You are here

  • Home
  • Archive
  • Volume 8, Issue 11
  • Adverse pregnancy and neonatal outcomes associated with Neisseria gonorrhoeae, Mycoplasma genitalium, M. hominis, Ureaplasma urealyticum and U. parvum: a systematic review and meta-analysis protocol

Article Text

Article menu

Download PDFPDF

XML
Obstetrics and gynaecology
Protocol
Adverse pregnancy and neonatal outcomes associated with Neisseria gonorrhoeae, Mycoplasma genitalium, M. hominis, Ureaplasma urealyticum and U. parvum: a systematic review and meta-analysis protocol
  1. Lisa M Vallely1,
  2. Dianne Egli-Gany2,
  3. William Pomat3,
  4. Caroline SE Homer4,5,
  5. Rebecca Guy6,
  6. Handan Wand7,
  7. Bronwyn Silver8,
  8. Alice R Rumbold9,
  9. John M Kaldor1,
  10. Nicola Low2,
  11. Andrew J Vallely1,10
  1. 1 Public Health Interventions Research Group, Kirby Institute, University of New South Wales, Sydney, New South Wales, Australia
  2. 2 Institute of Social and Preventive Medicine, University of Bern, Bern, Switzerland
  3. 3 Director, Papua New Guinea Institute of Medical Research, Goroka, Eastern Highlands Province, Papua New Guinea
  4. 4 Centre for Midwifery, Child and Family Health, University of Technology Sydney, Sydney, New South Wales, Australia
  5. 5 Co-Program Director Maternal and Child Health, Burnet Institute, Melbourne, Victoria, Australia
  6. 6 Surveillance and Evaluation Research, The Kirby Institute, University of New South Wales, Sydney, New South Wales, Australia
  7. 7 Biostatistics and Databases program, The Kirby Institute, University of New South Wales, Sydney, New South Wales, Australia
  8. 8 Public Health Division, Central Australian Aboriginal Congress, Alice Springs, Australia
  9. 9 Robinson Research Institute, University of Adelaide, Adelaide, Australia
  10. 10 Sexual and Reproductive Health Unit, Papua New Guinea Institute of Medical Research, Goroka, Papua New Guinea
  1. Correspondence to Dr Lisa M Vallely; lvallely{at}kirby.unsw.edu.au

Abstract

Introduction Several bacterial sexually transmitted and genital mycoplasma infections during pregnancy have been associated with poor pregnancy and perinatal outcomes. Comprehensive and systematic information about associations between sexually transmitted infections (STI) and genital infections in pregnancy and adverse perinatal outcomes is needed to improve understanding about the evidence for causal associations between these infections and adverse pregnancy and neonatal outcomes. Our primary objective is to systematically review the literature about associations between: (1) Neisseria gonorrhoeae in pregnancy and preterm birth; (2) Mycoplasma genitalium in pregnancy and preterm birth; (3) M. hominis, Ureaplasma urealyticum and/or U. parvum in pregnancy and preterm birth.

Methods and analysis We will undertake a systematic search of Medline, Excerpta Medica database and the Cochrane Library and Cumulative Index to Nursing and Allied Health Literature. Following an initial screening of titles by one reviewer, abstracts will be independently assessed by two reviewers before screening of full-text articles. To exclude a manuscript, both reviewers need to agree on the decision. Any discrepancies will be resolved by discussion, or the adjudication of a third reviewer. Studies will be included if they report testing for one or more of N. gonorrhoeae, M. genitalium, M. hominis, U. urealyticum and/or U. parvum during pregnancy and report pregnancy and/or birth outcomes. In this review, the primary outcome is preterm birth. Secondary outcomes are premature rupture of membranes, low birth weight, spontaneous abortion, stillbirth, neonatal mortality and ophthalmia neonatorum. We will use standard definitions, or definitions reported by study authors. We will examine associations between exposure and outcome in forest plots, using the I2 statistic to examine between study heterogeneity. Where appropriate, we will use meta-analysis to combine results of individual studies.

Ethics and dissemination This systematic review of published literature does not require ethical committee approval. Results of this review will be published in a peer reviewed, open access journal.

PROSPERO registration number CRD42016050962.

