| Literature DB >> 27521270 |
Michael Thomas Wong1, David Eng Hui Ong2, Frances Sheau Huei Lim3, Karen Wei Weng Teng4, Naomi McGovern4, Sriram Narayanan4, Wen Qi Ho4, Daniela Cerny5, Henry Kun Kiaang Tan6, Rosslyn Anicete6, Bien Keem Tan7, Tony Kiat Hon Lim8, Chung Yip Chan9, Peng Chung Cheow9, Ser Yee Lee9, Angela Takano8, Eng-Huat Tan10, John Kit Chung Tam11, Ern Yu Tan12, Jerry Kok Yen Chan13, Katja Fink4, Antonio Bertoletti14, Florent Ginhoux4, Maria Alicia Curotto de Lafaille4, Evan William Newell15.
Abstract
Depending on the tissue microenvironment, T cells can differentiate into highly diverse subsets expressing unique trafficking receptors and cytokines. Studies of human lymphocytes have primarily focused on a limited number of parameters in blood, representing an incomplete view of the human immune system. Here, we have utilized mass cytometry to simultaneously analyze T cell trafficking and functional markers across eight different human tissues, including blood, lymphoid, and non-lymphoid tissues. These data have revealed that combinatorial expression of trafficking receptors and cytokines better defines tissue specificity. Notably, we identified numerous T helper cell subsets with overlapping cytokine expression, but only specific cytokine combinations are secreted regardless of tissue type. This indicates that T cell lineages defined in mouse models cannot be clearly distinguished in humans. Overall, our data uncover a plethora of tissue immune signatures and provide a systemic map of how T cell phenotypes are altered throughout the human body.Entities:
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Year: 2016 PMID: 27521270 DOI: 10.1016/j.immuni.2016.07.007
Source DB: PubMed Journal: Immunity ISSN: 1074-7613 Impact factor: 31.745