TY - JOUR
T1 - Interventions affecting the nitric oxide pathway versus placebo or no therapy for fetal growth restriction in pregnancy
AU - Pels, Anouk
AU - Ganzevoort, Wessel
AU - Kenny, Louise C.
AU - Baker, Philip N.
AU - von Dadelszen, Peter
AU - Gluud, Christian
AU - Kariya, Chirag T.
AU - Leemhuis, Aleid G.
AU - Groom, Katie M.
AU - Sharp, Andrew N.
AU - Magee, Laura A.
AU - Jakobsen, Janus C.
AU - Mol, Ben Willem J.
AU - Papageorghiou, Aris T.
N1 - Funding Information: -Trial funding: the trial was funded by the Netherlands Organization for Health Research and Development (project No. 836021023). Funding Information: As part of the pre-publication editorial process, this protocol has been commented on by three peers (an editor and two referees who are external to the editorial team). This project was supported by the National Institute for Health Research (NIHR), via Cochrane Infrastructure funding to Cochrane Pregnancy and Childbirth. The views and opinions expressed therein are those of the review authors and do not necessarily reflect those of the Evidence Synthesis Programme, the NIHR, National Health Service (NHS) or the Department of Health and Social Care. We thank Nia Roberts for her contribution to the published protocol for this review. Funding Information: -Trial funding: this report is independent research funded by the Medical Research Council (MRC) and managed by the National Institute for Health Research (NIHR) on behalf of the MRC–NIHR partnership. The views expressed in this publication are those of the authors and not necessarily those of the MRC, National Health Service, NIHR, or the Department of Health. Funding Information: -Trial funding: Italian National Research Council (CNR) and the Ministry of University and Scientific Research (MIUR) Funding Information: -Trial funding: this work was supported by the Japan Agency for Medical Research and Development (AMED) as part of the Project for Baby and Infant in Research of Health and Development to Adolescent and Young Adults, by the Japan Society for the Promotion of Science KAKENHI (Grant Number 17K16846), and in part by the Takeda Science Foundation. Funding Information: Aris T Papageorghiou: I am employed as a consultant in the NHS; and as an academic at the U niversity. I also provide obstetric ultrasound in the private health sector. My research is mostly funded by public bodies, research councils, foundations and charities in the U K, Europe and U SA (currently: HTA/NIHR; EPSRC/NIHR; RCU K/GCRF; NIHR/BRC; ERC; NIH; Bill & Melinda Gates Foundation). The NIHR funded the Maternal sildenafil for severe fetal growth restriction (STRIDER) trial, and this Cochrane review was conceived and planned during a STRIDER meeting, but not funded directly. I have previously participated in research where companies contributed to a grant (GE, Philips, Samsung, Premaitha Health). As an academic I oOen participate in research meetings at other hospitals or universities; these are unpaid but travel to attend meetings is usually provided. Some of these were sponsored by industry to the host institutions (Roche, Philips, Samsung, GE). I participate as a speaker in educational events that have, on occasion, received industrial sponsorship to cover travel, accomodation and honoraria. I receive royalties for medical text-books I have published (Informa Healthcare, Oxford U niversity Press). I am a co-founder, shareholder, and senior scientific advisor for Intelligent U ltrasound, a company that aims to improve clinical ultrasound. For this I receive payments, managed through Oxford U niversity Innovations, a subsidiary of the U niversity of Oxford that manages technology transfer and academic consultingactivities. Finally, I am a Editor-in-Chief for BJOG, for which I am paid a stipend; VisitingProfessor at BeijingCapital U niversity (not remunerated); a board member of the journal U ltrasound in Obstetrics and Gynecology (not remunerated); and Chair of the Expert Working Group, Obs & Gyn, Health & Social Care