  • sexually transmitted infections
  • adverse pregnancy outcome
  • systematic review
  • genital mycoplasmas
  • preterm birth
  • meta analysis

This is an open access article distributed in accordance with the Creative Commons Attribution Non Commercial (CC BY-NC 4.0) license, which permits others to distribute, remix, adapt, build upon this work non-commercially, and license their derivative works on different terms, provided the original work is properly cited, appropriate credit is given, any changes made indicated, and the use is non-commercial. See: http://creativecommons.org/licenses/by-nc/4.0/.

https://doi.org/10.1136/bmjopen-2018-024175

Statistics from Altmetric.com

    Request Permissions

    If you wish to reuse any or all of this article please use the link below which will take you to the Copyright Clearance Center’s RightsLink service. You will be able to get a quick price and instant permission to reuse the content in many different ways.

    Strengths and limitations of this study

    • This systematic review is, as far as we are aware, the first to address associations between adverse pregnancy and neonatal outcomes and the sexually transmitted pathogens Neisseria gonorrhoeae and Mycoplasma genitalium, and associations with other genital mycoplasmas.

    • The systematic review, which covers more than one infection, will be efficient because these infections are often tested for and reported in the same study.

    • This review will appraise the quality of each study according to the study design (ie, cross-sectional, case–control, cohort or clinical trial).

    • The results of this review can be used to estimate the burden of disease due to these sexually transmitted and genital infections.

    • A limitation of this review is that we will only be able to examine associations separately for Ureaplasma urealyticum and U. parvum in more recent studies because older studies did not distinguish between the two species.

    Introduction  

    Several bacterial sexually transmitted infections (STI) during pregnancy have been reported to be associated with poor pregnancy outcomes.1–3 Chlamydia trachomatis (CT, chlamydia), Neisseria gonorrhoeae (NG), Trichomonas vaginalis (TV, trichomoniasis) and Mycoplasma genitalium (MG) have all been associated with one or more of the following: premature rupture of membranes (PROM), preterm birth and low birth weight (LBW)1–10; CT and NG are also recognised as causes of neonatal conjunctivitis and CT is a cause of neonatal pneumonia.11 Other genital mycoplasmas in the reproductive tract are M. hominis, Ureaplasma urealyticum and U. parvum. Combined testing for these organisms is common and they are very frequently found in the vagina.12 Routine testing and treatment of asymptomatic non-pregnant women are discouraged because the evidence that they cause disease is questionable.13 Detection of these organisms during pregnancy has been reported in some studies, however, to be associated with spontaneous abortion, stillbirth, preterm birth, LBW and perinatal morbidity and mortality.13–15 In a large cohort study in south Asia, Ureaplasma spp (U. urealyticum and U. parvum together) were the second most common organism identified in infants with signs of serious bacterial infection than from healthy babies and were more commonly isolated from sick than healthy infants.16 Bacterial culture for U. urealyticum does not distinguish between two closely related species, U. urealyticum and U. parvum and associations with each of these subspecies and adverse pregnancy outcomes are not consistent.17 18

    Comprehensive and systematic information about associations between STI, other genital infections in pregnancy and adverse pregnancy and perinatal outcomes is needed to improve understanding about the evidence for causal associations, to contribute to estimates of the global burden of STI and to determine the potential impact of preventive interventions. For example, associations between syphilis in pregnancy and preterm birth, LBW, stillbirth and systemic congenital infection are well-established, the burden of disease has been estimated and a global strategy for elimination of congenital syphilis is in place.19–21 For other STI and reproductive tract infections, the consistency and causal nature of associations are not as clear. Much of the published work on STI, reproductive tract infections and their association with adverse birth outcomes comes from middle-income and high-income countries, with less evidence from low-income settings which have the highest prevalence rates of STI in pregnancy.1 22

