Treatment of Patients With Metastatic Cancer Using a Major Histocompatibility Complex Class II–Restricted T-Cell Receptor Targeting the Cancer Germline Antigen MAGE-A3

Yong‐Chen Lu; Linda L. Parker; Tangying Lu; Zhili Zheng; Mary Ann Toomey; Donald E. White; Xin Yao; Yong F. Li; Paul F. Robbins; Steven A. Feldman; Pierre van der Bruggen; Christopher A. Klebanoff; Stephanie L. Goff; Richard M. Sherry; Udai S. Kammula; James C. Yang; Steven A. Rosenberg

doi:10.1200/jco.2017.74.5463

Treatment of Patients With Metastatic Cancer Using a Major Histocompatibility Complex Class II–Restricted T-Cell Receptor Targeting the Cancer Germline Antigen MAGE-A3

Yong‐Chen Lu(Bristol-Myers Squibb (Germany)), Linda L. Parker(Bristol-Myers Squibb (Germany)), Tangying Lu(Bristol-Myers Squibb (Germany)), Zhili Zheng(Bristol-Myers Squibb (Germany)), Mary Ann Toomey(Bristol-Myers Squibb (Germany)), Donald E. White(Bristol-Myers Squibb (Germany)), Xin Yao(Bristol-Myers Squibb (Germany)), Yong F. Li(Bristol-Myers Squibb (Germany)), Paul F. Robbins(Bristol-Myers Squibb (Germany)), Steven A. Feldman(Bristol-Myers Squibb (Germany)), Pierre van der Bruggen(Bristol-Myers Squibb (Germany)), Christopher A. Klebanoff(Bristol-Myers Squibb (Germany)), Stephanie L. Goff(Bristol-Myers Squibb (Germany)), Richard M. Sherry(Bristol-Myers Squibb (Germany)), Udai S. Kammula(Bristol-Myers Squibb (Germany)), James C. Yang(Bristol-Myers Squibb (Germany)), Steven A. Rosenberg(Bristol-Myers Squibb (Germany))

Journal of Clinical Oncology

August 15, 2017

10.1200/jco.2017.74.5463

Cited by 271Open Access

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Abstract

Purpose Adoptive transfer of genetically modified T cells is being explored as a treatment for patients with metastatic cancer. Most current strategies use genes that encode major histocompatibility complex (MHC) class I–restricted T-cell receptors (TCRs) or chimeric antigen receptors to genetically modify CD8 + T cells or bulk T cells for treatment. Here, we evaluated the safety and efficacy of an adoptive CD4 + T-cell therapy using an MHC class II–restricted, HLA-DPB1*0401–restricted TCR that recognized the cancer germline antigen, MAGE-A3 (melanoma-associated antigen-A3). Patients and Methods Patients received a lymphodepleting preparative regimen, followed by adoptive transfer of purified CD4 + T cells, retrovirally transduced with MAGE-A3 TCR plus systemic high-dose IL-2. A cell dose escalation was conducted, starting at 10 7 total cells and escalating at half-log increments to approximately 10 11 cells. Nine patients were treated at the highest dose level (0.78 to 1.23 × 10 11 cells). Results Seventeen patients were treated. During the cell dose-escalation phase, an objective complete response was observed in a patient with metastatic cervical cancer who received 2.7 × 10 9 cells (ongoing at ≥ 29 months). Among nine patients who were treated at the highest dose level, objective partial responses were observed in a patient with esophageal cancer (duration, 4 months), a patient with urothelial cancer (ongoing at ≥ 19 months), and a patient with osteosarcoma (duration, 4 months). Most patients experienced transient fevers and the expected hematologic toxicities from lymphodepletion pretreatment. Two patients experienced transient grade 3 and 4 transaminase elevations. There were no treatment-related deaths. Conclusion These results demonstrate the safety and efficacy of administering autologous CD4 + T cells that are genetically engineered to express an MHC class II–restricted antitumor TCR that targets MAGE-A3. This clinical trial extends the reach of TCR gene therapy for patients with metastatic cancer.

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