TIL therapy broadens the tumor-reactive CD8(+) T cell compartment in melanoma patients

Pia Kvistborg; Chengyi Jenny Shu; Bianca Heemskerk; Manuel Fankhauser; Charlotte Albæk Thrue; Mireille Toebes; Nienke van Rooij; Carsten Linnemann; Marit M van Buuren; Jos H M Urbanus; Joost B Beltman; Per thor Straten; Yong F Li; Paul F Robbins; Michal J Besser; Jacob Schachter; Gemma G Kenter; Mark E Dudley; Steven A Rosenberg; John B A G Haanen; Sine Reker Hadrup; Ton N M Schumacher

doi:10.4161/onci.18851

TIL therapy broadens the tumor-reactive CD8(+) T cell compartment in melanoma patients

Pia Kvistborg, Chengyi Jenny Shu, Bianca Heemskerk, Manuel Fankhauser, Charlotte Albæk Thrue, Mireille Toebes, Nienke van Rooij, Carsten Linnemann, Marit M van Buuren, Jos H M Urbanus, Joost B Beltman, Per thor Straten , Yong F Li, Paul F Robbins, Michal J Besser, Jacob Schachter, Gemma G Kenter, Mark E Dudley, Steven A Rosenberg, John B A G HaanenSine Reker Hadrup, Ton N M Schumacher

Center for Cancer Immune Therapy (CCIT)

162 Citations (Scopus)

Abstract

There is strong evidence that both adoptive T cell transfer and T cell checkpoint blockade can lead to regression of human melanoma. However, little data are available on the effect of these cancer therapies on the tumor-reactive T cell compartment. To address this issue we have profiled therapy-induced T cell reactivity against a panel of 145 melanoma-associated CD8(+) T cell epitopes. Using this approach, we demonstrate that individual tumor-infiltrating lymphocyte cell products from melanoma patients contain unique patterns of reactivity against shared melanoma-associated antigens, and that the combined magnitude of these responses is surprisingly low. Importantly, TIL therapy increases the breadth of the tumor-reactive T cell compartment in vivo, and T cell reactivity observed post-therapy can almost in full be explained by the reactivity observed within the matched cell product. These results establish the value of high-throughput monitoring for the analysis of immuno-active therapeutics and suggest that the clinical efficacy of TIL therapy can be enhanced by the preparation of more defined tumor-reactive T cell products.

Original language	English
Journal	OncoImmunology
Volume	1
Issue number	4
Pages (from-to)	409-418
Number of pages	10
ISSN	2162-4011
DOIs	https://doi.org/10.4161/onci.18851
Publication status	Published - 2012

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Kvistborg, P., Shu, C. J., Heemskerk, B., Fankhauser, M., Thrue, C. A., Toebes, M., van Rooij, N., Linnemann, C., van Buuren, M. M., Urbanus, J. H. M., Beltman, J. B., thor Straten , P., Li, Y. F., Robbins, P. F., Besser, M. J., Schachter, J., Kenter, G. G., Dudley, M. E., Rosenberg, S. A., ... Schumacher, T. N. M. (2012). TIL therapy broadens the tumor-reactive CD8(+) T cell compartment in melanoma patients. OncoImmunology, 1(4), 409-418. https://doi.org/10.4161/onci.18851

Kvistborg, P, Shu, CJ, Heemskerk, B, Fankhauser, M, Thrue, CA, Toebes, M, van Rooij, N, Linnemann, C, van Buuren, MM, Urbanus, JHM, Beltman, JB, thor Straten , P, Li, YF, Robbins, PF, Besser, MJ, Schachter, J, Kenter, GG, Dudley, ME, Rosenberg, SA, Haanen, JBAG, Hadrup, SR & Schumacher, TNM 2012, 'TIL therapy broadens the tumor-reactive CD8(+) T cell compartment in melanoma patients', OncoImmunology, vol. 1, no. 4, pp. 409-418. https://doi.org/10.4161/onci.18851