    Systematic reviews that synthesise findings from different studies can help to examine the consistency and risk of bias of the body of evidence. To date, systematic reviews about adverse pregnancy outcomes have examined associations with CT,23 TV24 and MG.25 For CT, there are published and ongoing reviews. Silva et al 23 reported on 12 studies published up to January 2010 and found that CT infection during pregnancy was associated with an increased risk of preterm labour, LBW and perinatal mortality. A protocol in the online database PROSPERO shows that another systematic review about CT and adverse pregnancy outcomes is ongoing.26 For TV, a systematic review by Silver et al 24 included 11 studies published up to May 2013 and found that antenatal TV infection was associated with increased risk of preterm birth, PROM and small for gestational age infants. For MG, a systematic review by Lis et al 25 included nine studies published up to June 2014 and found that MG was associated with preterm birth and spontaneous abortion. Nucleic acid amplification tests (NAATs) for MG are only now becoming widely available, so a new systematic review of evidence about MG is warranted.25 For NG and adverse pregnancy and neonatal outcomes we are unaware of any systematic reviews. Multiplex NAATs now include targets for M. hominis, U. urealyticum and U. parvum. We are unaware of a systematic review that has synthesised quantitative data about associations between these genital mycoplasmas and adverse pregnancy outcomes. M. hominis, in particular, is strongly associated with bacterial vaginosis (BV) which itself is strongly associated with adverse pregnancy outcomes.15 The use of antibiotic therapy for treating BV in pregnancy has been found to eradicate BV during pregnancy but did not reduce the risk of preterm birth, or preterm, prelabour rupture of membranes.27 It would be useful to examine whether or not co-existing BV modifies any association between genital mycoplasmas and adverse pregnancy outcomes. STIs and genital mycoplasmas can co-occur and the use of multiplex NAATs means that findings about multiple organisms are increasingly presented together.13 28 A single search strategy that includes terms for different pathogens and outcomes could make the work of a systematic review more efficient.

    Objectives

    The overall aim of this systematic review is to examine associations between selected infections in pregnancy and adverse pregnancy and/or neonatal outcomes. We have the following specific objectives:

    1. To determine whether NG infection during pregnancy increases the risk of preterm birth.

    2. To determine whether MG infection during pregnancy increases the risk of preterm birth.

    3. To determine whether infection with the genital tract infections M. hominis, U. urealyticum and U. parvum during pregnancy increase the risk of preterm birth.

    4. To examine associations between each of the named infections during pregnancy and other adverse pregnancy or neonatal outcomes: LBW, PROM, spontaneous abortion; perinatal mortality; ophthalmia neonatorum.

    Methods and analysis

    We wrote the systematic review protocol in accordance with the Preferred Reporting Items for Systematic Reviews and Meta-Analyses Protocols guidelines29 (online supplementary file 1), adapting it where necessary to our review of observational research studies. If we need to amend the protocol, we will update the PROSPERO record with the date of each amendment, accompanied by a description of the change and the rationale.

    Supplementary file 1

    Eligibility criteria

    Studies will be selected if they report one or more pregnancy, perinatal or neonatal outcome in women with NG, MG, M. hominis, U. urealyticum and/or U. parvum.

    Study design

    We will include any study design with data that allows comparison between women with and without one of the included infections. Eligible study designs include case–control, cross-sectional, cohort studies and clinical trials. Individual case reports, case series without a control group and opinion articles will not be included.

    Participants

    Women who have been tested during pregnancy for NG, MG, M. hominis, U. urealyticum or U. parvum using a laboratory diagnostic test, for example culture or NAAT, and for whom pregnancy and/or neonatal health outcomes are reported.

    Infections

    For studies that report more than one of the eligible infections, we will only include studies for which we can extract data separately for each infection, with the exception of U. urealyticum. We will assume that studies reporting on U. urealyticum alone have not differentiated between U. urealyticum and U. parvum. We assume that studies published after 2000 and reporting separate results for U. urealyticum and U. parvum have conducted tests that distinguish between these organisms.

    Exposures or interventions

    For observational study designs, the exposures of interest are: (1) NG; (2) MG; (3) M. hominis, U. urealyticum and/or U. parvum infection, diagnosed using a recognised laboratory test. For intervention studies, the intervention of interest is antibiotic treatment for a detected NG, MG, other genital mycoplasma infection or antibiotic prophylaxis. The comparator is women who did not receive antibiotic treatment for NG, MG or other genital mycoplasma infection.

    Exclusion criteria

    Individual case reports, case series, opinion articles and studies without a control group will be excluded.

    Studies including only mycoplasma infections without differentiating between specific mycoplasmas and articles that pool different STI and mycoplasma infections together will be excluded.

    Information sources

    We will search Medline, Excerpta Medica database and the Cochrane Library and Cumulative Index to Nursing and Allied Health Literature to identify relevant studies in humans only. We will not apply language or date limits to the search, but will only include articles published in English or German.

