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Now showing items 1 - 16 of 361

  • Robust and persistent reactivation of SIV and HIV by N-803 and depletion of CD8+ cells

    McBrien, Julia Bergild   Mavigner, Maud   Franchitti, Lavinia   Smith, S. Abigail   White, Erick   Tharp, Gregory K.   Walum, Hasse   Busman-Suhay, Kathleen   Aguilera-Sandoval, Christian R.   Thayer, William O.   Spagnuolo, Rae Ann   Kovarova, Martina   Wahl, Angela   Cervasi, Barbara   Margolis, David M.   Vanderford, Thomas H.   Carnathan, Diane G.   Paiardini, Mirko   Lifson, Jeffrey D.   Lee, John H.   Safrit, Jeffrey T.   Bosinger, Steven E.   Estes, Jacob D.   Derdeyn, Cynthia A.   Garcia, J. Victor   Kulpa, Deanna A.   Chahroudi, Ann   Silvestri, Guido  

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  • Nef-Mediated CD3-TCR Downmodulation Dampens Acute Inflammation and Promotes SIV Immune Evasion

    Joas, Simone   Sauermann, Ulrike   Roshani, Berit   Klippert, Antonina   Daskalaki, Maria   Mätz-Rensing, Kerstin   Stolte-Leeb, Nicole   Heigele, Anke   Tharp, Gregory K.   Gupta, Prachi Mehrotra   Nelson, Sydney   Bosinger, Steven   Parodi, Laura   Giavedoni, Luis   Silvestri, Guido   Sauter, Daniel   Stahl-Hennig, Christiane   Kirchhoff, Frank  

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  • Caspase-8 Collaborates with Caspase-11 to Drive Tissue Damage and Execution of Endotoxic Shock

    Manda, Pratyusha   Feng, Yanjun   Lyons, John D.   Berger, Scott B.   Otani, Shunsuke   DeLaney, Alexandra   Tharp, Gregory K.   Maner-Smith, Kristal   Burd, Eileen M.   Schaeffer, Michelle   Hoffman, Sandra   Capriotti, Carol   Roback, Linda   Young, Cedrick B.   Liang, Zhe   Ortlund, Eric A.   DiPaolo, Nelson C.   Bosinger, Steven   Bertin, John   Gough, Peter J.   Brodsky, Igor E.   Coopersmith, Craig M.   Shayakhmetov, Dmitry M.   Mocarski, Edward S.  

    The execution of shock following high dose E. coli lipopolysaccharide (LPS) or bacterial sepsis in mice required pro-apoptotic caspase-8 in addition to pro-pyroptotic caspase-11 and gasdermin D. Hematopoietic cells produced MyD88- and TRIF-dependent inflammatory cytokines sufficient to initiate shock without any contribution from cas pase-8 or caspase-11. Both proteases had to be present to support tumor necrosis factor- and interferon-beta-dependent tissue injury first observed in the small intestine and later in spleen and thymus. Caspase-11 enhanced the activation of caspase-8 and extrinsic cell death machinery within the lower small intestine. Neither caspase-8 nor caspase-11 was individually sufficient for shock. Both caspases collaborated to amplify inflammatory signals associated with tissue damage. Therefore, combined pyroptotic and apoptotic signaling mediated endotoxemia independently of RIPK1 kinase activity and RIPK3 function. These observations bring to light the relevance of tissue compartmentalization to disease processes in vivo where cytokines act in parallel to execute diverse cell death pathways.
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  • Transcriptome analysis of GVHD reveals aurora kinase A as a targetable pathway for disease prevention

    Furlan, Scott N.   Watkins, Benjamin   Tkachev, Victor   Flynn, Ryan   Cooley, Sarah   Ramakrishnan, Swetha   Singh, Karnail   Giver, Cindy   Hamby, Kelly   Stempora, Linda   Garrett, Aneesah   Chen, Jingyang   Betz, Kayla M.   Ziegler, Carly G. K.   Tharp, Gregory K.   Bosinger, Steven E.   Promislow, Daniel E. L.   Miller, Jeffrey S.   Waller, Edmund K.   Blazar, Bruce R.   Kean, Leslie S.  

