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1. Spatial proteomics reveals phenotypic and functional differences in T cell and macrophage subsets during villitis of unknown etiology

Author

Petra K. Lothert, Bohdana Fedyshyn, Sylvie Girard, Rana Chakraborty, Andrew P. Norgan, and Elizabeth Ann L. Enninga

Subjects
Medicine, Science
Abstract

Abstract Villitis of unknown etiology (VUE) is a prevalent inflammatory pathology of the placenta characterized by infiltration of maternal T cells and accumulation of fetal macrophages into chorionic villi. VUE is associated with a variety of adverse clinical outcomes, including fetal growth restriction and fetal demise. Evaluation of the phenotypic and functional differences between two immune cell types associated with this pathology, namely T cells and macrophages, was completed to gain a deeper understanding of the immuno-pathogenesis of VUE. GeoMx Digital Spatial Profiling was performed on placental tissue from 4 high grade VUE cases and 4 controls with no underlying pathology. Placental tissues were fluorescently labeled with CD3 and CD68 antibodies and oligo-conjugated antibodies against 48 protein targets. Overall, T cells in VUE exhibited upregulated markers of activation, memory, and antigen experience compared to controls and were altered based on placental location (villi vs. decidua). Additionally, villous macrophages in VUE upregulated costimulatory and major histocompatibility complex class I and II molecules compared to controls and macrophage subtypes in the decidua. Data herein provides new mechanistic insights into T cell and macrophage biology in VUE which contribute to this abnormal immune response to pregnancy.

Published
2024
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2. Maternal SARS-CoV-2 infection in pregnancy disrupts gene expression in Hofbauer cells with limited impact on cytotrophoblasts.

Author

Elizabeth Ann L Enninga, Huy Quang Quach, Jin Sung Jang, Maria Cristina Miranda de Araujo Correia, Yaroslav Fedyshyn, Bohdana Fedyshyn, Maureen Lemens, Dawn Littlefield, Supriya Behl, Elise Sintim-Aboagye, Maria C Mejia Plazas, Maria C Cardenas, Shree Chakraborty, Satoko Yamaoka, Hideki Ebihara, Akhilesh Pandey, Hu Li, Andrew D Badley, Erica L Johnson, Jie Sun, Andrew P Norgan, Regan N Theiler, and Rana Chakraborty

Subjects
Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5
Abstract

BackgroundHofbauer cells (HBCs) and cytotrophoblasts (CTBs) are major cell populations in placenta. The indirect impact of maternal SARS-CoV-2 disease on these cells that are not directly infected has not been extensively studied. Herein, we profiled gene expression in HBCs and CTBs isolated from placentae of recovered pregnant subjects infected with SARS-CoV-2 during all trimesters of pregnancy, placentae from subjects with active infection, SARS-CoV-2 vaccinated subjects, and those who were unexposed to the virus.MethodsPlacentae were collected within 4 h post-delivery and membrane-free tissues were enzymatically digested for the isolation of HBCs and CTBs. RNA extracted from HBCs and CTBs were sequenced using 150bp paired-end reads. Differentially expressed genes (DEGs) were identified by DESeq2 package in R and enriched in GO Biological Processes, KEGG Pathway, Reactome Gene Sets, Hallmark Gene Sets, and Canonical Pathways. Protein-protein interactions among the DEGs were modelled using STRING and BioGrid.ResultsPregnant subjects (n = 30) were recruited and categorized into six groups: infected with SARS-CoV-2 in i) the first (1T, n = 4), ii) second (2T, n = 5), iii) third (3T, n = 5) trimester, iv) tested positive at delivery (Delivery, n = 5), v) never infected (Control, n = 6), and vi) fully mRNA-vaccinated by delivery (Vaccinated, n = 5). Compared to the Control group, gene expression analysis showed that HBCs from infected subjects had significantly altered gene expression profiles, with the 2T group having the highest number of DEGs (1,696), followed by 3T and 1T groups (1,656 and 958 DEGs, respectively). These DEGs were enriched for pathways involved in immune regulation for host defense, including production of cytokines, chemokines, antimicrobial proteins, ribosomal assembly, neutrophil degranulation inflammation, morphogenesis, and cell migration/adhesion. Protein-protein interaction analysis mapped these DEGs with oxidative phosphorylation, translation, extracellular matrix organization, and type I interferon signaling. Only 95, 23, and 8 DEGs were identified in CTBs of 1T, 2T, and 3T groups, respectively. Similarly, 11 and 3 DEGs were identified in CTBs and HBCs of vaccinated subjects, respectively. Reassuringly, mRNA vaccination did not induce an inflammatory response in placental cells.ConclusionsOur studies demonstrate a significant impact of indirect SARS-CoV-2 infection on gene expression of inner mesenchymal HBCs, with limited effect on lining CTB cells isolated from pregnant subjects infected and recovered from SARS-CoV-2. The pathways associated with these DEGs identify potential targets for therapeutic intervention.