Information Centre (not remunerated). He reports not being involved in any decisionsrelatingtothestudy(inclusion/exclusion,riskofbias,dataextraction,GRADE)andthesetaskswerecarriedoutbyothermembers of the review team who were not directly involved in the U K STRIDER trial. Funding Information: -Trial funding: Canadian Institutes of Health Research (Grant Number: MOP-137077) Funding Information: Louise C Kenny is Executive Pro-Vice Chancellor of the Faculty of Health and Life Sciences at the U niversity of Liverpool and Professor of Maternal and Fetal Health and as such has numerous grant applications under review at any given time. Anouk Pels: has been paid by Alere to give invited symposia on a proprietary screeningtest for preeclampsia. She is the editor of Ten Teachers and has received royalties from the publishers. She is also a limited shareholder in Metabolomic Diagnostics, an SME who have licensed technology that she has developed pertaining to the screening of preeclampsia. She is a co-investigator for the U K STRIDER trial, funded by the National Institute for Health Research and Medical Research Council. She reports not being involved in any decisions relating to the study (inclusion/exclusion, risk of bias, data extraction, GRADE) and these tasks were carried out by other members of the review team who were not directly involved in the U K STRIDER trial. Funding Information: -Trial funding: this study is funded by the Research Foundation (Project No. 200697) of Henan - Provincial Health Authority. Funding Information: Aris T. Papageorghiou is supported by the NIHR BRC Funding Information: -Trial funding: this study was supported by the Delegation a la Recherche Clinique (DRC) of the U niver-sity Medical Center of Nantes (CHU de Nantes), and we thank Veyron France Laboratories for supplying ARG and placebo. Funding Information: -Trial funding: the trial was funded by the Health Research Council of New Zealand (13/242) with additional support from Cure Kids (3565), both grants were awarded through external peer reviewed processes. The funders had no role in trial design; data collection, analysis, or interpretation; or writing of the report. Funding Information: Chirag T Kariya: CTK is is a co-investigator for the Canadian STRIDER trial, funded by Canadian Institute of Health Research (CIHR) grant to the U niversity of British Columbia that included support to travel to meetings for the study, conducting study related activities and salary support. They report not being involved in any decisions relating to the study (inclusion/exclusion, risk of bias, data extraction, GRADE) and these tasks were carried out by other members of the review team who were not directly involved in the Canadian STRIDER trial. Publisher Copyright: Copyright © 2023 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd.
PY - 2023/7/10
Y1 - 2023/7/10
N2 - Background: Fetal growth restriction (FGR) is a condition of poor growth of the fetus in utero. One of the causes of FGR is placental insufficiency. Severe early-onset FGR at < 32 weeks of gestation occurs in an estimated 0.4% of pregnancies. This extreme phenotype is associated with a high risk of fetal death, neonatal mortality, and neonatal morbidity. Currently, there is no causal treatment, and management is focused on indicated preterm birth to prevent fetal death. Interest has risen in interventions that aim to improve placental function by administration of pharmacological agents affecting the nitric oxide pathway causing vasodilatation. Objectives: The objective of this systematic review and aggregate data meta-analysis is to assess the beneficial and harmful effects of interventions affecting the nitric oxide pathway compared with placebo, no therapy, or different drugs affecting this pathway against each other, in pregnant women with severe early-onset FGR. Search methods: We searched Cochrane Pregnancy and Childbirth’s Trials Register, ClinicalTrials.gov, the WHO International Clinical Trials Registry Platform (ICTRP) (16 