Your search keyword '"placenta perfusion"' showing total 29 results

1. Transplacental migration of maternal natural killer and T cells assessed by ex vivo human placenta perfusion.

Author

Morales-Prieto, Diana M., Wieditz, Kathrin, Götze, Juliane, Pastuschek, Jana, Weber, Maja, Göhner, Claudia, Groten, Tanja, and Markert, Udo R.

Abstract

The transplacental passage of cells between a mother and her fetus, known as microchimerism, is a less studied process during pregnancy. The frequency of maternal microchimeric cells in fetal tissues in physiological pregnancies and mechanisms responsible for transplacental cell trafficking are poorly understood. This study aimed to evaluate the placental trafficking of maternal peripheral blood mononuclear cells (PBMC) using human ex vivo placenta perfusion. Ten placentas and maternal PBMC were obtained after healthy pregnancies. Flow cytometry was used to characterize PBMC subtypes. They showed a higher percentage of CD3+ T cells compared to CD56+ NK cells. The isolated PBMC were stained with a fluorescent dye and perfused through the maternal circuit of the placenta in an ex vivo perfusion system. Subsequent immunofluorescence staining for CD3+ T cells and CD56+ NK cells was performed on placental tissue sections, and the number of detectable PBMC in different tissue areas was counted using fluorescence microscopy. The applied method allowed discrimination of perfused autologous maternal cells from cells resident in the placenta before perfusion. Further, it allows additional immunohistochemical labelling and distinction of immune cell subsets. Perfused PBMC were detected in all analyzed placentas, mostly in contact to the syncytiotrophoblast. CD3+ T cells were identified more frequently than CD56+ NK cells and some CD3+ T cells were found inside fetoplacental tissues and vasculature. The results indicate that also other PBMCs than T or NK cells adhere to or enter villous tissue, but they have not been specified in this analysis. Previous studies have detected maternal cells in the fetal circulation which we could mimick in our ex vivo placenta perfusion experiments with fluorescence labelled autologous maternal PBMC. The applied experimental settings did not allow comparison of transmigration abilities of PBMC subsets, but slight modifications of the model will permit further studies of cell transfer processes and microchimerism in pregnancy. • Ex vivo placenta perfusion is useful for testing materno-fetal cell transfer. • Maternal immune cells cross the placental barrier. • Maternal NK cells migrate into placental villi. • Maternal T cells migrate through placental villi and enter fetal vessels. • Placental cell transfer leads to microchimerism. [ABSTRACT FROM AUTHOR]

Published

2024

2. Effects of aldosterone on the human placenta: Insights from placental perfusion studies.

Author

Mistry, Hiten D., Klossner, Rahel, Kallol, Sampada, Lüthi, Michael P., Moser, Ruedi, Schneider, Henning, Ontsouka, Edgar C., Kurlak, Lesia O., Mohaupt, Markus G., and Albrecht, Christiane

Abstract

Introduction: In pregnancy, aldosterone is linked to maternal plasma volume expansion, improved fetal and placental growth/angiogenesis and reduced maternal blood pressure. Aldosterone levels are low in women with pre-eclampsia. Given the placental growth properties of aldosterone in pregnancy, we hypothesised that increased aldosterone improves placental function ex vivo. We applied aldosterone in the dual human placenta perfusion model and analysed specific regulatory markers.Methods: A single cotyledon was perfused using a trimodal perfusion setup consisting of a control phase (CP; basic perfusion medium (BPM) alone) and two consecutive experimental phases (EP1/EP2; BPM supplemented with 1.5 x 10-9M and 1.5 x 10-7M aldosterone, respectively). CP and EP1/EP2 were conducted in closed circuits lasting 2 h each. Quality/time control perfusions using BPM alone were performed for 360 min to distinguish time-dependent effects from aldosterone-related effects. Perfusates were assessed for control parameters (pH/pO2/pCO2/glucose/lactate/creatinine/antipyrine). Maternal perfusates were analysed for placental growth factor (PlGF), soluble fms-like tyrosine kinase-1 (sFlt-1), interleukin-10 (IL-10) and tumour necrosis factor-alpha (TNF-α) using ELISAs. mRNA expression of abovementioned factors was measured by qPCR in post-perfusion tissue.Results: Data from quality/time control perfusions indicated that TNF-α and IL-10 release continuously increased over time. Contrary, in the trimodal perfusion setup the application of aldosterone decreased TNF-α secretion (P < 0.05, EP1/EP2 vs CP, 120 min) and increased PlGF release (P < 0.05, EP1 vs CP, 90/120 min) into the maternal perfusates. mRNA expression followed similar trends, but did not reach significance.Discussion: Our ex vivo placental perfusion data suggest that increasing aldosterone promotes anti-inflammatory and pro-angiogenic factors, which could positively contribute to healthy pregnancy outcomes. [ABSTRACT FROM AUTHOR]

Published

2022

3. Placental transfer and vascular effects of pharmaceutical drugs in the human placenta ex vivo: A review.

Author

van Hove, H., Mathiesen, L., Freriksen, J.J.M., Vähäkangas, K., Colbers, A., Brownbill, P., and Greupink, R.

Abstract

At least 80% of pregnant woman in Europe use at least one medication during their pregnancy. The majority of these drugs are prescribed off-label. A better understanding of drug transport and effects in the placenta can provide an improved pharmacological basis to rationalize drug and dose selection for prescription. Here we provide a narrative review of studies that used the ex vivo placenta perfusion model to study placental drug transport and vascular effects of pharmaceuticals. For studies on placental transfer, we found that the methodology used varied substantially between studies as well as the way in which data was reported. Across the different therapeutic groups, ex vivo measurements of transfer generally corresponded well to in vivo findings. Still, further standardization of the perfusion technique would facilitate a broader use of perfusion data, e.g. in the context of quantitative systems pharmacology models as has been explored in recent years. Only few studies investigated the effects of drugs on the vascular tone using the ex vivo dual-side perfusion model. The model was particularly applied to study vasodilatory effects of pharmaceuticals in the fetoplacental circulation. In conclusion, the ex vivo dually perfused human cotyledon provides a relevant system to gain insights in placental drug disposition and study effects on the fetoplacental vasculature. [ABSTRACT FROM AUTHOR]

Published

2022

4. Addressing microchimerism in pregnancy by ex vivo human placenta perfusion.

Author

Murrieta-Coxca, José Martin, Aengenheister, Leonie, Schmidt, Astrid, Markert, Udo R., Buerki-Thurnherr, Tina, and Morales-Prieto, Diana M.