    Search strategy

    The search strategy includes Medical Subject Headings (MeSH) and keywords related to pregnancy, infections (NG, MG, M. hominis, U. urealyticum and/or U. parvum) and pregnancy, birth and neonatal outcomes (table 1). The ‘explode’ function will be applied to each MeSH heading.

    View this table:
    Table 1

    Search strategy

    We will search each database from its earliest date, including online publication. To identify additional relevant studies, we will search the reference lists of included studies or relevant reviews identified during the search. LV, the lead author of this manuscript, who is also the lead person for this planned review, will conduct the search.

    Study records

    Data management

    Search results will be imported into an Endnote (Clarivate Analytics 2017, Boston) library and all duplicates will be removed. We will use REDCap (Research Electronic Data Capture, Vanderbilt University, TN), a secure web application for building and managing online databases for screening and data extraction. DEG will design and pilot the forms for screening and data extraction. All extracted data will be imported into Stata V.14.0 (StataCorp LLC, TX) for analysis.

    Selection process

    We will conduct screening for inclusion in three stages:

    1. One reviewer (LV) will review each title and decide on records that can be excluded immediately using selected criteria (online supplementary material 2). All other records advance to the next stage.

    2. In the second stage, two reviewers (LV, DE-G) will independently screen all titles and abstracts against the eligibility criteria. To exclude a record, both reviewers need to agree on the decision. Any record excluded by a single reviewer is checked by the second reviewer and discrepancies will be resolved by discussion, or by the adjudication of a third reviewer.

    3. In the third stage, two reviewers (LV, DE-G) will screen the full text of each record independently against the eligibility criteria. To exclude a manuscript, both reviewers need to agree on the decision. Any manuscript excluded by a single reviewer is checked by the second reviewer and discrepancies will be resolved by discussion, or by the adjudication of a third reviewer. Reasons for exclusion of any study at stage three will be recorded.

    Supplementary file 2

    Data collection process

    Two reviewers will extract data independently. The reviewers will compare their findings and resolve discrepancies through discussion, or by asking a third reviewer to adjudicate. Where necessary we will contact the authors of selected manuscripts for missing or additional information.

    Data items

    Table 2 outlines data items that will be extracted, including study characteristics, participant characteristics, presence or absence of infection and pregnancy and neonatal outcomes.

    View this table:
    Table 2

    Data items to be extracted

    Outcomes

    There are several potential adverse outcomes of pregnancy, and perinatal or neonatal outcomes. In this review we will use standard and recommended definitions 30 or, if these are not consistently defined, use the  case defintions reported by the authors.  The following outcomes will be considered:

    Primary outcome

    • Preterm birth, defined as birth before 37 completed weeks’ gestation (including extremely preterm, very preterm and moderate to late preterm).30

    Secondary outcomes

    • PROM, including preterm (before 37 completed weeks gestation) rupture of membranes.

    • LBW, defined as birth weight less than 2500 g.31

    • Spontaneous abortion (miscarriage) (or as defined by study).

    • Perinatal mortality

      • Stillbirth/fetal death in utero at more than 20 weeks gestation (or as defined by study).

      • Neonatal mortality (death in the first 28 days of life).

    • Ophthalmia neonatorum.

    Risk of bias in individual studies

    Two reviewers will assess the methodological quality and risk of bias of each study included in the review independently, using study specific checklists published by the UK National Institute for Health and Care Excellence.32 33 The checklists enable the reviewer to appraise the internal and external validity of a study after considering key aspects relating to study design, including population characteristics; definition of exposure variables; outcomes assessed and methods of analyses. Based on these four aspects, an overall assessment of the internal and external validity of each study will be considered. Where the two reviewers disagree, a third reviewer will adjudicate.

    Data synthesis and analysis

    We will conduct separate data synthesis and analysis, first for the STI NG and MG and then for the other genital mycoplasma infections M. hominis, U. urealyticum and U. parvum. The stepwise approach will make our review process more efficient. We will apply the same procedures for each group of infections.

    We will develop a table summarising the key characteristics of each included study, including author, study year, setting, study design, number of participants and outcomes.

