Your search keyword '"Even Y"' showing total 26 results

1. Potent suppression of HIV-1 cell attachment by Kudzu root extract

Author

Mediouni, S., Jablonski, J. A., Tsuda, S., Richard, A., Kessing, C., Andrade, M. V., Biswas, A., Even, Y., Tellinghuisen, T., Choe, H., Cameron, M., Stevenson, M., and Valente, S. T.

Published

2018

2. Discussion of wildlife trade before and during the COVID-19 pandemic in professional opinion pieces and scientific articles

Author

Wang, Yifu, Tilley, Hannah B, Phalke, Sagarika, Andersson, Astrid A, Dingle, Caroline, Hatten, Chloe E R, Leung, Even Y M, Murphy, Derek, Wierucka, Kaja, Mumby, Hannah S, Wang, Yifu, Tilley, Hannah B, Phalke, Sagarika, Andersson, Astrid A, Dingle, Caroline, Hatten, Chloe E R, Leung, Even Y M, Murphy, Derek, Wierucka, Kaja, and Mumby, Hannah S

Abstract

Wildlife trade is a multi-billion-dollar sector that impacts a wide range of species, and thus is of significant research and conservation interest. Wildlife trade has also become a prominent topic in the public-facing media, where coverage has intensified following the outbreak of the global COVID-19 pandemic due to the potential connection between wildlife trade and the origin of the SARS Cov2 virus. Given the importance of the media in shaping public understanding and discourse of complex topics such as wildlife trade, this could impact the implementation of and public support for policy decisions. In this study, we followed a standardised protocol to extract wildlife trade-related discussion from 285 professional opinion pieces (NGO reports or articles in conservation-themed forums) and 107 scientific articles published in two time periods: “pre-COVID” (June 1–December 31, 2019) and “during-COVID” (January 1–May 31, 2020). We compared opinion pieces and scientific articles across the two time periods and to each other to investigate potential differences in the presentation of wildlife trade and associated speakers. We found a shift in the way that wildlife trade was discussed in professional opinion pieces between the periods, in that the discussion became less specific in terms of defining the legality and purpose of trade, and the animal groups involved in the “during-COVID” period. The generalised framing of wildlife trade in our dataset also coincided with an increased discussion of highly generalised management strategies, such as blanket bans on wildlife trade. We also found that publications included more quotes from researchers in the “during-COVID” period. In both professional opinion pieces and scientific articles, we found that quotations or research were often from speakers whose affiliation region was different to the geographic range of the trade they were speaking about. This highlights the importance of incorporating local knowledge and consider

Published

2022

3. After migration into blood circulation, hematopoietic stem cells can stably self-renew and maintain bone marrow while being skewed toward myeloid lineage when submitted to serial transplantation

Author

Chang C, Even Y, Fabio M.V. Rossi, and Yi L

Subjects

Haematopoiesis, Myeloid, medicine.anatomical_structure, Lineage (genetic), Serial Transplantation, medicine, Cancer research, hemic and immune systems, Bone marrow, Stem cell, Biology, Homeostasis, Granulocyte colony-stimulating factor

Abstract

Hematopoietic stem cells (HSCs) mainly reside in bone marrow (BM) within niches providing an appropriate environment for their survival and self-renewal. Although, small numbers of HSCs can quit their residing environment to migrate into blood circulation and re-engraft elsewhere in BM. Mobilizing agents such as granulocyte colony stimulating factor (G-CSF) can amplify this process by inducing massive HSC mobilization into blood circulation. This method is widely used in clinics to treat hematological disorders. However, in physiological conditions, the properties of HSCs after migration (called migratory HSCs) remain incompletely characterized. In this study, we investigated the capacity of migratory HSCs to self-renew, reconstitute and maintain BM. We show that after migration, HSCs can stably self-renew and maintain BM in homeostasis. However, while stably repopulating BM of irradiated recipients, migratory HSCs show a defect in lymphoid lineage reconstitution when subjected to serial transplantations. Our findings provide interesting knowledge on HSC properties after migration, which may benefits therapeutic research on HSC-based therapies to treat hematological disorders.

