NY-ESO-1-specific redirected T cells with endogenous TCR knockdown mediate tumor response and cytokine release syndrome

Mikiya Ishihara; Shigehisa Kitano; Shinichi Kageyama; Yoshihiro Miyahara; Noboru Yamamoto; Hidefumi Kato; Hideyuki Mishima; Hiroyoshi Hattori; Takeru Funakoshi; Takashi Kojima; Tetsuro Sasada; Eiichi Sato; Sachiko Okamoto; Daisuke Tomura; Ikuei Nukaya; Hideto Chono; Junichi Mineno; Muhammad Faris Kairi; Phuong Diem Hoang Nguyen; Yannick Simoni; Alessandra Nardin; Evan Newell; Michael Fehlings; Hiroaki Ikeda; Takashi Watanabe; Hiroshi Shiku

doi:10.1136/jitc-2021-003811

NY-ESO-1-specific redirected T cells with endogenous TCR knockdown mediate tumor response and cytokine release syndrome

J Immunother Cancer. 2022 Jun;10(6):e003811. doi: 10.1136/jitc-2021-003811.

Authors

Mikiya Ishihara¹, Shigehisa Kitano^{2

3}, Shinichi Kageyama⁴, Yoshihiro Miyahara⁵, Noboru Yamamoto³, Hidefumi Kato⁶, Hideyuki Mishima⁷, Hiroyoshi Hattori⁸, Takeru Funakoshi⁹, Takashi Kojima¹⁰, Tetsuro Sasada¹¹, Eiichi Sato¹², Sachiko Okamoto¹³, Daisuke Tomura¹³, Ikuei Nukaya¹³, Hideto Chono¹³, Junichi Mineno¹³, Muhammad Faris Kairi¹⁴, Phuong Diem Hoang Nguyen¹⁴, Yannick Simoni¹⁴, Alessandra Nardin¹⁴, Evan Newell¹⁴, Michael Fehlings¹⁴, Hiroaki Ikeda¹⁵, Takashi Watanabe⁵, Hiroshi Shiku⁵

Affiliations

¹ Cancer Center, Mie University Hospital, Tsu, Japan.
² Division of Cancer Immunotherapy Development, Advanced Medical Development Center, The Cancer Institute Hospital of Japanese Foundation for Cancer Research, Tokyo, Japan.
³ Department of Experimental Therapeutics, National Cancer Institue Hospital, Tokyo, Japan.
⁴ Departments of Immuno-Gene Therapy and Personalized Cancer Immunotherapy, Mie University Graduate School of Medicine, Tsu, Japan kageyama@med.mie-u.ac.jp.
⁵ Departments of Immuno-Gene Therapy and Personalized Cancer Immunotherapy, Mie University Graduate School of Medicine, Tsu, Japan.
⁶ Department of Transfusion Medicine, Aichi Medical University, Nagakute, Japan.
⁷ Cancer Center, Aichi Medical University, Nagakute, Japan.
⁸ Laboratory of Advanced Therapy, Clinical Research Center, National Hospital Organization Nagoya Medical Center, Nagoya, Japan.
⁹ Department of Dermatology, Keio University School of Medicine, Tokyo, Japan.
¹⁰ Department of Gastroenterology and Gastrointestinal Oncology, National Cancer Center Hospital East, Kashiwa, Japan.
¹¹ Division of Cancer Immunotherapy, Kanagawa Cancer Center Research Institute, Yokohama, Japan.
¹² Institute of Medical Science, Tokyo Medical University, Tokyo, Japan.
¹³ Takara Bio Inc, Kusatsu, Japan.
¹⁴ ImmunoScape Pte. Ltd, Singapore.
¹⁵ Department of Oncology, Nagasaki University Graduate School of Biomedical Sciences, Nagasaki, Japan.

Abstract

Background: Because of the shortage of ideal cell surface antigens, the development of T-cell receptor (TCR)-engineered T cells (TCR-T) that target intracellular antigens such as NY-ESO-1 is a promising approach for treating patients with solid tumors. However, endogenous TCRs in vector-transduced T cells have been suggested to impair cell-surface expression of transduced TCR while generating mispaired TCRs that can become self-reactive.

Methods: We conducted a first-in-human phase I clinical trial with the TCR-transduced T-cell product (TBI-1301) in patients with NY-ESO-1-expressing solid tumors. In manufacturing TCR-T cells, we used a novel affinity-enhanced NY-ESO-1-specific TCR that was transduced by a retroviral vector that enables siRNA (small interfering RNA)-mediated silencing of endogenous TCR. The patients were divided into two cohorts. Cohort 1 was given a dose of 5×10⁸ cells (whole cells including TCR-T cells) preconditioned with 1500 mg/m² cyclophosphamide. Cohort 2 was given 5× 10⁹ cells preconditioned with 1500 mg/m² cyclophosphamide.

Results: In vitro study showed that both the CD8⁺ and CD4⁺ T fractions of TCR-T cells exhibited cytotoxic effects against NY-ESO-1-expressing tumor cells. Three patients and six patients were allocated to cohort 1 and cohort 2, respectively. Three of the six patients who received 5×10⁹ cells showed tumor response, while three patients developed early-onset cytokine release syndrome (CRS). One of the patients developed a grade 3 lung injury associated with the infiltration of the TCR-T cells. No siRNA-related adverse events other than CRS were observed. Cytokines including interleukin 6 I and monocyte chemotactic protein-1/chemokine (C-C motif) ligand (CCL2)increased in the sera of patients with CRS. In vitro analysis showed these cytokines were not secreted from the T cells infused. A significant fraction of the manufactured T cells in patients with CRS was found to express either CD244, CD39, or both at high levels.

Conclusions: The trial showed that endogenous TCR-silenced and affinity-enhanced NY-ESO-1 TCR-T cells were safely administered except for grade 3 lung injury. The TCR-T cell infusion exhibited significant tumor response and early-onset CRS in patients with tumors that express NY-ESO-1 at high levels. The differentiation properties of the manufactured T cells may be prognostic for TCR-T-related CRS.

Trial registration number: NCT02366546.

Keywords: cell engineering; clinical trials as topic; cytokines; immunotherapy, adoptive.

Publication types

Clinical Trial, Phase I

MeSH terms

Antigens, Neoplasm
Cyclophosphamide
Cytokine Release Syndrome* / therapy
Cytokines / metabolism
Humans
Immunotherapy*
Membrane Proteins
Neoplasms* / immunology
Neoplasms* / therapy
Receptors, Antigen, T-Cell* / genetics
T-Lymphocytes* / immunology

Substances

Antigens, Neoplasm
CTAG1B protein, human
Cytokines
Membrane Proteins
Receptors, Antigen, T-Cell
Cyclophosphamide

Associated data

ClinicalTrials.gov/NCT02366546