Your search keyword '"Vähäkangas, Kirsi"' showing total 9 results

1. Transplacental passage of lamotrigine in a human placental perfusion system in vitro and in maternal and cord blood in vivo.

Author

Myllynen PK, Pienimäki PK, and Vähäkangas KH

Subjects

Antipyrine blood, Chromatography, High Pressure Liquid, Dose-Response Relationship, Drug, Female, Humans, Hydrogen-Ion Concentration, In Vitro Techniques, Lamotrigine, Time Factors, Anticonvulsants blood, Fetal Blood metabolism, Maternal-Fetal Exchange, Placenta metabolism, Pregnancy blood, Triazines blood

Abstract

Objective: We studied transplacental passage of lamotrigine (3,5-diamino-6-[2,3-dichlorophenyl]-1,2,4-triazine; LTG) using an ex vivo human placental perfusion method and in in vivo samples., Methods: Term placentas from healthy mothers without medications were perfused in a recirculating dual perfusion system. LTG (2.5 microg/ml, n=4; 10 microg/ml, n=4) and reference compound antipyrine (100 microg/ml) were added into the maternal circulation. The disappearance of drugs from the maternal circulation and appearance into the foetal circulation was followed every 15 min up to 2 h. Drug concentrations were analysed using high-performance liquid chromatography. In addition to human placental perfusions, we analysed LTG concentrations in maternal vein and cord blood samples after delivery from two epileptic mothers receiving LTG therapy during pregnancy., Results: LTG was detectable in the foetal circulation at 15 min in all of the perfusions, indicating rapid transfer. Maternal and foetal concentrations reached equilibrium at 60 min with both concentrations used. The feto-maternal ratio was 1.26+/-0.20 with 10 microg/ml LTG and 0.83+/-0.41 with 2.5 microg/ml LTG at the end of the perfusion. The transfer of LTG from the maternal to the foetal compartment at 120 min was 28.9+/-10.7% with 2.5 microg/ml LTG and 37.8+/-3.2% with 10 microg/ml LTG (p>0.05). In the serum samples from epileptic mothers, the cord blood maternal concentration ratio was 1.02 in one pair and 1.55 in the other., Conclusions: LTG crossed the placenta easily and rapidly, indicating that the maternal treatment leads to a considerable foetal exposure.

Published

2003

2. Experimental human placental models for studying uptake, transport and toxicity of micro- and nanoplastics

Author

Dusza, Hanna M., van Boxel, Jeske, van Duursen, Majorie B.M., Forsberg, Markus M., Legler, Juliette, and Vähäkangas, Kirsi H.

Subjects

Environmental Engineering, In vitro, SDG 3 - Good Health and Well-being, Pregnancy, Placenta, Microplastics, Environmental Chemistry, Nanoplastics, Pollution, Waste Management and Disposal, Ex vivo

Abstract

Micro- and nanoplastics (MNPs) are ubiquitous in the environment and have recently been found in human lungs, blood and placenta. However, data on the possible effects of MNPs on human health is extremely scarce. The potential toxicity of MNPs during pregnancy, a period of increased susceptibility to environmental insults, is of particular concern. The placenta provides a unique interface between maternal and fetal circulation which is essential for in utero survival and healthy pregnancy. Placental toxicokinetics and toxicity of MNPs are still largely unexplored and the limited studies performed up to now focus mainly on polystyrene particles. Practical and ethical considerations limit research options in humans, and extrapolation from animal studies is challenging due to marked differences between species. Nevertheless, diverse in vitro and ex vivo human placental models exist e.g., plasma membrane vesicles, mono-culture and co-culture of placental cells, placenta-on-a-chip, villous tissue explants, and placental perfusion that can be used to advance this research area. The objective of this concise review is to recapitulate different human placental models, summarize the current understanding of placental uptake, transport and toxicity of MNPs and define knowledge gaps. Moreover, we provide perspectives for future research urgently needed to assess the potential hazards and risks of MNP exposure to maternal and fetal health.