Published

2021

4. Elaboration of an Interaction Model Between Zolpidem and the ω1 Modulatory Site of GABAA Receptor Using Site-Directed Mutagenesis

Author

Olivier, A., Renard, S., Even, Y., Besnard, F., Graham, D., Sevrin, M., George, P., Gundertofte, Klaus, editor, and Jørgensen, Flemming Steen, editor

Published

2000

5. Oregano Oil and Its Principal Component, Carvacrol, Inhibit HIV-1 Fusion into Target Cells

Author

Mediouni, S., primary, Jablonski, J. A., additional, Tsuda, S., additional, Barsamian, A., additional, Kessing, C., additional, Richard, A., additional, Biswas, A., additional, Toledo, F., additional, Andrade, V. M., additional, Even, Y., additional, Stevenson, M., additional, Tellinghuisen, T., additional, Choe, H., additional, Cameron, M., additional, Bannister, T. D., additional, and Valente, S. T., additional

Published

2020

6. THE "ANTI-HERO" AND HIS STRIVING FOR HEROISM IN BRENNER'S WRITINGS / ה"לא גיבור הרוצה להיות גיבור" ביצירתו הסיפורית של י"ח ברנר

Author

אבן, יוסף and Even, Y.

Published

1969

7. Discussion of wildlife trade before and during the COVID-19 pandemic in professional opinion pieces and scientific articles

Author

Yifu Wang, Hannah B. Tilley, Sagarika Phalke, Astrid A. Andersson, Caroline Dingle, Chloe E.R Hatten, Even Y.M. Leung, Derek Murphy, Kaja Wierucka, and Hannah S. Mumby

Subjects

Coronavirus, Discourse analysis, Endangered species, NGO report, Policy, Public-facing media, Ecology, QH540-549.5

Abstract

Wildlife trade is a multi-billion-dollar sector that impacts a wide range of species, and thus is of significant research and conservation interest. Wildlife trade has also become a prominent topic in the public-facing media, where coverage has intensified following the outbreak of the global COVID-19 pandemic due to the potential connection between wildlife trade and the origin of the SARS Cov2 virus. Given the importance of the media in shaping public understanding and discourse of complex topics such as wildlife trade, this could impact the implementation of and public support for policy decisions. In this study, we followed a standardised protocol to extract wildlife trade-related discussion from 285 professional opinion pieces (NGO reports or articles in conservation-themed forums) and 107 scientific articles published in two time periods: “pre-COVID” (June 1–December 31, 2019) and “during-COVID” (January 1–May 31, 2020). We compared opinion pieces and scientific articles across the two time periods and to each other to investigate potential differences in the presentation of wildlife trade and associated speakers. We found a shift in the way that wildlife trade was discussed in professional opinion pieces between the periods, in that the discussion became less specific in terms of defining the legality and purpose of trade, and the animal groups involved in the “during-COVID” period. The generalised framing of wildlife trade in our dataset also coincided with an increased discussion of highly generalised management strategies, such as blanket bans on wildlife trade. We also found that publications included more quotes from researchers in the “during-COVID” period. In both professional opinion pieces and scientific articles, we found that quotations or research were often from speakers whose affiliation region was different to the geographic range of the trade they were speaking about. This highlights the importance of incorporating local knowledge and considering the diversity of speakers and interviewees in both research and the public-facing media about the wildlife trade.

Published

2022

8. NUP98-HOXA10hd-Expanded Hematopoietic Stem Cells Efficiently Reconstitute Bone Marrow of Mismatched Recipients and Induce Tolerance

Author

Even, Y., primary, Bennett, J. L., additional, Sekulovic, S., additional, So, L., additional, Yi, L., additional, McNagny, K., additional, Humphries, R. K., additional, and Rossi, F. M. V., additional

Published

2011

9. Development of Stable Cell Lines Expressing Different Subtypes of GabaAReceptors

Author

Besnard, F., primary, Even, Y., additional, Itier, V., additional, Granger, P., additional, Partiséti, M., additional, Avenet, P., additional, Depoortere, H., additional, and Graham, D., additional

Published

1997

10. Development of Stable Cell Lines Expressing Different Subtypes of GabaA Receptors.

Author

Besnard, F., Even, Y., Itier, V., Granger, P., Partiséti, M., Avenet, P., Depoortere, H., and Graham, D.

