4.7 Article

Therapeutic Vaccines against Hepatocellular Carcinoma in the Immune Checkpoint Inhibitor Era: Time for Neoantigens?

Journal

Publisher

MDPI
DOI: 10.3390/ijms23042022

Keywords

hepatocellular carcinoma; immunotherapy; vaccines; neoantigens; immune checkpoint inhibitors

Funding

  1. ERANET-TRANSCAN-2 within HORIZON 2020 [TRS 201600000383]
  2. Instituto de Salud Carlos III
  3. Fondo Europeo de Desarrollo Regional Una manera de hacer Europa [PI20/00260]
  4. Murchante contra el cancer initiative
  5. Gobierno de Navarra (Dpto de Salud) [054-2021]
  6. FEDER [0011-1411-2020-000011, 0011-1411-2020-000010]
  7. Instituto de Salud Carlos III [PI18/00556]
  8. FEDER funds Una manera de hacer Europa
  9. Gobierno de Navarra Dpto
  10. de Salud [045-2017]
  11. FEDER funds, UE
  12. FEDER 2014-2020 Una manera de hacer Europa
  13. Dpto. de Industria Ayudas a Centros Tecnologicos y Organismos de Investigacion [GN2020 PC196-197]

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Immune checkpoint inhibitors (ICI) show promising results but still have limitations in hepatocellular carcinoma (HCC) immunotherapy. Understanding immune elements in the tumor microenvironment may help personalize therapies and improve non-responder patients. Vaccination and boosting responses against tumor-specific antigens may complement ICI treatment in certain HCC cases.
Immune checkpoint inhibitors (ICI) have been used as immunotherapy for hepatocellular carcinoma (HCC) with promising but still limited results. Identification of immune elements in the tumor microenvironment of individual HCC patients may help to understand the correlations of responses, as well as to design personalized therapies for non-responder patients. Immune-enhancing strategies, such as vaccination, would complement ICI in those individuals with poorly infiltrated tumors. The prominent role of responses against mutated tumor antigens (neoAgs) in ICI-based therapies suggests that boosting responses against these epitopes may specifically target tumor cells. In this review we summarize clinical vaccination trials carried out in HCC, the available information on potentially immunogenic neoAgs in HCC patients, and the most recent results of neoAg-based vaccines in other tumors. Despite the low/intermediate mutational burden observed in HCC, data obtained from neoAg-based vaccines in other tumors indicate that vaccines directed against these tumor-specific antigens would complement ICI in a subset of HCC patients.

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