Published
2024
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3. NDST1 Preferred Promoter Confirmation and Identification of Corresponding Transcriptional Inhibitors as Substrate Reduction Agents for Multiple Mucopolysaccharidosis Disorders.

Author

Ilona Tkachyova, Xiaolian Fan, Anne-Marie LamHonWah, Bohdana Fedyshyn, Ingrid Tein, Don J Mahuran, and Andreas Schulze

Subjects
Medicine, Science
Abstract

The stepwise degradation of glycosaminoglycans (GAGs) is accomplished by twelve lysosomal enzymes. Deficiency in any of these enzymes will result in the accumulation of the intermediate substrates on the pathway to the complete turnover of GAGs. The accumulation of these undegraded substrates in almost any tissue is a hallmark of all Mucopolysaccharidoses (MPS). Present therapeutics based on enzyme replacement therapy and bone marrow transplantation have low effectiveness for the treatment of MPS with neurological complications since enzymes used in these therapies are unable to cross the blood brain barrier. Small molecule-based approaches are more promising in addressing neurological manifestations. In this report we identify a target for developing a substrate reduction therapy (SRT) for six MPS resulting from the abnormal degradation of heparan sulfate (HS). Using the minimal promoter of NDST1, one of the first modifying enzymes of HS precursors, we established a luciferase based reporter gene assay capable of identifying small molecules that could potentially reduce HS maturation and therefore lessen HS accumulation in certain MPS. From the screen of 1,200 compounds comprising the Prestwick Chemical library we identified SAHA, a histone deacetylase inhibitor, as the drug that produced the highest inhibitory effects in the reporter assay. More importantly SAHA treated fibroblasts expressed lower levels of endogenous NDST1 and accumulated less 35S GAGs in patient cells. Thus, by using our simple reporter gene assay we have demonstrated that by inhibiting the transcription of NDST1 with small molecules, identified by high throughput screening, we can also reduce the level of sulfated HS substrate in MPS patient cells, potentially leading to SRT.

Published
2016
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4. Supplementary Table 7 from Essential Gene Profiles in Breast, Pancreatic, and Ovarian Cancer Cells

Author

Jason Moffat, Benjamin G. Neel, Robert Rottapel, Jeffrey L. Wrana, Troy Ketela, Maliha Haider, Josee Normand, Christine Misquitta, Patricia Mero, Alla Buzina, Dahlia Kasimer, Alessandro Datti, Frederick S. Vizeacoumar, Franco J. Vizeacoumar, Glauber C. Brito, Marianna Luhova, Bohdana Fedyshyn, Dewald van Dyk, Judice L.Y. Koh, Yaroslav Fedyshyn, Mauricio Medrano, Fabrice Sircoulomb, Paul M. Krzyzanowski, Konstantina Karamboulas, Azin Sayad, Fernando Suarez, Kevin R. Brown, and Richard Marcotte

Abstract

XLS file - 41K

Published
2023

5. Supplementary Table 9 from Essential Gene Profiles in Breast, Pancreatic, and Ovarian Cancer Cells

Author

Jason Moffat, Benjamin G. Neel, Robert Rottapel, Jeffrey L. Wrana, Troy Ketela, Maliha Haider, Josee Normand, Christine Misquitta, Patricia Mero, Alla Buzina, Dahlia Kasimer, Alessandro Datti, Frederick S. Vizeacoumar, Franco J. Vizeacoumar, Glauber C. Brito, Marianna Luhova, Bohdana Fedyshyn, Dewald van Dyk, Judice L.Y. Koh, Yaroslav Fedyshyn, Mauricio Medrano, Fabrice Sircoulomb, Paul M. Krzyzanowski, Konstantina Karamboulas, Azin Sayad, Fernando Suarez, Kevin R. Brown, and Richard Marcotte