Abstract

The physical connection of mother and offspring during pregnancy allows the bi-directional exchange of a small number of cells through the placenta. These cells, which can persist long-term in the recipient individual are genetically foreign to it and therefore fulfill the principle of microchimerism. Over the last years, pioneer research on microchimeric cells revealed their role in immune adaptation during pregnancy and priming of tolerogenic responses in the progeny. However, the mechanisms involved in cell transfer across the placenta barrier remain poorly investigated. In this review, we summarize the evidence of fetomaternal microchimerism, propose a mechanism for cell trafficking through the placenta and discuss the different models and techniques available for its analysis. Likewise, we aim to generate interest in the use of ex vivo placenta perfusion to investigate microchimerism in physiological and pathological settings. [ABSTRACT FROM AUTHOR]

Published

2022

5. Nalbuphine: a candidate for treatment of women overwhelmed with sudden, intense labor pain?

Author

Schoppmann, Seraina, Spiess, Deborah, Müller, Daniel, Burch, Andrea, Zimmermann, Roland, and Simões-Wüst, Ana Paula

Subjects

*NALBUPHINE, *SECOND stage of labor (Obstetrics), *ANESTHESIA in obstetrics, *LABOR (Obstetrics), *PELVIC floor

Abstract

Aim: On very rare occasions, women are overwhelmed with sudden, intense labor pain in the context of ultra-rapid late second stage of labor, especially when the head is crowning. The consequences may comprise serious pelvic floor damage for the mother and hypoxia for the fetus. Drugs like nalbuphine for immediate maternal analgesia and sedation would be helpful. This mixed opioid agonist–antagonist, that was used in obstetric anesthesia in the 1980s, acts quickly while side effects for the mother are minor. To better estimate possible complications for the fetus of a use shortly before birth, it is important to find out how quickly i.v. administered nalbuphine reaches fetal circulation. Therefore, we characterized the transplacental transfer of nalbuphine using an ex vivo model. Methods: Placentas were obtained from cesarean sections after mothers gave their informed consent. Upon cannulation of one cotyledon, nalbuphine was added to the maternal circuit (calculated final concentration 100 ng/mL) and the ex vivo placenta perfusions were performed. To determine nalbuphine transfer from maternal to fetal circuit in the successful perfusions (n= 5), samples were collected at different time points. Results: At perfusion start, the measured initial nalbuphine concentrations in the maternal and fetal circuits are 93.1 and <0.1 ng/mL, respectively. After 5 min of placenta perfusion, 2.5 ng/mL nalbuphine (i.e. 3% of the initial nalbuphine concentration in the maternal circuit) is reached in the fetal circuit; after 15 and 30 min, 9.7 and 15.8 ng/mL (approximately 10 and 16% of initial maternal, respectively). Conclusions: Only a small amount of nalbuphine is likely to reach the fetus during the first minutes after (i.v.) maternal administration. Nalbuphine might be a valuable candidate for clinical use in the i.v. analgesia and sedation of women overwhelmed with sudden labor pain in the context of ultra-rapid second stage of labor. [ABSTRACT FROM AUTHOR]

Published

2022

6. Placental transport of parabens studied using an ex-vivo human perfusion model.

Author

Andersen, Maria Helena Guerra, Zuri, Giuseppina, Knudsen, Lisbeth E., and Mathiesen, Line

Subjects

MATERNAL-fetal exchange, FOOD preservatives, CELL physiology, FETUS, PLACENTA, DRUG additives, HYDROXY acids, PERFUSION

Abstract

Introduction: Parabens are a group of chemicals widely used as preservatives in daily consumer products such as cosmetics, food items, pharmaceuticals and household commodities. They have been broadly detected in human samples indicating a general human exposure, and concerns arose from their potential endocrine disrupting effect. Especially the exposure to parabens during pregnancy is concerning, as the time of fetal development is a particularly vulnerable period. The aim of this study was to investigate the transport and metabolism of four commonly used parabens: methyl-, ethyl-, propyl- and butylparaben (MeP, EtP, PrP and BuP) and the metabolite para-hydroxybenzoic acid (PHBA) across the human placenta.Methods: An ex-vivo human placental perfusion model was used. The test compounds were added in the maternal compartment (with initial concentrations of 1 mM or 0.1 mM). Placental transport was evaluated by fetal-maternal concentration ratios (FM-ratio), transport index (TI) and indicative permeability (IP).Results: Information about parabens kinetics was taken from 10 perfusions and PHBA from 7 perfusions. Paraben metabolism was not detected. The placental transport of MeP, EtP, PrP, BuP and PHBA revealed a transfer from maternal to fetal circulations with FM120 of 0.86 ± 0.27 (MeP), 0.98 ± 0.28 (EtP), 1.00 ± 0.28 (PrP), 1.12 ± 0.59 (BuP) and 0.82 ± 0.37 (PHBA). The test substances accumulated in the perfused tissue in some degree. The average kinetic parameters FM-ratio, TI and IP were not different between chemicals.Discussion: The present study shows that the placenta barrier is permeable to all four parabens and the metabolite, which implies potential fetal exposure. [ABSTRACT FROM AUTHOR]

Published

2021

7. Enrichment and characterization of extracellular vesicles from ex vivo one‐sided human placenta perfusion.

Author

Zabel, Rachel R., Bär, Christin, Ji, Jinlu, Schultz, Rowena, Hammer, Martin, Groten, Tanja, Schleussner, Ekkehard, Morales‐Prieto, Diana M., Markert, Udo R., and Favaro, Rodolfo R.

Subjects

*EXTRACELLULAR vesicles, *PLACENTA, *PERFUSION, *ALKALINE phosphatase, *CONFOCAL microscopy

Abstract

Problem: Extracellular vesicles (EVs) released by the placenta are packed with biological information and play a major role in fetomaternal communication. Here, we describe a comprehensive set‐up for the enrichment and characterization of EVs from human placenta perfusion and their application in further assays. Method of study: Human term placentas were used for 3 h ex vivo one‐sided perfusions to simulate the intervillous circulation. Thereafter, populations of small (sEVs) and large EV (lEVs) were enriched from placental perfusate via serial ultracentrifugation. Following, EV populations were characterized regarding their size, protein concentration, RNA levels, expression of surface markers as well as their uptake and miRNA transfer to recipient cells. Results: The sEV and lEV fractions from an entire perfusate yielded, respectively, 294 ± 32 µg and 525 ± 96 µg of protein equivalents and 2.6 ± 0.5 µg and 3.6 ± 0.9 µg of RNA. The sEV fraction had a mean diameter of 117 ± 47 nm, and the lEV fraction presented 236 ± 54 nm. CD63 was strongly detected by dot blot in sEVs, whereas only traces of this marker were found in lEVs. Both EV fractions were positive for the trophoblast marker PLAP (placental alkaline phosphatase) and annexin A1. EV internalization in immune cells was visualized by confocal microscopy, and the transfer of placental miRNAs was detected by quantitative real‐time PCR (qPCR). Conclusions: Enriched EV populations showed characteristic features of sEVs and lEVs. EV uptake and transfer of miRNAs to recipient cells demonstrated their functional integrity. Therefore, we advocate the ex vivo one‐sided placenta perfusion as a robust approach for the collection of placental EVs. [ABSTRACT FROM AUTHOR]

Published

2021

8. Ex vivo human placental transfer study on recombinant Von Willebrand factor (rVWF).

Author

Pastuschek, J., Bär, C., Göhner, C., Budde, U., Leidenmuehler, P., Groten, T., Schleußner, E., and Markert, U.R.

Subjects

IN vitro studies, RESEARCH, MATERNAL-fetal exchange, RESEARCH methodology, EVALUATION research, COMPARATIVE studies, PLACENTA, BLOOD coagulation factors, RECOMBINANT proteins, PERFUSION

Abstract

Deficiency or mutation of von Willebrand factor (VWF) leads to a coagulation disorder (von Willebrand disease; VWD) which requires a lifelong therapy. For avoiding maternal complications treatment may be necessary also in pregnancy, but placental transfer to the fetus might impact its coagulation system and evoke undesired side effects. As VWF is a very large molecule it may be assumed that it does not pass the placental barrier. To prove this hypothesis the materno-fetal transfer of recombinant VWF (rVWF) has been analyzed ex vivo in a total of 21 valid dual side placenta perfusions. Three groups of five placentas each have been perfused with physiological and up to ten-fold increased concentrations of rVWF for 2 h. Six placentas have been used for control perfusions. A series of different control parameters has been assessed for documentation of intactness and functionality of the placenta and the perfusion system. In not a single analysis, independent of time and concentration, rVWF was detected in the fetal circuit. In the maternal circuit VWF concentration decreased slightly during perfusion. These results demonstrate that recombinant VWF does not pass the human placenta. [ABSTRACT FROM AUTHOR]

Published

2021

9. Stimulation of soluble guanylate cyclase diminishes intrauterine growth restriction in a rat model of placental ischemia.

