Standard care informed by the result of a placental growth factor blood test versus standard care alone in women with reduced fetal movement at or after 36+0 weeks' gestation: a pilot randomised controlled trial

Lindsay Armstrong-Buisseret; Peter J Godolphin; Lucy Bradshaw; Eleanor Mitchell; Sam Ratcliffe; Claire Storey; Alexander E P Heazell

doi:10.1186/s40814-020-0561-z

Standard care informed by the result of a placental growth factor blood test versus standard care alone in women with reduced fetal movement at or after 36⁺⁰ weeks' gestation: a pilot randomised controlled trial

Pilot Feasibility Stud. 2020 Feb 13:6:23. doi: 10.1186/s40814-020-0561-z. eCollection 2020.

Authors

Lindsay Armstrong-Buisseret¹, Peter J Godolphin¹, Lucy Bradshaw¹, Eleanor Mitchell¹, Sam Ratcliffe², Claire Storey³, Alexander E P Heazell^{2

4}

Affiliations

¹ 1Nottingham Clinical Trials Unit (NCTU), Building 42, University of Nottingham, University Park, Nottingham, NG7 2RD UK.
² 2Maternal and Fetal Health Research Centre, 5th Floor (Research), St Mary's Hospital, Oxford Road, Manchester, M13 9WL UK.
³ 3International Stillbirth Alliance, c/o Maternal and Fetal Health Research Centre, 5th Floor (Research,), St Mary's Hospital, Oxford Road, Manchester, M13 9WL UK.
⁴ 4St. Mary's Hospital, Manchester University Hospitals NHS Foundation Trust, Manchester Academic Health Science Centre, Manchester, M13 9WL UK.

Abstract

Background: Biomarkers of placental function can potentially aid the diagnosis and prediction of pregnancy complications. This randomised controlled pilot trial assessed whether for women with reduced fetal movement (RFM), intervention directed by the measurement of a placental biomarker in addition to standard care was feasible and improved pregnancy outcome compared with standard care alone.

Methods: Women aged 16-50 years presenting at eight UK maternity units with RFM between 36⁺⁰ and 41⁺⁰ weeks' gestation with a viable singleton pregnancy and no indication for immediate delivery were eligible. Participants were randomised 1:1 in an unblinded manner to standard care and a biomarker blood test result revealed and acted on (intervention arm) or standard care where the biomarker result was not available (control arm). The objectives were to determine the feasibility of a main trial by recruiting 175-225 participants over 9 months and to provide proof of concept that informing care by measurement of placental biomarkers may improve outcome. Feasibility was assessed via the number of potentially eligible women, number recruited, reasons for non-recruitment and compliance. Proof of concept outcomes included the rates of the induction of labour and caesarean birth, and a composite adverse pregnancy outcome.

Results: Overall, 2917 women presented with RFM ≥ 36 weeks, 352 were approached to participate and 216 (61%) were randomised (intervention n = 109, control n = 107). The main reason for not approaching women was resource/staff issues (n = 1510). Ninety-seven women declined the trial, mainly due to not liking blood tests (n = 24) or not wanting to be in a trial (n = 21). Compliance with the trial interventions was 100% in both arms. Labour was induced in 97 (45%) participants (intervention n = 49, control n = 48), while 17 (9%) had planned caesarean sections (intervention n = 9, control n = 8). Overall, 9 (8%) babies in the intervention arm had the composite adverse pregnancy outcome versus 4 (4%) in the control arm.

Conclusions: A main trial using a placental biomarker in combination with delivery, as indicated by the biomarker, in women with RFM is feasible. The frequency of adverse outcomes in this population is low, hence, a large sample size would be required along with consideration of the most appropriate outcome measures.

Trial registration: ISRCTN, ISRCTN12067514; registered 8 September 2017.

Keywords: Adverse pregnancy outcome; Feasibility study; Placental biomarker; Placental dysfunction; Reduced fetal movement; sFlt-1/PlGF ratio.

Grants and funding

CS-2013-13-009/DH_/Department of Health/United Kingdom