Chemotherapy and radiation therapy elicits tumor specific T cell responses in a breast cancer patient

David Bernal-Estévez; Ramiro Sánchez; Rafael E. Tejada; Carlos Parra-López

doi:10.1186/s12885-016-2625-2

Chemotherapy and radiation therapy elicits tumor specific T cell responses in a breast cancer patient

David Bernal-Estévez
, Ramiro Sánchez
, Rafael E. Tejada
, Carlos Parra-López

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

29 Scopus citations

Abstract

Background: Experimental evidence and clinical studies in breast cancer suggest that some anti-tumor therapy

regimens generate stimulation of the immune system that accounts for tumor clinical responses, however,

demonstration of the immunostimulatory power of these therapies on cancer patients continues to be a

formidable challenge. Here we present experimental evidence from a breast cancer patient with complete clinical

response after 7 years, associated with responsiveness of tumor specific T cells.

Methods: T cells were obtained before and after anti-tumor therapy from peripheral blood of a 63-years old

woman diagnosed with ductal breast cancer (HER2/neu+++, ER-, PR-, HLA-A*02:01) treated with surgery, followed

by paclitaxel, trastuzumab (suspended due to cardiac toxicity), and radiotherapy. We obtained a leukapheresis

before surgery and after 8 months of treatment. Using in vitro cell cultures stimulated with autologous monocytederived dendritic cells (DCs) that produce high levels of IL-12, we characterize by flow cytometry the phenotype of

tumor associated antigens (TAAs) HER2/neu and NY-ESO 1 specific T cells. The ex vivo analysis of the TCR-Vβ

repertoire of TAA specific T cells in blood and Tumor Infiltrating Lymphocytes (TILs) were performed in order to

correlate both repertoires prior and after therapy.

Results: We evidence a functional recovery of T cell responsiveness to polyclonal stimuli and expansion of TAAs

specific CD8+ T cells using peptide pulsed DCs, with an increase of CTLA-4 and memory effector phenotype after

anti-tumor therapy. The ex vivo analysis of the TCR-Vβ repertoire of TAA specific T cells in blood and TILs showed

that whereas the TCR-Vβ04-02 clonotype is highly expressed in TILs the HER2/neu specific T cells are expressed

mainly in blood after therapy, suggesting that this particular TCR was selectively enriched in blood after anti-tumor

therapy.

Conclusions: Our results show the benefits of anti-tumor therapy in a breast cancer patient with clinical complete

response in two ways, by restoring the responsiveness of T cells by increasing the frequency and activation in

peripheral blood of tumor specific T cells present in the tumor before therapy.

Original language	English
Article number	591
Pages (from-to)	1-13
Number of pages	13
Journal	BMC Cancer
Volume	16
Issue number	1
DOIs	https://doi.org/10.1186/s12885-016-2625-2
State	Published - 03 Aug 2016
Externally published	Yes

Keywords

Breast cancer
Chemotherapy
CTLA-4
HER2/neu
T cells
TCR repertoire
Type I alpha dendritic cells

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1186/s12885-016-2625-2

Cite this

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title = "Chemotherapy and radiation therapy elicits tumor specific T cell responses in a breast cancer patient",

abstract = "Background: Experimental evidence and clinical studies in breast cancer suggest that some anti-tumor therapyregimens generate stimulation of the immune system that accounts for tumor clinical responses, however,demonstration of the immunostimulatory power of these therapies on cancer patients continues to be aformidable challenge. Here we present experimental evidence from a breast cancer patient with complete clinicalresponse after 7 years, associated with responsiveness of tumor specific T cells.Methods: T cells were obtained before and after anti-tumor therapy from peripheral blood of a 63-years oldwoman diagnosed with ductal breast cancer (HER2/neu+++, ER-, PR-, HLA-A*02:01) treated with surgery, followedby paclitaxel, trastuzumab (suspended due to cardiac toxicity), and radiotherapy. We obtained a leukapheresisbefore surgery and after 8 months of treatment. Using in vitro cell cultures stimulated with autologous monocytederived dendritic cells (DCs) that produce high levels of IL-12, we characterize by flow cytometry the phenotype oftumor associated antigens (TAAs) HER2/neu and NY-ESO 1 specific T cells. The ex vivo analysis of the TCR-Vβrepertoire of TAA specific T cells in blood and Tumor Infiltrating Lymphocytes (TILs) were performed in order tocorrelate both repertoires prior and after therapy.Results: We evidence a functional recovery of T cell responsiveness to polyclonal stimuli and expansion of TAAsspecific CD8+ T cells using peptide pulsed DCs, with an increase of CTLA-4 and memory effector phenotype afteranti-tumor therapy. The ex vivo analysis of the TCR-Vβ repertoire of TAA specific T cells in blood and TILs showedthat whereas the TCR-Vβ04-02 clonotype is highly expressed in TILs the HER2/neu specific T cells are expressedmainly in blood after therapy, suggesting that this particular TCR was selectively enriched in blood after anti-tumortherapy.Conclusions: Our results show the benefits of anti-tumor therapy in a breast cancer patient with clinical completeresponse in two ways, by restoring the responsiveness of T cells by increasing the frequency and activation inperipheral blood of tumor specific T cells present in the tumor before therapy.",

keywords = "Breast cancer, Chemotherapy, CTLA-4, HER2/neu, T cells, TCR repertoire, Type I alpha dendritic cells",

author = "David Bernal-Est{\'e}vez and Ramiro S{\'a}nchez and Tejada, \{Rafael E.\} and Carlos Parra-L{\'o}pez",

note = "Publisher Copyright: {\textcopyright} 2016 The Author(s).",

year = "2016",

month = aug,

day = "3",

doi = "10.1186/s12885-016-2625-2",

language = "English",

volume = "16",

pages = "1--13",

journal = "BMC Cancer",

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T1 - Chemotherapy and radiation therapy elicits tumor specific T cell responses in a breast cancer patient

AU - Bernal-Estévez, David

AU - Sánchez, Ramiro

AU - Tejada, Rafael E.