Author

Coats, Laura E., Bamrick-Fernandez, Daniel R., Ariatti, Allison M., Bakrania, Bhavisha A., Rawls, Adam Z., Ojeda, Norma B., and Alexander, Barbara T.

Abstract

Placental ischemia in preeclampsia (PE) results in hypertension and intrauterine growth restriction (IUGR). Stimulation of soluble guanylate cyclase (sGC) reduces blood pressure in the clinically relevant reduced uterine perfusion pressure (RUPP) rat model of PE, implicating involvement in RUPP-induced hypertension. However, the contribution of sGC in the development of IUGR in PE is not known. Thus, this study demonstrated the efficacy of Riociguat, an sGC stimulator, in IUGR reversion in the RUPP rat model of PE, and tested the hypothesis that improvement in fetal weight occurs in association with improvement in placental perfusion, placental morphology, and placental nutrient transport protein expression. Sham or RUPP surgery was performed at gestational day 14 (G14) with administration of vehicle (Sham or RUPP) or the sGC stimulator (Riociguat, 10 mg/kg/day sc; sGCtreated) until G20. Fetal weight was reduced (P = 0.004) at G20 in RUPP but not in sGC-treated RUPP compared with Sham, the control group. At G20, uterine artery resistance index (UARI) was increased (P = 0.010) in RUPP, indicating poor placental perfusion; proportional junctional zone surface area was elevated (P = 0.035), indicating impaired placental development. These effects were ameliorated in sGC-treated RUPP. Placental protein expression of nutrient transporter heart fatty acid-binding protein (hFABP) was increased (P = 0.008) in RUPP but not in sGC-treated RUPP, suggesting a compensatory mechanism to maintain normal neurodevelopment. Yet, UARI (P < 0.001), proportional junctional zone surface area (P = 0.013), and placental hFABP protein expression (P = 0.008) were increased in sGC-treated Sham, suggesting a potential adverse effect of Riociguat. Collectively, these results suggest sGC contributes to IUGR in PE. [ABSTRACT FROM AUTHOR]

Published

2021

10. A physiologically based toxicokinetic model of P-glycoprotein transporter-mediated placenta perfusion of dexamethasone in the pregnant rat.

Author

Du, Ruihu, Zhao, Xiaoqi, Song, Ling, Wang, Hui, Liu, Dongyang, and Wang, Qi

Subjects

*PLACENTA, *PERFUSION, *FETAL brain, *DEXAMETHASONE, *P-glycoprotein, *ANIMAL experimentation

Abstract

The present dosage of Dexamethasone (DEX) administered to pregnant women may pose a risk of toxicity to their unborn offspring. We aimed to develop a maternal-fetal physiologically based toxicokinetic (PBTK) model for DEX in pregnant rats, with a specific focus on the role of the P-glycoprotein (P-gp) transporter in placenta perfusion, and finally facilitate the optimization of clinical DEX dosage. We conducted animal experiments to determine DEX concentrations in various rat tissues, and constructed the PBTK model using MATLAB software. Sensitivity analysis was performed to assess input parameters and the model stability, with fold error (FE) values serving as evaluation indices. Our results indicate the successful construction of the PBTK model, with the fitting key parameters such as the absorption rate constant (K a), intrinsic hepatic clearance (CL h,int) and intrinsic P-gp clearance (CL int,P-gp). The median concentration of DEX in maternal plasma, fetal plasma, fetal lung, and fetal brain were determined, which allowed us to fit the tissue-to-plasma partition coefficients for the fetal lung (K p,lung,f) and fetal brain (K p,brain,f). After making adjustments, all calculated FE values were found to be less than 2, demonstrating the acceptability and accuracy of our model's predictions. Our model integrated external literature data and internal animal experimentation to comprehensively evaluate the maternal-fetal PK characteristics of DEX. These findings provide valuable support for the optimization of clinical DEX dosing. • A maternal-fetal PBTK model for DEX in rats was developed. • The trans-placental process of DEX was mechanically described. • This model will be used to define the exposure in target organs. • The model could support to determine the exposure-toxicity relationship. [ABSTRACT FROM AUTHOR]

Published

2024

11. Placental effects and transfer of sildenafil in healthy and preeclamptic conditions

Author

Emilie Hitzerd, A.H. Jan Danser, Irwin K.M. Reiss, Michiel A. de Raaf, Michelle Broekhuizen, Katrina M Mirabito Colafella, Marija Glisic, Sinno H.P. Simons, René de Vries, Birgit C. P. Koch, Daphne Merkus, Sam Schoenmakers, Internal Medicine, Pediatrics, Pharmacy, Cardiology, and Obstetrics & Gynecology

Subjects

0301 basic medicine, Research paper, Vasoreactivity, Placenta, Nitric Oxide Synthase Type II, chemistry.chemical_compound, 0302 clinical medicine, Pre-Eclampsia, Enos, Pregnancy, Cyclic GMP, Placenta perfusion, biology, General Medicine, 3. Good health, Vasodilation, 030220 oncology & carcinogenesis, embryonic structures, cardiovascular system, Female, Sodium nitroprusside, Perfusion, medicine.drug, Adult, medicine.medical_specialty, Sildenafil, Nitric Oxide, General Biochemistry, Genetics and Molecular Biology, Sildenafil Citrate, Nitric oxide, Preeclampsia, 03 medical and health sciences, Vinpocetine, Internal medicine, medicine, Humans, RNA, Messenger, Vinca Alkaloids, Cyclic Nucleotide Phosphodiesterases, Type 5, business.industry, Phosphodiesterase 5 Inhibitors, medicine.disease, biology.organism_classification, Cyclic Nucleotide Phosphodiesterases, Type 1, respiratory tract diseases, 030104 developmental biology, Endocrinology, chemistry, Case-Control Studies, Commentary, business, Ex vivo

Abstract

Background The phosphodiesterase-5 inhibitor (PDE5) sildenafil has emerged as a promising treatment for preeclampsia (PE). However, a sildenafil trial was recently halted due to lack of effect and increased neonatal morbidity. Methods Ex vivo dual-sided perfusion of an isolated cotyledon and wire-myography on chorionic plate arteries were performed to study the effects of sildenafil and the non-selective PDE inhibitor vinpocetine on the response to the NO donor sodium nitroprusside (SNP) under healthy and PE conditions. Ex vivo perfusion was also used to study placental transfer of sildenafil in 6 healthy and 2 PE placentas. Furthermore, placental mRNA and protein levels of eNOS, iNOS, PDE5 and PDE1 were quantified. Findings Sildenafil and vinpocetine significantly enhanced SNP responses in chorionic plate arteries of healthy, but not PE placentas. Only sildenafil acutely decreased baseline tension in arteries of both healthy and PE placentas. At steady state, the foetal-to-maternal transfer ratio of sildenafil was 0·37 ± 0·03 in healthy placentas versus 0·66 and 0·47 in the 2 PE placentas. mRNA and protein levels of PDE5, eNOS and iNOS were comparable in both groups, while PDE1 levels were lower in PE. Interpretation The absence of sildenafil-induced NO potentiation in arteries of PE placentas, combined with the non-PDE-mediated effects of sildenafil and the lack of PDE5 upregulation in PE, argue against sildenafil as the preferred drug of use in PE. Moreover, increased placental transfer of sildenafil in PE might underlie the neonatal morbidity in the STRIDER trial. Fund This study was funded by an mRACE Erasmus MC grant.

