File. PRISMA checklist.

Preferred Reporting Items for Systematic review and Meta-Analysis Protocols (PRISMA-P) 2015 checklist.

(DOC)

Click here for additional data file.^{(83.5KB, doc)}

S2 File. Proposed data abstraction form.

(PDF)

Click here for additional data file.^{(165KB, pdf)}

S3 File. Data abstraction form for analysis.

(PDF)

Click here for additional data file.^{(147.1KB, pdf)}

Funding Statement

The author received no specific funding for this work.

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24.Higgins JPT, Thompson SG, Deeks JJ, Altman DG. Measuring inconsistency in meta-analyses. BMJ [Internet]. 2003;327:557–60. Available from: http://www.bmj.com/cgi/doi/10.1136/bmj.327.7414.557. [DOI] [PMC free article] [PubMed] [Google Scholar]
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27.Salanti G, Ades AE, Ioannidis JPA. Graphical methods and numerical summaries for presenting results from multiple-treatment meta-analysis: an overview and tutorial. J Clin Epidemiol [Internet]. 2011;64:163–71. Available from: https://linkinghub.elsevier.com/retrieve/pii/S0895435610001691. doi: 10.1016/j.jclinepi.2010.03.016 [DOI] [PubMed] [Google Scholar]
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PLoS One. doi: 10.1371/journal.pone.0263336.r001

Decision Letter 0

Jamie Matu

6 Oct 2021

PONE-D-21-28908Comparative effectiveness of non-pharmacological interventions on maternal and neonatal outcomes in gestational diabetes mellitus patients: A systematic review and network meta-analysis protocol of randomized controlled trials.PLOS ONE

Dear Dr. Saha,

Thank you for submitting your manuscript to PLOS ONE. After careful consideration, we feel that it has merit but does not fully meet PLOS ONE’s publication criteria as it currently stands. Therefore, we invite you to submit a revised version of the manuscript that addresses the points raised during the review process. Please also remember PLOS ONE does not copyedit accepted manuscripts, so the language in submitted articles must be clear, correct, and unambiguous.

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PLOS ONE

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Reviewers' comments:

Reviewer's Responses to Questions

Comments to the Author

1. Does the manuscript provide a valid rationale for the proposed study, with clearly identified and justified research questions?

The research question outlined is expected to address a valid academic problem or topic and contribute to the base of knowledge in the field.

Reviewer #1: Yes

Reviewer #2: Partly

**********

2. Is the protocol technically sound and planned in a manner that will lead to a meaningful outcome and allow testing the stated hypotheses?

The manuscript should describe the methods in sufficient detail to prevent undisclosed flexibility in the experimental procedure or analysis pipeline, including sufficient outcome-neutral conditions (e.g. necessary controls, absence of floor or ceiling effects) to test the proposed hypotheses and a statistical power analysis where applicable. As there may be aspects of the methodology and analysis which can only be refined once the work is undertaken, authors should outline potential assumptions and explicitly describe what aspects of the proposed analyses, if any, are exploratory.

Reviewer #1: Yes

Reviewer #2: Partly

**********

3. Is the methodology feasible and described in sufficient detail to allow the work to be replicable?

Descriptions of methods and materials in the protocol should be reported in sufficient detail for another researcher to reproduce all experiments and analyses. The protocol should describe the appropriate controls, sample size calculations, and replication needed to ensure that the data are robust and reproducible.

Reviewer #1: No

Reviewer #2: Yes

**********

4. Have the authors described where all data underlying the findings will be made available when the study is complete?

The PLOS Data policy requires authors to make all data underlying the findings described in their manuscript fully available without restriction, with rare exception, at the time of publication. The data should be provided as part of the manuscript or its supporting information, or deposited to a public repository. For example, in addition to summary statistics, the data points behind means, medians and variance measures should be available. If there are restrictions on publicly sharing data—e.g. participant privacy or use of data from a third party—those must be specified.