Abstract

XLS file - 22K

Published
2023

6. Supplementary Table 3 from Essential Gene Profiles in Breast, Pancreatic, and Ovarian Cancer Cells

Author

Jason Moffat, Benjamin G. Neel, Robert Rottapel, Jeffrey L. Wrana, Troy Ketela, Maliha Haider, Josee Normand, Christine Misquitta, Patricia Mero, Alla Buzina, Dahlia Kasimer, Alessandro Datti, Frederick S. Vizeacoumar, Franco J. Vizeacoumar, Glauber C. Brito, Marianna Luhova, Bohdana Fedyshyn, Dewald van Dyk, Judice L.Y. Koh, Yaroslav Fedyshyn, Mauricio Medrano, Fabrice Sircoulomb, Paul M. Krzyzanowski, Konstantina Karamboulas, Azin Sayad, Fernando Suarez, Kevin R. Brown, and Richard Marcotte

Abstract

XLS file - 51K

Published
2023

7. Supplementary Table 5d from Essential Gene Profiles in Breast, Pancreatic, and Ovarian Cancer Cells

Author

Jason Moffat, Benjamin G. Neel, Robert Rottapel, Jeffrey L. Wrana, Troy Ketela, Maliha Haider, Josee Normand, Christine Misquitta, Patricia Mero, Alla Buzina, Dahlia Kasimer, Alessandro Datti, Frederick S. Vizeacoumar, Franco J. Vizeacoumar, Glauber C. Brito, Marianna Luhova, Bohdana Fedyshyn, Dewald van Dyk, Judice L.Y. Koh, Yaroslav Fedyshyn, Mauricio Medrano, Fabrice Sircoulomb, Paul M. Krzyzanowski, Konstantina Karamboulas, Azin Sayad, Fernando Suarez, Kevin R. Brown, and Richard Marcotte

Abstract

XLS file - 49K

Published
2023

8. Supplementary Methods from Essential Gene Profiles in Breast, Pancreatic, and Ovarian Cancer Cells

Author

Jason Moffat, Benjamin G. Neel, Robert Rottapel, Jeffrey L. Wrana, Troy Ketela, Maliha Haider, Josee Normand, Christine Misquitta, Patricia Mero, Alla Buzina, Dahlia Kasimer, Alessandro Datti, Frederick S. Vizeacoumar, Franco J. Vizeacoumar, Glauber C. Brito, Marianna Luhova, Bohdana Fedyshyn, Dewald van Dyk, Judice L.Y. Koh, Yaroslav Fedyshyn, Mauricio Medrano, Fabrice Sircoulomb, Paul M. Krzyzanowski, Konstantina Karamboulas, Azin Sayad, Fernando Suarez, Kevin R. Brown, and Richard Marcotte

Abstract

PDF file - 217K

Published
2023

9. Supplementary Table 8 from Essential Gene Profiles in Breast, Pancreatic, and Ovarian Cancer Cells

Author

Jason Moffat, Benjamin G. Neel, Robert Rottapel, Jeffrey L. Wrana, Troy Ketela, Maliha Haider, Josee Normand, Christine Misquitta, Patricia Mero, Alla Buzina, Dahlia Kasimer, Alessandro Datti, Frederick S. Vizeacoumar, Franco J. Vizeacoumar, Glauber C. Brito, Marianna Luhova, Bohdana Fedyshyn, Dewald van Dyk, Judice L.Y. Koh, Yaroslav Fedyshyn, Mauricio Medrano, Fabrice Sircoulomb, Paul M. Krzyzanowski, Konstantina Karamboulas, Azin Sayad, Fernando Suarez, Kevin R. Brown, and Richard Marcotte