    For cross-sectional studies, cohort studies and clinical trials, the measure of association will usually be the risk ratio (RR, with 95% CI) and for case–control studies the measure of association will usually be the OR (with 95% CI). We will use the measure of association and 95% CI presented by the authors and we will check the calculation of the point estimate, where possible, with raw data extracted from the article. Study authors might also report effect estimates that control for potential confounding factors. Where adjusted estimates of effect obtained from multivariable regression analyses are reported, we will extract the estimate (with 95% CI) and will record the variables included in the multivariable model. We have prespecified three variables that are likely to cause confounding, resulting in an overestimation of the association between the infection of interest and pregnancy and perinatal outcomes. We will record whether each of the following variables is included in multivariable analyses: younger age, lower socioeconomic position and presence of other STI or reproductive tract infections.

    We will display associations first in forest plots to show the measure of association for each exposure-outcome pair, stratified by study design. We will use the I2 test to estimate the proportion of variability in point estimates that can be attributed to between study heterogeneity for reasons other than chance.34 As a guide, we will consider Ivalues <50% as evidence of low heterogeneity, 50%–75% as moderate heterogeneity and >75% as severe heterogeneity. We will investigate reasons for heterogeneity by stratification or, where there are enough studies, meta-regression. We will conduct sensitivity analyses to determine any effect of the following characteristics on the results: standard versus author-defined outcome definitions; low versus high risk of bias. We will conduct subgroup analyses to investigate the following possible sources of heterogeneity: country or region of study; diagnostic test (NAAT, culture, other); trimester of pregnancy when infection was detected (first, second, third); decade of study (pre-1980, 1980–1989, 1990–1999, 2000 or later); presence or absence of BV.

    Where appropriate, for outcomes reported by two or more studies of the same design, we will use meta-analysis to estimate a summary RR (95% CI) or OR (95% CI). If heterogeneity is moderate or severe, we will use a random effects model.35 The random effects model estimates the average effect across all studies and assumes that the true strength of association differs between studies. If heterogeneity is absent or low, we will use a fixed effects model. The fixed effects model assumes that the effect is similar across all studies and that variation between studies is due only to chance. We will conduct separate analyses for studies that record the presence of exposure before the outcome and studies in which exposure and outcome are measured at the same time.

    We will examine the results of adjusted analyses using the same approach as for unadjusted estimates.

    All data will be analysed using Stata V.14.0 (StataCorp LLC, TX).

    Meta-biases

    If there are more than 10 studies examining an exposure-outcome association, we will look for evidence of publication bias using funnel plots. We will examine these visually for evidence of asymmetry and use the Begg and Mazumdar rank correlation test for asymmetry.36

    We have not planned to look for evidence of selective reporting within studies.

    Confidence in cumulative evidence

    We will use the Grading of Research Evidence Assessment and Development approach to assess the body of evidence, considering the observational study designs,37 and provide a descriptive assessment of certainty in the cumulative evidence.

    Patient and public involvement

    Patients and/or the public were not involved in the development of this review protocol. We will publish the findings in open access publications which are available for the public to read and make use of the data.

    Discussion

    This systematic review will fill gaps in knowledge about potential associations between STI and reproductive tract infections, and adverse pregnancy and perinatal outcomes. Our systematic review will address infections that have not previously been assessed in a systematic review (NG) and some genital mycoplasmas.

    The association between STI and other genital infections, and adverse pregnancy and perinatal outcomes has been documented from a number of high- and middle-income settings.2 5 8 We will search multiple information sources and expect to find additional studies conducted in less well-resourced settings. Additional steps to minimise bias include independent assessments by two reviewers to reduce bias in the selection of studies and extraction of data and consideration of adjusted effect sizes and specific prespecified confounding factors in the analysis. However, we also anticipate some challenges that are specific to our review. First, we are reviewing the association between U. urealyticum and adverse pregnancy outcomes. U. urealyticum is now recognised to comprise two species, U. urealyticum and U. parvum. We will only be able to examine associations for these separate species in more recent studies, reducing the number of studies available for analysis. Second, we might not be able to determine whether trimester of pregnancy in which infection occurs results in different outcomes. Infections diagnosed in the third trimester might have been present throughout. Conversely, infections diagnosed early in pregnancy might already have been treated. We will take these factors into account when interpreting the findings.

    Studies that synthesise information about complications of STI and reproductive tract infections can be used in the estimation of the burden of disease. Until now, global burden of disease estimates of the burden of disease due to bacterial STI other than syphilis only include disability resulting from pelvic inflammatory disease and infertility. Ultimately, the findings of this review could help to improve decisions about both the prevention and clinical management of NG and genital mycoplasma infections in pregnancy.