Reviewer #1: No

Reviewer #2: No

**********

5. Is the manuscript presented in an intelligible fashion and written in standard English?

PLOS ONE does not copyedit accepted manuscripts, so the language in submitted articles must be clear, correct, and unambiguous. Any typographical or grammatical errors should be corrected at revision, so please note any specific errors here.

Reviewer #1: Yes

Reviewer #2: No

**********

6. Review Comments to the Author

Please use the space provided to explain your answers to the questions above and, if applicable, provide comments about issues authors must address before this protocol can be accepted for publication. You may also include additional comments for the author, including concerns about research or publication ethics.

You may also provide optional suggestions and comments to authors that they might find helpful in planning their study.

(Please upload your review as an attachment if it exceeds 20,000 characters)

Reviewer #1: In general this is a well designed systematic review / meta-analysis, that is already registered on PROSPERO. A good deal of thought has gone into the searches and terms used. I think it will make a useful contribution to the literature.

A couple of minor issues.

I would use the updated PRISMA guidelines and Checklist, rather than the 2015 version.

PMA isn't defined for the reader, presumably it is primary meta-analysis?

It isn't entirely clear what the effect sizes will be in the meta-analysis, and which formulas will be used to compute these effect sizes and so on.

Are the authors planning to look at other measures of bias, e.g. small study / publication bias? If so, what techniques will be used.

Reviewer #2: Major comments:

The use of non-pharmacologic lifestyle intervention (specifically, diet and exercise) and monitoring of blood glucose levels for the initial management of gestational diabetes (GDM) is standard of care. The determination of which of these accepted interventions has a more pronounced impact on pre-specific maternal and neonatal outcomes among women with GDM and their offspring would be of interest. However, the authors do not describe a study to compare effectiveness of currently accepted interventions for the management of GDM, but instead describe a comparison of non-pharmacologic interventions that are not adopted by current international guidelines due to a lack of evidence for benefit.

Thus, the hypothesis and goals of the review are not clear or consistent in the abstract or introduction of this manuscript. Furthermore, the validity of comparing across interventions such as omega-3 supplementation or smartphone applications, which prior studies did not show to differ from placebo, and why a network meta-analysis of these interventions should be performed, is questionable. Finally, the manuscript is not fully intelligible and some aspects are difficult to follow.

Minor comments:

-Inclusion criteria must be more specific: the types of interventions that will be included must be described and specified (eg., vitamin D, omega-3, low carb diet, etc. etc.); the specific outcomes that will be evaluated must be described and specified

-How many authors will perform the review specifically? (“3 or more”?)

-Page 10: “Both pharmacological and non-pharmacological interventions will not get included in the same NMA model.” – what pharmacologic interventions are referred to here, as the review purports to compare non-pharmacologic interventions?

**********

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Reviewer #1: No

Reviewer #2: No

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PLoS One. 2022 Jan 27;17(1):e0263336. doi: 10.1371/journal.pone.0263336.r002

Author response to Decision Letter 0

18 Oct 2021

RESPONSE TO REVIEWERS’ COMMENTS

Dear Reviewers,

Thank you for reading the manuscript critically and sharing your insightful comments and suggestions. The manuscript has been thoroughly revised based on your advice. Additionally, several sentences have been edited to ensure a concise and logical presentation. Two manuscript copies, one with track changes enabled and another clean version with changes in the colored text, are also submitted. Below are the point-wise responses to your comments.

1. Does the manuscript provide a valid rationale for the proposed study, with clearly identified and justified research questions?

The research question outlined is expected to address a valid academic problem or topic and contribute to the base of knowledge in the field.

Reviewer #1: Yes

REPLY:

Thank you for your feedback.

Reviewer #2: Partly

REPLY:

Thank you for your comment. The rationale has been reinforced further based on your other comments below. A clarification has been added now to the ‘Introduction’ section (the last two paras particularly).

2. Is the protocol technically sound and planned in a manner that will lead to a meaningful outcome and allow testing the stated hypotheses?

Reviewer #1: Yes

REPLY:

Thank you for your feedback.