AU - Parra-López, Carlos

PY - 2016/8/3

Y1 - 2016/8/3

N2 - Background: Experimental evidence and clinical studies in breast cancer suggest that some anti-tumor therapyregimens generate stimulation of the immune system that accounts for tumor clinical responses, however,demonstration of the immunostimulatory power of these therapies on cancer patients continues to be aformidable challenge. Here we present experimental evidence from a breast cancer patient with complete clinicalresponse after 7 years, associated with responsiveness of tumor specific T cells.Methods: T cells were obtained before and after anti-tumor therapy from peripheral blood of a 63-years oldwoman diagnosed with ductal breast cancer (HER2/neu+++, ER-, PR-, HLA-A*02:01) treated with surgery, followedby paclitaxel, trastuzumab (suspended due to cardiac toxicity), and radiotherapy. We obtained a leukapheresisbefore surgery and after 8 months of treatment. Using in vitro cell cultures stimulated with autologous monocytederived dendritic cells (DCs) that produce high levels of IL-12, we characterize by flow cytometry the phenotype oftumor associated antigens (TAAs) HER2/neu and NY-ESO 1 specific T cells. The ex vivo analysis of the TCR-Vβrepertoire of TAA specific T cells in blood and Tumor Infiltrating Lymphocytes (TILs) were performed in order tocorrelate both repertoires prior and after therapy.Results: We evidence a functional recovery of T cell responsiveness to polyclonal stimuli and expansion of TAAsspecific CD8+ T cells using peptide pulsed DCs, with an increase of CTLA-4 and memory effector phenotype afteranti-tumor therapy. The ex vivo analysis of the TCR-Vβ repertoire of TAA specific T cells in blood and TILs showedthat whereas the TCR-Vβ04-02 clonotype is highly expressed in TILs the HER2/neu specific T cells are expressedmainly in blood after therapy, suggesting that this particular TCR was selectively enriched in blood after anti-tumortherapy.Conclusions: Our results show the benefits of anti-tumor therapy in a breast cancer patient with clinical completeresponse in two ways, by restoring the responsiveness of T cells by increasing the frequency and activation inperipheral blood of tumor specific T cells present in the tumor before therapy.

AB - Background: Experimental evidence and clinical studies in breast cancer suggest that some anti-tumor therapyregimens generate stimulation of the immune system that accounts for tumor clinical responses, however,demonstration of the immunostimulatory power of these therapies on cancer patients continues to be aformidable challenge. Here we present experimental evidence from a breast cancer patient with complete clinicalresponse after 7 years, associated with responsiveness of tumor specific T cells.Methods: T cells were obtained before and after anti-tumor therapy from peripheral blood of a 63-years oldwoman diagnosed with ductal breast cancer (HER2/neu+++, ER-, PR-, HLA-A*02:01) treated with surgery, followedby paclitaxel, trastuzumab (suspended due to cardiac toxicity), and radiotherapy. We obtained a leukapheresisbefore surgery and after 8 months of treatment. Using in vitro cell cultures stimulated with autologous monocytederived dendritic cells (DCs) that produce high levels of IL-12, we characterize by flow cytometry the phenotype oftumor associated antigens (TAAs) HER2/neu and NY-ESO 1 specific T cells. The ex vivo analysis of the TCR-Vβrepertoire of TAA specific T cells in blood and Tumor Infiltrating Lymphocytes (TILs) were performed in order tocorrelate both repertoires prior and after therapy.Results: We evidence a functional recovery of T cell responsiveness to polyclonal stimuli and expansion of TAAsspecific CD8+ T cells using peptide pulsed DCs, with an increase of CTLA-4 and memory effector phenotype afteranti-tumor therapy. The ex vivo analysis of the TCR-Vβ repertoire of TAA specific T cells in blood and TILs showedthat whereas the TCR-Vβ04-02 clonotype is highly expressed in TILs the HER2/neu specific T cells are expressedmainly in blood after therapy, suggesting that this particular TCR was selectively enriched in blood after anti-tumortherapy.Conclusions: Our results show the benefits of anti-tumor therapy in a breast cancer patient with clinical completeresponse in two ways, by restoring the responsiveness of T cells by increasing the frequency and activation inperipheral blood of tumor specific T cells present in the tumor before therapy.

KW - Breast cancer

KW - Chemotherapy

KW - CTLA-4

KW - HER2/neu

KW - T cells

KW - TCR repertoire

KW - Type I alpha dendritic cells

UR - https://www.scopus.com/pages/publications/84988433754

U2 - 10.1186/s12885-016-2625-2

DO - 10.1186/s12885-016-2625-2

M3 - Article

C2 - 27484900

AN - SCOPUS:84988433754

SN - 1471-2407

VL - 16

SP - 1

EP - 13

JO - BMC Cancer

JF - BMC Cancer

IS - 1

M1 - 591

ER -

Chemotherapy and radiation therapy elicits tumor specific T cell responses in a breast cancer patient

Abstract

Keywords

UN SDGs

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