Immunological alterations after immunotherapy with short lived HBV-TCR T cells associates with long-term treatment response in HBV-HCC

Anthony Tanoto Tan; Fanping Meng; Jiehua Jin; Ji-Yuan Zhang; Si-Yu Wang; Lei Shi; Ming Shi; Yuanyuan Li; Yunbo Xie; Li-Min Liu; Chun-Bao Zhou; Alicia Chua; Zi Zong Ho; Junqing Luan; Jinfang Zhao; Jing Li; Lu-En Wai; Sarene Koh; Tingting Wang; Antonio Bertoletti; Fu-Sheng Wang

doi:10.1002/hep4.1857

Immunological alterations after immunotherapy with short lived HBV-TCR T cells associates with long-term treatment response in HBV-HCC

Hepatol Commun. 2022 Apr;6(4):841-854. doi: 10.1002/hep4.1857. Epub 2021 Dec 21.

Authors

Anthony Tanoto Tan^#¹, Fanping Meng^#^{2

3}, Jiehua Jin^#², Ji-Yuan Zhang^{2

3}, Si-Yu Wang², Lei Shi², Ming Shi^{2

3}, Yuanyuan Li², Yunbo Xie², Li-Min Liu², Chun-Bao Zhou², Alicia Chua⁴, Zi Zong Ho⁴, Junqing Luan², Jinfang Zhao², Jing Li², Lu-En Wai^{4

5}, Sarene Koh^{4

5}, Tingting Wang⁴, Antonio Bertoletti^{1

5}, Fu-Sheng Wang^{2

3}

Affiliations

¹ Emerging Infectious Diseases, Duke-NUS Medical School, Singapore.
² Treatment and Research Center for Infectious Diseases, The Fifth Medical Center of PLA General Hospital, Beijing, China.
³ National Clinical Research Center, The Fifth Medical Center of PLA General Hospital, Beijing, China.
⁴ Lion TCR Pte Ltd., Singapore.
⁵ Singapore Immunology Network, Agency for Science and Technology (A*STAR), Singapore.

^# Contributed equally.

Abstract

The application of hepatitis B virus (HBV)-T-cell receptor (TCR) T-cell immunotherapy in patients with HBV-related hepatocellular carcinoma (HBV-HCC) has been apathetic, as the expression of HBV antigens by both normal HBV-infected hepatocytes and HCC cells with HBV-DNA integration increases the risk of on-target off-tumor severe liver inflammatory events. To increase the safety of this immunotherapeutic approach, we developed messenger RNA (mRNA) HBV-TCR-redirected T cells that-due to the transient nature of mRNA-are functionally short lived and can be infused in escalating doses. The safety of this approach and its clinical potential against primary HBV-HCC have never been analyzed in human trials; thus, we studied the clinical and immunological parameters of 8 patients with chronic HBV infection and diffuse nonoperable HBV-HCC treated at weekly intervals with escalating doses (1 × 10⁴ , 1 × 10⁵ , 1 × 10⁶ , and 5 × 10⁶ TCR+ T cells/kg body weight) of T cells modified with HBV-TCR encoding mRNA. The treatment was well tolerated with no severe systemic inflammatory events, cytokine storm, or neurotoxicity observed in any of these patients throughout treatment. Instead, we observed a destruction of the tumor lesion or a prolonged stable disease in 3 of 8 patients. Importantly, the patients without clinically relevant reductions of HCC did not display any detectable peripheral blood immunological alterations. In contrast, signs of transient localized liver inflammation, activation of the T-cell compartment, and/or elevations of serum chemokine (C-X-C motif) ligand (CXCL) 9 and CXCL10 levels were detected in patients with long-term clinical benefit. Conclusion: We show that despite the reduced in vivo half-life (3-4 days), adoptive transfer of mRNA HBV-TCR T cells into patients with HBV-HCC show long-term clinical benefit that was associated with transient immunological alterations.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Carcinoma, Hepatocellular* / therapy
Hepatitis B virus / genetics
Humans
Immunotherapy
Liver Neoplasms* / therapy
RNA, Messenger
Receptors, Antigen, T-Cell / genetics
T-Lymphocytes

Substances

RNA, Messenger
Receptors, Antigen, T-Cell