    Ethics and dissemination

    We will present our results at an international medical conference that focuses on the prevention and treatment of STI. We will publish the results of this review in a peer reviewed, open access medical journal.

    References

    1. 1.
      2. Mullick S ,
      3. Watson-Jones D ,
      4. Beksinska M , et al
      . Sexually transmitted infections in pregnancy: prevalence, impact on pregnancy outcomes, and approach to treatment in developing countries. Sex Transm Infect 2005;81:294302.doi:10.1136/sti.2002.004077
      OpenUrlAbstract/FREE Full Text
    2. 2.
      2. Blas MM ,
      3. Canchihuaman FA ,
      4. Alva IE , et al
      . Pregnancy outcomes in women infected with Chlamydia trachomatis: a population-based cohort study in Washington State. Sex Transm Infect 2007;83:3148.doi:10.1136/sti.2006.022665
      OpenUrlAbstract/FREE Full Text
    3. 3.
      2. Cotch MF ,
      3. Pastorek JG ,
      4. Nugent RP , et al
      . Trichomonas vaginalis associated with low birth weight and preterm delivery. The Vaginal Infections and Prematurity Study Group. Sex Transm Dis 1997;24:35360.
      OpenUrlCrossRefPubMedWeb of Science
    4. 4.
      2. Gravett MG ,
      3. Nelson HP ,
      4. DeRouen T , et al
      . Independent associations of bacterial vaginosis and Chlamydia trachomatis infection with adverse pregnancy outcome. JAMA 1986;256:1899903.doi:10.1001/jama.1986.03380140069024
      OpenUrlCrossRefPubMedWeb of Science
    5. 5.
      2. Chow JM ,
      3. Kang MS ,
      4. Samuel MC , et al
      . Assessment of the association of chlamydia trachomatis infection and adverse perinatal outcomes with the use of population-based chlamydia case report registries and birth records. Public Health Rep 2009;124 Suppl 2:2430.doi:10.1177/00333549091240S205
      OpenUrl
    6. 6.
      2. Donders GG ,
      3. Desmyter J ,
      4. De Wet DH , et al
      . The association of gonorrhoea and syphilis with premature birth and low birthweight. Genitourin Med 1993;69:98101.doi:10.1136/sti.69.2.98
      OpenUrlPubMedWeb of Science
    7. 7.
      2. Elliott B ,
      3. Brunham RC ,
      4. Laga M , et al
      . Maternal gonococcal infection as a preventable risk factor for low birth weight. J Infect Dis 1990;161:5316.doi:10.1093/infdis/161.3.531
      OpenUrlCrossRefPubMed
    8. 8.
      2. Johnson HL ,
      3. Ghanem KG ,
      4. Zenilman JM , et al
      . Sexually transmitted infections and adverse pregnancy outcomes among women attending inner city public sexually transmitted diseases clinics. Sex Transm Dis 2011;38:16771.doi:10.1097/OLQ.0b013e3181f2e85f
      OpenUrlCrossRefPubMed
    9. 9.
      2. Rours GI ,
      3. Duijts L ,
      4. Moll HA , et al
      . Chlamydia trachomatis infection during pregnancy associated with preterm delivery: a population-based prospective cohort study. Eur J Epidemiol 2011;26:493502.doi:10.1007/s10654-011-9586-1
      OpenUrlCrossRefPubMed
    10. 10.
      2. Hitti J ,
      3. Garcia P ,
      4. Totten P , et al
      . Correlates of cervical Mycoplasma genitalium and risk of preterm birth among Peruvian women. Sex Transm Dis 2010;37:815.doi:10.1097/OLQ.0b013e3181bf5441
      OpenUrlCrossRefPubMed
    11. 11.
      2. Beem MO ,
      3. Saxon EM
      . Respiratory-tract colonization and a distinctive pneumonia syndrome in infants infected with Chlamydia trachomatis. N Engl J Med 1977;296:30610.doi:10.1056/NEJM197702102960604
      OpenUrlCrossRefPubMedWeb of Science
    12. 12.
      2. Donders GGG ,
      3. Ruban K ,
      4. Bellen G , et al
      . Mycoplasma/Ureaplasma infection in pregnancy: to screen or not to screen. J Perinat Med 2017;45:50515.doi:10.1515/jpm-2016-0111
      OpenUrl
    13. 13.