@article{c74aee5ae43d43998d6c0d8b1b6784f0,

title = "TIL therapy broadens the tumor-reactive CD8(+) T cell compartment in melanoma patients",

abstract = "There is strong evidence that both adoptive T cell transfer and T cell checkpoint blockade can lead to regression of human melanoma. However, little data are available on the effect of these cancer therapies on the tumor-reactive T cell compartment. To address this issue we have profiled therapy-induced T cell reactivity against a panel of 145 melanoma-associated CD8(+) T cell epitopes. Using this approach, we demonstrate that individual tumor-infiltrating lymphocyte cell products from melanoma patients contain unique patterns of reactivity against shared melanoma-associated antigens, and that the combined magnitude of these responses is surprisingly low. Importantly, TIL therapy increases the breadth of the tumor-reactive T cell compartment in vivo, and T cell reactivity observed post-therapy can almost in full be explained by the reactivity observed within the matched cell product. These results establish the value of high-throughput monitoring for the analysis of immuno-active therapeutics and suggest that the clinical efficacy of TIL therapy can be enhanced by the preparation of more defined tumor-reactive T cell products.",

author = "Pia Kvistborg and Shu, \{Chengyi Jenny\} and Bianca Heemskerk and Manuel Fankhauser and Thrue, \{Charlotte Alb{\ae}k\} and Mireille Toebes and \{van Rooij\}, Nienke and Carsten Linnemann and \{van Buuren\}, \{Marit M\} and Urbanus, \{Jos H M\} and Beltman, \{Joost B\} and \{thor Straten\}, Per and Li, \{Yong F\} and Robbins, \{Paul F\} and Besser, \{Michal J\} and Jacob Schachter and Kenter, \{Gemma G\} and Dudley, \{Mark E\} and Rosenberg, \{Steven A\} and Haanen, \{John B A G\} and Hadrup, \{Sine Reker\} and Schumacher, \{Ton N M\}",

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doi = "10.4161/onci.18851",

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T1 - TIL therapy broadens the tumor-reactive CD8(+) T cell compartment in melanoma patients

AU - Kvistborg, Pia

AU - Shu, Chengyi Jenny

AU - Heemskerk, Bianca

AU - Fankhauser, Manuel

AU - Thrue, Charlotte Albæk

AU - Toebes, Mireille

AU - van Rooij, Nienke

AU - Linnemann, Carsten

AU - van Buuren, Marit M

AU - Urbanus, Jos H M

AU - Beltman, Joost B

AU - thor Straten , Per

AU - Li, Yong F

AU - Robbins, Paul F

AU - Besser, Michal J

AU - Schachter, Jacob

AU - Kenter, Gemma G

AU - Dudley, Mark E

AU - Rosenberg, Steven A

AU - Haanen, John B A G

AU - Hadrup, Sine Reker

AU - Schumacher, Ton N M

PY - 2012

Y1 - 2012

N2 - There is strong evidence that both adoptive T cell transfer and T cell checkpoint blockade can lead to regression of human melanoma. However, little data are available on the effect of these cancer therapies on the tumor-reactive T cell compartment. To address this issue we have profiled therapy-induced T cell reactivity against a panel of 145 melanoma-associated CD8(+) T cell epitopes. Using this approach, we demonstrate that individual tumor-infiltrating lymphocyte cell products from melanoma patients contain unique patterns of reactivity against shared melanoma-associated antigens, and that the combined magnitude of these responses is surprisingly low. Importantly, TIL therapy increases the breadth of the tumor-reactive T cell compartment in vivo, and T cell reactivity observed post-therapy can almost in full be explained by the reactivity observed within the matched cell product. These results establish the value of high-throughput monitoring for the analysis of immuno-active therapeutics and suggest that the clinical efficacy of TIL therapy can be enhanced by the preparation of more defined tumor-reactive T cell products.

AB - There is strong evidence that both adoptive T cell transfer and T cell checkpoint blockade can lead to regression of human melanoma. However, little data are available on the effect of these cancer therapies on the tumor-reactive T cell compartment. To address this issue we have profiled therapy-induced T cell reactivity against a panel of 145 melanoma-associated CD8(+) T cell epitopes. Using this approach, we demonstrate that individual tumor-infiltrating lymphocyte cell products from melanoma patients contain unique patterns of reactivity against shared melanoma-associated antigens, and that the combined magnitude of these responses is surprisingly low. Importantly, TIL therapy increases the breadth of the tumor-reactive T cell compartment in vivo, and T cell reactivity observed post-therapy can almost in full be explained by the reactivity observed within the matched cell product. These results establish the value of high-throughput monitoring for the analysis of immuno-active therapeutics and suggest that the clinical efficacy of TIL therapy can be enhanced by the preparation of more defined tumor-reactive T cell products.

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U2 - 10.4161/onci.18851

DO - 10.4161/onci.18851

M3 - Journal article

C2 - 22754759

SN - 2162-4011

VL - 1

SP - 409

EP - 418

JO - OncoImmunology

JF - OncoImmunology

IS - 4

ER -

TIL therapy broadens the tumor-reactive CD8(+) T cell compartment in melanoma patients

Abstract

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