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), Department of Oncology, Copenhagen University Hospital , Herlev, Denmark.

157 Citationer (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.

Originalsprog	Engelsk
Tidsskrift	OncoImmunology
Vol/bind	1
Udgave nummer	4
Sider (fra-til)	409-418
Antal sider	10
ISSN	2162-4011
DOI	https://doi.org/10.4161/onci.18851
Status	Udgivet - 2012

Adgang til dokumentet

10.4161/onci.18851

Citationsformater

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, bind 1, nr. 4, s. 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}",

year = "2012",

doi = "10.4161/onci.18851",

language = "English",

volume = "1",

pages = "409--418",

journal = "OncoImmunology",

issn = "2162-4011",

publisher = "Landes Bioscience",

number = "4",

}

TY - JOUR

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.

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

Adgang til dokumentet

Fingeraftryk

Citationsformater