T-cell receptor gene therapy for human papillomavirus-associated epithelial cancers: A first-in-human, phase I/II study

Stacey L. Doran; Sanja Stevanović; Sabina Adhikary; Jared J. Gartner; Li Jia; Mei Li M. Kwong; William C. Faquin; Stephen M. Hewitt; Richard M. Sherry; James C. Yang; Steven A. Rosenberg; Christian S. Hinrichs

doi:10.1200/JCO.18.02424

T-cell receptor gene therapy for human papillomavirus-associated epithelial cancers: A first-in-human, phase I/II study

Stacey L. Doran, Sanja Stevanović, Sabina Adhikary, Jared J. Gartner, Li Jia, Mei Li M. Kwong, William C. Faquin, Stephen M. Hewitt, Richard M. Sherry, James C. Yang, Steven A. Rosenberg, Christian S. Hinrichs

Research output: Contribution to journal › Article › peer-review

213 Scopus citations

Abstract

PURPOSE: Genetically engineered T-cell therapy is an emerging treatment of hematologic cancers with potential utility in epithelial cancers. We investigated T-cell therapy for the treatment of metastatic human papillomavirus (HPV)-associated epithelial cancers. METHODS: This phase I/II, single-center trial enrolled patients with metastatic HPV16-positive cancer from any primary tumor site who had received prior platinum-based therapy. Treatment consisted of autologous genetically engineered T cells expressing a T-cell receptor directed against HPV16 E6 (E6 T-cell receptor T cells), a conditioning regimen, and systemic aldesleukin. RESULTS: Twelve patients were treated in the study. No dose-limiting toxicities were observed in the phase I portion. Two patients, both in the highest-dose cohort, experienced objective tumor responses. A patient with three lung metastases experienced complete regression of one tumor and partial regression of two tumors, which were subsequently resected; she has no evidence of disease 3 years after treatment. All patients demonstrated high levels of peripheral blood engraftment with E6 T-cell receptor T cells 1 month after treatment (median, 30%; range, 4% to 53%). One patient's resistant tumor demonstrated a frameshift deletion in interferon gamma receptor 1, which mediates response to interferon gamma, an essential molecule for T-cell-mediated antitumor activity. Another patient's resistant tumor demonstrated loss of HLA-A*02:01, the antigen presentation molecule required for this therapy. A tumor from a patient who responded to treatment did not demonstrate genetic defects in interferon gamma response or antigen presentation. CONCLUSION: Engineered T cells can induce regression of epithelial cancer. Tumor resistance was observed in the context of T-cell programmed death-1 expression and defects in interferon gamma and antigen presentation pathway components. These findings have important implications for development of cellular therapy in epithelial cancers.

Original language	English (US)
Pages (from-to)	2759-2768
Number of pages	10
Journal	Journal of Clinical Oncology
Volume	37
Issue number	30
DOIs	https://doi.org/10.1200/JCO.18.02424
State	Published - 2019
Externally published	Yes

All Science Journal Classification (ASJC) codes

Oncology
Cancer Research

Access to Document

10.1200/JCO.18.02424

Cite this

Doran, S. L., Stevanović, S., Adhikary, S., Gartner, J. J., Jia, L., Kwong, M. L. M., Faquin, W. C., Hewitt, S. M., Sherry, R. M., Yang, J. C., Rosenberg, S. A., & Hinrichs, C. S. (2019). T-cell receptor gene therapy for human papillomavirus-associated epithelial cancers: A first-in-human, phase I/II study. Journal of Clinical Oncology, 37(30), 2759-2768. https://doi.org/10.1200/JCO.18.02424

@article{8671e6b156c84109ac873d13aade0843,

title = "T-cell receptor gene therapy for human papillomavirus-associated epithelial cancers: A first-in-human, phase I/II study",

abstract = "PURPOSE: Genetically engineered T-cell therapy is an emerging treatment of hematologic cancers with potential utility in epithelial cancers. We investigated T-cell therapy for the treatment of metastatic human papillomavirus (HPV)-associated epithelial cancers. METHODS: This phase I/II, single-center trial enrolled patients with metastatic HPV16-positive cancer from any primary tumor site who had received prior platinum-based therapy. Treatment consisted of autologous genetically engineered T cells expressing a T-cell receptor directed against HPV16 E6 (E6 T-cell receptor T cells), a conditioning regimen, and systemic aldesleukin. RESULTS: Twelve patients were treated in the study. No dose-limiting toxicities were observed in the phase I portion. Two patients, both in the highest-dose cohort, experienced objective tumor responses. A patient with three lung metastases experienced complete regression of one tumor and partial regression of two tumors, which were subsequently resected; she has no evidence of disease 3 years after treatment. All patients demonstrated high levels of peripheral blood engraftment with E6 T-cell receptor T cells 1 month after treatment (median, 30%; range, 4% to 53%). One patient's resistant tumor demonstrated a frameshift deletion in interferon gamma receptor 1, which mediates response to interferon gamma, an essential molecule for T-cell-mediated antitumor activity. Another patient's resistant tumor demonstrated loss of HLA-A*02:01, the antigen presentation molecule required for this therapy. A tumor from a patient who responded to treatment did not demonstrate genetic defects in interferon gamma response or antigen presentation. CONCLUSION: Engineered T cells can induce regression of epithelial cancer. Tumor resistance was observed in the context of T-cell programmed death-1 expression and defects in interferon gamma and antigen presentation pathway components. These findings have important implications for development of cellular therapy in epithelial cancers.",

author = "Doran, {Stacey L.} and Sanja Stevanovi{\'c} and Sabina Adhikary and Gartner, {Jared J.} and Li Jia and Kwong, {Mei Li M.} and Faquin, {William C.} and Hewitt, {Stephen M.} and Sherry, {Richard M.} and Yang, {James C.} and Rosenberg, {Steven A.} and Hinrichs, {Christian S.}",

