Brain cancer induces systemic immunosuppression through release of non-steroid soluble mediators

Katayoun Ayasoufi; Christian K. Pfaller; Laura Evgin; Roman H. Khadka; Zachariah P. Tritz; Emma N. Goddery; Cori E. Fain; Lila T. Yokanovich; Benjamin T. Himes; Fang Jin; Jiaying Zheng; Matthew R. Schuelke; Michael J. Hansen; Wesley Tung; Ian F. Parney; Larry R. Pease; Richard G. Vile; Aaron J. Johnson

doi:10.1093/brain/awaa343

Brain cancer induces systemic immunosuppression through release of non-steroid soluble mediators

Katayoun Ayasoufi, Christian K. Pfaller, Laura Evgin, Roman H. Khadka, Zachariah P. Tritz, Emma N. Goddery, Cori E. Fain, Lila T. Yokanovich, Benjamin T. Himes, Fang Jin, Jiaying Zheng, Matthew R. Schuelke, Michael J. Hansen, Wesley Tung, Ian F. Parney, Larry R. Pease, Richard G. Vile, Aaron J. Johnson

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

36 Scopus citations

Abstract

Immunosuppression of unknown aetiology is a hallmark feature of glioblastoma and is characterized by decreased CD4 T-cell counts and downregulation of major histocompatibility complex class II expression on peripheral blood monocytes in patients. This immunosuppression is a critical barrier to the successful development of immunotherapies for glioblastoma. We recapitulated the immunosuppression observed in glioblastoma patients in the C57BL/6 mouse and investigated the aetiology of low CD4 T-cell counts. We determined that thymic involution was a hallmark feature of immunosuppression in three distinct models of brain cancer, including mice harbouring GL261 glioma, B16 melanoma, and in a spontaneous model of diffuse intrinsic pontine glioma. In addition to thymic involution, we determined that tumour growth in the brain induced significant splenic involution, reductions in peripheral T cells, reduced MHC II expression on blood leucocytes, and a modest increase in bone marrow resident CD4 T cells. Using parabiosis we report that thymic involution, declines in peripheral T-cell counts, and reduced major histocompatibility complex class II expression levels were mediated through circulating blood-derived factors. Conversely, T-cell sequestration in the bone marrow was not governed through circulating factors. Serum isolated from glioma-bearing mice potently inhibited proliferation and functions of T cells both in vitro and in vivo. Interestingly, the factor responsible for immunosuppression in serum is non-steroidal and of high molecular weight. Through further analysis of neurological disease models, we determined that the immunosuppression was not unique to cancer itself, but rather occurs in response to brain injury. Non-cancerous acute neurological insults also induced significant thymic involution and rendered serum immunosuppressive. Both thymic involution and serum-derived immunosuppression were reversible upon clearance of brain insults. These findings demonstrate that brain cancers cause multifaceted immunosuppression and pinpoint circulating factors as a target of intervention to restore immunity.

Original language	English (US)
Pages (from-to)	3629-3652
Number of pages	24
Journal	Brain
Volume	143
Issue number	12
DOIs	https://doi.org/10.1093/brain/awaa343
State	Published - Dec 1 2020
Externally published	Yes

Keywords

T cells
glioblastoma
immunosuppression
neuroimmunology
thymus

ASJC Scopus subject areas

Clinical Neurology

UN SDGs

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

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10.1093/brain/awaa343

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Ayasoufi, K., Pfaller, C. K., Evgin, L., Khadka, R. H., Tritz, Z. P., Goddery, E. N., Fain, C. E., Yokanovich, L. T., Himes, B. T., Jin, F., Zheng, J., Schuelke, M. R., Hansen, M. J., Tung, W., Parney, I. F., Pease, L. R., Vile, R. G., & Johnson, A. J. (2020). Brain cancer induces systemic immunosuppression through release of non-steroid soluble mediators. Brain, 143(12), 3629-3652. https://doi.org/10.1093/brain/awaa343