Published

2023

3. Smoking during pregnancy in Finland – Trends in the MATEX cohort.

Author

Rumrich, Isabell K., Vähäkangas, Kirsi, Viluksela, Matti, Gissler, Mika, Surcel, Heljä-Marja, Korhonen, Antti, De Ruyter, Hanna, and Hänninen, Otto

Subjects

*AGE distribution, *LONGITUDINAL method, *MATERNAL age, *PREGNANCY & psychology, *SELF-evaluation, *SMOKING, *SMOKING cessation, *SOCIOECONOMIC factors, *PREGNANCY

Abstract

Aims: In Finland, smoking rates in the general population are decreasing due to increased awareness of the adverse effects and tightened tobacco legislation. However, previous studies have shown that smoking in pregnant Finnish women remained as high as in the general Finnish female population at around 15% in 2010. Our aim was to describe temporal and spatial trends in smoking behaviour, and determinants of changes in smoking behaviour between first and second pregnancy. Methods : Self-reported smoking from the Finnish Medical Birth Register covered the years 1991–2015 (N =1,435,009). The association of maternal age and socioeconomic status with smoking rate was analysed. Spatial trends were assessed at municipality level. Results : The overall smoking rate during early pregnancy remained fairly stable at around 15% from 1991 to 2015, but increased in teenage and young women below 25 years of age. The mean smoking rate (36%) was higher in these age groups than in older pregnant women (11%). Through the study period the smoking rate remained higher in blue collar workers compared with higher socioeconomic groups. Between the first and second child, on average only 4% of women started to smoke and 41% quitted. Smoking rates developed less favourably in Eastern Finland. Conclusions : The observed increase in smoking rate during pregnancy in teenage and young women is concerning. Pregnancy is a trigger point for smoking cessation in a big fraction of pregnant women. More studies are needed to explain the opposite trends of smoking rates in Northern and Western Finland compared with Eastern Finland. [ABSTRACT FROM AUTHOR]

Published

2019

4. Maternal use of drugs and preeclampsia.

Author

Sahlman, Heidi, Koponen, Marjaana, El‐Nezami, Hani, Vähäkangas, Kirsi, and Keski‐Nisula, Leea

Subjects

PREECLAMPSIA, VITAL records (Births, deaths, etc.), BENZODIAZEPINES, UNIVERSITY hospitals, NONOPIOID analgesics, PREGNANCY

Abstract

Aims: The aim was to compare and describe maternal use of drugs between women with preeclampsia and controls and to estimate the possible association with preeclampsia. Methods: The study cohort was collected from the Kuopio University Hospital Birth Register, which includes information about all women who gave birth in Kuopio University Hospital during the years 2002–2016, including information from approximately 36 000 parturients, of whom 1252 had preeclampsia. Maternal use of 16 groups of drugs during pregnancy was analysed from all women with preeclampsia and 1256 controls. Results: Every second woman had used at least 1 drug during pregnancy but those with preeclampsia had used significantly more than the controls (cases 59.5% vs controls 35.5%; p < 0.001). In both study groups, the most commonly used drugs were antibiotics (cases 19.5%, controls 17.0%), antihypertensives (cases 29.0%, controls 7.6%) and paracetamol (cases 13.1%, controls 5.9%). Women with preeclampsia had used significantly more benzodiazepines, paracetamol, antihypertensives and acid‐suppressive drugs than the women in the control group (p < 0.05). Conclusions: Women with preeclampsia were more likely to use medicines during pregnancy. While the association between benzodiazepines, antihypertensives and acid‐suppressive drugs and preeclampsia may be explained by reverse causation, the association of paracetamol with preeclampsia remains to be clarified. Because paracetamol is a frequently used drug, more information about its safety during pregnancy including its role in preeclampsia is urgently needed. [ABSTRACT FROM AUTHOR]

