Chiara Mandò scite author profile

Intrauterine growth restriction (IUGR) and pregnancy hypertensive disorders such as preeclampsia (PE) associated with IUGR share a common placental phenotype called “placental insufficiency”, originating in early gestation when high availability of energy is required. Here, we assess mitochondrial content and the expression and activity of respiratory chain complexes (RCC) in placental cells of these pathologies. We measured mitochondrial (mt)DNA and nuclear respiratory factor 1 ( NRF1) expression in placental tissue and cytotrophoblast cells, gene and protein expressions of RCC (real-time PCR and Western blotting) and their oxygen consumption, using the innovative technique of high-resolution respirometry. We analyzed eight IUGR, six PE, and eight uncomplicated human pregnancies delivered by elective cesarean section. We found lower mRNA levels of complex II, III, and IV in IUGR cytotrophoblast cells but no differences at the protein level, suggesting a posttranscriptional compensatory regulation. mtDNA was increased in IUGR placentas. Both mtDNA and NRF1 expression were instead significantly lower in their isolated cytotrophoblast cells. Finally, cytotrophoblast RCC activity was significantly increased in placentas of IUGR fetuses. No significant differences were found in PE placentas. This study provides genuine new data into the complex physiology of placental oxygenation in IUGR fetuses. The higher mitochondrial content in IUGR placental tissue is reversed in cytotrophoblast cells, which instead present higher mitochondrial functionality. This suggests different mitochondrial content and activity depending on the placental cell lineage. Increased placental oxygen consumption might represent a limiting step in fetal growth restriction, preventing adequate oxygen delivery to the fetus.

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Epigenetic modulation of theIGF2/H19imprinted domain in human embryonic and extra-embryonic compartments and its possible role in fetal growth restriction

Tabano

Colapietro²,

Cetin

et al. 2010

Epigenetics

115

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Maternal blood mitochondrial DNA content during normal and intrauterine growth restricted (IUGR) pregnancy

Colleoni

Lattuada

Garretto

et al. 2010

American Journal of Obstetrics and Gynecology

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Preliminary metabolomics analysis of placenta in maternal obesity

et al. 2018

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Placental metabolome analysis of obese pregnancies showed differences in metabolites involved in antioxidant defenses, nucleotide production, as well as lipid synthesis and energy production, supporting a shift towards higher placental metabolism. OB placentas also showed a specific fatty acids profile suggesting a disruption of LC-PUFA biomagnification. This study can lay the foundation to further metabolomic placental characterization in maternal obesity. Metabolic signatures in obese placentas may reflect changes occurring in the intrauterine metabolic environment, which may affect the development of adult diseases.

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Chiara Mandò

Placental mitochondrial content and function in intrauterine growth restriction and preeclampsia

Epigenetic modulation of theIGF2/H19imprinted domain in human embryonic and extra-embryonic compartments and its possible role in fetal growth restriction

Maternal blood mitochondrial DNA content during normal and intrauterine growth restricted (IUGR) pregnancy

Preliminary metabolomics analysis of placenta in maternal obesity

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