Published

1997

11. Evaluation of intravenous cannula and administration set fixation methods.

Author

Fried E, Shochat T, Har-even Y, Cohen Y, Fried, Elchanan, Shochat, Tzippora, Har-even, Yoel, and Cohen, Yitzhak

Abstract

Intravenous cannula and administration set fixation is crucial for fluid resuscitation and intravenous administration of medications. Because conventional hospital fixations are insufficient for the military field scenario, two consecutive, prospective, randomized, clinical trials were performed in the Israel Defense Forces Medical School, to determine the most effective fixation method in the military arena. Gauze bandage, adhesive bandage, Coban wrap, and plastic wrap fixation methods were tested for field conditions and intravenous fluid flow. The results showed that plastic wrap is the fastest fixation method, withstands field conditions with minimal negative effects on the intravenous fluid flow, and is the most cost-effective. [ABSTRACT FROM AUTHOR]

Published

2005

12. Discussion of wildlife trade before and during the COVID-19 pandemic in professional opinion pieces and scientific articles.

Author

Wang Y, Tilley HB, Phalke S, Andersson AA, Dingle C, Hatten CER, Leung EYM, Murphy D, Wierucka K, and Mumby HS

Abstract

Wildlife trade is a multi-billion-dollar sector that impacts a wide range of species, and thus is of significant research and conservation interest. Wildlife trade has also become a prominent topic in the public-facing media, where coverage has intensified following the outbreak of the global COVID-19 pandemic due to the potential connection between wildlife trade and the origin of the SARS Cov2 virus. Given the importance of the media in shaping public understanding and discourse of complex topics such as wildlife trade, this could impact the implementation of and public support for policy decisions. In this study, we followed a standardised protocol to extract wildlife trade-related discussion from 285 professional opinion pieces (NGO reports or articles in conservation-themed forums) and 107 scientific articles published in two time periods: "pre-COVID" (June 1-December 31, 2019) and "during-COVID" (January 1-May 31, 2020). We compared opinion pieces and scientific articles across the two time periods and to each other to investigate potential differences in the presentation of wildlife trade and associated speakers. We found a shift in the way that wildlife trade was discussed in professional opinion pieces between the periods, in that the discussion became less specific in terms of defining the legality and purpose of trade, and the animal groups involved in the "during-COVID" period. The generalised framing of wildlife trade in our dataset also coincided with an increased discussion of highly generalised management strategies, such as blanket bans on wildlife trade. We also found that publications included more quotes from researchers in the "during-COVID" period. In both professional opinion pieces and scientific articles, we found that quotations or research were often from speakers whose affiliation region was different to the geographic range of the trade they were speaking about. This highlights the importance of incorporating local knowledge and considering the diversity of speakers and interviewees in both research and the public-facing media about the wildlife trade., Competing Interests: The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: Hannah S Mumby reports financial support was provided by Branco Weiss-Society In Science Fellowship. Hannah S Mumby reports financial support was provided by Association for the Study of Animal Behaviour., (© 2022 The Authors.)

Published

2022

13. Physiological and comparative proteomic analyzes reveal immune defense response of the king scallop Pecten maximus in presence of paralytic shellfish toxin (PST) from Alexandrium minutum.

Author

Even Y, Pousse E, Chapperon C, Artigaud S, Hégaret H, Bernay B, Pichereau V, Flye-Sainte-Marie J, and Jean F

Subjects

Animals, Immunity, Marine Toxins toxicity, Proteomics, Seafood, Shellfish, Dinoflagellida physiology, Pecten metabolism, Pectinidae metabolism