Abstract

XLS file - 303K

Published
2023

10. Supplementary Table 1 from Essential Gene Profiles in Breast, Pancreatic, and Ovarian Cancer Cells

Author

Jason Moffat, Benjamin G. Neel, Robert Rottapel, Jeffrey L. Wrana, Troy Ketela, Maliha Haider, Josee Normand, Christine Misquitta, Patricia Mero, Alla Buzina, Dahlia Kasimer, Alessandro Datti, Frederick S. Vizeacoumar, Franco J. Vizeacoumar, Glauber C. Brito, Marianna Luhova, Bohdana Fedyshyn, Dewald van Dyk, Judice L.Y. Koh, Yaroslav Fedyshyn, Mauricio Medrano, Fabrice Sircoulomb, Paul M. Krzyzanowski, Konstantina Karamboulas, Azin Sayad, Fernando Suarez, Kevin R. Brown, and Richard Marcotte

Abstract

XLS file - 15.2MB

Published
2023

11. Supplementary Table 6 from Essential Gene Profiles in Breast, Pancreatic, and Ovarian Cancer Cells

Author

Jason Moffat, Benjamin G. Neel, Robert Rottapel, Jeffrey L. Wrana, Troy Ketela, Maliha Haider, Josee Normand, Christine Misquitta, Patricia Mero, Alla Buzina, Dahlia Kasimer, Alessandro Datti, Frederick S. Vizeacoumar, Franco J. Vizeacoumar, Glauber C. Brito, Marianna Luhova, Bohdana Fedyshyn, Dewald van Dyk, Judice L.Y. Koh, Yaroslav Fedyshyn, Mauricio Medrano, Fabrice Sircoulomb, Paul M. Krzyzanowski, Konstantina Karamboulas, Azin Sayad, Fernando Suarez, Kevin R. Brown, and Richard Marcotte

Abstract

XLS file - 75K

Published
2023

12. Supplementary Table 4 from Essential Gene Profiles in Breast, Pancreatic, and Ovarian Cancer Cells

Author

Jason Moffat, Benjamin G. Neel, Robert Rottapel, Jeffrey L. Wrana, Troy Ketela, Maliha Haider, Josee Normand, Christine Misquitta, Patricia Mero, Alla Buzina, Dahlia Kasimer, Alessandro Datti, Frederick S. Vizeacoumar, Franco J. Vizeacoumar, Glauber C. Brito, Marianna Luhova, Bohdana Fedyshyn, Dewald van Dyk, Judice L.Y. Koh, Yaroslav Fedyshyn, Mauricio Medrano, Fabrice Sircoulomb, Paul M. Krzyzanowski, Konstantina Karamboulas, Azin Sayad, Fernando Suarez, Kevin R. Brown, and Richard Marcotte

Abstract

XLS file - 32K

Published
2023

13. Supplementary Table 2 from Essential Gene Profiles in Breast, Pancreatic, and Ovarian Cancer Cells

Author

Jason Moffat, Benjamin G. Neel, Robert Rottapel, Jeffrey L. Wrana, Troy Ketela, Maliha Haider, Josee Normand, Christine Misquitta, Patricia Mero, Alla Buzina, Dahlia Kasimer, Alessandro Datti, Frederick S. Vizeacoumar, Franco J. Vizeacoumar, Glauber C. Brito, Marianna Luhova, Bohdana Fedyshyn, Dewald van Dyk, Judice L.Y. Koh, Yaroslav Fedyshyn, Mauricio Medrano, Fabrice Sircoulomb, Paul M. Krzyzanowski, Konstantina Karamboulas, Azin Sayad, Fernando Suarez, Kevin R. Brown, and Richard Marcotte

Abstract

XLS file - 55K

Published
2023

14. Supplementary Figures 1-8 from Essential Gene Profiles in Breast, Pancreatic, and Ovarian Cancer Cells

Author

Jason Moffat, Benjamin G. Neel, Robert Rottapel, Jeffrey L. Wrana, Troy Ketela, Maliha Haider, Josee Normand, Christine Misquitta, Patricia Mero, Alla Buzina, Dahlia Kasimer, Alessandro Datti, Frederick S. Vizeacoumar, Franco J. Vizeacoumar, Glauber C. Brito, Marianna Luhova, Bohdana Fedyshyn, Dewald van Dyk, Judice L.Y. Koh, Yaroslav Fedyshyn, Mauricio Medrano, Fabrice Sircoulomb, Paul M. Krzyzanowski, Konstantina Karamboulas, Azin Sayad, Fernando Suarez, Kevin R. Brown, and Richard Marcotte

