Your search keyword '"C. Patrick Case"' showing total 20 results

1. Sex-specific differences in the mechanisms for enhanced thromboxane A2-mediated vasoconstriction in adult offspring exposed to prenatal hypoxia

Author

Murilo E. Graton, Floor Spaans, Rose He, Paulami Chatterjee, Raven Kirschenman, Anita Quon, Tom J. Phillips, C. Patrick Case, and Sandra T. Davidge

Subjects

Pregnancy complications, Prenatal hypoxia, Developmental origins of health and disease, Placental treatment, Coronary arteries, Mesenteric arteries, Medicine, Physiology, QP1-981

Abstract

Abstract Background Prenatal hypoxia, a common pregnancy complication, leads to impaired cardiovascular outcomes in the adult offspring. It results in impaired vasodilation in coronary and mesenteric arteries of the adult offspring, due to reduced nitric oxide (NO). Thromboxane A2 (TxA2) is a potent vasoconstrictor increased in cardiovascular diseases, but its role in the impact of prenatal hypoxia is unknown. To prevent the risk of cardiovascular disease by prenatal hypoxia, we have tested a maternal treatment using a nanoparticle-encapsulated mitochondrial antioxidant (nMitoQ). We hypothesized that prenatal hypoxia enhances vascular TxA2 responses in the adult offspring, due to decreased NO modulation, and that this might be prevented by maternal nMitoQ treatment. Methods Pregnant Sprague–Dawley rats received a single intravenous injection (100 µL) of vehicle (saline) or nMitoQ (125 µmol/L) on gestational day (GD)15 and were exposed to normoxia (21% O2) or hypoxia (11% O2) from GD15 to GD21 (term = 22 days). Coronary and mesenteric arteries were isolated from the 4-month-old female and male offspring, and vasoconstriction responses to U46619 (TxA2 analog) were evaluated using wire myography. In mesenteric arteries, L-NAME (pan-NO synthase (NOS) inhibitor) was used to assess NO modulation. Mesenteric artery endothelial (e)NOS, and TxA2 receptor expression, superoxide, and 3-nitrotyrosine levels were assessed by immunofluorescence. Results Prenatal hypoxia resulted in increased U46619 responsiveness in coronary and mesenteric arteries of the female offspring, and to a lesser extent in the male offspring, which was prevented by nMitoQ. In females, there was a reduced impact of L-NAME in mesenteric arteries of the prenatal hypoxia saline-treated females, and reduced 3-nitrotyrosine levels. In males, L-NAME increased U46619 responses in mesenteric artery to a similar extent, but TxA2 receptor expression was increased by prenatal hypoxia. There were no changes in eNOS or superoxide levels. Conclusions Prenatal hypoxia increased TxA2 vasoconstrictor capacity in the adult offspring in a sex-specific manner, via reduced NO modulation in females and increased TP expression in males. Maternal placental antioxidant treatment prevented the impact of prenatal hypoxia. These findings increase our understanding of how complicated pregnancies can lead to a sex difference in the programming of cardiovascular disease in the adult offspring. Graphical Abstract

Published

2024

2. Treating the placenta to prevent adverse effects of gestational hypoxia on fetal brain development

Author

Tom J. Phillips, Hannah Scott, David A. Menassa, Ashleigh L. Bignell, Aman Sood, Jude S. Morton, Takami Akagi, Koki Azuma, Mark F. Rogers, Catherine E. Gilmore, Gareth J. Inman, Simon Grant, Yealin Chung, Mais M. Aljunaidy, Christy-Lynn Cooke, Bruno R. Steinkraus, Andrew Pocklington, Angela Logan, Gavin P. Collett, Helena Kemp, Peter A. Holmans, Michael P. Murphy, Tudor A. Fulga, Andrew M. Coney, Mitsuru Akashi, Sandra T. Davidge, and C. Patrick Case

Subjects

Medicine, Science

Abstract

Abstract Some neuropsychiatric disease, including schizophrenia, may originate during prenatal development, following periods of gestational hypoxia and placental oxidative stress. Here we investigated if gestational hypoxia promotes damaging secretions from the placenta that affect fetal development and whether a mitochondria-targeted antioxidant MitoQ might prevent this. Gestational hypoxia caused low birth-weight and changes in young adult offspring brain, mimicking those in human neuropsychiatric disease. Exposure of cultured neurons to fetal plasma or to secretions from the placenta or from model trophoblast barriers that had been exposed to altered oxygenation caused similar morphological changes. The secretions and plasma contained altered microRNAs whose targets were linked with changes in gene expression in the fetal brain and with human schizophrenia loci. Molecular and morphological changes in vivo and in vitro were prevented by a single dose of MitoQ bound to nanoparticles, which were shown to localise and prevent oxidative stress in the placenta but not in the fetus. We suggest the possibility of developing preventative treatments that target the placenta and not the fetus to reduce risk of psychiatric disease in later life.

