Static and dynamic responses to hyperoxia of normal placenta across gestation with T2*‐weighted MRI sequences

Author:

Bartin R.12ORCID,Melbourne A.34,Bobet L.2,Gauchard G.2,Menneglier A.2,Grevent D.25,Bussieres L.12,Siauve N.6,Salomon L. J.12ORCID

Affiliation:

1. Department of Fetal Medicine, Surgery and Imaging Hôpital Universitaire Necker‐Enfants Malades, AP‐HP Paris France

2. Plateforme LUMIERE Hôpital Universitaire Necker‐Enfants Malades, URP 7328 and PACT, affiliated to Imagine Institut, Université de Paris, Faculté de Médecine Paris France

3. Department of Medical Physics and Biomedical Engineering University College London London UK

4. School of Biomedical Engineering & Imaging Sciences Kings College London London UK

5. Department of Pediatric Radiology Hôpital Universitaire Necker‐Enfants Malades, AP‐HP Paris France

6. Department of Radiology Hôpital Louis Mourier, AP‐HP Colombes France

Abstract

ABSTRACTObjectivesT2*‐weighted magnetic resonance imaging (MRI) sequences have been identified as non‐invasive tools with which to study placental oxygenation in vivo. This study aimed to use these to investigate both static and dynamic responses to hyperoxia of the normal placenta across gestation.MethodsWe conducted a single‐center prospective study including 52 uncomplicated pregnancies. Two T2*‐weighted sequences (T2* relaxometry) were performed, one before and one after maternal hyperoxia. The distribution of placental T2* values was modeled by fitting a gamma probability density function (T2* ), describing the structure of the histogram using the mean T2* value, the shape parameter (α) and the rate (β). A dynamic acquisition (blood‐oxygen‐level‐dependent (BOLD) MRI) was also performed before and during maternal oxygen supply, until placental oxygen saturation had been achieved. The signal change over time was modeled using a sigmoid function, to determine the intensity of enhancement (ΔBOLD (% with respect to baseline)), a temporal variation coefficient (λ (min–1), controlling the slope of the curve) and the maximum steepness (Vmax (% of placental enhancement/min)).ResultsThe histogram analysis of the T2* values in normoxia showed a whole‐placenta variation, with a decreasing linear trend in the mean T2* value (Pearson's correlation coefficient (R) = −0.83 (95% CI, −0.9 to −0.71), P < 0.001), along with an increasingly peaked and narrower distribution of T2* values with advancing gestation. After maternal hyperoxia, the mean T2* ratios (mean T2*hyperoxia/mean T2*baseline) were positively correlated with gestational age, while the other histogram parameters remained stable, suggesting a translation of the histogram towards higher values with a similar appearance after maternal hyperoxia. ΔBOLD showed a non‐linear increase across gestation. Conversely, λ showed an inverted trend across gestation, with a weaker correlation (R = −0.33 (95% CI, −0.58 to −0.02), P = 0.04, R2 = 0.1). As a combination of ΔBOLD and λ, the changes in Vmax throughout gestation were influenced mainly by the changes in ΔBOLD and showed a positive non‐linear correlation with gestational age.ConclusionsOur results suggest that the decrease in the T2* placental signal as gestation progresses does not reflect placental dysfunction. The BOLD dynamic signal change is representative of a free‐diffusion model of oxygenation and highlights the increasing differences in oxygen saturation between mother and fetus as gestation progresses (ΔBOLD) and in the placental permeability to oxygen (λ). © 2024 International Society of Ultrasound in Obstetrics and Gynecology.

Publisher

Wiley

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