Frontiers in Immunology (Jan 2019)

TCR Repertoire Analysis Reveals Mobilization of Novel CD8+ T Cell Clones Into the Cancer-Immunity Cycle Following Anti-CD4 Antibody Administration

  • Hiroyasu Aoki,
  • Hiroyasu Aoki,
  • Satoshi Ueha,
  • Satoshi Ueha,
  • Shigeyuki Shichino,
  • Shigeyuki Shichino,
  • Haru Ogiwara,
  • Haru Ogiwara,
  • Shin-ichi Hashimoto,
  • Shin-ichi Hashimoto,
  • Shin-ichi Hashimoto,
  • Kazuhiro Kakimi,
  • Satoru Ito,
  • Satoru Ito,
  • Satoru Ito,
  • Kouji Matsushima,
  • Kouji Matsushima

DOI
https://doi.org/10.3389/fimmu.2018.03185
Journal volume & issue
Vol. 9

Abstract

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Depletion of CD4+ cells using an anti-CD4 monoclonal antibody (anti-CD4 mAb) induces the expansion of tumor-reactive CD8+ T cells and strong antitumor effects in several murine tumor models. However, it is not known whether the anti-CD4 mAb treatment activates a particular or a broad spectrum of tumor-reactive CD8+ T cell clones. To investigate the changes in the TCR repertoire induced by the anti-CD4 mAb treatment, we performed unbiased high-throughput TCR sequencing in a B16F10 mouse subcutaneous melanoma model. By Inter-Organ Clone Tracking analysis, we demonstrated that anti-CD4 mAb treatment increased the diversity and combined frequency of CD8+ T cell clones that overlapped among the tumor, draining lymph node (dLN), and peripheral blood repertoires. Interestingly, the anti-CD4 mAb treatment-induced expansion of overlapping clones occurred mainly in the dLN rather than in the tumor. Overall, the Inter-Organ Clone Tracking analysis revealed that anti-CD4 mAb treatment enhances the mobilization of a wide variety of tumor-reactive CD8+ T cell clones into the Cancer-Immunity Cycle and thus induces a robust antitumor immune response in mice.

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