Published

2017

3. Sex-Specific Effects of Nanoparticle-Encapsulated MitoQ (nMitoQ) Delivery to the Placenta in a Rat Model of Fetal Hypoxia

Author

Esha Ganguly, Mais M. Aljunaidy, Raven Kirschenman, Floor Spaans, Jude S. Morton, Thomas E. J. Phillips, C. Patrick Case, Christy-Lynn M. Cooke, and Sandra T. Davidge

Subjects

placenta, hypoxia, MitoQ, nanoparticles, sex difference, Physiology, QP1-981

Abstract

Pregnancy complications associated with chronic fetal hypoxia have been linked to the development of adult cardiovascular disease in the offspring. Prenatal hypoxia has been shown to increase placental oxidative stress and impair placental function in a sex-specific manner, thereby affecting fetal development. As oxidative stress is central to placental dysfunction, we developed a placenta-targeted treatment strategy using the antioxidant MitoQ encapsulated into nanoparticles (nMitoQ) to reduce placental oxidative/nitrosative stress and improve placental function without direct drug exposure to the fetus in order to avoid off-target effects during development. We hypothesized that, in a rat model of prenatal hypoxia, nMitoQ prevents hypoxia-induced placental oxidative/nitrosative stress, promotes angiogenesis, improves placental morphology, and ultimately improves fetal oxygenation. Additionally, we assessed whether there were sex differences in the effectiveness of nMitoQ treatment. Pregnant rats were intravenously injected with saline or nMitoQ (100 μl of 125 μM) on gestational day (GD) 15 and exposed to either normoxia (21% O2) or hypoxia (11% O2) from GD15 to 21. On GD21, placentae from both sexes were collected for detection of superoxide, nitrotyrosine, nitric oxide, CD31 (endothelial cell marker), and fetal blood spaces, Vegfa and Igf2 mRNA expression in the placental labyrinth zone. Prenatal hypoxia decreased male fetal weight, which was not changed by nMitoQ treatment; however, placental efficiency (fetal/placental weight ratio) decreased by hypoxia and was increased by nMitoQ in both males and females. nMitoQ treatment reduced the prenatal hypoxia-induced increase in placental superoxide levels in both male and female placentae but improved oxygenation in only female placentae. Nitrotyrosine levels were increased in hypoxic female placentae and were reduced by nMitoQ. Prenatal hypoxia reduced placental Vegfa and Igf2 expression in both sexes, while nMitoQ increased Vegfa and Igf2 expression only in hypoxic female placentae. In summary, our study suggests that nMitoQ treatment could be pursued as a potential preventative strategy against placental oxidative stress and programming of adult cardiovascular disease in offspring exposed to hypoxia in utero. However, sex differences need to be taken into account when developing therapeutic strategies to improve fetal development in complicated pregnancies, as nMitoQ treatment was more effective in placentae from females than males.

Published

2019

4. Placenta‐targeted treatment in hypoxic dams improves maturation and growth of fetal cardiomyocytes in vitro via the release of placental factors

Author

Sandra T. Davidge, Mais M. Aljunaidy, Floor Spaans, Esha Ganguly, C. Patrick Case, Jude S. Morton, Christy-Lynn M. Cooke, Raven Kirschenman, and Thomas E. Phillips

Subjects

Male, Ubiquinone, Physiology, Placenta, 030204 cardiovascular system & hematology, medicine.disease_cause, Antioxidants, Muscle hypertrophy, Fetal Development, Rats, Sprague-Dawley, Andrology, 03 medical and health sciences, chemistry.chemical_compound, Organophosphorus Compounds, 0302 clinical medicine, Pregnancy, Physiology (medical), medicine, Animals, Myocytes, Cardiac, Hypoxia, Cells, Cultured, MitoQ, Fetus, Nutrition and Dietetics, business.industry, General Medicine, Hypoxia (medical), Rats, Oxidative Stress, medicine.anatomical_structure, Fetal circulation, chemistry, Culture Media, Conditioned, embryonic structures, Gestation, Female, medicine.symptom, business, 030217 neurology & neurosurgery, Oxidative stress

Abstract

New findings What is the central question of this study? Does treatment of hypoxic dams with a placenta-targeted antioxidant prevent the release of placenta-derived factors that impair maturation or growth of fetal cardiomyocytes in vitro? What is the main finding and its importance? Factors released from hypoxic placentae impaired fetal cardiomyocyte maturation (induced terminal differentiation) and growth (increased cell size) in vitro, which was prevented by maternal treatment with a placenta-targeted antioxidant (nMitoQ). Moreover, there were no sex differences in the effects of placental factors on fetal cardiomyocyte maturation and growth. Overall, our data suggest that treatment targeted against placental oxidative stress could prevent fetal programming of cardiac diseases via the release of placental factors. Abstract Pregnancy complications associated with placental oxidative stress may impair fetal organ development through the release of placenta-derived factors into the fetal circulation. We assessed the effect of factors secreted from placentae previously exposed to prenatal hypoxia on fetal cardiomyocyte development and developed a treatment strategy that targets placental oxidative stress by encapsulating the antioxidant MitoQ into nanoparticles (nMitoQ). We used a rat model of prenatal hypoxia (gestational day (GD) 15-21), which was treated with saline or nMitoQ on GD15. On GD21, placentae were harvested, placed in culture, and conditioned medium (containing placenta-derived factors) was collected after 24 h. This conditioned medium was then added to cultured cardiomyocytes from control dam fetuses. Conditioned medium from prenatally hypoxic placentae increased the percentage of binucleated cardiomyocytes (marker of terminal differentiation) and the size of mononucleated and binucleated cardiomyocytes (sign of hypertrophy), effects that were prevented by nMitoQ treatment. Our data suggest that factors derived from placentae previously exposed to prenatal hypoxia lead to abnormal fetal cardiomyocyte development, and show that treatment against placental oxidative stress may prevent fetal programming of cardiac disease.

