| Literature DB >> 33128876 |
Daniela Pais Ferreira1, Joana Gomes Silva1, Tania Wyss2, Silvia A Fuertes Marraco1, Léonardo Scarpellino3, Mélanie Charmoy1, Roeltje Maas4, Imran Siddiqui1, Li Tang5, Johanna A Joyce6, Mauro Delorenzi7, Sanjiv A Luther3, Daniel E Speiser1, Werner Held8.
Abstract
Central memory CD8+ T cells (Tcm) control systemic secondary infections and can protect from chronic infection and cancer as a result of their stem-cell-like capacity to expand, differentiate, and self-renew. Central memory is generally thought to emerge following pathogen clearance and to form based on the de-differentiation of cytolytic effector cells. Here, we uncovered rare effector-phase CD8+ T cells expressing high amounts of the transcription factor Tcf7 (Tcf1) that showed no evidence of prior cytolytic differentiation and that displayed key hallmarks of Tcm cells. These effector-phase Tcf7hi cells quantitatively yielded Tcm cells based on lineage tracing. Mechanistically, Tcf1 counteracted the differentiation of Tcf7hi cells and sustained the expression of conserved adult stem-cell genes that were critical for CD8+ T cell stemness. The discovery of stem-cell-like CD8+ T cells during the effector response to acute infection provides an opportunity to optimize Tcm cell formation by vaccination.Entities:
Keywords: CD8(+) T cells; Granzyme; LCMV infection; T cell factor 1 (Tcf1) (Tcf7); central memory; effector differentiation; stemness; vaccination
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Year: 2020 PMID: 33128876 DOI: 10.1016/j.immuni.2020.09.005
Source DB: PubMed Journal: Immunity ISSN: 1074-7613 Impact factor: 31.745