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  1. Home
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Browsing by Author "Jiajie Hou"

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    PublicationErratum
    Correction to: The NK cell granule protein NKG7 regulates cytotoxic granule exocytosis and inflammation (Nature Immunology, (2020), 21, 10, (1205-1218), 10.1038/s41590-020-0758-6)
    (Nature Research, 2024) Susanna S. Ng; Fabian De Labastida Rivera; Juming Yan; Dillon Corvino; Indrajit Das; Ping Zhang; Rachel Kuns; Shashi Bhushan Chauhan; Jiajie Hou; Xian-Yang Li; Teija C. M. Frame; Benjamin A. McEnroe; Eilish Moore; Jinrui Na; Jessica A. Engel; Megan S. F. Soon; Bhawana Singh; Andrew J. Kueh; Marco J. Herold; Marcela Montes de Oca; Siddharth Sankar Singh; Patrick T. Bunn; Amy Roman Aguilera; Mika Casey; Matthias Braun; Nazanin Ghazanfari; Shivangi Wani; Yulin Wang; Fiona H. Amante; Chelsea L. Edwards; Ashraful Haque; William C. Dougall; Om Prakash Singh; Alan G. Baxter; Michele W. L. Teng; Alex Loukas; Norelle L. Daly; Nicole Cloonan; Mariapia A. Degli-Esposti; Jude Uzonna; William R. Heath; Tobias Bald; Siok-Keen Tey; Kyohei Nakamura; Geoffrey R. Hill; Rajiv Kumar; Shyam Sundar; Mark J. Smyth; Christian R. Engwerda
    Correction to: Nature Immunologyhttps://doi.org/10.1038/s41590-020-0758-6, published online 24 August 2020. The Chief Editor is correcting this article at the request of the corresponding author, Christian Engwerda. An investigation by QIMR Berghofer Medical Research Institute found that the original Figs. 7e, 7h (upper panel) and 8a and Extended Data Fig. 5b (EO771 data only) were based on experiments for which no evidence of their conduct or primary data could be confirmed. As such, the data from the underlying experiments are believed to have been fabricated or are unreliable, respectively. The four panels have been removed from Figs. 7 and 8 and Extended Data Fig. 5 (see Supplementary Information for a list of edits and original article for comparison). The major finding of the paper that NKG7 regulates cytotoxic granule exocytosis and inflammation remains unaffected. No concerns have been raised regarding other data in the paper. © The Author(s), under exclusive licence to Springer Nature America, Inc. 2024.
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    PublicationArticle
    The NK cell granule protein NKG7 regulates cytotoxic granule exocytosis and inflammation
    (Nature Research, 2020) Susanna S. Ng; Fabian De Labastida Rivera; Juming Yan; Dillon Corvino; Indrajit Das; Ping Zhang; Rachel Kuns; Shashi Bhushan Chauhan; Jiajie Hou; Xian-Yang Li; Teija C. M. Frame; Benjamin A. McEnroe; Eilish Moore; Jinrui Na; Jessica A. Engel; Megan S. F. Soon; Bhawana Singh; Andrew J. Kueh; Marco J. Herold; Marcela Montes de Oca; Siddharth Sankar Singh; Patrick T. Bunn; Amy Roman Aguilera; Mika Casey; Matthias Braun; Nazanin Ghazanfari; Shivangi Wani; Yulin Wang; Fiona H. Amante; Chelsea L. Edwards; Ashraful Haque; William C. Dougall; Om Prakash Singh; Alan G. Baxter; Michele W. L. Teng; Alex Loukas; Norelle L. Daly; Nicole Cloonan; Mariapia A. Degli-Esposti; Jude Uzonna; William R. Heath; Tobias Bald; Siok-Keen Tey; Kyohei Nakamura; Geoffrey R. Hill; Rajiv Kumar; Shyam Sundar; Mark J. Smyth; Christian R. Engwerda
    Immune-modulating therapies have revolutionized the treatment of chronic diseases, particularly cancer. However, their success is restricted and there is a need to identify new therapeutic targets. Here, we show that natural killer cell granule protein 7 (NKG7) is a regulator of lymphocyte granule exocytosis and downstream inflammation in a broad range of diseases. NKG7 expressed by CD4+ and CD8+ T cells played key roles in promoting inflammation during visceral leishmaniasis and malaria—two important parasitic diseases. Additionally, NKG7 expressed by natural killer cells was critical for controlling cancer initiation, growth and metastasis. NKG7 function in natural killer and CD8+ T cells was linked with their ability to regulate the translocation of CD107a to the cell surface and kill cellular targets, while NKG7 also had a major impact on CD4+ T cell activation following infection. Thus, we report a novel therapeutic target expressed on a range of immune cells with functions in different immune responses. © 2020, The Author(s), under exclusive licence to Springer Nature America, Inc.
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