      2. Horner P ,
      3. Donders G ,
      4. Cusini M , et al
      . Should we be testing for urogenital mycoplasma hominis, ureaplasma parvum and ureaplasma urealyticum in men and women? - a position statement from the European STI guidelines editorial board. J Eur Acad Dermatol Venereol 2018;32:184551.doi:10.1111/jdv.15146
      OpenUrl
    14. 14.
      2. Minkoff H ,
      3. Grunebaum AN ,
      4. Schwarz RH , et al
      . Risk factors for prematurity and premature rupture of membranes: a prospective study of the vaginal flora in pregnancy. Am J Obstet Gynecol 1984;150:96572.doi:10.1016/0002-9378(84)90392-2
      OpenUrlCrossRefPubMedWeb of Science
    15. 15.
      2. Taylor-Robinson D ,
      3. Lamont RF
      . Mycoplasmas in pregnancy. BJOG 2011;118:16474.doi:10.1111/j.1471-0528.2010.02766.x
      OpenUrlCrossRefPubMed
    16. 16.
      2. Saha SK ,
      3. Schrag SJ ,
      4. El Arifeen S , et al
      . Causes and incidence of community-acquired serious infections among young children in south Asia (ANISA): an observational cohort study. Lancet 2018;392:14559.doi:10.1016/S0140-6736(18)31127-9
      OpenUrl
    17. 17.
      2. Cassell GH ,
      3. Waites KB ,
      4. Watson HL , et al
      . Ureaplasma urealyticum intrauterine infection: role in prematurity and disease in newborns. Clin Microbiol Rev 1993;6:6987.doi:10.1128/CMR.6.1.69
      OpenUrlAbstract/FREE Full Text
    18. 18.
      2. Kataoka S ,
      3. Yamada T ,
      4. Chou K , et al
      . Association between preterm birth and vaginal colonization by mycoplasmas in early pregnancy. J Clin Microbiol 2006;44:515.doi:10.1128/JCM.44.1.51-55.2006
      OpenUrlAbstract/FREE Full Text
    19. 19.
      WHO. Investment case for eliminating mother-to-child transmission of syphilis: Promoting better maternal and child health and stronger health system. Geneva: World Health Organization, 2012.
    20. 20.
      2. McDermott J ,
      3. Steketee R ,
      4. Larsen S , et al
      . Syphilis-associated perinatal and infant mortality in rural Malawi. Bull World Health Organ 1993;71:77380.
      OpenUrlPubMedWeb of Science
    21. 21.
      2. Newman L ,
      3. Kamb M ,
      4. Hawkes S , et al
      . Global estimates of syphilis in pregnancy and associated adverse outcomes: analysis of multinational antenatal surveillance data. PLoS Med 2013;10:e1001396.doi:10.1371/journal.pmed.1001396
      OpenUrlCrossRefPubMed
    22. 22.
      WHO. Sexually Transmitted Infections Fact Sheet No. 110. Geneva: World Health Organization, 2013.
    23. 23.
      2. Silva MJ ,
      3. Florêncio GL ,
      4. Gabiatti JR , et al
      . Perinatal morbidity and mortality associated with chlamydial infection: a meta-analysis study. Braz J Infect Dis 2011;15:5339.doi:10.1590/S1413-86702011000600006
      OpenUrlCrossRefPubMed
    24. 24.
      2. Silver BJ ,
      3. Guy RJ ,
      4. Kaldor JM , et al
      . Trichomonas vaginalis as a cause of perinatal morbidity: a systematic review and meta-analysis. Sex Transm Dis 2014;41:36976.doi:10.1097/OLQ.0000000000000134
      OpenUrlCrossRefPubMed
    25. 25.
      2. Lis R ,
      3. Rowhani-Rahbar A ,
      4. Manhart LE
      . Mycoplasma genitalium infection and female reproductive tract disease: a meta-analysis. Clin Infect Dis 2015;61:41826.doi:10.1093/cid/civ312
      OpenUrlCrossRefPubMed
    26. 26.
      2. Mao J ,
      3. Tang W ,
      4. Fu R , et al
      . Adverse outcomes associated with Chlamydia trachomatis infection in women: a systematic review and meta-analysis: PROSPERO: CRD42017056818. 2017.
    27. 27.
      2. Brocklehurst P ,
      3. Gordon A ,
      4. Heatley E , et al
      . Antibiotics for treating bacterial vaginosis in pregnancy. Cochrane Database Syst Rev 2013;1:CD000262.doi:10.1002/14651858.CD000262.pub4
