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RUP response to COVID-19 crisis: learn about the steps we are taking and find relevant content.

Newest Articles
Article
| November 20 2020
Featured Figure
Novel mechanisms of sensitivity to LPS/infection
Katharina Richard, Kurt H. Piepenbrink, Kari Ann Shirey, Archana Gopalakrishnan, Shreeram Nallar, Daniel J. Prantner, Darren J. Perkins, Wendy Lai, Alexandra Vlk, Vladimir Y. Toshchakov, Chiguang Feng, Rachel Fanaroff, Andrei E. Medvedev, Jorge C.G. Blanco, Stefanie N. Vogel
We developed mice expressing Tlr4 SNPs homologous to those expressed in humans and associated with infectious and inflammatory diseases. Cellular and molecular analyses of TLR4 signaling in wild-type vs. TLR4-SNP mice revealed novel mechanisms of LPS hyporesponsiveness and altered disease susceptibility.
Article
| November 19 2020
Featured Figure
In vivo efficacy of anti–SARS-CoV-2 antibodies
Alexandra Schäfer, Frauke Muecksch, Julio C.C. Lorenzi, Sarah R. Leist, Melissa Cipolla, Stylianos Bournazos, Fabian Schmidt, Rachel M. Maison, Anna Gazumyan, David R. Martinez, Ralph S. Baric, Davide F. Robbiani, Theodora Hatziioannou, Jeffrey V. Ravetch, Paul D. Bieniasz, Richard A. Bowen, Michel C. Nussenzweig, Timothy P. Sheahan
Human monoclonal antibody potency in vitro does not uniformly correlate with its in vivo neutralization of SARS-CoV-2. Antibody Fc-effector function is important for in vivo neutralization, and antibody combinations show superior efficacy compared with single antibodies.
Brief Definitive Report
| November 17 2020
Featured Figure
Clonal fate mapping of CD4 T cells
Achia Khatun, Moujtaba Y. Kasmani, Ryan Zander, David M. Schauder, Jeremy P. Snook, Jian Shen, Xiaopeng Wu, Robert Burns, Yi-Guang Chen, Chien-Wei Lin, Matthew A. Williams, Weiguo Cui
The naive polyclonal CD4 T cell repertoire can differentiate into multiple lineages during acute viral infection, with some clones exhibiting a preferred lineage choice, as revealed by scRNA-seq and scTCR-seq. TCR motifs can partially skew clone-intrinsic lineage preferences toward the TFH fate.
Article
| November 12 2020
Featured Figure
Humoral correlates of protection for typhoid fever
Celina Jin, Jennifer Hill, Bronwyn M. Gunn, Wen-Han Yu, Lindsay C. Dahora, Elizabeth Jones, Mari Johnson, Malick M. Gibani, Rachel L. Spreng, S. Munir Alam, Anna Nebykova, Helene B. Juel, S. Moses Dennison, Kelly E. Seaton, Jonathan K. Fallon, Georgia D. Tomaras, Galit Alter, Andrew J. Pollard
Distinct protective humoral signatures are induced by Vi-conjugate and Vi-polysaccharide vaccines. Shared humoral features across both vaccines suggest that protection against typhoid fever is mediated through a combination of qualitative features of the polyclonal humoral response (avidity and innate immune cell functional responses) in addition to antibody quantity.
Technical Advances and Resources
| November 11 2020
Featured Figure
Gut microbiomes in healthy donors and patients with cancer
Allyson L. Byrd, Menghan Liu, Kei E. Fujimura, Svetlana Lyalina, Deepti R. Nagarkar, Bruno Charbit, Jacob Bergstedt, Etienne Patin, Oliver J. Harrison, Lluís Quintana-Murci, Ira Mellman, Darragh Duffy, Matthew L. Albert, the Milieu Intérieur Consortium
By characterizing gut microbiome composition across 946 healthy donors, Byrd et al. demonstrate strong influences of age and biological sex. Additionally, they define global shifts in the gut microbiome composition of patients with non-gastrointestinal tumors compared with healthy donors.
Article
| November 10 2020
Featured Figure
Unconventional T cells controlled by FAS
Maria Elena Maccari, Sebastian Fuchs, Patrick Kury, Geoffroy Andrieux, Simon Völkl, Bertram Bengsch, Myriam Ricarda Lorenz, Maximilian Heeg, Jan Rohr, Sabine Jägle, Carla N. Castro, Miriam Groß, Ursula Warthorst, Christoph König, Ilka Fuchs, Carsten Speckmann, Julian Thalhammer, Friedrich G. Kapp, Markus G. Seidel, Gregor Dückers, Stefan Schönberger, Catharina Schütz, Marita Führer, Robin Kobbe, Dirk Holzinger, Christian Klemann, Petr Smisek, Stephen Owens, Gerd Horneff, Reinhard Kolb, Nora Naumann-Bartsch, Maurizio Miano, Julian Staniek, Marta Rizzi, Tomas Kalina, Pascal Schneider, Anika Erxleben, Rolf Backofen, Arif Ekici, Charlotte M. Niemeyer et al.
Maccari et al. identify a physiological population of highly proliferative CD38+CD45RA+, IL-10–producing TCRαβ+ T cells. They can be CD4+, CD8+, or double-negative and are controlled by FAS and CTLA4, while their survival is enhanced by mTOR and STAT3 signals.
Technical Advances and Resources
| November 06 2020
Featured Figure
Murine 4G-CAR-T cells co-engineered to express IL-15
Evripidis Lanitis, Giorgia Rota, Paris Kosti, Catherine Ronet, Aodrenn Spill, Bili Seijo, Pedro Romero, Denarda Dangaj, George Coukos, Melita Irving
This work presents robust tools for the transduction and expansion of murine CAR-T cells and demonstrates the impact of murine IL-15 co-expression on CAR-T cell expansion, phenotype, function, and tumor microenvironment reprogramming in immunocompetent mice.

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Related Articles from Rockefeller University Press

Current Issue
Volume 217,
Issue 11,
November 2, 2020
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Reviews & Opinions
Found in Translation
| November 23 2020
Featured Figure
Adoptive cell therapy: Living drugs against cancer
Tamara Laskowski, Katayoun Rezvani
Tamara Laskowski and Katayoun Rezvani discuss the recent advances of adoptive cell therapy in cancer.
Insights
| November 13 2020
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A knockout combination for MPN stem cells
Megan Bywater, Steven W. Lane
Arsenic trioxide in combination with IFNα is able to deplete MPN stem cells, leading to reduced transplantation and even long-term treatment-free remission in disease control.
Insights
| November 13 2020
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The BAFFling persistence of memory B cells
Jeremy F. Brooks, Julie Zikherman
The pathways involved in the persistence of memory B cells are largely unknown. In this issue, two groups (Müller-Winkler et al. and Lau et al.) take complementary approaches to identify an essential role for BAFFR in the survival of memory B cells.
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Neuroscience 2019

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