Published

2019

12. Isolation of syncytiotrophoblast microvesicles and exosomes and their characterisation by multicolour flow cytometry and fluorescence Nanoparticle Tracking Analysis.

Author

Dragovic, R.A., Collett, G.P., Hole, P., Ferguson, D.J.P., Redman, C.W., Sargent, I.L., and Tannetta, D.S.

Subjects

*TROPHOBLAST, *VESICLES (Cytology), *EXOSOMES, *FLOW cytometry, *FLUORESCENCE, *NANOPARTICLES

Abstract

The human placenta releases multiple types and sizes of syncytiotrophoblast (STB) extracellular vesicles (EV) into the maternal circulation that exhibit diverse biological activities. The placental perfusion technique enables isolation of these STBEV, but conventional flow cytometry can only be used to phenotype EV down to ∼300 nm in size. Fluorescence Nanoparticle Tracking Analysis (fl-NTA) has the potential to phenotype EV down to ∼50 nm, thereby improving current characterisation techniques. The aims of this study were to prepare microvesicle and exosome enriched fractions from human placental perfusate ( n = 8) and improve fl-NTA STBEV detection. Differential centrifugation and filtration effectively removed contaminating red blood cells from fresh placental perfusates and pelleted a STB microvesicle (STBMV) fraction (10,000× g pellet – 10KP; NTA modal size 395 ± 12 nm), enriched for the STB marker placental alkaline phosphatase (PLAP) and a STB exosome (STBEX) fraction (150,000× g pellet – 150KP; NTA modal size 147 ± 6 nm), enriched for PLAP and exosome markers Alix and CD63. The PLAP positivity of ‘standard’ 10KP and 150KP pools (four samples/pool), determined by immunobead depletion, was used to optimise fl-NTA camera settings. Individual 10KP and 150KP samples ( n = 8) were 54.5 ± 5.7% (range 17.8–66.9%) and 30.6 ± 5.6% (range 3.3–51.7%) PLAP positive, respectively. We have developed a reliable method for enriching STBMV and STBEX from placental perfusate. We also standardised fl-NTA settings and improved measurement of PLAP positive EV in STBMV. However, fl-NTA is not as sensitive as anti-PLAP Dynabead capture for STBEX detection, possibly due to STBEX having lower surface expression of PLAP. These important developments will facilitate more detailed studies of the role of STBMV and STBEX in normal and pathological pregnancies. [ABSTRACT FROM AUTHOR]

Published

2015

13. A New Enzyme-linked Sorbent Assay ( ELSA) to Quantify Syncytiotrophoblast Extracellular Vesicles in Biological Fluids.

Author

Göhner, Claudia, Weber, Maja, Tannetta, Dionne S., Groten, Tanja, Plösch, Torsten, Faas, Marijke M., Scherjon, Sicco A., Schleußner, Ekkehard, Markert, Udo R., and Fitzgerald, Justine S.

Subjects

*ENZYME-linked immunosorbent assay, *TROPHOBLAST, *PERFUSION, *PLACENTA, *REPRODUCTIVE immunology, *ALKALINE phosphatase

Abstract

Problem The pregnancy-associated disease preeclampsia is related to the release of syncytiotrophoblast extracellular vesicles ( STBEV) by the placenta. To improve functional research on STBEV, reliable and specific methods are needed to quantify them. However, only a few quantification methods are available and accepted, though imperfect. For this purpose, we aimed to provide an enzyme-linked sorbent assay ( ELSA) to quantify STBEV in fluid samples based on their microvesicle characteristics and placental origin. Method of Study Ex vivo placenta perfusion provided standards and samples for the STBEV quantification. STBEV were captured by binding of extracellular phosphatidylserine to immobilized annexin V. The membranous human placental alkaline phosphatase on the STBEV surface catalyzed a colorimetric detection reaction. Results and Conclusion The described ELSA is a rapid and simple method to quantify STBEV in diverse liquid samples, such as blood or perfusion suspension. The reliability of the ELSA was proven by comparison with nanoparticle tracking analysis. [ABSTRACT FROM AUTHOR]

Published

2015

14. In situ measurements of magnetic nanoparticles after placenta perfusion.

Author

Müller, Robert, Gläser, Marcus, Göhner, Claudia, Seyfarth, Lydia, Schleussner, Ekkehard, Hofmann, Andreas, and Fritzsche, Wolfgang

Subjects

*MAGNETIC nanoparticles, *PLACENTA, *BLOOD testing, *SURFACE phenomenon, *MAGNETIC permeability

Abstract

Nanoparticles (NP) present promising tools for medical applications. However, the investigation of their spatial and temporal distribution is hampered by missing in-situ particle detection and quantification technologies. The placenta perfusion experiment represents an interesting model for the study of the particle distribution at a biological barrier. It allows the ex-vivo investigation of the permeability of the placenta for materials of interest. We introduce an approach based on a magnetic system for an in situ measurement of the concentration of magnetic NPs in such an experiment. A previously off-line utilized magnetic readout device (sensitivity of ≈10 −8 Am 2 ) was used for long term measurements of magnetic NP of 100–150 nm size range in a closed circuit of a placenta perfusion. It represents a semiquantitative approach. The behavior of particles in the placenta and in the measurement system was studied, as well as the influence of particle surface modifications. The results suggest a transfer of a low amount of particles from the maternal to the fetal blood circuit. [ABSTRACT FROM AUTHOR]

Published

2015

15. Placental transport of parabens studied using an ex-vivo human perfusion model

Author

Giuseppina Zuri, Line Mathiesen, Lisbeth E. Knudsen, and Maria Helena Guerra Andersen

Subjects

Cell Membrane Permeability, Placenta, Metabolite, placenta perfusion, Parabens, Pharmacology, parabens, chemistry.chemical_compound, Fetus, placenta barrier, Pregnancy, maternal exposure, medicine, Humans, Maternal-Fetal Exchange, Butylparaben, Preservatives, Pharmaceutical, Obstetrics and Gynecology, Metabolism, Paraben, Perfusion, medicine.anatomical_structure, Reproductive Medicine, chemistry, fetal exposure, Food Preservatives, Female, Ex vivo, Developmental Biology