    Graft-versus-host disease (GVHD) is the most common complication of hematopoietic stem cell transplant (HCT). However, our understanding of the molecular pathways that cause this disease remains incomplete, leading to inadequate treatment strategies. To address this, we measured the gene expression profile of nonhuman primate (NHP) T cells during acute GVHD. Utilizing microarray technology, we measured the expression profiles of CD3(+) T cells from five cohorts: allogeneic transplant recipients receiving (i) no immunoprophylaxis (No Rx), (ii) sirolimus monotherapy (Siro), (iii) tacrolimus-methotrexate (Tac-Mtx), as well as (iv) autologous transplant recipients (Auto) and (v) healthy controls (HC). This comparison allowed us to identify transcriptomic signatures specific for alloreactive T cells and determine the impact of both mTOR (mechanistic target of rapamycin) and calcineurin inhibition on GVHD. We found that the transcriptional profile of unprophylaxed GVHD was characterized by significant perturbation of pathways regulating T cell proliferation, effector function, and cytokine synthesis. Within these pathways, we discovered potentially druggable targets not previously implicated in GVHD, prominently including aurora kinase A (AURKA). Utilizing a murine GVHD model, we demonstrated that pharmacologic inhibition of AURKA could improve survival. Moreover, we found enrichment of AURKA transcripts both in allo-proliferating T cells and in sorted T cells from patients with clinical GVHD. These data provide a comprehensive elucidation of the T cell transcriptome in primate acute GVHD and suggest that AURKA should be considered a target for preventing GVHD, which, given the many available AURKA inhibitors in clinical development, could be quickly deployed for the prevention of GVHD.
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  • Enhanced Killing of Triple-Negative Breast Cancer Cells by Reassortant Reovirus and Topoisomerase Inhibitors

    Rodríguez Stewart, Roxana M.   Berry, Jameson T.L.   Berger, Angela K.   Yoon, Sung Bo   Hirsch, Aspen L.   Guberman, Jaime A.   Patel, Nirav B.   Tharp, Gregory K.   Bosinger, Steven E.   Mainou, Bernardo A.  

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  • BALDR:a computational pipeline for paired heavy and light chain immunoglobulin reconstruction in single-cell RNA-seq data

    Upadhyay, Amit A.   Kauffman, Robert C.   Wolabaugh, Amber N.   Cho, Alice   Patel, Nirav B.   Reiss, Samantha M.   Havenar-Daughton, Colin   Dawoud, Reem A.   Tharp, Gregory K.   Sanz, Inaki   Pulendran, Bali   Crotty, Shane   Lee, F. Eun-Hyung   Wrammert, Jens   Bosinger, Steven E.  

    B cells play a critical role in the immune response by producing antibodies, which display remarkable diversity. Here we describe a bioinformatic pipeline, BALDR (BCR Assignment of Lineage using De novo Reconstruction) that accurately reconstructs the paired heavy and light chain immunoglobulin gene sequences from Illumina single-cell RNA-seq data. BALDR was accurate for clonotype identification in human and rhesus macaque influenza vaccine and simian immunodeficiency virus vaccine induced vaccine-induced plasmablasts and naive and antigen-specific memory B cells. BALDR enables matching of clonotype identity with single-cell transcriptional information in B cell lineages and will have broad application in the fields of vaccines, human immunodeficiency virus broadly neutralizing antibody development, and cancer. BALDR is available at https://github.com/BosingerLab/BALDR.
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  • The 14 Fibs of Gregory K by Greg Pincus

    Andracki, Thaddeus  

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  • Gregory K. Mislick and Daniel A. Nussbaum: Cost Estimation—Methods and Tools

    Jones, Ken  

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  • Gregory K. Mislick and Daniel A. Nussbaum: Cost Estimation—Methods and Tools

    Jones   Ken  

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  • Book Review: Rajendra K. Srivastava and Gregory Metz Thomas, The Future of Branding

    Chatterjee   Rajashri  

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  • Book Review: Rajendra K. Srivastava and Gregory Metz Thomas, The Future of Branding

    Chatterjee, Rajashri  

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  • Ingram, Gregory K.; Hong, Yu-Hung (eds.) (2011): Climate Change and Land Policies

    Prof. Dr. Fabian Thiel  

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  • Ingram, Gregory K.; Hong, Yu-Hung (eds.) (2011): Climate Change and Land Policies

    Prof. Dr. Fabian Thiel  

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  • Climate Change and Land Policies, edited by Gregory K. Ingram and Yu-Hung Hong

    George Pomeroy  

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  • Probability: Modeling and Applications to Random Processesby Gregory K. Miller

    Review by: John Haigh  

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  • Climate Change and Land Policies, edited by Gregory K. Ingram and Yu-Hung Hong

    George Pomeroy  

    No abstract is available for this article.
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