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February 01, 2010

  • Date:05MondaySeptember 2011

    Giant titanium wave function in gallium oxide: a potential spin-bus system?

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    Time
    09:30 - 09:30
    Location
    Perlman Chemical Sciences Building
    LecturerDr. Frederic Mentink
    Organizer
    Department of Chemical and Biological Physics
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    Lecture
  • Date:05MondaySeptember 2011

    Studying mechanisms of immune cell activation at the single molecule level

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    Time
    13:00 - 13:00
    Location
    Wolfson Building for Biological Research
    LecturerDr. Eilon Sherman
    Laboratory of Cellular and Molecular Biology, CCR, NCI, NIH, Bethesda, MD, USA
    Organizer
    Department of Systems Immunology
    Contact
    AbstractShow full text abstract about Cells transduce information across their plasma membrane via...»
    Cells transduce information across their plasma membrane via engagement of surface receptors and the subsequent recruitment of intracellular proteins to these receptors. Such receptor-regulated cellular signaling often results in the formation of transient, heterogeneous protein complexes and macro-molecular clusters that serve to amplify, relay and regulate the incoming signals. Important examples include signaling complexes downstream of receptor tyrosine kinases (RTKs), immune receptors and G protein-coupled receptors (GPCRs). Although these signaling structures play a crucial role in health and disease, including immune activation, cancer, and HIV infection, the detailed biophysical mechanisms by which they assemble and serve to activate cells remain poorly understood due to shortcomings in current research techniques.
    We have developed and applied two-color photoactivated localization microscopy (PALM) to study the organization, structure and function of signaling complexes in the activation of immune (T) cells, at the single molecule level. Using this method, individual molecules can be identified and localized with resolution down to ~20nm. Second-order and clustering statistics were applied to resolve size-distributions of signaling complexes and molecular interactions at the plasma membrane of the cells. Our results show that nanoclusters, signaling complexes as small as dimers and trimers, govern the earliest events of T cell activation through dynamic interactions. Importantly, we show that these signaling complexes assume, in several ways, novel patterns of nanoscale organization that are crucial for cell activation. Taking a multidisciplinary approach, including the use of genetic mutagenesis, targeted drugs, statistical analysis and Monte-Carlo simulations, we could trace mechanisms that govern the formation of these patterns. Such mechanisms include combinations of dynamic protein-protein and protein-lipid interactions, hop-diffusion, confinement and patterning by the cell cytoskeleton and plasma membrane. These results extend our understanding of the mechanism of immune cell activation, findings also relevant to other receptor systems. I will further discuss novel research techniques that we have developed to better study critical signaling pathways in live interacting cells and in molecular detail.
    Lecture
  • Date:05MondaySeptember 2011

    Cytoskeletal signaling networks in cancer metastasis: invadopodia put their foot in the door

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    Time
    14:00 - 14:00
    Location
    Max and Lillian Candiotty Building
    LecturerDr. Hava Henn
    Yale Univ School of Medicine and Albert Einstein College of Medicine, USA
    Organizer
    Department of Immunology and Regenerative Biology
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    Lecture
  • Date:06TuesdaySeptember 2011

    The Benoziyo Center for Neurological Diseases lecture

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    Time
    10:00 - 11:00
    Title
    The miswired brain: from neurodevelopment to psychopathology
    Location
    Arthur and Rochelle Belfer Building for Biomedical Research
    LecturerKevin Mitchell
    Smurfit Institute of Genetics Trinity College Dublin Dublin, Ireland
    Organizer
    Department of Biomolecular Sciences
    Contact
    Lecture
  • Date:06TuesdaySeptember 2011