Published

2020

5. In vitro placenta barrier model using primary human trophoblasts, underlying connective tissue and vascular endothelium

Author

Dionne Tannetta, Michiya Matsusaki, Paul Verkade, Simon Grant, John D. Aplin, Gavin Collett, Jon Hanley, Aman Sood, Fiona Day, Nagaraj D. Halemani, Catherine Murdoch-Davis, Akihiro Nishiguchi, Jennifer McGarvey, Ian L. Sargent, Helena Kemp, Mitsuru Akashi, Catherine E. Gilmore, and C. Patrick Case

Subjects

Endothelium, Placenta, Biophysics, Connective tissue, Bioengineering, 02 engineering and technology, Biology, Biomaterials, 03 medical and health sciences, Pregnancy, Human Umbilical Vein Endothelial Cells, medicine, Humans, Secretion, Cells, Cultured, reproductive and urinary physiology, Connective Tissue Cells, 030304 developmental biology, Neurons, 0303 health sciences, Fetus, Trophoblast, 021001 nanoscience & nanotechnology, Embryonic stem cell, In vitro, Trophoblasts, Cell biology, medicine.anatomical_structure, Mechanics of Materials, embryonic structures, Ceramics and Composites, Female, Endothelium, Vascular, 0210 nano-technology

Abstract

Fetal development may be compromised by adverse events at the placental interface between mother and fetus. However, it is still unclear how the communication between mother and fetus occurs through the placenta. In vitro - models of the human placental barrier, which could help our understanding and which recreate three-dimensional (3D) structures with biological functionalities and vasculatures, have not been reported yet. Here we present a 3D-vascularized human primary placental barrier model which can be constructed in 1 day. We illustrate the similarity of our model to first trimester human placenta, both in its structure and in its ability to respond to altered oxygen and to secrete factors that cause damage cells across the barrier including embryonic cortical neurons. We use this model to highlight the possibility that both the trophoblast and the endothelium within the placenta might play a role in the fetomaternal dialogue.

Published

2019

6. Nanoparticle‐encapsulated antioxidant improves placental mitochondrial function in a sexually dimorphic manner in a rat model of prenatal hypoxia

Author

Floor Spaans, C. Patrick Case, Christy-Lynn M. Cooke, Raven Kirschenman, Esha Ganguly, Claudia D. Holody, Sandra T. Davidge, Michael P. Murphy, Thomas E. Phillips, and Hélène Lemieux

Subjects

Male, 0301 basic medicine, Ubiquinone, Placenta, Cell Respiration, Biology, Fetal Hypoxia, medicine.disease_cause, Mitochondrial Dynamics, Biochemistry, Antioxidants, Rats, Sprague-Dawley, Andrology, 03 medical and health sciences, chemistry.chemical_compound, Organophosphorus Compounds, Sex Factors, 0302 clinical medicine, Pregnancy, Genetics, medicine, Animals, Molecular Biology, Fetus, MitoQ, Hypoxia (medical), Mitochondria, Rats, 030104 developmental biology, medicine.anatomical_structure, Mitochondrial biogenesis, chemistry, mitochondrial fusion, embryonic structures, Nanoparticles, Gestation, Female, medicine.symptom, 030217 neurology & neurosurgery, Oxidative stress, Biotechnology

Abstract

Pregnancy complications associated with prenatal hypoxia lead to increased placental oxidative stress. Previous studies suggest that prenatal hypoxia can reduce mitochondrial respiratory capacity and mitochondrial fusion, which could lead to placental dysfunction and impaired fetal development. We developed a placenta-targeted treatment strategy using a mitochondrial antioxidant, MitoQ, encapsulated into nanoparticles (nMitoQ) to reduce placental oxidative stress and (indirectly) improve fetal outcomes. We hypothesized that, in a rat model of prenatal hypoxia, nMitoQ improves placental mitochondrial function and promotes mitochondrial fusion in both male and female placentae. Pregnant rats were treated with saline or nMitoQ on gestational day (GD) 15 and exposed to normoxia (21% O2 ) or hypoxia (11% O2 ) from GD15-21. On GD21, male and female placental labyrinth zones were collected for mitochondrial respirometry assessments, mitochondrial content, and markers of mitochondrial biogenesis, fusion and fission. Prenatal hypoxia reduced complex IV activity and fusion in male placentae, while nMitoQ improved complex IV activity in hypoxic male placentae. In female placentae, prenatal hypoxia decreased respiration through the S-pathway (complex II) and increased N-pathway (complex I) respiration, while nMitoQ increased fusion in hypoxic female placentae. No changes in mitochondrial content, biogenesis or fission were found. In conclusion, nMitoQ improved placental mitochondrial function in male and female placentae from fetuses exposed to prenatal hypoxia, which may contribute to improved placental function. However, the mechanisms (ie, changes in mitochondrial respiratory capacity and mitochondrial fusion) were distinct between the sexes. Treatment strategies targeted against placental oxidative stress could improve placental mitochondrial function in complicated pregnancies.

