Molecular Therapy: Nucleic Acids (Jan 2013)

A Practical Approach to Immunotherapy of Hepatocellular Carcinoma Using T Cells Redirected Against Hepatitis B Virus

  • Sarene Koh,
  • Noriko Shimasaki,
  • Rossarin Suwanarusk,
  • Zi Zong Ho,
  • Adeline Chia,
  • Nasirah Banu,
  • Shanshan Wu Howland,
  • Alice Soh Meoy Ong,
  • Adam J Gehring,
  • Hans Stauss,
  • Laurent Renia,
  • Matti Sällberg,
  • Dario Campana,
  • Antonio Bertoletti

DOI
https://doi.org/10.1038/mtna.2013.43
Journal volume & issue
Vol. 2, no. C

Abstract

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Hepatocellular carcinoma (HCC) cells often have hepatitis B virus (HBV)-DNA integration and can be targeted by HBV-specific T cells. The use of viral vectors to introduce exogenous HBV-specific T-cell receptors (TCR) on T cells to redirect their specificity is complex and expensive to implement in clinical trials. Moreover, it raises safety concerns related to insertional mutagenesis and potential toxicity of long-lived HBV-specific T cells in patients with persistent infection. To develop a more practical and safer approach to cell therapy of HCC, we used electroporation of mRNA encoding anti-HBV TCR. Approximately 80% of CD8+ T cells expressed functional HBV TCR 24 hours postelectroporation, an expression efficiency much higher than that obtained by retroviral transduction (~18%). Antigen-specific cytokine production of electroporated T cells was efficient within 72-hour period, after which the redirected T cells lost their HBV-specific function. Despite this transient functionality, the TCR-electroporated T cells efficiently prevented tumor seeding and suppressed the growth of established tumors in a xenograft model of HCC. Finally, we established a method for large-scale TCR mRNA electroporation that yielded large numbers of highly functional clinical-grade anti-HBV T cells. This method represents a practical approach to cell therapy of HCC and its inherently self-limiting toxicity suggests potential for application in other HBV-related pathologies.

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