Abstract

The king scallop, Pecten maximus is a highly valuable seafood in Europe. Over the last few years, its culture has been threatened by toxic microalgae during harmful algal blooms, inducing public health concerns. Indeed, phycotoxins accumulated in bivalves can be harmful for human, especially paralytic shellfish toxins (PST) synthesized by the microalgae Alexandrium minutum. Deleterious effects of these toxic algae on bivalves have also been reported. However, its impact on bivalves such as king scallop is far from being completely understood. This study combined ecophysiological and proteomic analyzes to investigate the early response of juvenile king scallops to a short term exposure to PST producing A. minutum. Our data showed that all along the 2-days exposure to A. minutum, king scallops exhibited transient lower filtration and respiration rates and accumulated PST. Significant inter-individual variability of toxin accumulation potential was observed among individuals. Furthermore, we found that ingestion of toxic algae, correlated to toxin accumulation was driven by two factors: 1/ the time it takes king scallop to recover from filtration inhibition and starts to filtrate again, 2/ the filtration level to which king scallop starts again to filtrate after inhibition. Furthermore, at the end of the 2-day exposure to A. minutum, proteomic analyzes revealed an increase of the killer cell lectin-like receptor B1, involved in adaptative immune response. Proteins involved in detoxification and in metabolism were found in lower amount in A. minutum exposed king scallops. Proteomic data also showed differential accumulation in several structure proteins such as β-actin, paramyosin and filamin A, suggesting a remodeling of the mantle tissue when king scallops are subjected to an A. minutum exposure., (Copyright © 2022 Elsevier B.V. All rights reserved.)

Published

2022

14. Strong constitutive expression divergence among strains but no evidence of differential expression associated with sexual reproduction in Alexandrium minutum.

Author

Seveno J, Even Y, and Le Gac M

Subjects

Gene Expression, Reproduction, Saxitoxin, Cyanobacteria, Dinoflagellida genetics

Abstract

Sexual reproduction remains poorly characterized in dinoflagellates. This is especially the case at the molecular level. Here crossing experiments were performed among strains of the toxic dinoflagellate Alexandrium minutum belonging to two genetically divergent groups. Gene expression was compared between sexually compatible and incompatible crosses at the time of gamete fusion and resting cyst (~zygote) formation. Not a single transcript was identified as differentially expressed between compatible and incompatible crosses at these two crucial time points of the dinoflagellate life cycle. However, several thousands of transcripts displayed constitutive expression differences between strains. This was especially the case between the strains belonging to the genetically divergent groups. A few hundreds of transcripts were also identified as differentially expressed between strains belonging to opposite mating types. Some of these transcripts displayed homology with the SxtA protein, known to be involved in saxitoxin production in cyanobacteria, as well as with proteins potentially involved in mating in fungi., (Copyright © 2020 Elsevier Ltd. All rights reserved.)

Published

2020

15. CDK13, a Kinase Involved in Pre-mRNA Splicing, Is a Component of the Perinucleolar Compartment.

Author

Even Y, Escande ML, Fayet C, and Genevière AM

Subjects

CDC2 Protein Kinase chemistry, Cell Line, Tumor, Chromosomal Proteins, Non-Histone metabolism, Cyclins metabolism, Humans, Mitosis, Phosphoproteins metabolism, Protein Structure, Tertiary, RNA Precursors metabolism, RNA-Binding Proteins metabolism, Nucleolin, CDC2 Protein Kinase metabolism, Cell Compartmentation, Cell Nucleolus metabolism, RNA Precursors genetics, RNA Splicing genetics

Abstract

The perinucleolar compartment (PNC) is a subnuclear stucture forming predominantly in cancer cells; its prevalence positively correlates with metastatic capacity. Although several RNA-binding proteins have been characterized in PNC, the molecular function of this compartment remains unclear. Here we demonstrate that the cyclin-dependent kinase 13 (CDK13) is a newly identified constituent of PNC. CDK13 is a kinase involved in the regulation of gene expression and whose overexpression was found to alter pre-mRNA processing. In this study we show that CDK13 is enriched in PNC and co-localizes all along the cell cycle with the PNC component PTB. In contrast, neither the cyclins K and L, known to associate with CDK13, nor the potential kinase substrates accumulate in PNC. We further show that CDK13 overexpression increases PNC prevalence suggesting that CDK13 may be determinant for PNC formation. This result linked to the finding that CDK13 gene is amplified in different types of cancer indicate that this kinase can contribute to cancer development in human.

Published

2016

16. Prolonged self-renewal activity unmasks telomerase control of telomere homeostasis and function of mouse hematopoietic stem cells.