Published

2021

7. Placental treatment improves cardiac tolerance to ischemia/reperfusion insult in adult male and female offspring exposed to prenatal hypoxia

Author

Sandra T. Davidge, Raven Kirschenman, Christy-Lynn M. Cooke, Jennie Vu, Thomas J. Phillips, Floor Spaans, Anita Quon, C. Patrick Case, and Nataliia Hula

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Offspring, Ubiquinone, Placenta, Ischemia, medicine.disease_cause, Antioxidants, Rats, Sprague-Dawley, 03 medical and health sciences, 0302 clinical medicine, Organophosphorus Compounds, Pregnancy, Internal medicine, Medicine, Animals, Hypoxia, Pharmacology, Fetus, business.industry, Age Factors, Hypoxia (medical), medicine.disease, 3. Good health, Phospholamban, Rats, 030104 developmental biology, Endocrinology, Cardiovascular Diseases, 030220 oncology & carcinogenesis, Prenatal Exposure Delayed Effects, Reperfusion Injury, Gestation, Nanoparticles, Female, medicine.symptom, business, Oxidative stress

Abstract

Offspring born from complicated pregnancies are at greater risk of cardiovascular disease in adulthood. Prenatal hypoxia is a common pregnancy complication that results in placental oxidative stress and impairs fetal development. Adult offspring exposed to hypoxia during fetal life are more susceptible to develop cardiac dysfunction, and show decreased cardiac tolerance to an ischemia/reperfusion (I/R) insult. To improve offspring cardiac outcomes, we have assessed the use of a placenta-targeted intervention during hypoxic pregnancies, by encapsulating the mitochondrial antioxidant MitoQ into nanoparticles (nMitoQ). We hypothesized that maternal nMitoQ treatment during hypoxic pregnancies improves cardiac tolerance to I/R insult in adult male and female offspring. Pregnant Sprague-Dawley rats were exposed to normoxia (21 % O2) or hypoxia (11 % O2) from gestational day 15-20, after injection with 100 μL saline or nMitoQ (125 μM) on GD15 (n=6-8/group). Male and female offspring were aged to 4 months. Both male and female offspring from hypoxic pregnancies showed reduced cardiac tolerance to I/R (assessed ex vivo using the isolated working heart technique) which was ameliorated by nMitoQ treatment. To identify potential molecular mechanisms for the changes in cardiac tolerance to I/R, cardiac levels/phosphorylation of proteins important for intracellular Ca2+ cycling were assessed with Western blotting. In prenatally hypoxic male offspring, improved cardiac recovery from I/R by nMitoQ was accompanied by increased cardiac phospholamban and phosphatase 2Ce levels, and a trend to decreased Ca2+/calmodulin-dependent protein kinase IIδ phosphorylation. In contrast, in female offspring, nMitoQ treatment in hypoxic pregnancies increased phospholamban and protein kinase Ce phosphorylation. Maternal nMitoQ treatment improves cardiac tolerance to I/R insult in adult offspring and thus has the potential to improve the later-life trajectory of cardiovascular health of adult offspring born from pregnancies complicated by prenatal hypoxia.

Published

2020

8. DNA damage signalling from the placenta to foetal blood as a potential mechanism for childhood leukaemia initiation

Author

C. Patrick Case, Camille Malouf, Nahid Zareian, Katrin Ottersbach, Allison Blair, Natalie Brown, Christopher Badie, Chrysa Kapeni, Duncan M. Baird, Jon D. Lane, and Els Mansell

Subjects

0301 basic medicine, Myeloid, DNA damage, Placenta, lcsh:Medicine, Article, 03 medical and health sciences, 0302 clinical medicine, Pregnancy, medicine, Humans, lcsh:Science, reproductive and urinary physiology, Chromosome Aberrations, Multidisciplinary, business.industry, Stem Cells, lcsh:R, Infant, Newborn, Fibroblasts, Precursor Cell Lymphoblastic Leukemia-Lymphoma, medicine.disease, Trophoblasts, Leukemia, Haematopoiesis, Leukemia, Myeloid, Acute, 030104 developmental biology, medicine.anatomical_structure, Cord blood, Culture Media, Conditioned, Immunology, embryonic structures, Carcinogens, Female, lcsh:Q, Bone marrow, Stem cell, business, 030217 neurology & neurosurgery, DNA Damage, Signal Transduction

Abstract

For many diseases with a foetal origin, the cause for the disease initiation remains unknown. Common childhood acute leukaemia is thought to be caused by two hits, the first in utero and the second in childhood in response to infection. The mechanism for the initial DNA damaging event are unknown. Here we have used in vitro, ex vivo and in vivo models to show that a placental barrier will respond to agents that are suspected of initiating childhood leukaemia by releasing factors that cause DNA damage in cord blood and bone marrow cells, including stem cells. We show that DNA damage caused by in utero exposure can reappear postnatally after an immune challenge. Furthermore, both foetal and postnatal DNA damage are prevented by prenatal exposure of the placenta to a mitochondrially-targeted antioxidant. We conclude that the placenta might contribute to the first hit towards leukaemia initiation by bystander-like signalling to foetal haematopoietic cells.

