Tumor emergence is sensed by self-specific CD44hi memory Tregs that create a dominant tolerogenic environment for tumors in mice
Guillaume Darrasse-Jèze, … , Katrina Podsypanina, David Klatzmann
Guillaume Darrasse-Jèze, … , Katrina Podsypanina, David Klatzmann
Published August 3, 2009
Citation Information: J Clin Invest. 2009;119(9):2648-2662. https://doi.org/10.1172/JCI36628.
View: Text | PDF
Research Article Immunology

Tumor emergence is sensed by self-specific CD44hi memory Tregs that create a dominant tolerogenic environment for tumors in mice

Abstract

Early responses of Tregs and effector T cells (Teffs) to their first encounter with tumor cells have been poorly characterized. Here we have shown, in both implanted and in situ–induced mouse tumor models, that the appearance of tumor cells is immediately sensed by CD44hi memory Tregs that are specific for self antigens. The rapid response of these Tregs preceded and prevented activation of naive antitumor Teffs. The relative speed of the Treg versus the Teff response within the first 2–4 days determined the outcome of the antitumor immune response: tolerance or rejection. If antitumor memory Teffs were present at the time of tumor emergence, both Tregs and Teffs were recruited and activated with memory kinetics; however, the Tregs were unable to control the Teffs, which eradicated the tumor cells. This balance between effector and regulatory responses did not depend on the number of Tregs and Teffs, but rather on their memory status. Thus, in the natural setting, dominant tolerogenic immunosurveillance by self-specific memory Tregs protects tumors, just as it protects normal tissues. More generally, our results reveal that the timing of Treg and Teff engagement, determined by their memory status, is an important mode of regulation of immune responses.

Authors

Guillaume Darrasse-Jèze, Anne-Sophie Bergot, Aurélie Durgeau, Fabienne Billiard, Benoît L. Salomon, José L. Cohen, Bertrand Bellier, Katrina Podsypanina, David Klatzmann

×

Figure 4

Early Treg proliferation in dLNs is that of amTregs and is MHC class II dependent.

Options: View larger image (or click on image) Download as PowerPoint
Early Treg proliferation in dLNs is that of amTregs and is MHC class II ...
(A) We adoptively transferred 1-day 4T1 tumor-bearing Thy1.2 mice with naive CD44lo or CD44hi amTregs purified from unmanipulated Thy1.1 BALB/c mice and CFSE labeled prior to inoculation. CFSE proliferation profiles of naive and amTregs among CD4+Foxp3+Thy1.1+ donor cells were evaluated at day 5 after adoptive transfer in dLNs and ndLNs. Each panel is representative of 3 mice. (B) Proliferation of Tregs at tumor emergence is dependent on MHC class II signaling. MHC-IIΔ/Δ or C57BL/6 mice with or without 1 day B16F10 tumor received CFSE-labeled Thy1.1 congenic cells from normal mice. Division profiles of Thy1.1+ donor cells were evaluated by flow cytometry at day 6 in dLNs, ndLNs, or nLNs (n = 3 per group). In A and B, numbers within histograms denote the percentages of CFSE and CFSEint cells, as defined in Figure 1A, and corresponding percentages are also shown graphically. *P < 0.001 versus respective control.