Published

2019

5. Drug transporters in the human blood-placental barrier

Author

Vähäkangas, Kirsi and Myllynen, Päivi

Subjects

Pharmaceutical Preparations, Pregnancy, Placenta, embryonic structures, Reviews, Animals, Humans, ATP-Binding Cassette Transporters, Female, Carrier Proteins, Maternal-Fetal Exchange, Multidrug Resistance-Associated Protein 2

Abstract

Studies on the increasing number of transporters found in the placental barrier are gaining momentum, because of their tissue-specific expression, significance in physiology and disease, and the possible utilization of the emerging knowledge in pharmacology. In the placenta, both syncytiotrophoblast and fetal capillary endothelium express transporters. Fetal exposure is determined by the net effect of combination of transporters, their nature and localization in relation to placental cells and their substrate specificity. Although the significance of placental transporters on human fetal drug exposure is almost an unstudied field so far, their potential use to design drugs that do not cross the placenta is already being pursued. It is thus of interest to review the existing knowledge of human placental transporters. Transporters in all groups which take part in drug transport are found in human placenta. Especially, ATP-binding cassette transporters ABCG2/breast cancer resistance protein, ABCB1/P-glycoprotein and ABCC2/MRP2 are all expressed at the apical surface of syncytiotrophoblast facing maternal blood and are putatively important protective proteins both for placental tissue and the fetus, because they are efflux transporters and their substrates include many drugs and also environmental chemicals. Such protective effect has been shown in animals, but these results cannot be directly extrapolated to humans due to interspecies differences in placental structure and function. Experimental models utilizing human placental tissue, especially human placental perfusion, offer valuable possibilities, which have been insufficiently studied so far.

Published

2009

6. Maternal Smoking and the Risk of Cancer in Early Life – A Meta-Analysis.

Author

Rumrich, Isabell Katharina, Viluksela, Matti, Vähäkangas, Kirsi, Gissler, Mika, Surcel, Heljä-Marja, and Hänninen, Otto

Subjects

HEALTH, SMOKING, CANCER risk factors, PREGNANCY complications, DEVELOPMENTAL biology, META-analysis

Abstract

Background: In spite of the well-known harmful effects on the fetus, many women continue smoking during pregnancy. Smoking as an important source of toxic chemicals may contribute to the developmental origin of diseases. Objectives: The aim of this work was to pursue the possible association between maternal smoking and cancer in early life. Specifically, we wanted to identify the associated early life cancer types, and to quantify the associations. Methods: In a systematic literature search 825 articles were identified in PubMed and Web of Science, and 55 more through the reference lists. Of these 62 fulfilled the criteria for inclusion in meta-analyses. Using Mantel-Haenszel or DerSimonian and Laird method, depending on heterogeneity of the studies, pooled estimates and 95% confidence intervals for eight cancer types were calculated. Results: Smoking during pregnancy was associated with an increased risk for for brain and central nervous system tumors (OR = 1.09; 95% CI = 1.02–1.17). Although the risk for lymphoma was also associated (OR = 1.21; 95% CI = 1.05–1.34), it did not hold up in subgroup analyses. Leukemia was not found to be associated with maternal smoking. Five other cancer types (bone, soft tissue, renal, hepatic, and germ cell cancer) were also examined, but the number of studies was too limited to exclude the possibility of maternal smoking as a risk factor for cancer in offspring. Conclusions: According to our meta-analyses, maternal smoking is associated with nervous system cancers, but not with leukemia in early life. Confirming or rejecting associations of maternal smoking with lymphoma and the five other cancer types requires further studies. [ABSTRACT FROM AUTHOR]