Author

Sekulovic S, Gylfadottir V, Vulto I, Gasparetto M, Even Y, Brookes C, Smith C, Eaves CJ, Lansdorp PM, Rossi FM, and Humphries RK

Subjects

Animals, Cell Proliferation, Gene Deletion, Gene Expression Regulation, Hematopoietic Stem Cell Transplantation, Hematopoietic Stem Cells cytology, Hematopoietic Stem Cells metabolism, Histones genetics, Mice, Mice, Inbred C57BL, Telomerase genetics, DNA Damage, Hematopoietic Stem Cells enzymology, Telomerase metabolism, Telomere

Abstract

Strategies for expanding hematopoietic stem cells (HSCs) could have significant utility for transplantation-based therapies. However, deleterious consequences of such manipulations remain unknown. Here we examined the impact of HSC self-renewal divisions in vitro and in vivo on their subsequent regenerative and continuing ability to sustain blood cell production in the absence of telomerase. HSC expansion in vitro was obtained using a NUP98-HOXA10hd transduction strategy and, in vivo, using a serial transplant protocol. We observed ~ 10kb telomere loss in leukocytes produced in secondary mice transplanted with HSCs regenerated in primary recipients of NUP98-HOXA10hd-transduced and in vitro-expanded Tert(-/-) HSCs 6 months before. The second generation leukocytes also showed elevated expression of γH2AX (relative to control) indicative of greater accumulating DNA damage. In contrast, significant telomere shortening was not detected in leukocytes produced from freshly isolated, serially transplanted wild-type (WT) or Tert(-/-) HSCs, suggesting that HSC replication posttransplant is not limited by telomere shortening in the mouse. These findings document a role of telomerase in telomere homeostasis, and in preserving HSC functional integrity on prolonged self-renewal stimulation.

Published

2011

17. Depot-specific differences in adipogenic progenitor abundance and proliferative response to high-fat diet.

Author

Joe AW, Yi L, Even Y, Vogl AW, and Rossi FM

Subjects

Adipocytes physiology, Adipose Tissue physiopathology, Animals, Bromodeoxyuridine, Cell Count, Cell Division physiology, Colony-Forming Units Assay, Dietary Fats metabolism, Disease Models, Animal, Female, Hyperplasia etiology, Hyperplasia physiopathology, Hypertrophy etiology, Hypertrophy physiopathology, Male, Metabolic Syndrome metabolism, Metabolic Syndrome physiopathology, Mice, Mice, Inbred C57BL, Stem Cells physiology, Adipocytes cytology, Adipose Tissue cytology, Cell Proliferation, Dietary Fats adverse effects, Food, Formulated adverse effects, Stem Cells cytology

Abstract

White adipose tissue (fat) is the primary organ for energy storage and its regulation has serious implications on human health. Excess fat tissue causes significant morbidity, and adipose tissue dysfunction caused by excessive adipocyte hypertrophy has been proposed to play a significant role in the pathogenesis of metabolic disease. Studies in both humans and animal models show that metabolic dysfunction is more closely associated with visceral than subcutaneous fat accumulation. Here, we show that in mice fed a high-fat diet, visceral fat (VAT) grows mostly by hypertrophy and subcutaneous fat (SAT) by hyperplasia, providing a rationale for the different effects of specific adipose depots on metabolic health. To address whether depot expansion is controlled at the level of stem/progenitor cells, we developed a strategy to prospectively identify adipogenic progenitors (APs) from both depots. Clonogenic assays and in vivo bromodeoxyuridine (BrdU) studies show that APs are eightfold more abundant in SAT than VAT, and that AP proliferation is significantly increased in SAT but not VAT in response to high-fat diet. Our results suggest that depot-specific differences in AP abundance and proliferation underlie whether a fat depot expands by hypertrophy or hyperplasia, and thus may have important implications on the development of metabolic disease. In addition, we provide the first evidence that dietary inputs can modulate the proliferation of adipogenic progenitors in adults.

Published

2009

18. CDK13, a new potential human immunodeficiency virus type 1 inhibitory factor regulating viral mRNA splicing.

Author

Berro R, Pedati C, Kehn-Hall K, Wu W, Klase Z, Even Y, Genevière AM, Ammosova T, Nekhai S, and Kashanchi F

Subjects

HeLa Cells, Humans, Immunoprecipitation, Protein Binding, CDC2 Protein Kinase metabolism, HIV-1 growth & development, RNA Splicing, RNA, Messenger metabolism, RNA, Viral metabolism, Virus Replication physiology, tat Gene Products, Human Immunodeficiency Virus metabolism

