| Literature DB >> 35857588 |
Bernardo S Reis1, Patrick W Darcy1, Iasha Z Khan1, Christine S Moon2, Adam E Kornberg2, Vanessa S Schneider1,3, Yelina Alvarez1, Olawale Eleso1, Caixia Zhu1, Marina Schernthanner1, Ainsley Lockhart1, Aubrey Reed1, Juliana Bortolatto1, Tiago B R Castro1, Angelina M Bilate1, Sergei Grivennikov4, Arnold S Han2, Daniel Mucida1,5.
Abstract
γδ T cells represent a substantial fraction of intestinal lymphocytes at homeostasis, but they also constitute a major lymphocyte population infiltrating colorectal cancers (CRCs); however, their temporal contribution to CRC development or progression remains unclear. Using human CRC samples and murine CRC models, we found that most γδ T cells in premalignant or nontumor colons exhibit cytotoxic markers, whereas tumor-infiltrating γδ T cells express a protumorigenic profile. These contrasting T cell profiles were associated with distinct T cell receptor (TCR)-Vγδ gene usage in both humans and mice. Longitudinal intersectional genetics and antibody-dependent strategies targeting murine γδ T cells enriched in the epithelium at steady state led to heightened tumor development, whereas targeting γδ subsets that accumulate during CRC resulted in reduced tumor growth. Our results uncover temporal pro- and antitumor roles for γδ T cell subsets.Entities:
Mesh:
Substances:
Year: 2022 PMID: 35857588 PMCID: PMC9326786 DOI: 10.1126/science.abj8695
Source DB: PubMed Journal: Science ISSN: 0036-8075 Impact factor: 63.714