Communications Medicine (Oct 2023)

Lenvatinib activates anti-tumor immunity by suppressing immunoinhibitory infiltrates in the tumor microenvironment of advanced hepatocellular carcinoma

  • Masami Yamauchi,
  • Atsushi Ono,
  • Kei Amioka,
  • Yasutoshi Fujii,
  • Hikaru Nakahara,
  • Yuji Teraoka,
  • Shinsuke Uchikawa,
  • Hatsue Fujino,
  • Takashi Nakahara,
  • Eisuke Murakami,
  • Wataru Okamoto,
  • Daiki Miki,
  • Tomokazu Kawaoka,
  • Masataka Tsuge,
  • Michio Imamura,
  • C. Nelson Hayes,
  • Waka Ohishi,
  • Takeshi Kishi,
  • Mizuki Kimura,
  • Natsumi Suzuki,
  • Koji Arihiro,
  • Hiroshi Aikata,
  • Kazuaki Chayama,
  • Shiro Oka

DOI
https://doi.org/10.1038/s43856-023-00390-x
Journal volume & issue
Vol. 3, no. 1
pp. 1 – 14

Abstract

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Abstract Background Lenvatinib, a multiple receptor tyrosine kinase inhibitor, might exert antitumor effects via tumor immune modulation. However, changes in the tumor immune microenvironment induced by lenvatinib are poorly understood. We investigated the effect of lenvatinib on immune features in clinical samples from patients with hepatocellular carcinoma. Methods Fifty-one patients with advanced hepatocellular carcinoma who received lenvatinib monotherapy as first-line treatment were enrolled. We collected blood sample (n = 51) and tumor tissue (n, baseline/four weeks after treatment initiation/post-progression = 50/8/12). DNA, RNA, and proteins extracted from the tissues were subjected to multi-omics analysis, and patients were classified into two groups according to baseline immune status. Each group was investigated in terms of the dynamics of tumor signaling. We also longitudinally analyzed circulating immune proteins and chemokines in peripheral blood. Results Here we show that lenvatinib has similar anti-tumor efficacy with objective response rate and progression-free survival in both Immune-Hot and Immune-Cold subtypes. Immune signatures associated with T-cell functions and interferon responses are enriched in the early phase of treatment, while signatures associated with immunoinhibitory cells are downregulated along with efficient vascular endothelial growth factor receptor and fibroblast growth factor receptor blockades. These findings are supported by imaging mass cytometry, T-cell receptor repertoire analysis and kinetics of circulating proteins. We also identify interleukin-8 and angiopoietin-2 as possible targets of intervention to overcome resistance to existing immunotherapies. Conclusions Our findings show the ability of lenvatinib to modulate tumor immunity in clinical samples of hepatocellular carcinoma.