Fractionated Radiotherapy with 3 x 8 Gy Induces Systemic Anti-Tumour Responses and Abscopal Tumour Inhibition without Modulating the Humoral Anti-Tumour Response

Thomas H. P. M. Habets; Tammy Oth; Ans Houben; Mirelle J. A. J. Huijskens; Birgit L. M. G. Senden-Gijsbers; Melanie C. A. Schnijderberg; Boudewijn Brans; Ludwig J. Dubois; Philippe Lambin; Marijke De Saint-Hubert; Wilfred T. V. Germeraad; Marcel G. J. Tilanus; Felix M. Mottaghy; Gerardus Bos; Joris Vanderlocht

doi:10.1371/journal.pone.0159515

Fractionated Radiotherapy with 3 x 8 Gy Induces Systemic Anti-Tumour Responses and Abscopal Tumour Inhibition without Modulating the Humoral Anti-Tumour Response

Thomas H. P. M. Habets, Tammy Oth, Ans Houben, Mirelle J. A. J. Huijskens, Birgit L. M. G. Senden-Gijsbers, Melanie C. A. Schnijderberg, Boudewijn Brans, Ludwig J. Dubois, Philippe Lambin, Marijke De Saint-Hubert, Wilfred T. V. Germeraad, Marcel G. J. Tilanus, Felix M. Mottaghy, Gerardus Bos, Joris Vanderlocht^*

^*Corresponding author for this work

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

Abstract

Accumulating evidence indicates that fractionated radiotherapy (RT) can result in distant non-irradiated (abscopal) tumour regression. Although preclinical studies indicate the importance of T cells in this infrequent phenomenon, these studies do not preclude that other immune mechanisms exhibit an addition role in the abscopal effect. We therefore addressed the question whether in addition to T cell mediated responses also humoral antitumour responses are modulated after fractionated RT and whether systemic dendritic cell (DC) stimulation can enhance tumour-specific antibody production. We selected the 67NR mammary carcinoma model since this tumour showed spontaneous antibody production in all tumour-bearing mice. Fractionated RT to the primary tumour was associated with a survival benefit and a delayed growth of a non-irradiated (contralateral) secondary tumour. Notably, fractionated RT did not affect anti-tumour antibody titers and the composition of the immunoglobulin (Ig) isotypes. Likewise, we demonstrated that treatment of tumour-bearing Balb/C mice with DC stimulating growth factor Flt3-L did neither modulate the magnitude nor the composition of the humoral immune response. Finally, we evaluated the immune infiltrate and Ig isotype content of the tumour tissue using flow cytometry and found no differences between treatment groups that were indicative for local antibody production. In conclusion, we demonstrate that the 67NR mammary carcinoma in Balb/C mice is associated with a pre-existing antibody response. And, we show that in tumour-bearing Balb/C mice with abscopal tumour regression such pre-existing antibody responses are not altered upon fractionated RT and/or DC stimulation with Flt3-L. Our research indicates that evaluating the humoral immune response in the setting of abscopal tumour regression is not invariably associated with therapeutic effects.

Original language	English
Article number	e0159515
Journal	PLOS ONE
Volume	11
Issue number	7
DOIs	https://doi.org/10.1371/journal.pone.0159515
Publication status	Published - 18 Jul 2016

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Habets, T. H. P. M., Oth, T., Houben, A., Huijskens, M. J. A. J., Senden-Gijsbers, B. L. M. G., Schnijderberg, M. C. A., Brans, B., Dubois, L. J., Lambin, P., De Saint-Hubert, M., Germeraad, W. T. V., Tilanus, M. G. J., Mottaghy, F. M., Bos, G., & Vanderlocht, J. (2016). Fractionated Radiotherapy with 3 x 8 Gy Induces Systemic Anti-Tumour Responses and Abscopal Tumour Inhibition without Modulating the Humoral Anti-Tumour Response. PLOS ONE, 11(7), Article e0159515. https://doi.org/10.1371/journal.pone.0159515

