The Identity of Human Tissue-Emigrant CD8+ T Cells
2020; Cell Press; Volume: 183; Issue: 7 Linguagem: Inglês
10.1016/j.cell.2020.11.019
ISSN1097-4172
AutoresMarcus Buggert, Laura A. Vella, Son Nguyen, Vincent H. Wu, Zeyu Chen, Takuya Sekine, André Perez‐Potti, Colby R. Maldini, Sasikanth Manne, Samuel Darko, Amy Ransier, Leticia Kuri-Cervantes, Alberto Sada Japp, Irene Bukh Brody, Martin A. Ivarsson, Jean-Baptiste Gorin, Olga Rivera‐Ballesteros, Laura Hertwig, Jack P. Antel, Matthew E. Johnson, Afam A. Okoye, Louis J. Picker, Golnaz Vahedi, Ernesto Sparrelid, Sian Llewellyn‐Lacey, Emma Gostick, Johan K. Sandberg, Niklas K. Björkström, Amit Bar‐Or, Yoav Dori, Ali Naji, David H. Canaday, Terri M. Laufer, Andrew D. Wells, David A. Price, Ian Frank, Daniel C. Douek, E. John Wherry, Maxim Itkin, Michael R. Betts,
Tópico(s)Immunotherapy and Immune Responses
ResumoLymphocyte migration is essential for adaptive immune surveillance. However, our current understanding of this process is rudimentary, because most human studies have been restricted to immunological analyses of blood and various tissues. To address this knowledge gap, we used an integrated approach to characterize tissue-emigrant lineages in thoracic duct lymph (TDL). The most prevalent immune cells in human and non-human primate efferent lymph were T cells. Cytolytic CD8+ T cell subsets with effector-like epigenetic and transcriptional signatures were clonotypically skewed and selectively confined to the intravascular circulation, whereas non-cytolytic CD8+ T cell subsets with stem-like epigenetic and transcriptional signatures predominated in tissues and TDL. Moreover, these anatomically distinct gene expression profiles were recapitulated within individual clonotypes, suggesting parallel differentiation programs independent of the expressed antigen receptor. Our collective dataset provides an atlas of the migratory immune system and defines the nature of tissue-emigrant CD8+ T cells that recirculate via TDL.
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