      OpenUrlCrossRefPubMed
    28. 28.
      2. Leli C ,
      3. Mencacci A ,
      4. Latino MA , et al
      . Prevalence of cervical colonization by Ureaplasma parvum, Ureaplasma urealyticum, Mycoplasma hominis and Mycoplasma genitalium in childbearing age women by a commercially available multiplex real-time PCR: An Italian observational multicentre study. J Microbiol Immunol Infect 2018;51:2205.doi:10.1016/j.jmii.2017.05.004
      OpenUrl
    29. 29.
      2. Shamseer L ,
      3. Moher D ,
      4. Clarke M , et al
      . Preferred reporting items for systematic review and meta-analysis protocols (PRISMA-P) 2015: elaboration and explanation. BMJ 2015;349:g7647.doi:10.1136/bmj.g7647
      OpenUrlAbstract/FREE Full Text
    30. 30.
      2. Blencowe H ,
      3. Cousens S ,
      4. Oestergaard MZ , et al
      . National, regional, and worldwide estimates of preterm birth rates in the year 2010 with time trends since 1990 for selected countries: a systematic analysis and implications. Lancet 2012;379:216272.doi:10.1016/S0140-6736(12)60820-4
      OpenUrlCrossRefPubMedWeb of Science
    31. 31.
      WHO. ICD-10: Version 2010. Geneva: World Health Organization, 2010.
    32. 32.
      NICE. Methods for the development of NICE public health guidance (third edition): Process and methods. UK: National Institute for Health and Care Excellence, 2012.
    33. 33.
      NICE. The social care guidance manual: Process and methods. UK: National Institute for Health and Care Excellence, 2013.
    34. 34.
      2. Higgins JP ,
      3. Thompson SG ,
      4. Deeks JJ , et al
      . Measuring inconsistency in meta-analyses. BMJ 2003;327:55760.doi:10.1136/bmj.327.7414.557
      OpenUrlFREE Full Text
    35. 35.
      2. Riley RD ,
      3. Higgins JP ,
      4. Deeks JJ
      . Interpretation of random effects meta-analyses. BMJ 2011;342:d549.doi:10.1136/bmj.d549
      OpenUrlFREE Full Text
    36. 36.
      2. Begg CB ,
      3. Mazumdar M
      . Operating characteristics of a rank correlation test for publication bias. Biometrics 1994;50:1088101.doi:10.2307/2533446
      OpenUrlCrossRefPubMedWeb of Science
    37. 37.
      2. Guyatt GH ,
      3. Oxman AD ,
      4. Sultan S , et al
      . GRADE guidelines: 9. Rating up the quality of evidence. J Clin Epidemiol 2011;64:13116.doi:10.1016/j.jclinepi.2011.06.004
      OpenUrlCrossRefPubMed

    Footnotes

    • LMV and DE-G contributed equally.

    • Contributors LMV is the guarantor of the protocol manuscript. LMV, DE-G, NL and AJV conceived the study and developed the review protocol. CSEH gave advice about the pregnancy outcomes. NL gave advice about the infection outcomes and systematic review methods. HW reviewed and advised on the statistical analyses. LV wrote the first draft of the manuscript. DE-G, NL and AJV helped to revise the manuscript. WP, RG, HW, CSEH, BS, AR and JMK contributed to the development and design of the protocol and in revising the manuscript. All authors read, provided feedback and approved the final manuscript.

    • Funding LMV receives salary support from the Australian National Health and Medical Research Council (NHMRC), through an early career fellowship. DE-G received salary support from r4d programme (Swiss Programme for Research on Global Issues for Development), grant number IZ07Z0-160909. These funders played no role in the development of the protocol or the planned analyses.

    • Competing interests None declared.

    • Patient consent Not required.

    • Ethics approval This systematic review does not use individual personal data and therefore does not require ethical committee approval.

    • Provenance and peer review Not commissioned; externally peer reviewed.