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title = "Fractionated Radiotherapy with 3 x 8 Gy Induces Systemic Anti-Tumour Responses and Abscopal Tumour Inhibition without Modulating the Humoral Anti-Tumour Response",

abstract = "Accumulating evidence indicates that fractionated radiotherapy (RT) can result in distant non-irradiated (abscopal) tumour regression. Although preclinical studies indicate the importance of T cells in this infrequent phenomenon, these studies do not preclude that other immune mechanisms exhibit an addition role in the abscopal effect. We therefore addressed the question whether in addition to T cell mediated responses also humoral antitumour responses are modulated after fractionated RT and whether systemic dendritic cell (DC) stimulation can enhance tumour-specific antibody production. We selected the 67NR mammary carcinoma model since this tumour showed spontaneous antibody production in all tumour-bearing mice. Fractionated RT to the primary tumour was associated with a survival benefit and a delayed growth of a non-irradiated (contralateral) secondary tumour. Notably, fractionated RT did not affect anti-tumour antibody titers and the composition of the immunoglobulin (Ig) isotypes. Likewise, we demonstrated that treatment of tumour-bearing Balb/C mice with DC stimulating growth factor Flt3-L did neither modulate the magnitude nor the composition of the humoral immune response. Finally, we evaluated the immune infiltrate and Ig isotype content of the tumour tissue using flow cytometry and found no differences between treatment groups that were indicative for local antibody production. In conclusion, we demonstrate that the 67NR mammary carcinoma in Balb/C mice is associated with a pre-existing antibody response. And, we show that in tumour-bearing Balb/C mice with abscopal tumour regression such pre-existing antibody responses are not altered upon fractionated RT and/or DC stimulation with Flt3-L. Our research indicates that evaluating the humoral immune response in the setting of abscopal tumour regression is not invariably associated with therapeutic effects.",

author = "Habets, {Thomas H. P. M.} and Tammy Oth and Ans Houben and Huijskens, {Mirelle J. A. J.} and Senden-Gijsbers, {Birgit L. M. G.} and Schnijderberg, {Melanie C. A.} and Boudewijn Brans and Dubois, {Ludwig J.} and Philippe Lambin and {De Saint-Hubert}, Marijke and Germeraad, {Wilfred T. V.} and Tilanus, {Marcel G. J.} and Mottaghy, {Felix M.} and Gerardus Bos and Joris Vanderlocht",

year = "2016",

month = jul,

day = "18",

doi = "10.1371/journal.pone.0159515",

language = "English",

volume = "11",

journal = "PLOS ONE",

issn = "1932-6203",

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Habets, THPM, Oth, T, Houben, A, Huijskens, MJAJ, Senden-Gijsbers, BLMG, Schnijderberg, MCA, Brans, B, Dubois, LJ , Lambin, P, De Saint-Hubert, M, Germeraad, WTV, Tilanus, MGJ, Mottaghy, FM , Bos, G & Vanderlocht, J 2016, 'Fractionated Radiotherapy with 3 x 8 Gy Induces Systemic Anti-Tumour Responses and Abscopal Tumour Inhibition without Modulating the Humoral Anti-Tumour Response', PLOS ONE, vol. 11, no. 7, e0159515. https://doi.org/10.1371/journal.pone.0159515

TY - JOUR

T1 - Fractionated Radiotherapy with 3 x 8 Gy Induces Systemic Anti-Tumour Responses and Abscopal Tumour Inhibition without Modulating the Humoral Anti-Tumour Response

AU - Habets, Thomas H. P. M.

AU - Oth, Tammy

AU - Houben, Ans

AU - Huijskens, Mirelle J. A. J.

AU - Senden-Gijsbers, Birgit L. M. G.

AU - Schnijderberg, Melanie C. A.

AU - Brans, Boudewijn

AU - Dubois, Ludwig J.

AU - Lambin, Philippe

AU - De Saint-Hubert, Marijke

AU - Germeraad, Wilfred T. V.

