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Free fetal haemoglobin in an early onset fetal growth restriction cohort (EVERREST) threatens placental function: A prospective multi-centre study Short version title: Free fetal haemoglobin in severe FGR
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  • Adam Brook,
  • Georgia BAYNES,
  • Jonathan SCARGILL,
  • Angelos EVANGELINOS,
  • Charlotte BRENNAN-RICHARDSON,
  • Freya DOW,
  • Yuval GINSBERG,
  • Tal Weissbach,
  • Jana Brodszki,
  • Eva HANSSON,
  • Anke Diemert,
  • Kurt Hecher,
  • Katarzyna MAKSYM,
  • Neil Marlow,
  • Rebecca Spencer,
  • Anna David,
  • Stefan Hansson,
  • Paul BROWNBILL
Adam Brook
University of Manchester
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Georgia BAYNES
University of Manchester
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Jonathan SCARGILL
Northern Care Alliance NHS Foundation Trust Oldham Care Organisation
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Angelos EVANGELINOS
University of Manchester
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Charlotte BRENNAN-RICHARDSON
University of Manchester
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Freya DOW
University of Manchester
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Yuval GINSBERG
Rambam Medical Centre
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Tal Weissbach
Sheba Medical Center
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Jana Brodszki
Institute of Clinical Sciences Lund Lund University and Skåne University Hospital
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Eva HANSSON
Institute of Clinical Sciences Lund Lund University and Skåne University Hospital
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Anke Diemert
University Medical Center Hamburg-Eppendorf
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Kurt Hecher
University Medical Center Hamburg-Eppendorf
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Katarzyna MAKSYM
University College London Elizabeth Garrett Anderson Institute for Women's Health
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Neil Marlow
University College London Elizabeth Garrett Anderson Institute for Women's Health
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Rebecca Spencer
University College London Elizabeth Garrett Anderson Institute for Women's Health
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Anna David
University College London Elizabeth Garrett Anderson Institute for Women's Health
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Stefan Hansson
Institute of Clinical Sciences Lund Lund University and Skåne University Hospital
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Paul BROWNBILL
University of Manchester

Corresponding Author:paul.brownbill@manchester.ac.uk

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Abstract

Objectives: To assess fetal circulating free fetal haemoglobin (fHbF) levels and heme defences, correlated to fetal circulatory biometry and fetal sex in severe early-onset fetal growth restriction. Design, Setting & Population: A prospective study severe early-onset fetal growth restriction pregnancies with close clinical management (EFW<3 rd centile and <600g at 20-26+6 weeks; N=20). Method & Main Outcome Measures: Temporal fetal vascular obstetric biometry was recorded. Cord blood fHbF and key heme-scavenger defences were measured and compared with normal term births (N=26) and births with late-onset FGR (N=12). Results: fHbF was elevated in early-onset FGR compared with normal pregnancy: 0.437(0.337/0.753) mg/mL; P<0.0001; 0.098(0.045/0.264) mg/mL; P<0.0001), respectively; whilst hemopexin was downregulated in early- and late-onset FGR compared to normal pregnancy: 36(14/81) μg/mL, P<0.001; 25(19/40) μg/mL, P<0.0001; 155(132/219) μg/mL, respectively; median(interquartile ranges). Early-onset FGR male fetuses had higher fetal haemoglobin compared with the normal males: 0.710(0.433/0.857) mg/mL; P<0.001; 0.099(0.043/0.246) mg/mL, respectively; median(interquartile ranges). In early-onset FGR, ratios of mid-cerebral artery and umbilical artery pulsatility indices correlated positively with heme-scavenger levels (hemopexin and a heme-handling composite measure: P<0.05 and P<0.01, respectively), indicating lower levels are associated with cerebral vascular redistribution. These heme handling measures also positively correlated with gestational age at delivery (P<0.01, both) and birthweight (P<0.001 and P<0.05, respectively). Conclusion: Free fetal haemoglobin overproduction may be one route to placental vascular compromise in early-onset FGR, implicated in reduced placental and fetal blood flow.
11 Sep 2024Submitted to BJOG: An International Journal of Obstetrics and Gynaecology
13 Sep 2024Submission Checks Completed
13 Sep 2024Assigned to Editor
13 Sep 2024Review(s) Completed, Editorial Evaluation Pending
04 Oct 2024Reviewer(s) Assigned
13 Nov 2024Editorial Decision: Revise Major