    From zebrafish to humans: what snapshots of antibody

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    Time
    13:30 - 13:30
    Location
    Wolfson Building for Biological Research
    LecturerMr. Joshua Weinstein
    Stanford University, from Stephen Quake’s lab
    Organizer
    Department of Systems Immunology
    Contact
    AbstractShow full text abstract about The adaptive immune system serves to enable a single individ...»
    The adaptive immune system serves to enable a single individual to defend against previously un-encountered pathogens by trial and error. The zebrafish is among the simplest organisms that systematically mutate DNA coding for antibodies – the proteins
    responsible for this defense. Recently, new high-throughput sequencing
    technologies have enabled the most complete picture yet of those
    populations of sequences coding for the antibody repertoires produced
    by individual fish. This talk will focus on the application of these
    tools to immune development and antigen-response in zebrafish and on their extension to vaccine-response in humans. Several unique and system-wide stereotypies are shown to arise across groups of organisms sharing either age or stimulus. Using these observations as a starting point, we develop a simple but powerful theoretical model that elucidates the interplay between antibody sequences and the dynamics
    of the B cells that produce them.
    Lecture
  • Date:07WednesdaySeptember 2011

    "Van der Waals Interactions in Biology, Chemistry, and Physics"

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    Time
    11:00 - 11:00
    Location
    Michael Sela Auditorium
    LecturerDr. Alexandre Tkatchenko
    Fritz Haber Institut, Berlin, Germany
    Organizer
    Department of Molecular Chemistry and Materials Science
    Contact
    Lecture
  • Date:07WednesdaySeptember 2011

    Controlling physiological processes down to the single cell level

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    Time
    14:00 - 14:00
    Location
    Max and Lillian Candiotty Building
    LecturerProf. David Ben Simon
    Dept. Statistical Physics Laboratory and Dept. of Biology Ecole Normale Superieure, Paris, France
    Organizer
    Department of Immunology and Regenerative Biology
    Contact
    Lecture
  • Date:08ThursdaySeptember 2011

    Seminar :Image Analysis and the use of image J

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    Time
    10:00 - 18:00
    Location
    Camelia Botnar Building
    Contact
    Lecture
  • Date:08ThursdaySeptember 2011

    Life Sciences Colloquium

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    Time
    11:00 - 11:00
    Title
    Damage Control - How the Pink1/Parkin pathway can regulate removal of impaired mitochondria by autophagy
    Location
    Dolfi and Lola Ebner Auditorium
    LecturerProf. Richard J. Youle
    National Institute of Neurological Disorders and Stroke NIH, USA
    Contact
    Colloquia
  • Date:08ThursdaySeptember 2011

    "Goldilocks and the 3 Bears"

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    Time
    17:30 - 17:30
    Title
    Musical Children's Theater
    Location
    Michael Sela Auditorium
    Contact
    Cultural Events
  • Date:09FridaySeptember 2011

    Give and Take Fair

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    Time
    10:30 - 13:00
    Location
    Ruthie & Samy Cohn Building for Magnetic Resonance Studies in Structural Biology
    Homepage
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    Cultural Events
  • Date:12MondaySeptember 2011

    3rd National Graduate Students Symposium in Organic Chemsity

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    Time
    All day
    Location
    Gerhard M.J. Schmidt Lecture Hall
    Chairperson
    Anitta Harrison
    Homepage
    Contact
    Conference
  • Date:12MondaySeptember 2011

    RNAi in Budding Yeast

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    Time
    13:00 - 13:00
    Location
    Arthur and Rochelle Belfer Building for Biomedical Research
    LecturerAnna Drinnenberg
    Whitehead Institute for Biomedical Research, Cambridge, MA
    Contact
    AbstractShow full text abstract about RNA interference (RNAi), a gene-silencing pathway triggered ...»
    RNA interference (RNAi), a gene-silencing pathway triggered by double-stranded RNA (dsRNA), is conserved in diverse eukaryotic species but has been lost in the model budding yeast, Saccharomyces cerevisiae.  We have shown that RNAi is present in other budding-yeast species, including Saccharomyces castellii, Klyuveromyces polysporus and Candida albicans.  To generate small interfering RNAs (siRNAs) these species use non-canonical Dicer proteins that probably emerged from a duplication event of another ribonuclease III enzyme in the budding-yeast lineage. The siRNAs in all three budding-yeast species mostly correspond to transposons and Y´ subtelomeric repeats indicating a role of RNAi in the regulation of such elements.  Reconstituting RNAi in S. cerevisiae by adding pathway components of S. castellii only subtly impacts cellular phenotype but destabilizes a cytoplasmically-inherited dsRNA virus known as Killer virus.  Cells that have lost the Killer virus are at a competitive disadvantage when exposed to the toxin secreted by cells that maintain Killer.  The incompatibility between RNAi and Killer viruses extends to other species; in that RNAi is absent in all fungal species known to possess dsRNA Killer viruses, whereas Killer is absent in closely related species that have retained RNAi.  Thus, the advantage imparted by acquiring and retaining killer viruses explains the persistence of RNAi-deficient species during fungal evolution.
    Lecture
  • Date:12MondaySeptember 2011