note = "Publisher Copyright: {\textcopyright} 2019 by American Society of Clinical Oncology",

year = "2019",

doi = "10.1200/JCO.18.02424",

language = "English (US)",

volume = "37",

pages = "2759--2768",

journal = "Journal of Clinical Oncology",

issn = "0732-183X",

publisher = "Lippincott Williams and Wilkins",

number = "30",

}

Doran, SL, Stevanović, S, Adhikary, S, Gartner, JJ, Jia, L, Kwong, MLM, Faquin, WC, Hewitt, SM, Sherry, RM, Yang, JC, Rosenberg, SA & Hinrichs, CS 2019, 'T-cell receptor gene therapy for human papillomavirus-associated epithelial cancers: A first-in-human, phase I/II study', Journal of Clinical Oncology, vol. 37, no. 30, pp. 2759-2768. https://doi.org/10.1200/JCO.18.02424

TY - JOUR

T1 - T-cell receptor gene therapy for human papillomavirus-associated epithelial cancers

T2 - A first-in-human, phase I/II study

AU - Doran, Stacey L.

AU - Stevanović, Sanja

AU - Adhikary, Sabina

AU - Gartner, Jared J.

AU - Jia, Li

AU - Kwong, Mei Li M.

AU - Faquin, William C.

AU - Hewitt, Stephen M.

AU - Sherry, Richard M.

AU - Yang, James C.

AU - Rosenberg, Steven A.

AU - Hinrichs, Christian S.

PY - 2019

Y1 - 2019

N2 - PURPOSE: Genetically engineered T-cell therapy is an emerging treatment of hematologic cancers with potential utility in epithelial cancers. We investigated T-cell therapy for the treatment of metastatic human papillomavirus (HPV)-associated epithelial cancers. METHODS: This phase I/II, single-center trial enrolled patients with metastatic HPV16-positive cancer from any primary tumor site who had received prior platinum-based therapy. Treatment consisted of autologous genetically engineered T cells expressing a T-cell receptor directed against HPV16 E6 (E6 T-cell receptor T cells), a conditioning regimen, and systemic aldesleukin. RESULTS: Twelve patients were treated in the study. No dose-limiting toxicities were observed in the phase I portion. Two patients, both in the highest-dose cohort, experienced objective tumor responses. A patient with three lung metastases experienced complete regression of one tumor and partial regression of two tumors, which were subsequently resected; she has no evidence of disease 3 years after treatment. All patients demonstrated high levels of peripheral blood engraftment with E6 T-cell receptor T cells 1 month after treatment (median, 30%; range, 4% to 53%). One patient's resistant tumor demonstrated a frameshift deletion in interferon gamma receptor 1, which mediates response to interferon gamma, an essential molecule for T-cell-mediated antitumor activity. Another patient's resistant tumor demonstrated loss of HLA-A*02:01, the antigen presentation molecule required for this therapy. A tumor from a patient who responded to treatment did not demonstrate genetic defects in interferon gamma response or antigen presentation. CONCLUSION: Engineered T cells can induce regression of epithelial cancer. Tumor resistance was observed in the context of T-cell programmed death-1 expression and defects in interferon gamma and antigen presentation pathway components. These findings have important implications for development of cellular therapy in epithelial cancers.

AB - PURPOSE: Genetically engineered T-cell therapy is an emerging treatment of hematologic cancers with potential utility in epithelial cancers. We investigated T-cell therapy for the treatment of metastatic human papillomavirus (HPV)-associated epithelial cancers. METHODS: This phase I/II, single-center trial enrolled patients with metastatic HPV16-positive cancer from any primary tumor site who had received prior platinum-based therapy. Treatment consisted of autologous genetically engineered T cells expressing a T-cell receptor directed against HPV16 E6 (E6 T-cell receptor T cells), a conditioning regimen, and systemic aldesleukin. RESULTS: Twelve patients were treated in the study. No dose-limiting toxicities were observed in the phase I portion. Two patients, both in the highest-dose cohort, experienced objective tumor responses. A patient with three lung metastases experienced complete regression of one tumor and partial regression of two tumors, which were subsequently resected; she has no evidence of disease 3 years after treatment. All patients demonstrated high levels of peripheral blood engraftment with E6 T-cell receptor T cells 1 month after treatment (median, 30%; range, 4% to 53%). One patient's resistant tumor demonstrated a frameshift deletion in interferon gamma receptor 1, which mediates response to interferon gamma, an essential molecule for T-cell-mediated antitumor activity. Another patient's resistant tumor demonstrated loss of HLA-A*02:01, the antigen presentation molecule required for this therapy. A tumor from a patient who responded to treatment did not demonstrate genetic defects in interferon gamma response or antigen presentation. CONCLUSION: Engineered T cells can induce regression of epithelial cancer. Tumor resistance was observed in the context of T-cell programmed death-1 expression and defects in interferon gamma and antigen presentation pathway components. These findings have important implications for development of cellular therapy in epithelial cancers.

UR - http://www.scopus.com/inward/record.url?scp=85073182819&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85073182819&partnerID=8YFLogxK

U2 - 10.1200/JCO.18.02424

DO - 10.1200/JCO.18.02424

M3 - Article

C2 - 31408414

AN - SCOPUS:85073182819

SN - 0732-183X

VL - 37

SP - 2759

EP - 2768

JO - Journal of Clinical Oncology

JF - Journal of Clinical Oncology

IS - 30

ER -

T-cell receptor gene therapy for human papillomavirus-associated epithelial cancers: A first-in-human, phase I/II study

Abstract

All Science Journal Classification (ASJC) codes

Access to Document

Other files and links

Fingerprint

Cite this