Reviewer #2: Partly

REPLY:

Thank you for your comment. The methodology has been elaborated further based on your comments below. Detailed responses are below (at ‘6. Review Comments to the Author’).

3. Is the methodology feasible and described in sufficient detail to allow the work to be replicable?

Reviewer #1: No

REPLY:

Thank you for your comment. The analysis plan has been clarified further based on comments made by both reviewers. Please also see replies below about the amendments made in eligibility criteria and analysis (at ‘6. Review Comments to the Author’).

Reviewer #2: Yes

REPLY:

Thank you for your feedback.

4. Have the authors described where all data underlying the findings will be made available when the study is complete?

Reviewer #1: No

REPLY:

A data availability statement is now included in the manuscript just before the references.

Reviewer #2: No

REPLY:

A data availability statement is now included in the manuscript just before the references.

5. Is the manuscript presented in an intelligible fashion and written in standard English?

Reviewer #1: Yes

REPLY:

Thank you for your feedback.

Reviewer #2: No

REPLY:

The manuscript has been hard edited meticulously. Besides responding to the reviewers' comments, every sentence was re-read and amended when required to ensure lexical integrity.

6. Review Comments to the Author

REPLY:

Thank you for finding the proposed review relevant.

A couple of minor issues.

I would use the updated PRISMA guidelines and Checklist, rather than the 2015 version.

REPLY:

Thanks for the comment. By 'updated PRISMA guideline,' if you are referring to the PRISMA-2020 guideline for systematic review and meta-analysis, please allow me to clarify that it will not apply to this manuscript since this is a protocol for a systematic review and not the review itself.

Nevertheless, based on your comment, I searched the PRISMA website for any updated version of the PRISMA-P statement. However, I couldn't find any updated version of PRISMA-P after 2015. Additionally, I contacted one of the authors of the PRISMA 2020 statement for the same, and I learned that the PRISMA-P 2015 version is the only version available for systematic review protocols presently.

A humble request, if you are referring to any other version of the PRISMA statement, kindly let me know.

PMA isn't defined for the reader, presumably it is primary meta-analysis?

REPLY:

I apologize for not mentioning the full form of the PMA. PMA stands for pairwise meta-analysis. The abbreviation's use has been updated accordingly in the manuscript.

It isn't entirely clear what the effect sizes will be in the meta-analysis, and which formulas will be used to compute these effect sizes and so on.

REPLY:

Thank you for the comments. These issues are now addressed in the manuscript. I quote the sentence for your kind reference- 'The ES estimation of categorical and continuous outcomes will ensue in the risk ratio and weighted or standardized mean difference, respectively, for both NMA and PMA.' NMA stands for network meta-analysis.

Regarding formulae, these are specified in the updated manuscript in the ‘Methods’ section under the subheading ‘Criteria for selecting outcomes for NMA.’

Are the authors planning to look at other measures of bias, e.g. small study / publication bias? If so, what techniques will be used.

REPLY:

Yes, publication bias assessment will happen. However, the description of it was incomplete in the manuscript. Thanks for pointing it out. Publication bias assessment will ensue using comparison-adjusted funnel plots, and this is now mentioned in the manuscript in the ‘Methods’ section (under subheading ‘RoB across studies’).

Reviewer #2: Major comments:

Thus, the hypothesis and goals of the review are not clear or consistent in the abstract or introduction of this manuscript.

REPLY:

Thank you for your comment. A modified rationale of the manuscript has been drafted (please see the last two paragraphs of the introduction section for these amendments). The manuscript now coins on the weaknesses of the existing trials and meta-analyses of these trials to reinforce its justification. Furthermore, to make the abstract and introduction consistent, the interventions and outcomes of interest are stated explicitly in both sections.

Furthermore, the validity of comparing across interventions such as omega-3 supplementation or smartphone applications, which prior studies did not show to differ from placebo, and why a network meta-analysis of these interventions should be performed, is questionable. Finally, the manuscript is not fully intelligible and some aspects are difficult to follow.