July 2022), and reference lists of retrieved studies. Selection criteria: We considered all randomised controlled comparisons of interventions affecting the nitric oxide pathway compared with placebo, no therapy, or another drug affecting this pathway in pregnant women with severe early-onset FGR of placental origin, for inclusion in this review. Data collection and analysis: We used standard Cochrane Pregnancy and Childbirth methods for data collection and analysis. Main results: We included a total of eight studies (679 women) in this review, all of which contributed to the data and analysis. The identified studies report on five different comparisons: sildenafil compared with placebo or no therapy, tadalafil compared with placebo or no therapy, L-arginine compared with placebo or no therapy, nitroglycerin compared with placebo or no therapy and sildenafil compared with nitroglycerin. The risk of bias of included studies was judged as low or unclear. In two studies the intervention was not blinded. The certainty of evidence for our primary outcomes was judged as moderate for the intervention sildenafil and low for tadalafil and nitroglycerine (due to low number of participants and low number of events). For the intervention L-arginine, our primary outcomes were not reported. Sildenafil citrate compared to placebo or no therapy (5 studies, 516 women). Five studies (Canada, Australia and New Zealand, the Netherlands, the UK and Brazil) involving 516 pregnant women with FGR were included. We assessed the certainty of the evidence as moderate. Compared with placebo or no therapy, sildenafil probably has little or no effect on all-cause mortality (risk ratio (RR) 1.01, 95% confidence interval (CI) 0.80 to 1.27, 5 studies, 516 women); may reduce fetal mortality (RR 0.82, 95% CI 0.60 to 1.12, 5 studies, 516 women), and increase neonatal mortality (RR 1.45, 95% CI 0.90 to 2.33, 5 studies, 397 women), although the results are uncertain for fetal and neonatal mortality as 95% confidence intervals are wide crossing the line of no effect. Tadalafil compared with placebo or no therapy (1 study, 87 women). One study (Japan) involving 87 pregnant women with FGR was included. We assessed the certainty of the evidence as low. Compared with placebo or no therapy, tadalafil may have little or no effect on all-cause mortality (risk ratio 0.20, 95% CI 0.02 to 1.60, one study, 87 women); fetal mortality (RR 0.11, 95% CI 0.01 to 1.96, one study, 87 women); and neonatal mortality (RR 0.89, 95% CI 0.06 to 13.70, one study, 83 women). L-Arginine compared with placebo or no therapy (1 study, 43 women). One study (France) involving 43 pregnant women with FGR was included. This study did not assess our primary outcomes. Nitroglycerin compared to placebo or no therapy (1 studies, 23 women). One study (Brazil) involving 23 pregnant women with FGR was included. We assessed the certainty of the evidence as low. The effect on the primary outcomes is not estimable due to no events in women participating in both groups. Sildenafil citrate compared to nitroglycerin (1 study, 23 women). One study (Brazil) involving 23 pregnant women with FGR was included. We assessed the certainty of the evidence as low. The effect on the primary outcomes is not estimable due to no events in women participating in both groups. Authors' conclusions: Interventions affecting the nitric oxide pathway probably do not seem to influence all-cause (fetal and neonatal) mortality in pregnant women carrying a baby with FGR, although more evidence is needed. The certainty of this evidence is moderate for sildenafil and low for tadalafil and nitroglycerin. For sildenafil a fair amount of data are available from randomised clinical trials, but with low numbers of participants. Therefore, the certainty of evidence is moderate. For the other interventions investigated in this review there are insufficient data, meaning we do not know whether these interventions improve perinatal and maternal outcomes in pregnant women with FGR.
