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  • Granzyme A activates anothe... Granzyme A activates another way to die
    Lieberman, Judy Immunological reviews, 20/May , Volume: 235, Issue: 1
    Journal Article
    Peer reviewed
    Open access

    Granzyme A (GzmA) is the most abundant serine protease in killer cell cytotoxic granules. GzmA activates a novel programed cell death pathway that begins in the mitochondrion, where cleavage of ...
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  • Knocking down disease: a pr... Knocking down disease: a progress report on siRNA therapeutics
    Wittrup, Anders; Lieberman, Judy Nature reviews. Genetics, 09/2015, Volume: 16, Issue: 9
    Journal Article
    Peer reviewed
    Open access

    Small interfering RNAs (siRNAs), which downregulate gene expression guided by sequence complementarity, can be used therapeutically to block the synthesis of disease-causing proteins. The main ...
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  • Knocking 'em Dead: Pore-For... Knocking 'em Dead: Pore-Forming Proteins in Immune Defense
    Liu, Xing; Lieberman, Judy Annual review of immunology, 04/2020, Volume: 38, Issue: 1
    Journal Article
    Peer reviewed
    Open access

    Immune cells use a variety of membrane-disrupting proteins complement, perforin, perforin-2, granulysin, gasdermins, mixed lineage kinase domain-like pseudokinase (MLKL) to induce different kinds of ...
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  • Dysregulation of microRNA biogenesis and gene silencing in cancer
    Hata, Akiko; Lieberman, Judy Science signaling, 2015-Mar-17, Volume: 8, Issue: 368
    Journal Article
    Peer reviewed
    Open access

    MicroRNAs (miRNAs) are small noncoding RNAs that suppress the abundance of partially complementary mRNAs and inhibit their translation. Each miRNA can regulate hundreds of mRNAs, sometimes strongly ...
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  • miR-34 and p53: New Insight... miR-34 and p53: New Insights into a Complex Functional Relationship
    Navarro, Francisco; Lieberman, Judy PloS one, 07/2015, Volume: 10, Issue: 7
    Journal Article
    Peer reviewed
    Open access

    miR-34, a tumor suppressor miRNA family transcriptionally activated by p53, is considered a critical mediator of p53 function. However, knockout of the mouse miR-34 family has little or no effect on ...
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  • Cryo-EM structure of the ga... Cryo-EM structure of the gasdermin A3 membrane pore
    Ruan, Jianbin; Xia, Shiyu; Liu, Xing ... Nature (London), 05/2018, Volume: 557, Issue: 7703
    Journal Article
    Peer reviewed
    Open access

    Gasdermins mediate inflammatory cell death after cleavage by caspases or other, unknown enzymes. The cleaved N-terminal fragments bind to acidic membrane lipids to form pores, but the mechanism of ...
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  • Death by a thousand cuts: g... Death by a thousand cuts: granzyme pathways of programmed cell death
    Chowdhury, Dipanjan; Lieberman, Judy Annual review of immunology, 01/2008, Volume: 26
    Journal Article
    Peer reviewed
    Open access

    The granzymes are cell death-inducing enzymes, stored in the cytotoxic granules of cytotoxic T lymphocytes and natural killer cells, that are released during granule exocytosis when a specific ...
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  • The ABCs of granule-mediate... The ABCs of granule-mediated cytotoxicity: new weapons in the arsenal
    Lieberman, Judy Nature reviews. Immunology, 200305, 2003-May, 2003-05-01, 20030501, Volume: 3, Issue: 5
    Journal Article
    Peer reviewed
    Open access

    Granule exocytosis is the main pathway for the immune elimination of virus-infected cells and tumour cells by cytotoxic T lymphocytes and natural killer cells. After target-cell recognition, release ...
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  • Inflammasome-activated gasd... Inflammasome-activated gasdermin D causes pyroptosis by forming membrane pores
    Liu, Xing; Zhang, Zhibin; Ruan, Jianbin ... Nature (London), 07/2016, Volume: 535, Issue: 7610
    Journal Article
    Peer reviewed
    Open access

    Inflammatory caspases (caspases 1, 4, 5 and 11) are activated in response to microbial infection and danger signals. When activated, they cleave mouse and human gasdermin D (GSDMD) after Asp276 and ...
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  • Visualizing lipid-formulate... Visualizing lipid-formulated siRNA release from endosomes and target gene knockdown
    Wittrup, Anders; Ai, Angela; Liu, Xing ... Nature biotechnology, 08/2015, Volume: 33, Issue: 8
    Journal Article
    Peer reviewed
    Open access

    A central hurdle in developing small interfering RNAs (siRNAs) as therapeutics is the inefficiency of their delivery across the plasma and endosomal membranes to the cytosol, where they interact with ...
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