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Clinical Trial Details — Status: Not yet recruiting

Administrative data

NCT number NCT06200571
Other study ID # 537602
Secondary ID
Status Not yet recruiting
Phase
First received
Last updated
Start date March 1, 2024
Est. completion date December 31, 2032

Study information

Verified date December 2023
Source Norwegian University of Science and Technology
Contact Åse Turid R Svoren, PhD candidate
Phone +4795701611
Email ase.turid.rossevatn.svoren@helse-mr.no
Is FDA regulated No
Health authority
Study type Observational

Clinical Trial Summary

Primary outcome 1. to identify biological changes in nulliparous women at high risk for preeclampsia defined by combined screening by Fetal Medicine Foundation (FMF) 2. to identify biological effects of aspirin in nulliparous women with high risk for preeclampsia Secondary outcomes include findings of longitudinal development and predictive potential of biological markers associated with high-risk for preeclampsia and aspirin treatment. The main questions it aims to answer are: - Is high risk for preeclampsia associated with biological changes during pregnancy? - How does aspirin modulate the biological changes associated with high risk for preeclampsia? Nulliparous women will undergo routine clinical care at two regional hospitals with different treatment strategies, and selected to the study in three groups: low risk of preeclampsia, high risk of preeclampsia without aspirin, and high-risk of preeclampsia with aspirin treatment.


Description:

St. Olavs Hospital offers FMF-screening in week 11-14 and aspirin treatment through the "Implementing Screening for Preeclampsia in Norway With Aspirin Discontinuation at 24-28 Weeks - a Randomized Controlled Trial" (NCT06108947). FMF-screening and aspirin treatment are not part of routine clinical care at Alesund Hospital according to current recommendations from the Norwegian health authorities. Alesund Hospital will therefore perform FMF-screening only to determine the project specific study groups. Researchers will compare the three groups to identify biological changes associated with high risk for preeclampsia and the effect of aspirin. FMF- screening will be performed in week 11-14 after written, informed consent (approved by the the Regional Committee for Medical and Health Research Ethics in Central Norway (REK-midt), REK 537602). Screening includes patient history, blood pressure, uterine artery mean pulsatile index and serum placenta growth factor (PlGF). Standardized blood pressure will be measured by trained personnel. Ultrasound scans will be performed by FMF certified doctors and midwives working at Alesund Hospital and the Center for Fetal Medicine at St.Olavs Hospital in Trondheim. PlGF in maternal serum will be analyzed with Roche or Kryptor technology. The investigators will include around 200 women, 18 years or older, with a singleton live fetus, in three groups: - Nulliparous women with low risk for preeclampsia (at both hospitals) - Nulliparous women with high risk for preeclampsia without aspirin (at Alesund Hospital) - Nulliparous women with high risk for preeclampsia with aspirin (at St. Olavs Hospital) Follow-up: all three groups will have visits in week 22-24, 32 and 38, and standard antenatal care after 37 weeks until delivery. Fetal growth and Doppler will be assessed at the scheduled visits and according to clinical judgement by obstetricians at the outpatient clinic of the hospital. Women will have follow-up 6 months after birth. Blood and urine will be sampled at five time points for all three groups (week 11-14, 22-24, 32, 38 and 6 months after birth) for biological analyses. Placenta samples and umbilical venous blood will be sampled at delivery. Biological materials will be investigated to answer the research questions described. Biological changes in serum will be measured as cytokines by multiplex, metabolites by NMR-analysis, and lipids by NMR-analysis. Vascular changes in the placenta will be measured by histopathological evaluation. The study will be registered in Clinicaltrials.gov Funding and sponsors: The study is funded by Helse-Midt Norge RHF. The funding source has played no role in design of the study and will have no role in data collection, analyses, interpretation or publication. Participants: Ann-Charlotte Iversen, professor, Phd, Project leader Åse Turid Rossevatn Svoren, consultant, MD, Phd candidate, Kjell Åsmund Salvesen, professor, MD, PhD, Solveig Bjellmo, consultant, MD, Phd


Recruitment information / eligibility

Status Not yet recruiting
Enrollment 200
Est. completion date December 31, 2032
Est. primary completion date December 31, 2026
Accepts healthy volunteers Accepts Healthy Volunteers
Gender Female
Age group 18 Years and older
Eligibility Inclusion Criteria: - 18 years or older - nulliparous women - singleton live fetus - FMF risk > 1/100 (high risk), or < 1/150 (low risk) Exclusion Criteria: - not speaking Norwegian or English language - fetal anomalies diagnosed with ultrasound

Study Design


Related Conditions & MeSH terms


Locations

Country Name City State
Norway Alesund Hospital Ålesund
Norway St. Olavs Hospital Trondheim

Sponsors (3)

Lead Sponsor Collaborator
Norwegian University of Science and Technology Alesund Hospital, St. Olavs Hospital

Country where clinical trial is conducted

Norway, 

Outcome

Type Measure Description Time frame Safety issue
Primary Maternal serum cytokine profile in week 11-13, 22-24, 32 and 38 and 6 months post partum Significant difference between low and high-risk pregnancies defined by FMF-screening December 2028
Primary Maternal serum cytokine profile in week 11-13, 22-24, 32 and 38 and 6 months post partum Significant difference between high-risk pregnancies with and without aspirin December 2028
Secondary Maternal serum metabolite profile in week 11-13, 22-24, 32 and 38 and 6 months post partum Significant difference between low and high-risk pregnancies defined by FMF-screening December 2028
Secondary Maternal serum lipid profile in week 11-13, 22-24, 32 and 38 and 6 months post partum Significant difference between low and high-risk pregnancies defined by FMF-screening December 2028
Secondary Maternal serum metabolite profile in week 11-13, 22-24, 32 and 38 and 6 months post partum Significant difference between high-risk pregnancies with and without aspirin December 2028
Secondary Maternal serum lipid profile in week 11-13, 22-24, 32 and 38 and 6 months post partum Significant difference between high-risk pregnancies with and without aspirin December 2028
Secondary Maternal vascular malperfusion in the placenta Significant difference between low and high-risk pregnancies defined by FMF-screening December 2028
Secondary Fetal vascular malperfusion in the placenta Significant difference between low and high-risk pregnancies defined by FMF-screening December 2028
Secondary Maternal vascular malperfusion in the placenta Significant difference between high-risk pregnancies with and without aspirin December 2028
Secondary Fetal vascular malperfusion in the placenta Significant difference between high-risk pregnancies with and without aspirin December 2028
Secondary Fetal cord serum cytokine profile Significant difference between low and high-risk pregnancies defined by FMF-screening December 2028
Secondary Fetal cord serum metabolite profile Significant difference between low and high-risk pregnancies defined by FMF-screening December 2028
Secondary Fetal cord serum lipid profile Significant difference between low and high-risk pregnancies defined by FMF-screening December 2028
Secondary Fetal cord serum cytokine profile Significant difference between high-risk pregnancies with and without aspirin December 2028
Secondary Fetal cord serum metabolite profile Significant difference between high-risk pregnancies with and without aspirin December 2028
Secondary Fetal cord serum lipid profile Significant difference between high-risk pregnancies with and without aspirin December 2028
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