Published

2016

7. Human placental perfusion method in the assessment of transplacental passage of antiepileptic drugs

Author

Myllynen, Päivi, Pienimäki, Päivi, and Vähäkangas, Kirsi

Subjects

*EPILEPSY, *PLACENTA, *ANTICONVULSANTS, *PREGNANCY

Abstract

Abstract: Epilepsy is one of the most common neurological diseases, affecting about 0.5 to 1% of pregnant women. It is commonly accepted that older antiepileptic drugs bear teratogenic potential. So far, no agreement has been reached about the safest antiepileptic drug during pregnancy. It is known that nearly all drugs cross the placenta at least to some extent. Nowadays, there is very little information available of the pharmacokinetics of drugs in the feto-placental unit. Detailed information about drug transport across the placenta would be valuable for the development of safe and effective treatments. For reasons of safety, human studies on placental transfer are restricted to a limited number of drugs. Interspecies differences limit the extrapolation of animal data to humans. Several in vitro methods for the study of placental transfer have been developed over the past decades. The placental perfusion method is the only experimental method that has been used to study human placental transfer of substances in organized placental tissue. The aim of this article is to review human placental perfusion data on antiepileptic drugs. According to perfusion data, it seems that most of the antiepileptic drugs are transferred across the placenta meaning significant fetal exposure. [Copyright &y& Elsevier]

Published

2005

8. Human placental cell and tissue uptake of doxorubicin and its liposomal formulations.

Author

Soininen, Suvi K., Repo, Jenni K., Karttunen, Vesa, Auriola, Seppo, Vähäkangas, Kirsi H., and Ruponen, Marika

Subjects

*PLACENTA physiology, *DOXORUBICIN, *LIPOSOMES, *DRUG formularies, *DRUG toxicity, *PREGNANCY

Abstract

The anticancer drug doxorubicin and its liposomal formulations are in clinical use, doxorubicin also during pregnancy. However, little is known about how doxorubicin and its liposomal formulations are taken up by placental cells and whether they can cross human placenta. We therefore investigated quantitative cellular uptake and toxicity of doxorubicin and its two liposomal formulations, pH-sensitive liposomal doxorubicin (L-DOX) and commercially available pegylated liposomal doxorubicin (PL-DOX), in human placental choriocarcinoma (BeWo) cells. PL-DOX showed significantly lower cellular uptake and toxicity compared with doxorubicin and L-DOX. In preliminary studies with human placental perfusion, PL-DOX did not cross the placenta at all in 4 h, whereas doxorubicin and L-DOX crossed the placenta at low levels (max 12% of the dose). Furthermore, PL-DOX did not accumulate in placental tissue while doxorubicin did (up to 70% of the dose). Surface pegylation probably explains the low placental cell and tissue uptake of PL-DOX. Formulation of doxorubicin thus seems to enable a decrease of fetal exposure. [ABSTRACT FROM AUTHOR]

Published

2015

9. Kinetics of gold nanoparticles in the human placenta

Author

Myllynen, Päivi K., Loughran, Michael J., Howard, C. Vyvyan, Sormunen, Raija, Walsh, Adrian A., and Vähäkangas, Kirsi H.

Subjects

*NANOPARTICLES, *NANOSTRUCTURED materials, *PARTICLES, *NANOCRYSTALS

Abstract

Abstract: We studied the transfer of PEGylated gold nanoparticles through perfused human placenta. In ‘once-through’ perfusions using 15 and 30nm nanoparticles both maternal and fetal outflows were collected. Recirculating perfusions using 10 or 15nm nanoparticles lasted 6h. The gold concentration in samples was analysed on ICP-MS. The reference compound antipyrine crossed the placenta rapidly, as expected. In open perfusions nanoparticles were detected in maternal but not in fetal outflow, suggesting the lack of placental transfer. During 6h re-circulating perfusions, no particles were detected in fetal circulation. Using transmission electron microscopy (TEM) and silver enhancement, nanoparticles could be visualized in the placental tissue mainly in the trophoblastic cell layer. In in vitro experiments, nanoparticles were taken up by BeWo choriocarcinoma cells and retained inside the cells for an extended period of 48h. In conclusion, PEGylated gold nanoparticles of the size 10–30nm did not cross the perfused human placenta in detectable amounts into the fetal circulation within 6h. Whether PEGylated gold nanoparticles eventually are able to cross placenta and whether nanoparticles affect placental functions needs to be further studied. [Copyright &y& Elsevier]

Published

2008