Abstract

The human immunodeficiency virus type 1 (HIV-1) Tat is a 14-kDa viral protein that acts as a potent transactivator by binding to the transactivation-responsive region, a structured RNA element located at the 5' end of all HIV-1 transcripts. Tat transactivates viral gene expression by inducing the phosphorylation of the C-terminal domain of RNA polymerase II through several Tat-activated kinases and by recruiting chromatin-remodeling complexes and histone-modifying enzymes to the HIV-1 long terminal repeat. Histone acetyltransferases, including p300 and hGCN5, not only acetylate histones but also acetylate Tat at lysine positions 50 and 51 in the arginine-rich motif. Acetylated Tat at positions 50 and 51 interacts with a specialized protein module, the bromodomain, and recruits novel factors having this particular domain, such as P/CAF and SWI/SNF. In addition to having its effect on transcription, Tat has been shown to be involved in splicing. In this study, we demonstrate that Tat interacts with cyclin-dependent kinase 13 (CDK13) both in vivo and in vitro. We also found that CDK13 increases HIV-1 mRNA splicing and favors the production of the doubly spliced protein Nef. In addition, we demonstrate that CDK13 acts as a possible restriction factor, in that its overexpression decreases the production of the viral proteins Gag and Env and subsequently suppresses virus production. Using small interfering RNA against CDK13, we show that silencing of CDK13 leads to a significant increase in virus production. Finally, we demonstrate that CDK13 mediates its effect on splicing through the phosphorylation of ASF/SF2.

Published

2008

19. [Genome sequencing in the sea urchin embryo: what is new concerning the cell cycle?].

Author

Genevière AM, Aze A, and Even Y

Subjects

Animals, Cell Division, Mice, Models, Biological, Phylogeny, Sea Urchins classification, Species Specificity, Vertebrates genetics, Cell Cycle physiology, Embryo, Nonmammalian cytology, Genome, Sea Urchins embryology, Sea Urchins genetics

Abstract

Sea urchin is a classical research model system in developmental biology; moreover, the external fertilization and growth of embryos, their rapid division cycle, their transparency and the accessibility of these embryos to molecular visualization methods, made them good specimens to analyze the regulatory mechanisms of cell division. These features as well as the phylogenetic position of sea urchin, close to vertebrates but in an outgroup within the deuterostomes, led scientists working on this model to sequence the genome of the species S. purpuratus. The genome contains a full repertoire of cell cycle control genes. A comparison of this toolkit with those from vertebrates, nematodes, drosophila, as well as tunicates, provides new insight into the evolution of cell cycle control. While some gene subtypes have undergone lineage-specific expansions in vertebrates (i.e. cyclins, mitotic kinases,...), others seem to be lost in vertebrates, for instance the novel cyclin B identified in S. purpuratus. On the other hand, some genes which were previously thought to be vertebrate innovations, are also found in sea urchins (i.e. MCM9). To note is also the absence of cell cycle inhibitors of the INK type, which are apparently confined to vertebrates. The uncovered genomic repertoire of cell-cycle regulators will thus provide molecular tools that should further enhance future research on cell cycle control and developmental regulation in this model.

Published

2007

20. CDC2L5, a Cdk-like kinase with RS domain, interacts with the ASF/SF2-associated protein p32 and affects splicing in vivo.

Author

Even Y, Durieux S, Escande ML, Lozano JC, Peaucellier G, Weil D, and Genevière AM

Subjects

Animals, CDC2 Protein Kinase genetics, Cell Line, Cell Nucleus metabolism, Cell Nucleus ultrastructure, Humans, Lymphotoxin-alpha genetics, Lymphotoxin-alpha metabolism, Mice, Nuclear Proteins genetics, Protein Structure, Tertiary, Protein Subunits genetics, RNA-Binding Proteins, Recombinant Proteins genetics, Recombinant Proteins metabolism, Serine-Arginine Splicing Factors, Two-Hybrid System Techniques, CDC2 Protein Kinase metabolism, Nuclear Proteins metabolism, Protein Subunits metabolism, RNA Precursors metabolism, RNA Splicing