Published

2019

9. Maternal treatment with a placental-targeted antioxidant (MitoQ) impacts offspring cardiovascular function in a rat model of prenatal hypoxia

Author

Jude S. Morton, Christy-Lynn M. Cooke, Mais M. Aljunaidy, C. Patrick Case, Raven Kirschenman, Sandra T. Davidge, and Thomas E. Phillips

Subjects

0301 basic medicine, Male, Offspring, Ubiquinone, Placenta, Physiology, Intrauterine growth restriction, Gestational Age, Fetal Hypoxia, Antioxidants, Ventricular Function, Left, Rats, Sprague-Dawley, 03 medical and health sciences, chemistry.chemical_compound, Organophosphorus Compounds, Sex Factors, Pregnancy, medicine, Animals, Pharmacology, Fetus, MitoQ, business.industry, Age Factors, Hemodynamics, Hypoxia (medical), medicine.disease, Myocardial Contraction, 3. Good health, Disease Models, Animal, Oxidative Stress, 030104 developmental biology, medicine.anatomical_structure, chemistry, In utero, Cardiovascular Diseases, Maternal Exposure, Prenatal Exposure Delayed Effects, Gestation, Nanoparticles, Female, medicine.symptom, business

Abstract

Intrauterine growth restriction, a common consequence of prenatal hypoxia, is a leading cause of fetal morbidity and mortality with a significant impact on population health. Hypoxia may increase placental oxidative stress and lead to an abnormal release of placental-derived factors, which are emerging as potential contributors to developmental programming. Nanoparticle-linked drugs are emerging as a novel method to deliver therapeutics targeted to the placenta and avoid risking direct exposure to the fetus. We hypothesize that placental treatment with antioxidant MitoQ loaded onto nanoparticles (nMitoQ) will prevent the development of cardiovascular disease in offspring exposed to prenatal hypoxia. Pregnant rats were intravenously injected with saline or nMitoQ (125 μM) on gestational day (GD) 15 and exposed to either normoxia (21% O2) or hypoxia (11% O2) from GD15-21 (term: 22 days). In one set of animals, rats were euthanized on GD 21 to assess fetal body weight, placental weight and placental oxidative stress. In another set of animals, dams were allowed to give birth under normal atmospheric conditions (term: GD 22) and male and female offspring were assessed at 7 and 13 months of age for in vivo cardiac function (echocardiography) and vascular function (wire myography, mesenteric artery). Hypoxia increased oxidative stress in placentas of male and female fetuses, which was prevented by nMitoQ. 7-month-old male and female offspring exposed to prenatal hypoxia demonstrated cardiac diastolic dysfunction, of which nMitoQ improved only in 7-month-old female offspring. Vascular sensitivity to methacholine was reduced in 13-month-old female offspring exposed to prenatal hypoxia, while nMitoQ treatment improved vasorelaxation in both control and hypoxia exposed female offspring. Male 13-month-old offspring exposed to hypoxia showed an age-related decrease in vascular sensitivity to phenylephrine, which was prevented by nMitoQ. In summary, placental-targeted MitoQ treatment in utero has beneficial sex- and age-dependent effects on adult offspring cardiovascular function.

Published

2018

10. Treating the placenta to prevent adverse effects of gestational hypoxia on fetal brain development

Author

Hannah Scott, Bruno R. Steinkraus, C. Patrick Case, Ashleigh L. Bignell, Jude S. Morton, Gareth J. Inman, Andrew M. Coney, Tudor A. Fulga, Peter Holmans, Andrew Pocklington, David A. Menassa, Michael P. Murphy, Mark F. Rogers, Helena Kemp, Gavin Collett, Simon Grant, Mais M. Aljunaidy, Yealin Chung, Takami Akagi, Sandra T. Davidge, Thomas J. Phillips, Catherine E. Gilmore, Mitsuru Akashi, Christy-Lynn M. Cooke, Koki Azuma, Angela Logan, Aman Sood, Scott, Hannah [0000-0002-2497-549X], Pocklington, Andrew [0000-0002-2137-0452], and Apollo - University of Cambridge Repository

Subjects

0301 basic medicine, Organogenesis, Placenta, Gene Expression, medicine.disease_cause, Antioxidants, Fetal Development, chemistry.chemical_compound, 0302 clinical medicine, Pregnancy, Hypoxia, Microscopy, Confocal, Multidisciplinary, Brain, 3. Good health, Experimental models of disease, medicine.anatomical_structure, embryonic structures, Medicine, Female, medicine.symptom, medicine.medical_specialty, Offspring, Science, Article, 03 medical and health sciences, Fetus, Internal medicine, medicine, Animals, MitoQ, Disease model, business.industry, Trophoblast, Hypoxia (medical), medicine.disease, R1, Rats, Pregnancy Complications, Oxidative Stress, 030104 developmental biology, Endocrinology, chemistry, Schizophrenia, Reactive Oxygen Species, business, Biomarkers, 030217 neurology & neurosurgery, Oxidative stress

Abstract

Some neuropsychiatric disease, including schizophrenia, may originate during prenatal development, following periods of gestational hypoxia and placental oxidative stress. Here we investigated if gestational hypoxia promotes damaging secretions from the placenta that affect fetal development and whether a mitochondria-targeted antioxidant MitoQ might prevent this. Gestational hypoxia caused low birth-weight and changes in young adult offspring brain, mimicking those in human neuropsychiatric disease. Exposure of cultured neurons to fetal plasma or to secretions from the placenta or from model trophoblast barriers that had been exposed to altered oxygenation caused similar morphological changes. The secretions and plasma contained altered microRNAs whose targets were linked with changes in gene expression in the fetal brain and with human schizophrenia loci. Molecular and morphological changes in vivo and in vitro were prevented by a single dose of MitoQ bound to nanoparticles, which were shown to localise and prevent oxidative stress in the placenta but not in the fetus. We suggest the possibility of developing preventative treatments that target the placenta and not the fetus to reduce risk of psychiatric disease in later life.