REPLY:

Thanks for raising the issue. Your comment makes sense; a comparison between omega-3 supplementation versus smartphone application in terms of efficacy is perhaps two distant entities to make a meaningful comparison. Based on your comment, the analysis plan got updated to a more rationalized form. To describe using the above example, instead of comparing omega-3 supplementation versus smartphone, now juxtaposition will happen between the parent categories of these interventions (i.e., nutritional supplementation versus digital application).

The updated analysis plan will compare the following interventions- nutritional supplementation, digital intervention, structured exercise program, educational program, counseling service, or a combination of these.

An additional network meta-analysis will separately compare various nutritional supplements to address your concern in the subsequent comment. It will help understanding how supplements like vitamin D, probiotics, omega-3 fatty acids, etc., differ in terms of the occurrence of the perinatal outcomes in GDM patients and their neonates.

Please find this updated plan introduced briefly in the 'Introduction' section and described elaborately under the 'Methods' section (beneath the 'NMA' sub-heading).

Minor comments:

REPLY:

Thank you for the advice. The inclusion criteria have got updated now.

Regarding interventions', a list of interventions of interest has been specified (as stated in response to your previous comment). Also, following your suggestion, particular nutritional interventions will get compared in the additional network meta-analysis models (as specified in response to your previous comment).

However, an explicit list of nutritional interventions (like vitamin D, probiotics, omega-3 fatty acids, etc.) to be studied in the additional network meta-analysis models isn't prepared to keep the scope of the review broad. It will plausibly enhance the comprehensiveness (by allowing all possible nutritional supplement types tested in clinical trials on GDM patients to get included in the review) and rigor of the evidence.

Next, the reason for not including interventions like a low carbohydrate diet and self-monitoring of blood glucose in the proposed review is that these are part of standard GDM care. Notably, the non-pharmacological adjuncts to standard GDM care are the interventions of interest. In other words, the prospective review aims to study non-pharmacological interventions' roles on perinatal outcomes when combined with standard/usual GDM care.

Concerning outcomes, now specific outcomes of interest have been enlisted under the inclusion criteria as per your suggestion.

-How many authors will perform the review specifically? (“3 or more”?)

REPLY:

Three authors will perform the review.

REPLY:

Thanks for identifying the typing error. The sentence has been removed from the revised manuscript.

Thank you.

Attachment

Submitted filename: RESPONSE TO REVIEWERS.docx

Click here for additional data file.^{(26KB, docx)}

PLoS One. doi: 10.1371/journal.pone.0263336.r003

Decision Letter 1

Maria G Grammatikopoulou

4 Jan 2022

PONE-D-21-28908R1Comparative effectiveness of adjunct non-pharmacological interventions on maternal and neonatal outcomes in gestational diabetes mellitus patients: A systematic review and network meta-analysis protocol of randomized controlled trials.

PLOS ONE

Dear Dr. Saha,

Please submit your revised manuscript by Feb 18 2022 11:59PM. If you will need more time than this to complete your revisions, please reply to this message or contact the journal office at plosone@plos.org. When you're ready to submit your revision, log on to https://www.editorialmanager.com/pone/ and select the 'Submissions Needing Revision' folder to locate your manuscript file.

Please include the following items when submitting your revised manuscript:

A rebuttal letter that responds to each point raised by the academic editor and reviewer(s). You should upload this letter as a separate file labeled 'Response to Reviewers'.
A marked-up copy of your manuscript that highlights changes made to the original version. You should upload this as a separate file labeled 'Revised Manuscript with Track Changes'.
An unmarked version of your revised paper without tracked changes. You should upload this as a separate file labeled 'Manuscript'.

We look forward to receiving your revised manuscript.

Kind regards,

Maria G Grammatikopoulou

Academic Editor

PLOS ONE

Journal Requirements:

Please review your reference list to ensure that it is complete and correct. If you have cited papers that have been retracted, please include the rationale for doing so in the manuscript text, or remove these references and replace them with relevant current references. Any changes to the reference list should be mentioned in the rebuttal letter that accompanies your revised manuscript. If you need to cite a retracted article, indicate the article’s retracted status in the References list and also include a citation and full reference for the retraction notice.

