CX3CR1 identifies PD-1 therapy–responsive CD8+ T cells that withstand chemotherapy during cancer chemoimmunotherapy
Yiyi Yan, … , Roxana S. Dronca, Haidong Dong
Yiyi Yan, … , Roxana S. Dronca, Haidong Dong
Published April 19, 2018
Citation Information: JCI Insight. 2018;3(8):e97828. https://doi.org/10.1172/jci.insight.97828.
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Research Article Immunology Oncology

CX3CR1 identifies PD-1 therapy–responsive CD8+ T cells that withstand chemotherapy during cancer chemoimmunotherapy

Abstract

Although immune checkpoint inhibitors have resulted in durable clinical benefits in a subset of patients with advanced cancer, some patients who did not respond to initial anti–PD-1 therapy have been found to benefit from the addition of salvage chemotherapy. However, the mechanism responsible for the successful chemoimmunotherapy is not completely understood. Here we show that a subset of circulating CD8+ T cells expressing the chemokine receptor CX3CR1 are able to withstand the toxicity of chemotherapy and are increased in patients with metastatic melanoma who responded to chemoimmunotherapy (paclitaxel and carboplatin plus PD-1 blockade). These CX3CR1+CD8+ T cells have effector memory phenotypes and the ability to efflux chemotherapy drugs via the ABCB1 transporter. In line with clinical observation, our preclinical models identified an optimal sequencing of chemoimmunotherapy that resulted in an increase of CX3CR1+CD8+ T cells. Taken together, we found a subset of PD-1 therapy–responsive CD8+ T cells that were capable of withstanding chemotherapy and executing tumor rejection with their unique abilities of drug efflux (ABCB1), cytolytic activity (granzyme B and perforin), and migration to and retention (CX3CR1 and CD11a) at tumor sites. Future strategies to monitor and increase the frequency of CX3CR1+CD8+ T cells may help to design effective chemoimmunotherapy to overcome cancer resistance to immune checkpoint blockade therapy.

Authors

Yiyi Yan, Siyu Cao, Xin Liu, Susan M. Harrington, Wendy E. Bindeman, Alex A. Adjei, Jin Sung Jang, Jin Jen, Ying Li, Pritha Chanana, Aaron S. Mansfield, Sean S. Park, Svetomir N. Markovic, Roxana S. Dronca, Haidong Dong

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Figure 4

CX3CR1+Granzyme B+CD8+ T cells increased after chemoimmunotherapy.

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CX3CR1+Granzyme B+CD8+ T cells increased after chemoimmunotherapy. Once ...
Once B16F10 mouse melanoma tumors were palpable on day 7 after tumor injection, animals were randomly assigned to treatment groups. (A) Schedule of treatments. Mice were treated with i.p. injection of anti–PD-1 and –PD-L1 antibody (at 100 μg of each antibody) and collectively indicated as anti-PD IgG for a total of 5 doses at 3-day intervals. Carboplatin (40 μg/g) and paclitaxel (10 μg/g body weight) (collectively indicated as CP) were injected i.p. once either on day 7 or on day 10 after tumor injection. (B) Tumor growth. Data show the mean ± SEM of 5 mice per group; **P < 0.01 compared between day 7 and 10 treatment with CP plus anti-PD (2-way ANOVA). (C) The survival curve of treated animals as in B. *P < 0.05 compared between control and anti-PD plus day 10 CP (log-rank test). (D) Frequency of CX3CR1+Granzyme B+CD8+ T cells was measured in CD11ahiCD8+ cells isolated from tumor tissues on day 16 after tumor injection (*P < 0.05, n = 6, 2-way ANOVA). (E) B16F10 tumor growth in WT and PD-1–KO mice after treatment with CP) as in B on day 8 after tumor injection. One of 2 independent experiments (***P < 0.001, n = 3–5, 2-way ANOVA).