Abstract

PDF file - 310K

Published
2023

15. 2129. Maternal Transmission of SARS-CoV-2-specific Antibodies, but not Cytokines/Chemokines to Neonates Following Infection and Vaccination During Pregnancy

Author

Jonathon M Monroe, Sohan Punia, Huy Quang Quach, Elizabeth A Enninga, Yaroslav Fedyshyn, Bohdana Fedyshyn, Maureen Lemens, Dawn Littlefield, Elise Sintim-Aboagye, Maria C Mejia Plazas, Satoko Yamaoka, Hideki Ebihara, Akhilesh Pandey, Jie Sun, Erica L Johnson, Richard B Kennedy, Regan N Theiler, and Rana Chakraborty

Subjects
Infectious Diseases, Oncology
Abstract

Background Despite extensive studies of human immune responses to severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection and coronavirus disease 2019 (COVID-19) vaccination, research examining protective correlates of vertical transmission following maternal exposure in pregnancy remain limited. Here, we characterized antibody and cytokine responses in maternal and cord blood following infection or vaccination at various timepoints during gestation. Methods Spike S1 protein-specific binding antibodies and antibodies capable of blocking the interaction between the receptor binding domain (RBD) and the angiotensin converting enzyme 2 (ACE2) were measured in maternal and cord blood by ELISA. Serum concentrations of 74 cytokines/chemokines were measured by multiplex assay. Humoral responses and cytokine levels from matched maternal and fetal cord sera were compared and examined for potential correlations. Results We observed a highly significant correlation between Spike S1-specific antibody titer and RBD-ACE2 blocking antibody activity between maternal and fetal cord serum (p < 2.2e-16, R > 0.90). Blocking antibody activity was significantly higher for mothers infected during the 3rd trimester compared to earlier trimesters; however, vaccinated mothers developed and transferred higher antibody titers with greater RBD-ACE2 blocking antibody activity to their neonates than infected mothers. Furthermore, vaccine-induced Spike S1 IgG transfer ratios (fetal cord/maternal) were significantly higher than those induced by infection (p = 0.002). Multiplex assay showed significantly elevated levels of 33 cytokines/chemokines, mainly pro-inflammatory in infected maternal serum samples, while the paired fetal cord samples exhibited an anti-inflammatory cytokine predominance. Conclusion Our data support selective vertical transmission of potentially protective humoral responses against SARS-CoV-2, especially following vaccination in the 3rd trimester. The anti-inflammatory cytokine predominance in cord blood that persists despite maternal SARS-CoV-2 infection may offset the adverse outcomes of inflammation in pregnancy for the neonate. Disclosures All Authors: No reported disclosures.

Published
2022

16. Maternal Monocytes Respond to Cell-Free Fetal DNA and Initiate Key Processes of Human Parturition

Author

Elizabeth Ann L. Enninga, Nazanin Yeganeh Kazemi, Svetomir N. Markovic, Shari L. Sutor, Bohdana Fedyshyn, and Yaroslav Fedyshyn

Subjects
Fetus, Pregnancy, business.industry, Monocyte, Immunology, Parturition, medicine.disease, Corrections, Monocytes, Trophoblasts, Proinflammatory cytokine, Immune system, medicine.anatomical_structure, Cell-free fetal DNA, Placenta, Humans, Immunology and Allergy, Medicine, CXCL10, Female, business, Cell-Free Nucleic Acids
Abstract