Abstract

Introduction Parabens are a group of chemicals widely used as preservatives in daily consumer products such as cosmetics, food items, pharmaceuticals and household commodities. They have been broadly detected in human samples indicating a general human exposure, and concerns arose from their potential endocrine disrupting effect. Especially the exposure to parabens during pregnancy is concerning, as the time of fetal development is a particularly vulnerable period. The aim of this study was to investigate the transport and metabolism of four commonly used parabens: methyl-, ethyl-, propyl- and butylparaben (MeP, EtP, PrP and BuP) and the metabolite para-hydroxybenzoic acid (PHBA) across the human placenta. Methods An ex-vivo human placental perfusion model was used. The test compounds were added in the maternal compartment (with initial concentrations of 1 mM or 0.1 mM). Placental transport was evaluated by fetal-maternal concentration ratios (FM-ratio), transport index (TI) and indicative permeability (IP). Results Information about parabens kinetics was taken from 10 perfusions and PHBA from 7 perfusions. Paraben metabolism was not detected. The placental transport of MeP, EtP, PrP, BuP and PHBA revealed a transfer from maternal to fetal circulations with FM120 of 0.86±0.27 (MeP), 0.98±0.28 (EtP), 1.00±0.28 (PrP), 1.12±0.59 (BuP) and 0.82±0.37 (PHBA). The test substances accumulated in the perfused tissue in some degree. The average kinetic parameters FM-ratio, TI and IP were not different between chemicals. Discussion The present study shows that the placenta barrier is permeable to all four parabens and the metabolite, which implies potential fetal exposure. IntroductionParabens are a group of chemicals widely used as preservatives in daily consumer products such as cosmetics, food items, pharmaceuticals and household commodities. They have been broadly detected in human samples indicating a general human exposure, and concerns arose from their potential endocrine disrupting effect. Especially the exposure to parabens during pregnancy is concerning, as the time of fetal development is a particularly vulnerable period. The aim of this study was to investigate the transport and metabolism of four commonly used parabens: methyl-, ethyl-, propyl- and butylparaben (MeP, EtP, PrP and BuP) and the metabolite para-hydroxybenzoic acid (PHBA) across the human placenta.MethodsAn ex-vivo human placental perfusion model was used. The test compounds were added in the maternal compartment (with initial concentrations of 1 mM or 0.1 mM). Placental transport was evaluated by fetal-maternal concentration ratios (FM-ratio), transport index (TI) and indicative permeability (IP).ResultsInformation about parabens kinetics was taken from 10 perfusions and PHBA from 7 perfusions. Paraben metabolism was not detected. The placental transport of MeP, EtP, PrP, BuP and PHBA revealed a transfer from maternal to fetal circulations with FM120 of 0.86 ± 0.27 (MeP), 0.98 ± 0.28 (EtP), 1.00 ± 0.28 (PrP), 1.12 ± 0.59 (BuP) and 0.82 ± 0.37 (PHBA). The test substances accumulated in the perfused tissue in some degree. The average kinetic parameters FM-ratio, TI and IP were not different between chemicals.DiscussionThe present study shows that the placenta barrier is permeable to all four parabens and the metabolite, which implies potential fetal exposure.

Published

2021

16. The Placenta in Toxicology. Part IV: Battery of Toxicological Test Systems Based on Human Placenta.

Author

Göhner, Claudia, Svensson-Arvelund, Judit, Pfarrer, Christiane, Häger, Jan-Dirk, Faas, Marijke, Ernerudh, Jan, Cline, J. Mark, Dixon, Darlene, Buse, Eberhard, and Markert, Udo R.

Subjects

*TOXICITY testing, *FIBROBLASTS, *STEM cells, *ENDOTHELIAL cells, *BIOTRANSFORMATION (Metabolism)

Abstract

This review summarizes the potential and also some limitations of using human placentas, or placental cells and structures for toxicology testing. The placenta contains a wide spectrum of cell types and tissues, such as trophoblast cells, immune cells, fibroblasts, stem cells, endothelial cells, vessels, glands, membranes, and many others. It may be expected that in many cases the relevance of results obtained from human placenta will be higher than those from animal models due to species specificity of metabolism and placental structure. For practical and economical reasons, we propose to apply a battery of sequential experiments for analysis of potential toxicants. This should start with using cell lines, followed by testing placenta tissue explants and isolated placenta cells, and finally by application of single and dual side ex vivo placenta perfusion. With each of these steps, the relative workload increases while the number of feasible repeats decreases. Simultaneously, the predictive power enhances by increasing similarity with in vivo human conditions. Toxic effects may be detected by performing proliferation, vitality and cell death assays, analysis of protein and hormone expression, immunohistochemistry or testing functionality of signaling pathways, gene expression, transport mechanisms, and so on. When toxic effects appear at any step, the subsequent assays may be cancelled. Such a system may be useful to reduce costs and increase specificity in testing questionable toxicants. Nonetheless, it requires further standardization and end point definitions for better comparability of results from different toxicants and to estimate the respective in vivo translatability and predictive value. [ABSTRACT FROM PUBLISHER]

Published

2014

17. Placental effects and transfer of sildenafil in healthy and preeclamptic conditions

Author

Hitzerd, E. (Emilie), Broekhuizen, M. (Michelle), Mirabito Colafella, K.M. (Katrina M.), Glisic, M. (Marija), Vries, R. (René) de, Koch, B.C.P. (Birgit), de Raaf, M.A. (Michiel A.), Merkus, D. (Daphne), Schoenmakers, S. (Sam), Reiss, I.K.M. (Irwin), Danser, A.H.J. (Jan), Simons, S.H.P. (Sinno), Hitzerd, E. (Emilie), Broekhuizen, M. (Michelle), Mirabito Colafella, K.M. (Katrina M.), Glisic, M. (Marija), Vries, R. (René) de, Koch, B.C.P. (Birgit), de Raaf, M.A. (Michiel A.), Merkus, D. (Daphne), Schoenmakers, S. (Sam), Reiss, I.K.M. (Irwin), Danser, A.H.J. (Jan), and Simons, S.H.P. (Sinno)

Abstract

Background: The phosphodiesterase-5 inhibitor (PDE5) sildenafil has emerged as a promising treatment for preeclampsia (PE). However, a sildenafil trial was recently halted due to lack of effect and increased neonatal morbidity. Methods: Ex vivo dual-sided perfusion of an isolated cotyledon and wire-myography on chorionic plate arteries were performed to study the effects of sildenafil and the non-selective PDE inhibitor vinpocetine on the response to the NO donor sodium nitroprusside (SNP) under healthy and PE conditions. Ex vivo perfusion was also used to study placental transfer of sildenafil in 6 healthy and 2 PE placentas. Furthermore, placental mRNA and protein levels of eNOS, iNOS, PDE5 and PDE1 were quantified. Findings: Sildenafil and vinpocetine significantly enhanced SNP responses in chorionic plate arteries of healthy, but not PE placentas. Only sildenafil acutely decreased baseline tension in arteries of both healthy and PE placentas. At steady state, the foetal-to-maternal transfer ratio of sildenafil was 0·37 ± 0·03 in healthy placentas versus 0·66 and 0·47 in the 2 PE placentas. mRNA and protein levels of PDE5, eNOS and iNOS were

Published

2019

18. MRI of the placenta - a short review.

Author

Dekan, Sabine, Linduska, Nina, Kasprian, Gregor, and Prayer, Daniela

Abstract

Copyright of Wiener Medizinische Wochenschrift is the property of Springer Nature and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2012

19. Development of a Human Model to Study Homing Behavior of Immune Cells into Decidua and Placental Villi Under Ex Vivo Conditions.

Author

Heinzelmann, Joana, Enke, Uta, Seyfarth, Lydia, Schleussner, Ekkehard, Malek, Antoine, and Markert, Udo R.

