4.7 Article

Specific Notch receptor-ligand interactions control human TCR-αβ/γδ development by inducing differential Notch signal strength

期刊

JOURNAL OF EXPERIMENTAL MEDICINE
卷 210, 期 4, 页码 683-697

出版社

ROCKEFELLER UNIV PRESS
DOI: 10.1084/jem.20121798

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资金

  1. Odysseus program of the Fund for Scientific Research Flanders (FWO)
  2. FWO
  3. Flemish Institute for the advancement of Scientific-Technological Research in the Industry (IWT)
  4. Concerted Research Action of Ghent University (GOA)
  5. Interuniversity Attraction Poles Program (IUAP) from the Belgian Science Policy
  6. IWT
  7. Special Fund for Scientific Research (BOF) of the Ghent University
  8. Faculty of Medicine and Health Sciences from the Ghent University

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In humans, high Notch activation promotes gamma delta T cell development, whereas lower levels promote alpha beta-lineage differentiation. How these different Notch signals are generated has remained unclear. We show that differential Notch receptor-ligand interactions mediate this process. Whereas Delta-like 4 supports both TCR-alpha beta and -gamma delta development, Jagged1 induces mainly alpha beta-lineage differentiation. In contrast, Jagged2-mediated Notch activation primarily results in gamma delta T cell development and represses alpha beta-lineage differentiation by inhibiting TCR-beta formation. Consistently, TCR-alpha beta T cell development is rescued through transduction of a TCR-beta transgene. Jagged2 induces the strongest Notch signal through interactions with both Notch1 and Notch3, whereas Delta-like 4 primarily binds Notch1. In agreement, Notch3 is a stronger Notch activator and only supports gamma delta T cell development, whereas Notch1 is a weaker activator supporting both TCR-alpha beta and -gamma delta development. Fetal thymus organ cultures in JAG2-deficient thymic lobes or with Notch3-blocking antibodies confirm the importance of Jagged2/Notch3 signaling in human TCR-gamma delta differentiation. Our findings reveal that differential Notch receptor-ligand interactions mediate human TCR-alpha beta and -gamma delta T cell differentiation and provide a mechanistic insight into the high Notch dependency of human gamma delta T cell development.

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