T cell receptor grafting allows virological control of hepatitis B virus infection
Karin Wisskirchen, Janine Kah, Antje Malo, Theresa Asen, Tassilo Volz, Lena Allweiss, Jochen M. Wettengel, Marc Lütgehetmann, Stephan Urban, Tanja Bauer, Maura Dandri, Ulrike Protzer
Karin Wisskirchen, Janine Kah, Antje Malo, Theresa Asen, Tassilo Volz, Lena Allweiss, Jochen M. Wettengel, Marc Lütgehetmann, Stephan Urban, Tanja Bauer, Maura Dandri, Ulrike Protzer
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Research Article Immunology Virology

T cell receptor grafting allows virological control of hepatitis B virus infection

Abstract

T cell therapy is a promising means to treat chronic hepatitis B virus (HBV) infection and HBV-associated hepatocellular carcinoma. T cells engineered to express an HBV-specific T cell receptor (TCR) may cure an HBV infection upon adoptive transfer. We investigated the therapeutic potential and safety of T cells stably expressing high-affinity HBV envelope– or core–specific TCRs recognizing European and Asian HLA-A2 subtypes. Both CD8+ and CD4+ T cells from healthy donors and patients with chronic hepatitis B became polyfunctional effector cells when grafted with HBV-specific TCRs and eliminated HBV from infected HepG2-NTCP cell cultures. A single transfer of TCR-grafted T cells into HBV-infected, humanized mice controlled HBV infection, and virological markers declined by 4 to 5 log or below the detection limit. Engineered T cells specifically cleared infected hepatocytes without damaging noninfected cells when, as in a typical clinical setting, only a minority of hepatocytes were infected. Cell death was compensated by hepatocyte proliferation, and alanine amino transferase levels peaking between days 5 and 7 normalized again thereafter. Cotreatment with the entry inhibitor myrcludex B ensured long-term control of HBV infection. Thus, T cells stably transduced with highly functional TCRs have the potential to mediate clearance of HBV-infected cells, causing limited liver injury.

Authors

Karin Wisskirchen, Janine Kah, Antje Malo, Theresa Asen, Tassilo Volz, Lena Allweiss, Jochen M. Wettengel, Marc Lütgehetmann, Stephan Urban, Tanja Bauer, Maura Dandri, Ulrike Protzer

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Figure 3

Antiviral activity of T cells from patients with CHB.

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Antiviral activity of T cells from patients with CHB. (A) CD3+ T cells ...
(A) CD3+ T cells from 2 donors with CHB were isolated and transduced to express the HBV-specific TCRs 4GS20 (blue) and 6KC18 (red). TCR expression was quantified by flow cytometry. (B) Expansion of T cells during retroviral transduction with CD3/CD28 T activator Dynabeads and IL-2. (CF) HepG2-NTCP cells were infected with HBV at a MOI of 500 three weeks prior to coculture with TCR-grafted T cells from donors with CHB at an E/T ratio of 1:2. Since the ratio of CD4+ and CD8+ T cells varied substantially between the donors, effector cell numbers were calculated on the basis of TCR+ CD8+ T cells only. (C) Killing of target cells was measured using a real-time cell analyzer and is given as the normalized cell index relative to the starting point of the coculture. E/T of 1:2.7. (D) IFN-γ was determined in cell culture medium on day 2. Secreted HBeAg (E) and intracellular HBV cccDNA (F) levels were measured after 10 days of coculture. Data are presented as mean values of triplicate cocultures (n = 3).