Throughout gestation, the maternal immune system is tightly modulated to allow growth of a semiallogeneic fetus. During the third trimester, the maternal immune system shifts to a proinflammatory phenotype in preparation for labor. What induces this shift remains unclear. Cell-free fetal DNA (cffDNA) is shed by the placenta and enters maternal circulation throughout pregnancy. Levels of cffDNA are increased as gestation progresses and peak before labor, coinciding with a shift to proinflammatory maternal immunity. Furthermore, cffDNA is abnormally elevated in plasma from women with complications of pregnancy, including preterm labor. Given the changes in maternal immunity at the end of pregnancy and the role of sterile inflammation in the pathophysiology of spontaneous preterm birth, we hypothesized that cffDNA can act as a damage-associated molecular pattern inducing an inflammatory cytokine response that promotes hallmarks of parturition. To test this hypothesis, we stimulated human maternal leukocytes with cffDNA from primary term cytotrophoblasts or maternal plasma and observed significant IL-1β and CXCL10 secretion, which coincides with phosphorylation of IFN regulatory factor 3 and caspase-1 cleavage. We then show that human maternal monocytes are crucial for the immune response to cffDNA and can activate bystander T cells to secrete proinflammatory IFN-γ and granzyme B. Lastly, we find that the monocyte response to cffDNA leads to vascular endothelium activation, induction of myometrial contractility, and PGE2 release in vitro. Our results suggest that the immune response to cffDNA can promote key features of the parturition cascade, which has physiologic consequences relevant to the timing of labor.

Published
2021

17. Upregulation of HLA-Class I and II in Placentas Diagnosed with Villitis of Unknown Etiology

Author

Laurie L. Wakefield, Manish J. Gandhi, Sarah E. Kerr, Bohdana Fedyshyn, Elizabeth Ann L. Enninga, Rodrigo Ruano, Svetomir N. Markovic, and Alexey A. Leontovich

Subjects
Placenta Diseases, Placenta, Human leukocyte antigen, Immune system, HLA Antigens, Pregnancy, medicine, Humans, Lymphocytes, Inflammation, Fetus, medicine.diagnostic_test, business.industry, Obstetrics and Gynecology, medicine.disease, Up-Regulation, Transplant rejection, medicine.anatomical_structure, embryonic structures, Immunology, Female, Original Article, Chorionic Villi, business, Villitis of unknown etiology, Tissue typing
Abstract

The placenta utilizes many mechanisms to protect the haploidentical fetus from recognition by the maternal immune system. However, in cases of villitis of unknown etiology (VUE), maternal lymphocytes gain access into the placenta, causing significant health risks for the fetus. Evidence suggests that VUE is a rejection response between the mother and the haploidentical fetus. Therefore, we profiled human leukocyte antigen (HLA), an important predictor of transplant rejection, in VUE using placental tissue from ten patients with VUE and ten gestational age matched controls. Placentas were stained using novel multiplexed immunofluorescence (MxIF) to investigate morphology and HLA classes I and II. Gene expression was evaluated by microarray, and where available, tissue typing of mother/baby pairs was completed to determine HLA type. MxIF demonstrated strong CD8+ T cell infiltration and HLA class I staining both the distal and stem villi of VUE placentas. Compared to controls, VUE cases had significantly higher expression of HLA class II mRNA and pathway analysis demonstrated that 40% of the differentially expressed genes in VUE are related to tissue rejection. The data suggest that VUE resembles a rejection response between the mother and the fetus. It remains unknown what initiates immune recognition and why some mothers appear to be at higher risk for developing this condition than others. Understanding this etiology will be critical for developing effective interventions or prevention strategies during pregnancy. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (10.1007/s43032-019-00101-9) contains supplementary material, which is available to authorized users.

Published
2020

18. Increased cell‐free fetal DNA release after apoptosis and sterile inflammation in human trophoblast cells

Author

Svetomir N. Markovic, Rodrigo Ruano, Yaroslav Fedyshyn, Elizabeth Ann L. Enninga, Bohdana Fedyshyn, Rana Chakraborty, Isabel Yelsa, and Nazanin Yeganeh Kazemi

Subjects
Adult, Lipopolysaccharides, Immunology, CTBS, Cell, Apoptosis, Inflammation, Article, Cell Line, Andrology, Placenta, Humans, Immunology and Allergy, Medicine, HMGB1 Protein, Caspase 7, Caspase 3, Tumor Necrosis Factor-alpha, business.industry, Obstetrics and Gynecology, Trophoblast, DNA, Trophoblasts, medicine.anatomical_structure, Reproductive Medicine, Cell-free fetal DNA, Doxorubicin, embryonic structures, Female, Cytokine secretion, medicine.symptom, business, Cell-Free Nucleic Acids
Abstract