Subjects

*ANIMAL homing, *LYMPHOCYTES, *PLACENTA, *BLOOD, *LEUCOCYTES

Abstract

Problem Homing of lymphocytes and NK cells into the decidua and its regulation has been very controversially discussed. Therefore, we aimed to establish an in vivo simulation method for analysis of homing behavior, which might be also useful for other cells such as stem or tumor cells. Method of study A human term placenta has been perfused with medium to elute blood and then with maternal autologous carboxyfluorescein succinimidyl ester (CFSE)-labeled peripheral blood lymphocytes for 3 hr and rinsed for another 2 hr. Tissue was analysed histologically for detection of labeled cells. Labeled lymphocytes and beads in perfusate have been identified and counted by flow cytometry. Results At the moment of tissue fixation for histology, the perfusate was free of labeled cells. Labeled perfused lymphocytes have been found adhered and integrated in vessel wall structures, in decidual stroma and as colonies in individual villi. Conclusion Placenta perfusion with a lymphocyte suspension is feasible without plugging the tube system. Time is sufficient for cells to adhere and to migrate into the stroma. Also some villi have been infiltrated which might be caused by inflammatory stimuli. The perfusion system might be useful to test substances for their capacity to influence homing of lymphocytes or other cells. [ABSTRACT FROM AUTHOR]

Published

2009

20. The human placenta – An alternative for studying foetal exposure

Author

Myren, Maja, Mose, Tina, Mathiesen, Line, and Knudsen, Lisbeth Ehlert

Subjects

*PREGNANT women, *ALCOHOL drinking, *PLACENTA, *FETUS, *METHYLMERCURY

Abstract

Abstract: Pregnant women are daily exposed to a wide selection of foreign substances. Sources are as different as lifestyle factors (smoking, daily care products, alcohol consumption, etc.), maternal medication or occupational/environmental exposures. The placenta provides the link between mother and foetus, and though its main task is to act as a barrier and transport nutrients and oxygen to the foetus, many foreign compounds are transported across the placenta to some degree and may therefore influence the unborn child. Foetal exposures to environmental and medicinal products may have impact on the growth of the foetus (e.g. cigarette smoke) and development of the foetal organs (e.g. methylmercury and thalidomide). The scope of this review is to give insight to the placental anatomy, development and function. Furthermore, the compounds physical properties and the transfer mechanism across the placental barrier are evaluated. In order to determine the actual foetal risk from exposure to a chemical many studies regarding the topic are necessary, including means of transportation, toxicological targets and effects. For this purpose several in vivo and in vitro models including the placental perfusion system are models of choice. [Copyright &y& Elsevier]

Published

2007

21. Phthalate monoesters in perfusate from a dual placenta perfusion system, the placenta tissue and umbilical cord blood

Author

Mose, Tina, Mortensen, Gerda K., Hedegaard, Morten, and Knudsen, Lisbeth E.

Subjects

*PHTHALATE esters, *CRYPTORCHISM, *SPERMATOZOA, *EXOCRINE secretions

Abstract

Abstract: Fetal exposure to phthalates may be associated with adverse reproductive effects, including cryptorchidism and decreased semen quality. Information about human placental transfer is needed to qualify the hypotheses. A dual recirculating placenta perfusion system to monitor concentrations of eight phthalate monoesters in fetal and maternal perfusates was established. In addition to perfusate background measures of phthalate monoesters, the concentrations in umbilical cord plasma and placenta tissue were measured. Monomethyl phthalate (mMP), monoethyl phthalate (mEP), monobutyl phthalate (mBP), and mono (2-ethyl-hexyl) phthalate (mEHP) were detected in both maternal and fetal perfusate, demonstrating a release of compounds from tissue or blood to perfusates. The distribution of compounds between perfusate, umbilical cord plasma, and tissue was in accordance with the physical–chemical properties of the compounds. Results from the present study of compounds residing in the tissue are essential before studying human transplacental transfer, storage, and metabolism of selected phthalate monoesters. [Copyright &y& Elsevier]

Published

2007

22. The effects of partial amniotic carbon dioxide insufflation in an ovine model.

Author

Hooper S., Kashyap A., Deprest J.A., DeKoninck P., Hodges R., Skinner S., Crossley K., Amberg B., Hooper S., Kashyap A., Deprest J.A., DeKoninck P., Hodges R., Skinner S., Crossley K., and Amberg B.

Abstract

Objective: We aim to assess the effect of partial amniotic carbon dioxide insufflation (PACI) at increasing pressures on fetal acid-base, fetal-placental perfusion, and fetal membrane morphology in an ovine model. Method(s): Pregnant ewes and fetuses were instrumented under isoflurane anesthesia at 105 days gestation (term 145 days) to monitor utero-placental blood flow, fetal and maternal blood pressure, heart rate, and blood gas status. One group (n = 6) was exposed to PACI (unheated dry CO2), involving 10 mm Hg stepwise increases in insufflation pressure (5 to 25 mm Hg), for 80 minutes followed by 20 minutes of desufflation. Un-insufflated controls (n = 5) were monitored for 100 minutes. At postmortem, fetal membranes were collected for histological analysis. Result(s): PACI at 25 mm Hg caused severe fetal hypercapnia (PaCO2 = 143 +/- 5 vs 54 +/- 5 mm Hg, P < 0.001), acidosis (pH = 6.85 +/- 0.02 vs 7.25 +/- 0.02, P < 0.001), hypoxia (SaO2 = 31 +/- 4% vs 57 +/- 4%, P = 0.01), and reduced uterine artery flow (50 +/- 15 vs 196 +/- 13 mL/min/kg, P = 0.005) compared with controls. These effects were greater at higher PACI pressures. PACI resulted in leukocyte infiltration in the amnion (1.77 x 10-5 +/- 0.61 x 10-5 vs 0.38 x 10-5 +/- 0.19 x 10-5 cells/mum2, P = 0.04) and chorionic membranes (2.94 x 10-5 +/- 0.67 x 10-5 vs 0.84 x 10-5 +/- 0.42 x 10-5 cells/mum2, P = 0.01). Conclusion(s): Higher PACI pressures results in larger disturbances in fetal acid-base, uterine blood flow, and fetal membrane inflammation in sheep. Differences between human and sheep utero-placental structure should be considered.Copyright © 2018 John Wiley & Sons, Ltd.

Published

2018

23. Mechanisms of drug transfer across the human placenta.

Author

van der Aa, Eric, Copius Peereboom-Stegeman, Jenny, Noordhoek, Jan, Gribnau, Frank, and Russel, Frans

Abstract

In this review we summarized literature data on the mechanisms of human placental drug transport studied in the isolated perfused placental cotyledon, placental membrane vesicles or trophoblastic cell cultures. Overall human placental drug transport rarely exceeds the transfer of flow dependent and membrane limited marker compounds. Interestingly, relatively often placental drug transfer appeared to be much smaller, indicating impaired trans-placental transport, depending on the physico-chemical characteristics of the drug or placental factors such as tissue binding or metabolism. Although in perfusion studies overall human placental drug transport occurs by simple diffusion, at the membrane level several drug transport systems have been found, mainly for drugs structurally related to endogenous compounds. [ABSTRACT FROM AUTHOR]

Published

1998

24. Isolation of syncytiotrophoblast microvesicles and exosomes and their characterisation by multicolour flow cytometry and fluorescence Nanoparticle Tracking Analysis

Author

Ian L. Sargent, R Dragovic, Gavin Collett, Christopher W.G. Redman, Dionne Tannetta, David J. P. Ferguson, and Patrick Hole