Additional Editor Comments:

Please implement the improvements suggested by the 2 authors.

Season's greetings!

[Note: HTML markup is below. Please do not edit.]

Reviewers' comments:

Reviewer's Responses to Questions

Comments to the Author

1. Does the manuscript provide a valid rationale for the proposed study, with clearly identified and justified research questions?

The research question outlined is expected to address a valid academic problem or topic and contribute to the base of knowledge in the field.

Reviewer #3: Yes

Reviewer #4: Yes

**********

2. Is the protocol technically sound and planned in a manner that will lead to a meaningful outcome and allow testing the stated hypotheses?

Reviewer #3: Yes

Reviewer #4: Yes

**********

3. Is the methodology feasible and described in sufficient detail to allow the work to be replicable?

Reviewer #3: No

Reviewer #4: Yes

**********

4. Have the authors described where all data underlying the findings will be made available when the study is complete?

Reviewer #3: No

Reviewer #4: Yes

**********

5. Is the manuscript presented in an intelligible fashion and written in standard English?

Reviewer #3: Yes

Reviewer #4: Yes

**********

6. Review Comments to the Author

You may also provide optional suggestions and comments to authors that they might find helpful in planning their study.

(Please upload your review as an attachment if it exceeds 20,000 characters)

Reviewer #3: The authors provided us with a protocol for a systematic review and network meta-analysis for non-pharmacological interventions in gestational diabetes mellitus. The protocol is well structured and clear to read. Nevertheless, a variety of issues need to be covered before considered for publication.

1. Outcomes: It would be preferable to create an exhaustive list of outcomes based on the literature to ensure maximum objectiveness in the conducting of the review. This is not provided by the authors. Few examples are given e.g. preeclampsia. Still, it is to our belief necessary to prespecify (in the best possible way) outcome measures to be studied.

2. Details on reports providing information on more than one outcome have not been given.

3. Study selection: very weakly presented part. There is no specification of the program to be used or of the strategy (two separate authors etc). This needs to be analysed.

4. RoB evaluation using the 2011 tool needs to be justified. To our knowledge the tool has already been updated. Why is the newest form not chosen?

5. Prespecified forms of data extraction are not given. They are only described. Please provide a pdf version of the form.

6. Issues of the network meta-analysis are correct but are not backed up with bibliography. For example handling of zero events.

7. The biggest issue of the protocol is the search strategy. Even though information on the supplementary material is used to justify the choice of the protocol, we strongly disagree with the assumption of an RCT without adequate expansion of the search strategy. An in depth explanation is in order.

Reviewer #4: The present protocol is well designed and presented.

My comments are the following.

COMMENT 1. Only manuscripts in english are considered eligible for inclusion, please include more languages.

COMMENT 2. Please extend the search strategy to sources of grey literature.

**********

7. PLOS authors have the option to publish the peer review history of their article (what does this mean?). If published, this will include your full peer review and any attached files.

If you choose “no”, your identity will remain anonymous but your review may still be made public.

Do you want your identity to be public for this peer review? For information about this choice, including consent withdrawal, please see our Privacy Policy.

Reviewer #3: No

Reviewer #4: No

PLoS One. 2022 Jan 27;17(1):e0263336. doi: 10.1371/journal.pone.0263336.r004

Author response to Decision Letter 1

12 Jan 2022

Dear Reviewers,

I sincerely thank you for reading the manuscript and sharing your insightful comments. Please find two copies of the manuscript attached- one with track changes and the other a clean version.

The manuscript file accompanies four supporting documents-

1. S1 Table (relevancy wise search strings)

2. S1 File (PRISMA-P checklist)

3. S2 File (data abstraction form)

4. S3 File (data abstraction form for analysis)

Please find the responses to your comments below.