Abstract

The human CDC2L5 gene encodes a protein of unknown physiological function. This protein is closely related to the cyclin-dependent kinase (Cdks) family and contains an arginine/serine-rich (RS) domain. The Cdks were first identified as crucial regulators of cell-cycle progression, more recently they were found to be involved in transcription and mRNA processing. RS domains are mainly present in proteins regulating pre-mRNA splicing, suggesting CDC2L5 having a possible role in this process. In this study, we demonstrate that CDC2L5 is located in the nucleoplasm, at a higher concentration in speckles, the storage sites for splicing factors. Furthermore, this localization is dependent on the presence of the N-terminal sequence including the RS domain. Then, we report that CDC2L5 directly interacts with the ASF/SF2-associated protein p32, a protein involved in splicing regulation. Overexpression of CDC2L5 constructs disturbs constitutive splicing and switches alternative splice site selection in vivo. These results argue in favor of a functional role of the CDC2L5 kinase in splicing regulation., (2006 Wiley-Liss, Inc.)

Published

2006

21. Inhibition of cysteine protease activity disturbs DNA replication and prevents mitosis in the early mitotic cell cycles of sea urchin embryos.

Author

Concha C, Monardes A, Even Y, Morin V, Puchi M, Imschenetzky M, and Genevière AM

Subjects

Acrylates pharmacology, Animals, CDC2 Protein Kinase metabolism, Calpain antagonists & inhibitors, Cathepsins antagonists & inhibitors, Cell Nucleus drug effects, Cyclin B metabolism, Cytoplasm drug effects, Embryo, Nonmammalian cytology, Embryo, Nonmammalian metabolism, Leucine pharmacology, Tissue Distribution, Cell Cycle drug effects, Cysteine Proteinase Inhibitors pharmacology, DNA Replication drug effects, Leucine analogs & derivatives, Mitosis drug effects, Sea Urchins embryology

Abstract

Recent findings suggested that the role of cysteine proteases would not be limited to protein degradation in lysosomes but would also play regulatory functions in more specific cell mechanisms. We analyzed here the role of these enzymes in the control of cell cycle during embryogenesis. The addition of the potent cysteine protease inhibitor E64d to newly fertilized sea urchin eggs disrupted cell cycle progression, affecting nuclear as well as cytoplasmic characteristic events. Monitoring BrdU incorporation in E64d treated eggs demonstrated that DNA replication is severely disturbed. Moreover, this drug treatment inhibited male histones degradation, a step that is necessary for sperm chromatin remodeling and precedes the initiation of DNA replication in control eggs. This inhibition likely explains the DNA replication disturbance and suggests that S phase initiation requires cysteine protease activity. In turn, activation of the DNA replication checkpoint could be responsible for the consecutive block of nuclear envelope breakdown (NEB). However, in sea urchin early embryos this checkpoint doesn't control the mitotic cytoplasmic events that are not tightly coupled with NEB. Thus the fact that microtubule spindle is not assembled and cyclin B-cdk1 not activated under E64d treatment more likely rely on a distinct mechanism. Immunofluorescence experiments indicated that centrosome organization was deficient in absence of cysteine protease activity. This potentially accounts for mitotic spindle disruption and for cyclin B mis-localization in E64d treated eggs. We conclude that cysteine proteases are essential to trigger S phase and to promote M phase entry in newly fertilized sea urchin eggs., ((c) 2005 Wiley-Liss, Inc.)

Published

2005

22. The alpha, beta, gamma, delta-unsaturated aldehyde 2-trans-4-trans-decadienal disturbs DNA replication and mitotic events in early sea urchin embryos.

Author

Hansen E, Even Y, and Genevière AM

Subjects

Animals, Antimetabolites, Blotting, Western, Bromodeoxyuridine, CDC2 Protein Kinase metabolism, Cell Cycle drug effects, Chromatin drug effects, Chromatin ultrastructure, Cyclin B metabolism, Dose-Response Relationship, Drug, Embryo, Nonmammalian metabolism, Indicators and Reagents, Maturation-Promoting Factor metabolism, Microtubules drug effects, Microtubules ultrastructure, Spindle Apparatus drug effects, Aldehydes toxicity, DNA Replication drug effects, Mitosis drug effects, Sea Urchins metabolism

