| Literature DB >> 25308176 |
Waseem Qasim1, Maurizia Brunetto2, Adam J Gehring3, Shao-An Xue4, Anna Schurich4, Atefeh Khakpoor5, Hong Zhan1, Pietro Ciccorossi2, Kimberly Gilmour1, Daniela Cavallone2, Francesco Moriconi2, Farzin Farzhenah6, Alessandro Mazzoni2, Lucas Chan6, Emma Morris4, Adrian Thrasher1, Mala K Maini4, Ferruccio Bonino7, Hans Stauss4, Antonio Bertoletti8.
Abstract
HBV-DNA integration frequently occurs in HBV-related hepatocellular carcinoma (HCC), but whether HBV antigens are expressed in HCC cells and can be targeted by immune therapeutic strategies remains controversial. Here, we first characterized HBV antigen expression in HCC metastases, occurring in a patient who had undergone liver transplantation for HBV-related HCC. We then deployed for the first time in HCC autologous T cells, genetically modified to express an HBsAg specific T cell receptor, as therapy against chemoresistant extrahepatic metastases. We confirmed that HBV antigens were expressed in HCC metastases (but not in the donor liver) and demonstrated that tumour cells were recognized in vivo by lymphocytes, engineered to express an HBV-specific T cell receptor (TCR). Gene-modified T cells survived, expanded and mediated a reduction in HBsAg levels without exacerbation of liver inflammation or other toxicity. Whilst clinical efficacy was not established in this subject with end-stage metastatic disease, we confirm the feasibility of providing autologous TCR-redirected therapy against HCC and advocate this strategy as a novel therapeutic opportunity in hepatitis B-associated malignancies.Entities:
Keywords: HBV-specific CD8 T cells; Liver cancer; T cell therapy
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Year: 2014 PMID: 25308176 DOI: 10.1016/j.jhep.2014.10.001
Source DB: PubMed Journal: J Hepatol ISSN: 0168-8278 Impact factor: 25.083