Problem Cell-free fetal DNA (cffDNA) shed from the placenta can be detected in maternal blood and increases incrementally during gestation. Concentrations are further elevated with pregnancy complications. Specific activators of cffDNA release in such complications have not been identified. Here, we use trophoblast cells from early and term placenta to examine cffDNA release following apoptosis, infection, and sterile inflammatory stress. Method of study HTR8/SVneo cells were used to model first-trimester trophoblasts, and term cytotrophoblasts (CTBs) were isolated from placentae collected after uncomplicated deliveries. Trophoblasts were treated with varying concentrations of doxorubicin (DOX), lipopolysaccharide (LPS), or high-mobility group box protein 1 (HMGB1) for 18 h. Cells or supernatants were quantified for caspase-3/7 cleavage, pro-inflammatory cytokine secretion, and cffDNA release. Results Both HTR8/SVneo and CTBs underwent caspase-3/7 cleavage following DOX treatment, with HTR8/SVneo cells more sensitive to apoptosis than term CTBs. Apoptotic cells released more cffDNA in a dose-dependent manner. Treatment with LPS resulted in an increase in pro-inflammatory IL-6 release, particularly in term CTBs compared to early trophoblasts; however, LPS did not affect cffDNA release. Lastly, while neither cell released more TNF-α following stimulation with HMGB1, both HTR8/SVneo and CTBs released significantly more cffDNA in the presence of HMGB1. Conclusions These data show that apoptosis and sterile inflammation induced by DOX and HMGB1, respectively, cause an increase in cffDNA concentrations in both first-trimester and term trophoblasts. Understanding physiologic release of cffDNA during healthy and complicated pregnancy can identify new targets for the diagnosis and treatment of gestational complications.

Published
2021

20. Evaluating Markers of Immune Tolerance and Angiogenesis in Maternal Blood for an Association with Risk of Pregnancy Loss

Author

Rodrigo Ruano, Amy L. Weaver, Sarah C. Baumgarten, Chandra C. Shenoy, Chelsie C Van Oort, Elizabeth Ann L. Enninga, Bohdana Fedyshyn, and Michelle A. Wyatt

Subjects
medicine.medical_specialty, Angiogenesis, miscarriage, Article, Miscarriage, Immune tolerance, immunology, galectin-9, chemistry.chemical_compound, Immune system, medicine, Prospective cohort study, Pregnancy, vascular endothelial growth factor, business.industry, Obstetrics, General Medicine, medicine.disease, Vascular endothelial growth factor, chemistry, Medicine, Gestation, pregnancy loss, interleukin-4, business
Abstract

Pregnancy loss affects approximately 20% of couples. The lack of a clear cause complicates half of all miscarriages. Early evidence indicates the maternal immune system and angiogenesis regulation are both key players in implantation success or failure. Therefore, this prospective study recruited women in the first trimester with known viable intrauterine pregnancy and measured blood levels of immune tolerance proteins galectin-9 (Gal-9) and interleukin (IL)-4, and angiogenesis proteins (vascular endothelial growth factors (VEGF) A, C, and D) between 5 and 9 weeks gestation. Plasma concentrations were compared between groups defined based on (a) pregnancy outcome and (b) maternal history of miscarriage, respectively. In total, 56 women were recruited with 10 experiencing a miscarriage or pregnancy loss in the 2nd or 3rd trimester and 11 having a maternal history or miscarriage. VEGF-C was significantly lower among women with a miscarriage or pregnancy loss. Gal-9 and VEGF-A concentrations were decreased in women with a prior miscarriage. Identification of early changes in maternal immune and angiogenic factors during pregnancy may be a tool to improve patient counseling on pregnancy loss risk and future interventions to reduce miscarriage in a subset of women.