Abstract

The polyunsaturated aldehydes are highly reactive products of fatty acid peroxidation and combustion of organic materials, and they have been documented to have diverse cyctotoxic and genotoxic effects. The alpha,beta,gamma,delta-unsaturated aldehyde 2-trans-4-trans-decadienal is produced by marine microalgae, and it is known to inhibit cell proliferation and induce apoptosis in several different cell types. However, the molecular basis for the cell cycle arrest is not fully understood. We used sea urchin embryos to examine how some of the key events of the mitotic cell division were influenced by this polyunsaturated aldehyde. We found that cell divisions in embryos of Sphaerechinus granularis were inhibited by 2-trans-4-trans-decadienal in a dose dependent manner with an EC50 of 1.3 microM. Mitotic events in the nondividing eggs were characterized using immunofluorescent staining. DNA labelling revealed that pronuclear migration was inhibited, and a total absence of incorporation of the DNA-base analogue 5-bromo-2-deoxyuridine indicated that no DNA replication had occurred. Staining of alpha-tubulin subunits showed that tubulin-polymerization was disrupted and aberrations were induced in mitotic spindles. Furthermore, we monitored the activity of the G2-M promoting complex cyclin B-Cdk1 in newly fertilized sea urchin eggs, and found that this complex was not activated in embryos treated with 2-trans-4-trans-decadienal despite the accumulation of cyclin B.

Published

2004

23. Partial duplication of the eyebrows with other congenital malformations: a new syndrome.

Author

Gross-Kieselstein E and Har-Even Y

Subjects

Abnormalities, Multiple genetics, Child, Female, Genes, Recessive, Humans, Male, Syndrome, Abnormalities, Multiple pathology, Eyebrows abnormalities

Published

1989

24. Oculomotor apraxia: the presenting sign of Gaucher disease.

Author

Gross-Tsur V, Har-Even Y, Gutman I, and Amir N

Subjects

Child, Child, Preschool, Female, Gaucher Disease complications, Humans, Apraxias etiology, Eye Movements, Gaucher Disease physiopathology

Abstract

Oculomotor apraxia may be idiopathic or a symptom of a variety of diseases. In Gaucher disease, oculomotor deficit is characterized by a failure of volitional horizontal gaze with preservation of vertical movements. We present 2 sisters, 6 1/2 and 5 1/2 years of age, in whom the presenting sign was oculomotor apraxia. Oculomotor apraxia has not been previously reported as the presenting manifestation of Gaucher disease.

Published

1989

25. Familial variant of maxillonasal dysplasia?

Author

Gross-Kieselstein E, Har-Even Y, Navon P, and Branski D

Subjects

Child, Child, Preschool, Congenital Abnormalities diagnostic imaging, Female, Humans, Male, Maxilla diagnostic imaging, Nasal Bone diagnostic imaging, Radiography, Syndrome, Congenital Abnormalities genetics, Genetic Variation, Maxilla abnormalities, Nasal Bone abnormalities

Abstract

A rare syndrome comprising midfacial hypoplasia, lack of anterior nasal spine, and malocclusion is described. To the best of our knowledge, only sporadic cases with a similar cluster of defects have been reported, usually with the appellation of Binder syndrome. We describe an affected mother and daughter, thus suggesting a dominant mode of inheritance.

Published

1986

26. Antepartum fetal evaluation by assessment of fetal heart rate and fetal movements.

Author

Sadovsky E, Weinstein D, and Even Y

Subjects

Delivery, Obstetric, Evaluation Studies as Topic, Female, Fetal Diseases diagnosis, Humans, Infant, Newborn, Movement, Pregnancy, Risk, Fetal Heart physiology, Fetal Monitoring methods, Fetus physiology, Heart Rate

Abstract

Three antenatal monitoring tests--fetal movement acceleration test (FMAC-test), fetal heart rate-nonstress test (FHR-NST), and daily fetal movement recording (DFMR) were evaluated in 212 high risk pregnant women. While in 196 cases all three tests were normal, in 16 patients one to three tests showed pathological results. In the latter group, there was a significantly higher incidence of perinatal mortality, low Apgar score and growth retardation. Since false positives are known to occur in these tests, at least two should be pathological to warrant delivery in am attempt to prevent fetal death in utero. The sequence in which the pathology appears in the deteriorating fetus is as follows: the first to become non-reactive is the FMAC-test, followed by decreased fetal movements till cessation, and, finally, severe changes in the FHR-NST take place. The importance of this sequence of events is discussed.

Published

1981