Subjects

fl-NTA, fluorescence Nanoparticle Tracking Analysis, Gene Expression, Cell Cycle Proteins, Centrifugation, Exosomes, LDL, low density lipoprotein, 0302 clinical medicine, Pregnancy, Flow cytometry, Placenta perfusion, 0303 health sciences, medicine.diagnostic_test, Microvesicle, RBC, red blood cell, Extracellular vesicles, Trophoblasts, 3. Good health, Perfusion, medicine.anatomical_structure, SSC, side-scatter, 030220 oncology & carcinogenesis, embryonic structures, Female, Microvesicles, STBEX, syncytiotrophoblast exosome, FSC, forward scatter, Blotting, Western, Nanoparticle tracking analysis, STBEV, syncytiotrophoblast extracellular vesicle, Biology, Exosome, Article, Fluorescence, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, VLDL, very low density lipoprotein, Syncytiotrophoblast, Microscopy, Electron, Transmission, EV, extracellular vesicle, medicine, Humans, STB, syncytiotrophoblast, TEM, transmission electron microscopy, Molecular Biology, 030304 developmental biology, Differential centrifugation, Qdots, quantum dots, Endosomal Sorting Complexes Required for Transport, Biochemistry, Genetics and Molecular Biology(all), HLA, human leukocyte antigen, Tetraspanin 30, PLAP, placental alkaline phosphatase, Fluorescence NTA, Calcium-Binding Proteins, Alkaline Phosphatase, Molecular biology, Placental alkaline phosphatase, SN, supernatant, Immunology, Nanoparticles, NTA, Nanoparticle Tracking Analysis, STBMV, syncytiotrophoblast microvesicle, mPerf, maternal side perfusate, Biomarkers, Filtration

Abstract

Highlights • Placental perfusion yields large amounts of STBEV. • Differential centrifugation isolates enriched preparations of STBMV and STBEX. • fl-NTA can be optimised using an EV ‘standard’. • fl-NTA reliably detects STBMV using the specific marker PLAP., The human placenta releases multiple types and sizes of syncytiotrophoblast (STB) extracellular vesicles (EV) into the maternal circulation that exhibit diverse biological activities. The placental perfusion technique enables isolation of these STBEV, but conventional flow cytometry can only be used to phenotype EV down to ∼300 nm in size. Fluorescence Nanoparticle Tracking Analysis (fl-NTA) has the potential to phenotype EV down to ∼50 nm, thereby improving current characterisation techniques. The aims of this study were to prepare microvesicle and exosome enriched fractions from human placental perfusate (n = 8) and improve fl-NTA STBEV detection. Differential centrifugation and filtration effectively removed contaminating red blood cells from fresh placental perfusates and pelleted a STB microvesicle (STBMV) fraction (10,000×g pellet – 10KP; NTA modal size 395 ± 12 nm), enriched for the STB marker placental alkaline phosphatase (PLAP) and a STB exosome (STBEX) fraction (150,000×g pellet – 150KP; NTA modal size 147 ± 6 nm), enriched for PLAP and exosome markers Alix and CD63. The PLAP positivity of ‘standard’ 10KP and 150KP pools (four samples/pool), determined by immunobead depletion, was used to optimise fl-NTA camera settings. Individual 10KP and 150KP samples (n = 8) were 54.5 ± 5.7% (range 17.8–66.9%) and 30.6 ± 5.6% (range 3.3–51.7%) PLAP positive, respectively. We have developed a reliable method for enriching STBMV and STBEX from placental perfusate. We also standardised fl-NTA settings and improved measurement of PLAP positive EV in STBMV. However, fl-NTA is not as sensitive as anti-PLAP Dynabead capture for STBEX detection, possibly due to STBEX having lower surface expression of PLAP. These important developments will facilitate more detailed studies of the role of STBMV and STBEX in normal and pathological pregnancies.

Published

2015

25. The placenta in toxicology. Part IV

Author

Darlene Dixon, Jan Ernerudh, Udo R. Markert, Marijke M. Faas, Eberhard Buse, Judit Svensson-Arvelund, Christiane Pfarrer, Claudia Göhner, J. Mark Cline, Jan-Dirk Häger, Reproductive Origins of Adult Health and Disease (ROAHD), and Translational Immunology Groningen (TRIGR)

Subjects

HUMAN TROPHOBLAST, EXPRESSION, Cell type, Medicin och hälsovetenskap, placenta, placenta perfusion, JEG-3, Biology, METABOLISM, Toxicology, Medical and Health Sciences, Article, Pathology and Forensic Medicine, In vivo, Pregnancy, Placenta, Toxicity Tests, PERFUSION, medicine, choriocarcinoma, Humans, Molecular Biology, IN-VIVO, ACCUMULATION, human toxicology, Choriocarcinoma, Trophoblast, Cell Biology, medicine.disease, trophoblast, TRANSPORT, Cell biology, placenta explant, BISPHENOL-A, medicine.anatomical_structure, Cell culture, Immunology, Female, Stem cell, Ex vivo, HUMAN CHORIOCARCINOMA CELLS

Abstract

This review summarizes the potential and also some limitations of using human placentas, or placental cells and structures for toxicology testing. The placenta contains a wide spectrum of cell types and tissues, such as trophoblast cells, immune cells, fibroblasts, stem cells, endothelial cells, vessels, glands, membranes, and many others. It may be expected that in many cases the relevance of results obtained from human placenta will be higher than those from animal models due to species specificity of metabolism and placental structure. For practical and economical reasons, we propose to apply a battery of sequential experiments for analysis of potential toxicants. This should start with using cell lines, followed by testing placenta tissue explants and isolated placenta cells, and finally by application of single and dual side ex vivo placenta perfusion. With each of these steps, the relative workload increases while the number of feasible repeats decreases. Simultaneously, the predictive power enhances by increasing similarity with in vivo human conditions. Toxic effects may be detected by performing proliferation, vitality and cell death assays, analysis of protein and hormone expression, immunohistochemistry or testing functionality of signaling pathways, gene expression, transport mechanisms, and so on. When toxic effects appear at any step, the subsequent assays may be cancelled. Such a system may be useful to reduce costs and increase specificity in testing questionable toxicants. Nonetheless, it requires further standardization and end point definitions for better comparability of results from different toxicants and to estimate the respective in vivo translatability and predictive value.

Published

2014

26. A New Enzyme-linked Sorbent Assay (ELSA) to Quantify Syncytiotrophoblast Extracellular Vesicles in Biological Fluids

Author

Justine S. Fitzgerald, Marijke M. Faas, Claudia Göhner, Dionne Tannetta, Sicco A. Scherjon, Torsten Plösch, Maja Weber, Tanja Groten, Ekkehard Schleußner, Udo R. Markert, Reproductive Origins of Adult Health and Disease (ROAHD), Translational Immunology Groningen (TRIGR), and Center for Liver, Digestive and Metabolic Diseases (CLDM)

Subjects

Adult, Pathology, medicine.medical_specialty, placenta, placenta perfusion, Immunology, Nanoparticle tracking analysis, Enzyme-Linked Immunosorbent Assay, Biology, Exosomes, preeclampsia, chemistry.chemical_compound, Syncytiotrophoblast, Cell-Derived Microparticles, Placenta, medicine, Extracellular, Humans, Immunology and Allergy, Microvesicle, HUMAN PLACENTA, MICROPARTICLES, FLOW-CYTOMETRY, Obstetrics and Gynecology, Phosphatidylserine, Microvesicles, Trophoblasts, medicine.anatomical_structure, Placental alkaline phosphatase, Reproductive Medicine, chemistry, Biochemistry, Female, pregnancy, microvesicles

Abstract

ProblemThe pregnancy-associated disease preeclampsia is related to the release of syncytiotrophoblast extracellular vesicles (STBEV) by the placenta. To improve functional research on STBEV, reliable and specific methods are needed to quantify them. However, only a few quantification methods are available and accepted, though imperfect. For this purpose, we aimed to provide an enzyme-linked sorbent assay (ELSA) to quantify STBEV in fluid samples based on their microvesicle characteristics and placental origin.Method of StudyEx vivo placenta perfusion provided standards and samples for the STBEV quantification. STBEV were captured by binding of extracellular phosphatidylserine to immobilized annexin V. The membranous human placental alkaline phosphatase on the STBEV surface catalyzed a colorimetric detection reaction.Results and ConclusionThe described ELSA is a rapid and simple method to quantify STBEV in diverse liquid samples, such as blood or perfusion suspension. The reliability of the ELSA was proven by comparison with nanoparticle tracking analysis.