AU - Tilanus, Marcel G. J.

AU - Mottaghy, Felix M.

AU - Bos, Gerardus

AU - Vanderlocht, Joris

PY - 2016/7/18

Y1 - 2016/7/18

N2 - Accumulating evidence indicates that fractionated radiotherapy (RT) can result in distant non-irradiated (abscopal) tumour regression. Although preclinical studies indicate the importance of T cells in this infrequent phenomenon, these studies do not preclude that other immune mechanisms exhibit an addition role in the abscopal effect. We therefore addressed the question whether in addition to T cell mediated responses also humoral antitumour responses are modulated after fractionated RT and whether systemic dendritic cell (DC) stimulation can enhance tumour-specific antibody production. We selected the 67NR mammary carcinoma model since this tumour showed spontaneous antibody production in all tumour-bearing mice. Fractionated RT to the primary tumour was associated with a survival benefit and a delayed growth of a non-irradiated (contralateral) secondary tumour. Notably, fractionated RT did not affect anti-tumour antibody titers and the composition of the immunoglobulin (Ig) isotypes. Likewise, we demonstrated that treatment of tumour-bearing Balb/C mice with DC stimulating growth factor Flt3-L did neither modulate the magnitude nor the composition of the humoral immune response. Finally, we evaluated the immune infiltrate and Ig isotype content of the tumour tissue using flow cytometry and found no differences between treatment groups that were indicative for local antibody production. In conclusion, we demonstrate that the 67NR mammary carcinoma in Balb/C mice is associated with a pre-existing antibody response. And, we show that in tumour-bearing Balb/C mice with abscopal tumour regression such pre-existing antibody responses are not altered upon fractionated RT and/or DC stimulation with Flt3-L. Our research indicates that evaluating the humoral immune response in the setting of abscopal tumour regression is not invariably associated with therapeutic effects.

AB - Accumulating evidence indicates that fractionated radiotherapy (RT) can result in distant non-irradiated (abscopal) tumour regression. Although preclinical studies indicate the importance of T cells in this infrequent phenomenon, these studies do not preclude that other immune mechanisms exhibit an addition role in the abscopal effect. We therefore addressed the question whether in addition to T cell mediated responses also humoral antitumour responses are modulated after fractionated RT and whether systemic dendritic cell (DC) stimulation can enhance tumour-specific antibody production. We selected the 67NR mammary carcinoma model since this tumour showed spontaneous antibody production in all tumour-bearing mice. Fractionated RT to the primary tumour was associated with a survival benefit and a delayed growth of a non-irradiated (contralateral) secondary tumour. Notably, fractionated RT did not affect anti-tumour antibody titers and the composition of the immunoglobulin (Ig) isotypes. Likewise, we demonstrated that treatment of tumour-bearing Balb/C mice with DC stimulating growth factor Flt3-L did neither modulate the magnitude nor the composition of the humoral immune response. Finally, we evaluated the immune infiltrate and Ig isotype content of the tumour tissue using flow cytometry and found no differences between treatment groups that were indicative for local antibody production. In conclusion, we demonstrate that the 67NR mammary carcinoma in Balb/C mice is associated with a pre-existing antibody response. And, we show that in tumour-bearing Balb/C mice with abscopal tumour regression such pre-existing antibody responses are not altered upon fractionated RT and/or DC stimulation with Flt3-L. Our research indicates that evaluating the humoral immune response in the setting of abscopal tumour regression is not invariably associated with therapeutic effects.

U2 - 10.1371/journal.pone.0159515

DO - 10.1371/journal.pone.0159515

M3 - Article

C2 - 27427766

SN - 1932-6203

VL - 11

JO - PLOS ONE

JF - PLOS ONE

IS - 7

M1 - e0159515

ER -

Fractionated Radiotherapy with 3 x 8 Gy Induces Systemic Anti-Tumour Responses and Abscopal Tumour Inhibition without Modulating the Humoral Anti-Tumour Response

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