    Narcotic tolerance: A thing of the past?

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    Time
    14:00 - 14:00
    Location
    Max and Lillian Candiotty Building
    LecturerProf. Howard Gutstein
    Dept Biochemistry MD Anderson Cancer Center USA
    Organizer
    Department of Immunology and Regenerative Biology
    Contact
    Lecture
  • Date:13TuesdaySeptember 2011

    "Stimulus responsive adhesion of vesicles"

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    Time
    11:00 - 11:00
    Title
    Joint Seminar: Organic Chemistry & Materials and Interface
    Location
    Helen and Milton A. Kimmelman Building
    LecturerProf. Bart Jan RAVOO
    Organic Chemistry Institute and CeNTech, Westfälische Wilhelms-Universität Münster, Germany
    Organizer
    Department of Molecular Chemistry and Materials Science
    Contact
    AbstractShow full text abstract about Abstract: In the last years we have explored the formation o...»
    Abstract: In the last years we have explored the formation of vesicles of amphiphilic cyclodextrins and the molecular recognition of guest molecules at the surface of such host vesicles. On the one hand, the molecular recognition and interaction of bilayer vesicles is a versatile model system for the recognition, adhesion and fusion of biological cell membranes. On the other hand, the recognition-induced interaction of vesicles bridges the gap between colloid chemistry and supramolecular chemistry and gives rise to adaptive soft materials.
    In this lecture we will highlight our recent work on stimulus responsive adhesion of vesicles. We will show that photosensitive supramolecular linkers can give rise to light-responsive adhesion of vesicles as well as the light-induced capture and release of DNA in a supramolecular lipoplex. Furthermore, we will show that metal-binding supramolecular linkers can result in metal-ion responsive adhesion of vesicles. These dynamic supramolecular systems demonstrate that highly specific molecular recognition can guide the formation of adaptive soft materials.


    Lecture
  • Date:13TuesdaySeptember 2011

    "Iron-regulated Genes and the Host Response to Streptococcus pneumoniae"

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    Time
    13:00 - 13:00
    Location
    Wolfson Building for Biological Research
    LecturerDr. Edwin Swiatlo
    Division of Infectious Diseases University of Mississippi Medical Center Jackson, MS, USA
    Organizer
    Department of Systems Immunology
    Contact
    Lecture
  • Date:13TuesdaySeptember 2011

    To be announced

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    Time
    14:00 - 14:00
    Location
    Gerhard M.J. Schmidt Lecture Hall
    LecturerProf. John Kuryian
    To be announced
    Organizer
    Department of Chemical and Biological Physics
    Contact
    Lecture
  • Date:13TuesdaySeptember 2011

    Structural mechanisms of protein kinase regulation

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    Time
    14:00 - 14:00
    Location
    Gerhard M.J. Schmidt Lecture Hall
    LecturerProf. John Kuriyan
    Dept. Chemistry UC Berkeley
    Organizer
    Department of Immunology and Regenerative Biology
    Contact
    Lecture
  • Date:13TuesdaySeptember 2011

    "Without Borders" - Folk Music Festival

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    Time
    19:30 - 19:30
    Location
    Michael Sela Auditorium
    Contact
    Cultural Events
  • Date:14WednesdaySeptember 2011

    Cell Cycle Dynamics

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    Time
    12:00 - 12:00
    Location
    Arthur and Rochelle Belfer Building for Biomedical Research
    LecturerDr. Jan Skotheim
    Department of Biology Stanford University, CA
    Organizer
    Department of Molecular Genetics
    Contact
    Lecture

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