Published

2017

11. Secretions from placenta, after hypoxia/reoxygenation, can damage developing neurones of brain under experimental conditions

Author

Robert Keehan, Roberta Goodall, Oliver Beaumont, Akihiro Nishiguchi, Lizeth Lacharme-Lora, Michele Giugliano, Michiya Matsusaki, Christopher Coyle, Hiroyoshi Y. Tanaka, Tracey Masters, Nicki Cohen, Jon Hanley, Veronica H.L. Leinster, C. Patrick Case, Andrew D. Randall, Kristian Aquilina, Ian L. Sargent, Katja Simon, Nagaraj D. Halemani, Jennifer McGarvey, William Ind, Helena Kemp, Simon Grant, Emma Scull-Brown, Sharan Athwal, Aman Sood, Daniel J Curtis, Mitsuru Akashi, Rocco A Barone, Jon D. Lane, Thomas E. Phillips, Gavin Collett, Mitsunobu R. Kano, Leila Cornes, Xun Liu, Marianne Thoresen, and Dionne Tannetta

Subjects

Placenta, Dendrite, Settore BIO/09 - Fisiologia, Membrane Potentials, Tissue Culture Techniques, 0302 clinical medicine, Pregnancy, Hypoxia, Cells, Cultured, Parvalbumin, Cerebral Cortex, Neurons, 0303 health sciences, GABAA receptor, Glutamate receptor, Cerebral cortex, Development, Neurodevelopmental disorder, Neurone, Reoxygenation, Schizophrenia, Brain, Cell Hypoxia, medicine.anatomical_structure, Neurology, embryonic structures, Female, medicine.symptom, medicine.medical_specialty, Biology, 03 medical and health sciences, Fetus, Developmental Neuroscience, Internal medicine, Glial Fibrillary Acidic Protein, medicine, Animals, Humans, Rats, Wistar, 030304 developmental biology, Cytotrophoblast, Dose-Response Relationship, Drug, Dendrites, Hypoxia (medical), Embryo, Mammalian, Rats, Oxygen, Endocrinology, Animals, Newborn, Culture Media, Conditioned, Human medicine, Reactive Oxygen Species, 030217 neurology & neurosurgery, Immunostaining

Abstract

Some psychiatric diseases in children and young adults are thought to originate from adverse exposures during fetal life, including hypoxia and hypoxia/reoxygenation. The mechanism is not understood. Several authors have emphasised that the placenta is likely to play an important role as the key interface between mother and fetus. Here we have explored whether a first trimester human placenta or model barrier of primary human cytototrophoblasts might secrete factors, in response to hypoxia or hypoxia/reoxygenation, that could damage neurones. We find that the secretions in conditioned media caused an increase of [Ca2 +]i and mitochondrial free radicals and a decrease of dendritic lengths, branching complexity, spine density and synaptic activity in dissociated neurones from embryonic rat cerebral cortex. There was altered staining of glutamate and GABA receptors. We identify glutamate as an active factor within the conditioned media and demonstrate a specific release of glutamate from the placenta/cytotrophoblast barriers in vitro after hypoxia or hypoxia/reoxygenation. Injection of conditioned media into developing brains of P4 rats reduced the numerical density of parvalbumin-containing neurones in cortex, hippocampus and reticular nucleus, reduced immunostaining of glutamate receptors and altered cellular turnover. These results show that the placenta is able to release factors, in response to altered oxygen, that can damage developing neurones under experimental conditions.

Published

2014

12. DNA damaging bystander signalling from stem cells, cancer cells and fibroblasts after Cr(VI) exposure and its dependence on telomerase

Author

Maeve A. Caldwell, Duncan M. Baird, Lucy A. Crompton, Ryan Phillips, Nicola Cogan, C. Patrick Case, Miguel A. Rubio, Roger Newson, and Fiona M. Lyng

Subjects

Chromium, Telomerase, DNA damage, Health, Toxicology and Mutagenesis, Fluorescent Antibody Technique, Ascorbic Acid, Biology, Histones, Cancer stem cell, Genetics, Bystander effect, Humans, Telomerase reverse transcriptase, Thyroid Neoplasms, Molecular Biology, Cells, Cultured, Embryonic Stem Cells, Micronucleus Tests, Tumor Necrosis Factor-alpha, Bystander Effect, Fibroblasts, Molecular biology, Telomere, Cancer cell, Cancer research, Stem cell, DNA Damage, Signal Transduction

Abstract

The bystander effect is a feature of low dose radiation exposure and is characterized by a signaling process from irradiated cells to non irradiated cells, which causes DNA and chromosome damage in these 'nearest neighbour' cells. Here we show that a low and short dose of Cr(VI) can induce stem cells, cancer cells and fibroblasts to chronically secrete bystander signals, which cause DNA damage in neighboring cells. The Cr(VI) induced bystander signaling depended on the telomerase status of either cell. Telomerase negative fibroblasts were able to receive DNA damaging signals from telomerase positive or negative fibroblasts or telomerase positive cancer cells. However telomerase positive fibroblasts were resistant to signals from Cr(VI) exposed telomerase positive fibroblasts or cancer cells. Human embryonic stem cells, with positive Oct4 staining as a marker of pluripotency, showed no significant increase of DNA damage from adjacent Cr and mitomycin C exposed fibroblasts whilst those cells that were negatively stained did. This selectivity of DNA damaging bystander signaling could be an important consideration in developing therapies against cancer and in the safety and effectiveness of tissue engineering and transplantation using stem cells.