Review Comments to the Author

Author’s reply:

Thank you for the feedback. The updated version of this manuscript contains the following 17 outcomes as stated under the ‘Methods’ section in the manuscript –

1. Cesarean section

2. Pre-eclampsia

3. Polyhydramnios

4. Preterm birth

5. Macrosomia

6. Prolonged labor

7. Gestational hypertension

8. Premature rupture of membranes

9. Neonatal hypoglycemia

10. Neonatal hyperbilirubinemia

11. Congenital anomaly

12. Apgar scores at 1 min

13. Apgar scores at 5 min

14. Birth weight

15. Birth length

16. Gestational age at birth

17. Neonatal Corpulence Index

2. Details on reports providing information on more than one outcome have not been given.

Author’s reply:

Thank you for the comment. Now the following statement has been included in the revised manuscript to address the issue- “When multiple outcomes' data are reported in an article, it will get captured in the S2 and S3 Files and subsequently reported in the summary table of the proposed review.”

3. Study selection: very weakly presented part. There is no specification of the program to be used or of the strategy (two separate authors etc). This needs to be analysed.

Author’s reply:

Thank you for the comment. The study selection section has been revised, and the updated version is quoted here for your kind reference- “The retrieved citations will get uploaded in the Rayyan systematic reviews software for study selection.[18] After eliminating the duplicate articles, two review authors will independently skim through the titles and abstracts of the remaining and shortlist the seemingly eligible and dubious ones for full-text reading.” Kindly note, as the subheading “Role of review authors” states how a conflict in an opinion between the review authors will get resolved, it's not restated here.

4. RoB evaluation using the 2011 tool needs to be justified. To our knowledge the tool has already been updated. Why is the newest form not chosen?

Author’s reply:

Thank you for the comment. The updated version of the Cochrane RoB tool will be used. It’s quoted here from the revised manuscript for your kind reference- “The Revised Cochrane risk-of-bias tool for randomized trials (RoB 2) will be used for the RoB assessment of the respective studies.[19] Utilizing signaling questions, the RoB will get assessed in the following bias domains- randomization process, intended interventions, missing outcome data, outcome data measurement, and reported results. Each of the signaling questions can have any of the following answers based on the review authors' judgment- yes, probably yes, probably no, no, and no information. For each domain, an assessment of the algorithm-based evaluation of the signaling questions will transpire to incorporate necessary changes. The overall RoB judgment will depend on the evaluations made for respective domains (detailed elsewhere).[19] Two review authors will independently pursue the RoB assessment.” Kindly note, as the subheading “Role of review authors” states how a conflict in an opinion between the review authors will get resolved, it's not restated here.

5. Prespecified forms of data extraction are not given. They are only described. Please provide a pdf version of the form.

Author’s reply:

Thank you for the comment. Please find a draft data abstraction form attached to the revised manuscript. Besides, a draft data collection sheet for capturing data for meta-analysis is also included. Kindly refer to the attached S2 File and S3 File.

6. Issues of the network meta-analysis are correct but are not backed up with bibliography. For example handling of zero events.

Author’s reply:

Thank you for the feedback. Following additional relevant citations to back up the network meta-analysis are now included in the revised manuscript-

1. White IR. Network Meta-analysis. Stata J Promot Commun Stat Stata [Internet]. 2015;15:951–85. Available from: http://journals.sagepub.com/doi/10.1177/1536867X1501500403

2. Salanti G, Ades AE, Ioannidis JPA. Graphical methods and numerical summaries for presenting results from multiple-treatment meta-analysis: an overview and tutorial. J Clin Epidemiol [Internet]. 2011;64:163–71. Available from: https://linkinghub.elsevier.com/retrieve/pii/S0895435610001691

3. Rouse B, Chaimani A, Li T. Network meta-analysis: an introduction for clinicians. Intern Emerg Med [Internet]. 2017;12:103–11. Available from: http://link.springer.com/10.1007/s11739-016-1583-7

Author’s reply:

Thank you for the advice. An expanded search string is now included in the revised manuscript. For your kind reference, I am pasting it here from the revised manuscript- ‘(("nutrition*"[All Fields] OR ("vitamin s"[All Fields] OR "vitamine"[All Fields] OR "vitamines"[All Fields] OR "vitamins"[Pharmacological Action] OR "vitamins"[MeSH Terms] OR "vitamins"[All Fields] OR "vitamin"[All Fields]) OR "probitic"[All Fields] OR ("synbiotics"[MeSH Terms] OR "synbiotics"[All Fields] OR "synbiotic"[All Fields]) OR ("prebiotically"[All Fields] OR "prebiotics"[MeSH Terms] OR "prebiotics"[All Fields] OR "prebiotic"[All Fields]) OR ("calcification, physiologic"[MeSH Terms] OR ("calcification"[All Fields] AND "physiologic"[All Fields]) OR "physiologic calcification"[All Fields] OR "mineralization"[All Fields] OR "mineral s"[All Fields] OR "mineralisable"[All Fields] OR "mineralisation"[All Fields] OR "mineralisations"[All Fields] OR "mineralise"[All Fields] OR "mineralised"[All Fields] OR "mineralising"[All Fields] OR "mineralizations"[All Fields] OR "mineralize"[All Fields] OR "mineralized"[All Fields] OR "mineralizer"[All Fields] OR "mineralizers"[All Fields] OR "mineralizes"[All Fields] OR "mineralizing"[All Fields] OR "minerals"[MeSH Terms] OR "minerals"[All Fields] OR "mineral"[All Fields]) OR ("digital"[All Fields] OR "digitalisation"[All Fields] OR "digitalised"[All Fields] OR "digitalization"[All Fields] OR "digitalize"[All Fields] OR "digitalized"[All Fields] OR "digitalizer"[All Fields] OR "digitalizing"[All Fields] OR "digitally"[All Fields] OR "digitals"[All Fields] OR "digitization"[All Fields] OR "digitizations"[All Fields] OR "digitize"[All Fields] OR "digitized"[All Fields] OR "digitizer"[All Fields] OR "digitizers"[All Fields] OR "digitizes"[All Fields] OR "digitizing"[All Fields]) OR ("smartphone"[MeSH Terms] OR "smartphone"[All Fields] OR "smartphones"[All Fields] OR "smartphone s"[All Fields]) OR ("exercise"[MeSH Terms] OR "exercise"[All Fields] OR "exercises"[All Fields] OR "exercise therapy"[MeSH Terms] OR ("exercise"[All Fields] AND "therapy"[All Fields]) OR "exercise therapy"[All Fields] OR "exercise s"[All Fields] OR "exercised"[All Fields] OR "exerciser"[All Fields] OR "exercisers"[All Fields] OR "exercising"[All Fields]) OR ("educability"[All Fields] OR "educable"[All Fields] OR "educates"[All Fields] OR "education"[MeSH Subheading] OR "education"[All Fields] OR "educational status"[MeSH Terms] OR ("educational"[All Fields] AND "status"[All Fields]) OR "educational status"[All Fields] OR "education"[MeSH Terms] OR "education s"[All Fields] OR "educational"[All Fields] OR "educative"[All Fields] OR "educator"[All Fields] OR "educator s"[All Fields] OR "educators"[All Fields] OR "teaching"[MeSH Terms] OR "teaching"[All Fields] OR "educate"[All Fields] OR "educated"[All Fields] OR "educating"[All Fields] OR "educations"[All Fields]) OR ("counsel"[All Fields] OR "counseled"[All Fields] OR "counselings"[All Fields] OR "counselled"[All Fields] OR "counselling"[All Fields] OR "counseling"[MeSH Terms] OR "counseling"[All Fields] OR "counsellings"[All Fields] OR "counsels"[All Fields])) AND (("diabetes, gestational"[MeSH Terms] OR "gestational diabetes mellitus"[Title/Abstract] OR "GDM"[Title/Abstract]) AND "randomized controlled trial"[Publication Type] AND "randomized controlled trial"[Publication Type])) AND (randomizedcontrolledtrial[Filter]).’