AB - Background: Fetal growth restriction (FGR) is a condition of poor growth of the fetus in utero. One of the causes of FGR is placental insufficiency. Severe early-onset FGR at < 32 weeks of gestation occurs in an estimated 0.4% of pregnancies. This extreme phenotype is associated with a high risk of fetal death, neonatal mortality, and neonatal morbidity. Currently, there is no causal treatment, and management is focused on indicated preterm birth to prevent fetal death. Interest has risen in interventions that aim to improve placental function by administration of pharmacological agents affecting the nitric oxide pathway causing vasodilatation. Objectives: The objective of this systematic review and aggregate data meta-analysis is to assess the beneficial and harmful effects of interventions affecting the nitric oxide pathway compared with placebo, no therapy, or different drugs affecting this pathway against each other, in pregnant women with severe early-onset FGR. Search methods: We searched Cochrane Pregnancy and Childbirth’s Trials Register, ClinicalTrials.gov, the WHO International Clinical Trials Registry Platform (ICTRP) (16 July 2022), and reference lists of retrieved studies. Selection criteria: We considered all randomised controlled comparisons of interventions affecting the nitric oxide pathway compared with placebo, no therapy, or another drug affecting this pathway in pregnant women with severe early-onset FGR of placental origin, for inclusion in this review. Data collection and analysis: We used standard Cochrane Pregnancy and Childbirth methods for data collection and analysis. Main results: We included a total of eight studies (679 women) in this review, all of which contributed to the data and analysis. The identified studies report on five different comparisons: sildenafil compared with placebo or no therapy, tadalafil compared with placebo or no therapy, L-arginine compared with placebo or no therapy, nitroglycerin compared with placebo or no therapy and sildenafil compared with nitroglycerin. The risk of bias of included studies was judged as low or unclear. In two studies the intervention was not blinded. The certainty of evidence for our primary outcomes was judged as moderate for the intervention sildenafil and low for tadalafil and nitroglycerine (due to low number of participants and low number of events). For the intervention L-arginine, our primary outcomes were not reported. Sildenafil citrate compared to placebo or no therapy (5 studies, 516 women). Five studies (Canada, Australia and New Zealand, the Netherlands, the UK and Brazil) involving 516 pregnant women with FGR were included. We assessed the certainty of the evidence as moderate. Compared with placebo or no therapy, sildenafil probably has little or no effect on all-cause mortality (risk ratio (RR) 1.01, 95% confidence interval (CI) 0.80 to 1.27, 5 studies, 516 women); may reduce fetal mortality (RR 0.82, 95% CI 0.60 to 1.12, 5 studies, 516 women), and increase neonatal mortality (RR 1.45, 95% CI 0.90 to 2.33, 5 studies, 397 women), although the results are uncertain for fetal and neonatal mortality as 95% confidence intervals are wide crossing the line of no effect. Tadalafil compared with placebo or no therapy (1 study, 87 women). One study (Japan) involving 87 pregnant women with FGR was included. We assessed the certainty of the evidence as low. Compared with placebo or no therapy, tadalafil may have little or no effect on all-cause mortality (risk ratio 0.20, 95% CI 0.02 to 1.60, one study, 87 women); fetal mortality (RR 0.11, 95% CI 0.01 to 1.96, one study, 87 women); and neonatal mortality (RR 0.89, 95% CI 0.06 to 13.70, one study, 83 women). L-Arginine compared with placebo or no therapy (1 study, 43 women). One study (France) involving 43 pregnant women with FGR was included. This study did not assess our primary outcomes. Nitroglycerin compared to placebo or no therapy (1 studies, 23 women). One study (Brazil) involving 23 pregnant women with FGR was included. We assessed the certainty of the evidence as low. The effect on the primary outcomes is not estimable due to no events in women participating in both groups. Sildenafil citrate compared to nitroglycerin (1 study, 23 women). One study (Brazil) involving 23 pregnant women with FGR was included. We assessed the certainty of the evidence as low. The effect on the primary outcomes is not estimable due to no events in women participating in both groups. Authors' conclusions: Interventions affecting the nitric oxide pathway probably do not seem to influence all-cause (fetal and neonatal) mortality in pregnant women carrying a baby with FGR, although more evidence is needed. The certainty of this evidence is moderate for sildenafil and low for tadalafil and nitroglycerin. For sildenafil a fair amount of data are available from randomised clinical trials, but with low numbers of participants. Therefore, the certainty of evidence is moderate. For the other interventions investigated in this review there are insufficient data, meaning we do not know whether these interventions improve perinatal and maternal outcomes in pregnant women with FGR.
UR - http://www.scopus.com/inward/record.url?scp=85164290606&partnerID=8YFLogxK
U2 - https://doi.org/10.1002/14651858.CD014498
DO - https://doi.org/10.1002/14651858.CD014498
M3 - Review article
C2 - 37428872
SN - 1465-1858
VL - 2023
JO - Cochrane Database of Systematic Reviews
JF - Cochrane Database of Systematic Reviews
IS - 7
M1 - CD014498
ER -