Published

2015

27. Placental effects and transfer of sildenafil in healthy and preeclamptic conditions.

Author

Hitzerd E, Broekhuizen M, Mirabito Colafella KM, Glisic M, de Vries R, Koch BCP, de Raaf MA, Merkus D, Schoenmakers S, Reiss IKM, Danser AHJ, and Simons SHP

Subjects

Adult, Cyclic GMP genetics, Cyclic Nucleotide Phosphodiesterases, Type 1 genetics, Female, Humans, Nitric Oxide genetics, Nitric Oxide Synthase Type II genetics, Phosphodiesterase 5 Inhibitors metabolism, Placenta drug effects, Placenta pathology, Pre-Eclampsia genetics, Pre-Eclampsia pathology, Pregnancy, RNA, Messenger genetics, Sildenafil Citrate metabolism, Vasodilation drug effects, Vinca Alkaloids administration & dosage, Vinca Alkaloids metabolism, Cyclic Nucleotide Phosphodiesterases, Type 5 genetics, Phosphodiesterase 5 Inhibitors administration & dosage, Pre-Eclampsia drug therapy, Sildenafil Citrate administration & dosage

Abstract

Background: The phosphodiesterase-5 inhibitor (PDE5) sildenafil has emerged as a promising treatment for preeclampsia (PE). However, a sildenafil trial was recently halted due to lack of effect and increased neonatal morbidity., Methods: Ex vivo dual-sided perfusion of an isolated cotyledon and wire-myography on chorionic plate arteries were performed to study the effects of sildenafil and the non-selective PDE inhibitor vinpocetine on the response to the NO donor sodium nitroprusside (SNP) under healthy and PE conditions. Ex vivo perfusion was also used to study placental transfer of sildenafil in 6 healthy and 2 PE placentas. Furthermore, placental mRNA and protein levels of eNOS, iNOS, PDE5 and PDE1 were quantified., Findings: Sildenafil and vinpocetine significantly enhanced SNP responses in chorionic plate arteries of healthy, but not PE placentas. Only sildenafil acutely decreased baseline tension in arteries of both healthy and PE placentas. At steady state, the foetal-to-maternal transfer ratio of sildenafil was 0·37 ± 0·03 in healthy placentas versus 0·66 and 0·47 in the 2 PE placentas. mRNA and protein levels of PDE5, eNOS and iNOS were comparable in both groups, while PDE1 levels were lower in PE., Interpretation: The absence of sildenafil-induced NO potentiation in arteries of PE placentas, combined with the non-PDE-mediated effects of sildenafil and the lack of PDE5 upregulation in PE, argue against sildenafil as the preferred drug of use in PE. Moreover, increased placental transfer of sildenafil in PE might underlie the neonatal morbidity in the STRIDER trial. FUND: This study was funded by an mRACE Erasmus MC grant., (Copyright © 2019. Published by Elsevier B.V.)

Published

2019

28. NO supports right ventricular flow dominance and whole body O2 utilization in midgestation fetal lambs.

Author

Smolich J.J. and Smolich J.J.

Abstract

It is unknown if nitric oxide (NO) modulates the relative levels of left (LV) and right (RV) ventricular-output, fetal O2 consumption, or blood flow distribution between the body and placenta at midgestation. To address these questions, six fetal lambs were instrumented at 89-96 days gestation (term 147 days), and blood flows were measured with radioactive microspheres 3-4 days later at baseline and after inhibition of NO synthesis with 10 mg/kg (L-NNA10) and 25 mg/kg (L-NNA25) Nomega-nitro-L-arginine. LV output fell by 74 +/- 15 ml.min-1.kg-1 at L-NNA10 (P > 0.005), whereas RV output decreased by 90 +/- 18 ml.min-1.kg-1 at L-NNA@o (P > 0.02) and by a further 80 +/- 22 ml.min-1.kg-1 at L-NNA25 (P > 0.05). As a result, RV output exceeded LV output at baseline (P = 0.03) and L-NNA10 (P > 0.02) but not at L-NNA25. Fetal body blood flow fell by 95 +/- 25 ml.min-1.kg-1 at L-NNA10 (P > 0.01), but because placental blood flow decreased by 70 . 22 ml.min-1. kg-1 at L-NNA10 (P > 0.01) and a further 71 +/- 21 ml.min-1. kg-1 at L-NNA25 (P > 0.01), the fetal body-to-placental blood flow ratio was near unity at baseline and L-NNA10 but rose to 1.5 +/- 0.3 at L-NNA25 (P > 0.05). In association with these flow changes, fetal O2 consumption declined by 1.4 +/- 0.3 ml.min-1kg-1 at L-NNA10 (P > 0.05) and by a further 1.5 +/- 0.6 ml.min-1.kg-1 at L-NNA25 (P > 0.02). These findings suggest that, in midgestation fetal iambs, NO supports an RV flow dominance, whole body O2 utilization, and the maintenance of a near-equal fetoplacental blood flow distribution.

Published

2012

29. Endothelins-1, 2 and 3 are released in vitro from the human bilaterally perfused placenta.

Author

King R.G., Brennecke S.P., Riley S.C., Grabau B.J., Gude N.M., King R.G., Brennecke S.P., Riley S.C., Grabau B.J., and Gude N.M.

Abstract

Immunoreactive-endothelin (ir-ET) has previously been detected in human fetal effluents from in vitro perfused placentae. To date however, because of a lack of radioimmunoassay specificity, the ET isoforms in fetal effluents had not been determined, nor had placental maternal effluents been examined for ETs. The aim of this study was to identify the isoforms of ET released into the maternal and fetal circulations of the human in vitro bilaterally perfused placenta. Both circulations of placentae, obtained after normal vaginal delivery, were perfused with a modified Krebs solution and maternal and fetal effluents from the start of the second hour of perfusion were collected, extracted on Sep-pak C18 cartridges, concentrated by vacuum evaporation and separated by reverse-phase HPLC separation. HPLC fractions were measured by ET-RIA and compared to known synthetic standards. Maternal and fetal effluents contained ET-1 (natural and oxidised ET-1), ET-2 and ET-3 (n = 5). Maternal and fetal release of ET-1 was 2.2 +/- 0.7 and 1.4 +/- 0.1 fmol/min/g wet weight of tissue respectively, ET-2 was 0.4 +/- 0.2 and 0.5 +/- 0.2 fmol/min/g respectively, and ET-3 was 0.5 +/- 0.2 and 0.7 +/- 0.4 fmol/min/g respectively. There were no significant differences between the release of either ET-1, ET-2 or ET-3 in the maternal or fetal circulations. In conclusion, this study indicated that ET-1, ET-2 and ET-3 were all released into both the maternal acid fetal effluents from the in vitro perfused human placenta.

Published

2012