Thank you.

Reviewer #4: The present protocol is well designed and presented.

My comments are the following.

COMMENT 1. Only manuscripts in english are considered eligible for inclusion, please include more languages.

Author’s reply:

Thank you for your comment. The review authors are adept in the English language only. Moreover, no funding is available for hiring language translators. It is a potential limitation of the proposed review, now mentioned in the revised manuscript under the subheading ‘Limitation’ using the following text- “As review authors of the proposed review are adept in the English language only, articles published in any other language will not get included in this review.”

COMMENT 2. Please extend the search strategy to sources of grey literature.

Author’s reply:

Thank you for the comment. The search strategy has now been extended to a pre-print server medRxiv to include non-peer-reviewed articles. It has been stated in the revised manuscript using the following sentence- “Additional searches will ensue in the bibliography of articles recruited in this review and a preprint server, medRxiv.[17]”

Thank you.

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PLoS One. doi: 10.1371/journal.pone.0263336.r005

Decision Letter 2

Maria G Grammatikopoulou

18 Jan 2022

Comparative effectiveness of adjunct non-pharmacological interventions on maternal and neonatal outcomes in gestational diabetes mellitus patients: A systematic review and network meta-analysis protocol of randomized controlled trials.

PONE-D-21-28908R2

Dear Dr. Saha,

We’re pleased to inform you that your manuscript has been judged scientifically suitable for publication and will be formally accepted for publication once it meets all outstanding technical requirements.

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Additional Editor Comments (optional):

Reviewers' comments:

PLoS One. doi: 10.1371/journal.pone.0263336.r006

Acceptance letter

Maria G Grammatikopoulou

19 Jan 2022

PONE-D-21-28908R2

Dear Dr. Saha:

I'm pleased to inform you that your manuscript has been deemed suitable for publication in PLOS ONE. Congratulations! Your manuscript is now with our production department.

If your institution or institutions have a press office, please let them know about your upcoming paper now to help maximize its impact. If they'll be preparing press materials, please inform our press team within the next 48 hours. Your manuscript will remain under strict press embargo until 2 pm Eastern Time on the date of publication. For more information please contact onepress@plos.org.

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Kind regards,

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on behalf of

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Associated Data

This section collects any data citations, data availability statements, or supplementary materials included in this article.

Supplementary Materials

S1 Table. PubMed search strategy.

Proposed search strategy in PubMed and its relevance.

(DOCX)

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S1 File. PRISMA checklist.

Preferred Reporting Items for Systematic review and Meta-Analysis Protocols (PRISMA-P) 2015 checklist.

(DOC)

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S2 File. Proposed data abstraction form.

(PDF)

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S3 File. Data abstraction form for analysis.

(PDF)

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PERMALINK

Comparative effectiveness of adjunct non-pharmacological interventions on maternal and neonatal outcomes in gestational diabetes mellitus patients: A systematic review and network meta-analysis protocol of randomized controlled trials

Sumanta Saha

Roles

Abstract

Background

Materials and methods

Trial registration

Introduction

Methods

Eligibility criteria

Inclusion criteria

Exclusion criteria

Information sources and search strategy

Study selection

Data abstraction

Risk of bias (RoB) in individual studies

Role of review authors

Data synthesis

NMA

Criteria for selecting outcomes for NMA

ES

Network map

Transitivity and consistency

League tables and ranking probabilities

RoB across studies

Sensitivity analysis

Analytic tools

Reporting of the review

Confidence in cumulative evidence

Ethics and dissemination

Limitation

Supporting information

Funding Statement

References

Decision Letter 0

Jamie Matu

Roles

Author response to Decision Letter 0

Decision Letter 1

Maria G Grammatikopoulou

Roles

Author response to Decision Letter 1

Decision Letter 2

Maria G Grammatikopoulou

Roles

Acceptance letter

Maria G Grammatikopoulou

Roles

Associated Data

Supplementary Materials

ACTIONS

PERMALINK

RESOURCES

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