IL-2 therapy promotes suppressive ICOS+ Treg expansion in melanoma patients
Geok Choo Sim, … , Patrick Hwu, Laszlo Radvanyi
Geok Choo Sim, … , Patrick Hwu, Laszlo Radvanyi
Published December 2, 2013
Citation Information: J Clin Invest. 2014;124(1):99-110. https://doi.org/10.1172/JCI46266.
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Research Article Immunology

IL-2 therapy promotes suppressive ICOS+ Treg expansion in melanoma patients

Abstract

High-dose (HD) IL-2 therapy in patients with cancer increases the general population of Tregs, which are positive for CD4, CD25, and the Treg-specific marker Foxp3. It is unknown whether specific subsets of Tregs are activated and expanded during HD IL-2 therapy or whether activation of any particular Treg subset correlates with clinical outcome. Here, we evaluated Treg population subsets that were induced in patients with melanoma following HD IL-2 therapy. We identified a Treg population that was positive for CD4, CD25, Foxp3, and the inducible T cell costimulator (ICOS). This Treg population increased more than any other lymphocyte subset during HD IL-2 therapy and had an activated Treg phenotype, as indicated by high levels of CD39, CD73, and TGF-β. ICOS+ Tregs were the most proliferative lymphocyte population in the blood after IL-2 therapy. Patients with melanoma with enhanced expansion of ICOS+ Tregs in blood following the first cycle of HD IL-2 therapy had worse clinical outcomes than patients with fewer ICOS+ Tregs. However, there was no difference in total Treg expansion between HD IL-2 responders and nonresponders. These data suggest that increased expansion of the ICOS+ Treg population following the first cycle of HD IL-2 therapy may be predictive of clinical outcome.

Authors

Geok Choo Sim, Natalia Martin-Orozco, Lei Jin, Yan Yang, Sheng Wu, Edwina Washington, Deborah Sanders, Carol Lacey, Yijun Wang, Luis Vence, Patrick Hwu, Laszlo Radvanyi

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Figure 6

Changes in CD4+ICOS+ and CD4+CD25+Foxp3+ICOS+ T cells during HD IL-2 therapy in responding and nonresponding patients.

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Changes in CD4+ICOS+ and CD4+CD25+Foxp3+ICOS+ T cells during HD IL-2 the...
(A) Frequencies of CD4+ICOS+ T cells in the total viable lymphocyte gate are shown before and after cycle 1 of HD IL-2 therapy for a representative nonresponder (no. 027) and responder (no. 028). (B) Changes in the frequency of CD25+Foxp3+ in the gated CD4+ T cell subpopulation and (C) ICOS+ cells within the gated CD4+CD25+Foxp3+ subpopulation before and after cycle 1 of HD IL-2 therapy for the same nonresponder and responder. Frequencies of indicated cell subsets are indicated in AC. (D and E) Analysis of the fold changes in different ICOS+ and ICOS subsets during HD IL-2 therapy in nonresponding (n = 19) and responding (n = 7) patients. The indicated cell subsets were analyzed by flow cytometry before and 2 days after cycle 1 of therapy, and the fold change of each population was heat mapped by using an Excel conditional formatting program. Heat diagrams show the fold changes in the indicated T cell subsets as (D) the percentage of total peripheral blood lymphocytes in nonresponder and responders and (E) a percentage of the CD4+ subpopulation in nonresponders and responders (patient numbers are shown at the top of the heat map). The black bars on the right of each heat diagram indicate the CD4+ICOS+ subsets showing the greatest differences between responding and nonresponding patients. The asterisk denotes patient number 16 who received prior vaccination with recombinant MAGE-A3 vaccine before HD IL-2 therapy.