Published

2010

13. Evidence for bystander signalling between human trophoblast cells and human embryonic stem cells

Author

Barry Sampson, Simon Grant, Nicholas D. Allen, C. Patrick Case, Anna J. Jones, Sharan Athwal, Thomas F. Allison, Paul J. Gokhale, and Peter W. Andrews

Subjects

Embryonic stem cells, Cell signaling, DNA damage, Cellular differentiation, Human Embryonic Stem Cells, Apoptosis, Cell Communication, Stem cells, Biology, Article, Pluripotent stem cells, Metals, Heavy, medicine, Bystander effect, Humans, Induced pluripotent stem cell, QH426, reproductive and urinary physiology, Multidisciplinary, Tumor Necrosis Factor-alpha, Gap Junctions, Trophoblast, Cell Differentiation, Cell Cycle Checkpoints, Fibroblasts, Embryonic stem cell, Trophoblasts, Cell biology, medicine.anatomical_structure, Connexin 43, Cytokines, Stem cell, DNA Damage, Signal Transduction

Abstract

Maternal exposure during pregnancy to toxins can occasionally lead to miscarriage and malformation. It is currently thought that toxins pass through the placental barrier, albeit bi-layered in the first trimester and damage the fetus directly, albeit at low concentration. Here we examined the responses of human embryonic stem (hES) cells in tissue culture to two metals at low concentration. We compared direct exposures with indirect exposures across a bi-layered model of the placenta cell barrier. Direct exposure caused increased DNA damage without apoptosis or a loss of cell number but with some evidence of altered differentiation. Indirect exposure caused increased DNA damage and apoptosis but without loss of pluripotency. This was not caused by metal ions passing through the barrier. Instead the hES cells responded to signalling molecules (including TNF-α) secreted by the barrier cells. This mechanism was dependent on connexin 43 mediated intercellular ‘bystander signalling’ both within and between the trophoblast barrier and the hES colonies. These results highlight key differences between direct and indirect exposure of hES cells across a trophoblast barrier to metal toxins. It offers a theoretical possibility that an indirectly mediated toxicity of hES cells might have biological relevance to fetal development.

Published

2015

14. Understanding nanoparticle cellular entry: A physicochemical perspective

Author

C. Patrick Case, Wuge H. Briscoe, and Charlotte M. Beddoes

Subjects

Mechanism (biology), Chemistry, Cell Membrane, Nanoparticle, Nanotechnology, Surfaces and Interfaces, Environmental exposure, Endocytosis, Cell membrane, Colloid and Surface Chemistry, Membrane, medicine.anatomical_structure, Nanotoxicology, Related research, medicine, Humans, Nanoparticles, Physical and Theoretical Chemistry, Hydrophobic and Hydrophilic Interactions

Abstract

Understanding interactions between nanoparticles (NPs) with biological matter, particularly cells, is becoming increasingly important due to their growing application in medicine and materials, and consequent biological and environmental exposure. For NPs to be utilised to their full potential, it is important to correlate their functional characteristics with their physical properties, which may also be used to predict any adverse cellular responses. A key mechanism for NPs to impart toxicity is to gain cellular entry directly. Many parameters affect the behaviour of nanomaterials in a cellular environment particularly their interactions with cell membranes, including their size, shape and surface chemistry as well as factors such as the cell type, location and external environment (e.g. other surrounding materials, temperature, pH and pressure). Aside from in vitro and in vivo experiments, model cell membrane systems have been used in both computer simulations and physicochemical experiments to elucidate the mechanisms for NP cellular entry. Here we present a brief overview of the effects of NPs physical parameters on their cellular uptake, with focuses on 1) related research using model membrane systems and physicochemical methodologies; and 2) proposed physical mechanisms for NP cellular entrance, with implications to their nanotoxicity. We conclude with a suggestion that the energetic process of NP cellular entry can be evaluated by studying the effects of NPs on lipid mesophase transitions, as the molecular deformations and thus the elastic energy cost are analogous between such transitions and endocytosis. This presents an opportunity for contributions to understanding nanotoxicity from a physicochemical perspective.

Published

2014

15. Metallic debris from orthopaedic implants

Author

C. Patrick Case and Ian D. Learmonth

Subjects

Metallic debris, Metals, Surface Properties, business.industry, Neoplasms, Metallurgy, Humans, Medicine, General Medicine, Arthroplasty, Replacement, Middle Aged, business

Published

2007

16. Histology of failed metal-on-metal hip arthroplasty; three distinct sub-types

Author

Gordon C. Bannister, R.P. Baker, C. Patrick Case, and James R Berstock

Subjects

Male, Reoperation, Pathology, medicine.medical_specialty, medicine.medical_treatment, Radiography, Arthroplasty, Replacement, Hip, medicine, Humans, Orthopedics and Sports Medicine, Lymphocytes, Retrospective Studies, business.industry, Foreign-Body Reaction, Macrophages, Soft tissue, Histology, Metal debris, Middle Aged, Arthroplasty, Hip resurfacing, Surgery, Prosthesis Failure, Hip arthroplasty, Sub types, Metal-on-Metal Joint Prostheses, Female, Hip Prosthesis, business