Published
2021

22. Essential Gene Profiles in Breast, Pancreatic, and Ovarian Cancer Cells

Author

Troy Ketela, Robert Rottapel, Dewald van Dyk, Glauber C. Brito, Azin Sayad, Kevin R. Brown, Jason Moffat, Bohdana Fedyshyn, Benjamin G. Neel, Christine M. Misquitta, Judice L. Y. Koh, Paul M. Krzyzanowski, Frederick S. Vizeacoumar, Fernando Suarez, Alla Buzina, Josee Normand, Maliha Haider, Alessandro Datti, Yaroslav Fedyshyn, Franco J. Vizeacoumar, Dahlia Kasimer, Jeffrey L. Wrana, Marianna Luhova, Mauricio Medrano, Richard Marcotte, Patricia Mero, Fabrice Sircoulomb, and Konstantina Karamboulas

Subjects
Male, EXPRESSION, Breast Neoplasms, Genomics, TYROSINE KINASE, Computational biology, Biology, Bioinformatics, Article, Small hairpin RNA, SCREENS, LUNG-CANCER, Cell Line, Tumor, medicine, GENOME-WIDE RNAi, Humans, RNA, Small Interfering, Gene, Gene Library, Ovarian Neoplasms, COMPLEX, RECEPTOR FUNCTION, Cancer, AMPLIFICATION, GENOME-WIDE RNAi, LUNG-CANCER, PROSTATE-CANCER, RECEPTOR FUNCTION, TYROSINE KINASE, H-PRUNE, EXPRESSION, COMPLEX, AMPLIFICATION, SCREENS, medicine.disease, Phenotype, PROSTATE-CANCER, Pancreatic Neoplasms, Oncology, Essential gene, Cancer cell, H-PRUNE, Female, Transcriptome, Ovarian cancer
Abstract

Genomic analyses are yielding a host of new information on the multiple genetic abnormalities associated with specific types of cancer. A comprehensive description of cancer-associated genetic abnormalities can improve our ability to classify tumors into clinically relevant subgroups and, on occasion, identify mutant genes that drive the cancer phenotype ("drivers"). More often, though, the functional significance of cancer-associated mutations is difficult to discern. Genome-wide pooled short hairpin RNA (shRNA) screens enable global identification of the genes essential for cancer cell survival and proliferation, providing a "functional genomic" map of human cancer to complement genomic studies. Using a lentiviral shRNA library targeting ~16,000 genes and a newly developed, dynamic scoring approach, we identified essential gene profiles in 72 breast, pancreatic, and ovarian cancer cell lines. Integrating our results with current and future genomic data should facilitate the systematic identification of drivers, unanticipated synthetic lethal relationships, and functional vulnerabilities of these tumor types.This study presents a resource of genome-scale, pooled shRNA screens for 72 breast, pancreatic, and ovarian cancer cell lines that will serve as a functional complement to genomics data, facilitate construction of essential gene profiles, help uncover synthetic lethal relationships, and identify uncharacterized genetic vulnerabilities in these tumor types.This study presents a resource of genome-scale, pooled shRNA screens for 72 breast, pancreatic, and ovarian cancer cell lines that will serve as a functional complement to genomics data, facilitate construction of essential gene profiles, help uncover synthetic lethal relationships, and identify uncharacterized genetic vulnerabilities in these tumor types.

Published
2012

23. eSGA: E. coli synthetic genetic array analysis

Author

Butland, Gareth, primary, Babu, Mohan, additional, Díaz-Mejía, J Javier, additional, Bohdana, Fedyshyn, additional, Phanse, Sadhna, additional, Gold, Barbara, additional, Yang, Wenhong, additional, Li, Joyce, additional, Gagarinova, Alla G, additional, Pogoutse, Oxana, additional, Mori, Hirotada, additional, Wanner, Barry L, additional, Lo, Henry, additional, Wasniewski, Jas, additional, Christopoulos, Constantine, additional, Ali, Mehrab, additional, Venn, Pascal, additional, Safavi-Naini, Anahita, additional, Sourour, Natalie, additional, Caron, Simone, additional, Choi, Ja-Yeon, additional, Laigle, Ludovic, additional, Nazarians-Armavil, Anaies, additional, Deshpande, Avnish, additional, Joe, Sarah, additional, Datsenko, Kirill A, additional, Yamamoto, Natsuko, additional, Andrews, Brenda J, additional, Boone, Charles, additional, Ding, Huiming, additional, Sheikh, Bilal, additional, Moreno-Hagelsieb, Gabriel, additional, Greenblatt, Jack F, additional, and Emili, Andrew, additional

Published
2008
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