Abstract

The histological specimens from 29 failed metal-on-metal (MoM) hip arthroplasties treated at our institution were reviewed. Five patients had a failed MoM total hip arthroplasty (THA), and 24 patients a failed hip resurfacing. Clinical and radiographic features of each hip were correlated with the histological findings. We report three major histological subtypes. Patients either have a macrophage response to metal debris, a lymphocytic response (ALVAL) or a mixed picture of both. In addition we observe that the ALVAL response is located deep within tissue specimens, and can occur in environments of low wear debris. The macrophage response is limited to the surface of tissue specimens, with normal underlying tissue. Patients with subsequently confirmed ALVAL underwent revision surgery sooner than patients whose histology confirms a macrophage response (3.8 vs. 6.9 years p

Published

2013

17. Consequences of exposure to peri-articular injections of micro- and nano-particulate cobalt-chromium alloy

Author

Aman Sood, Chris Brown, C. Patrick Case, John Fisher, Lizeth Lacharme-Lora, Eileen Ingham, Roger B. Newson, and Blessing Mukonoweshuro

Subjects

Chromium, Materials science, Knee Joint, Biophysics, Nanoparticle, chemistry.chemical_element, Metal Nanoparticles, Prefrontal Cortex, Bioengineering, Injections, Intra-Articular, Biomaterials, Interferon-gamma, Mice, Bone Marrow, medicine, Animals, Particle Size, Chromosome Aberrations, Mice, Inbred C3H, Metallurgy, Radiochemistry, Cobalt-chrome, Cobalt, medicine.disease, Type IV hypersensitivity, Comet assay, chemistry, Mechanics of Materials, Ceramics and Composites, Interleukin-2, Nanometre, Female, Particle size, Chromium Alloys, Comet Assay, DNA Damage

Abstract

Metal hip replacements generate both metal particles and ions. The biological effects of peri-articular exposure to nanometre and micron sized cobalt chrome (CoCr) wear particles were investigated in a mouse model. Mice received injections of two clinically relevant doses of nanoparticles (32 nm), one of micron sized (2.9 μm) CoCr particles or vehicle alone into the right knee joint at 0, 6, 12 and 18 weeks. Mice were analysed for genotoxic and immunological effects 1, 4 and 40 weeks post exposure. Nanoparticles but not micron particles progressively corroded at the injection site. Micron sized particles were physically removed. No increase of Co or Cr was seen in peripheral blood between 1 and 40 weeks post exposure to particles. No significant inflammatory changes were observed in the knee tissues including ALVAL or necrosis. DNA damage was increased in bone marrow at one and forty weeks and in cells isolated from frontal cortex at 40 weeks after injection with nanoparticles. Mice exposed to the micron sized, but not nanoparticles became immunologically sensitized to Cr(III), Cr (VI) and Ni(II) over the 40 week period as determined by lymphocyte transformation and ELISpot (IFN-γ and IL-2) assays. The data indicated that the response to the micron sized particles was Th1 driven, indicative of type IV hypersensitivity. This study adds to understanding of the potential adverse biological reactions to metal wear products.

Published

2013

18. Changes in metal levels and chromosome aberrations in the peripheral blood of patients after metal-on-metal hip arthroplasty

Author

C. Patrick Case, Manjit Bhamra, Ann Doherty, Justine Turner, Dariusz Ladon, and Roger Newson

Subjects

Chromium, Pathology, medicine.medical_specialty, medicine.medical_treatment, Arthroplasty, Replacement, Hip, Physiology, Aneuploidy, Chromosomal translocation, Prosthesis Design, Translocation, Genetic, medicine, Humans, Orthopedics and Sports Medicine, Prospective Studies, Prospective cohort study, Whole blood, Aged, Aged, 80 and over, Chromosome Aberrations, Molybdenum, business.industry, Chromosome, Cobalt, Middle Aged, medicine.disease, Arthroplasty, Peripheral blood, Prosthesis Failure, Hip arthroplasty, Metals, sense organs, Hip Prosthesis, business

Abstract

A prospective study was performed to investigate changes in metal levels and chromosome aberrations in patients within 2 years of receiving metal-on-metal hip arthroplasties. There was a statistically significant increase of cobalt and chromium concentrations, with a small increase in molybdenum, in whole blood at 6, 12, and 24 months after surgery. There was also a statistically significant increase of both chromosome translocations and aneuploidy in peripheral blood lymphocytes at 6, 12, and 24 months after surgery. The changes were generally progressive with time, but the change in aneuploidy was much greater than in chromosome translocations. No statistically significant correlations were found in secondary analyses between chromosome translocation indices and cobalt or chromium concentration in whole blood. Although the clinical consequences of these changes, if any, are unknown, future epidemiological studies could usefully include direct comparisons of patients with implants of different composition.

Published

2004

19. Molecular Approaches to the Study of Pain

Author

C. Patrick Case, Richard A. Newton, Philip T. Davey, Val Piercy, Andrew A. Parsons, Sharon Bingham, Sally N. Lawson, Andrew D. Medhurst, Pravin Raval, and Gareth J. Sanger

Subjects

Biology

Published

2003

20. Prophylactic oral fluconazole and candida fungaemia

Author

Philip Whitehead, A. P. MacGowan, D. S. Reeves, NicholasM. Brown, C. Patrick Case, and David Felmingham

Subjects

medicine.medical_specialty, business.industry, Internal medicine, MEDLINE, Medicine, General Medicine, business, Fluconazole, medicine.drug

Published

1991