Ayasoufi, K, Pfaller, CK, Evgin, L, Khadka, RH, Tritz, ZP, Goddery, EN, Fain, CE, Yokanovich, LT, Himes, BT, Jin, F, Zheng, J, Schuelke, MR, Hansen, MJ, Tung, W, Parney, IF, Pease, LR, Vile, RG & Johnson, AJ 2020, 'Brain cancer induces systemic immunosuppression through release of non-steroid soluble mediators', Brain, vol. 143, no. 12, pp. 3629-3652. https://doi.org/10.1093/brain/awaa343

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title = "Brain cancer induces systemic immunosuppression through release of non-steroid soluble mediators",

abstract = "Immunosuppression of unknown aetiology is a hallmark feature of glioblastoma and is characterized by decreased CD4 T-cell counts and downregulation of major histocompatibility complex class II expression on peripheral blood monocytes in patients. This immunosuppression is a critical barrier to the successful development of immunotherapies for glioblastoma. We recapitulated the immunosuppression observed in glioblastoma patients in the C57BL/6 mouse and investigated the aetiology of low CD4 T-cell counts. We determined that thymic involution was a hallmark feature of immunosuppression in three distinct models of brain cancer, including mice harbouring GL261 glioma, B16 melanoma, and in a spontaneous model of diffuse intrinsic pontine glioma. In addition to thymic involution, we determined that tumour growth in the brain induced significant splenic involution, reductions in peripheral T cells, reduced MHC II expression on blood leucocytes, and a modest increase in bone marrow resident CD4 T cells. Using parabiosis we report that thymic involution, declines in peripheral T-cell counts, and reduced major histocompatibility complex class II expression levels were mediated through circulating blood-derived factors. Conversely, T-cell sequestration in the bone marrow was not governed through circulating factors. Serum isolated from glioma-bearing mice potently inhibited proliferation and functions of T cells both in vitro and in vivo. Interestingly, the factor responsible for immunosuppression in serum is non-steroidal and of high molecular weight. Through further analysis of neurological disease models, we determined that the immunosuppression was not unique to cancer itself, but rather occurs in response to brain injury. Non-cancerous acute neurological insults also induced significant thymic involution and rendered serum immunosuppressive. Both thymic involution and serum-derived immunosuppression were reversible upon clearance of brain insults. These findings demonstrate that brain cancers cause multifaceted immunosuppression and pinpoint circulating factors as a target of intervention to restore immunity.",

keywords = "T cells, glioblastoma, immunosuppression, neuroimmunology, thymus",

author = "Katayoun Ayasoufi and Pfaller, {Christian K.} and Laura Evgin and Khadka, {Roman H.} and Tritz, {Zachariah P.} and Goddery, {Emma N.} and Fain, {Cori E.} and Yokanovich, {Lila T.} and Himes, {Benjamin T.} and Fang Jin and Jiaying Zheng and Schuelke, {Matthew R.} and Hansen, {Michael J.} and Wesley Tung and Parney, {Ian F.} and Pease, {Larry R.} and Vile, {Richard G.} and Johnson, {Aaron J.}",

note = "Publisher Copyright: {\textcopyright} 2020 The Author(s) (2020). Published by Oxford University Press on behalf of the Guarantors of Brain. All rights reserved. For permissions, please email: journals.permissions@oup.com.",

year = "2020",

month = dec,

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doi = "10.1093/brain/awaa343",

language = "English (US)",

volume = "143",

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T1 - Brain cancer induces systemic immunosuppression through release of non-steroid soluble mediators

AU - Ayasoufi, Katayoun

AU - Pfaller, Christian K.

AU - Evgin, Laura

AU - Khadka, Roman H.

AU - Tritz, Zachariah P.

AU - Goddery, Emma N.

AU - Fain, Cori E.

AU - Yokanovich, Lila T.

AU - Himes, Benjamin T.

AU - Jin, Fang

AU - Zheng, Jiaying

AU - Schuelke, Matthew R.

AU - Hansen, Michael J.

AU - Tung, Wesley

AU - Parney, Ian F.

AU - Pease, Larry R.

AU - Vile, Richard G.

AU - Johnson, Aaron J.

N1 - Publisher Copyright: © 2020 The Author(s) (2020). Published by Oxford University Press on behalf of the Guarantors of Brain. All rights reserved. For permissions, please email: journals.permissions@oup.com.

PY - 2020/12/1

Y1 - 2020/12/1

N2 - Immunosuppression of unknown aetiology is a hallmark feature of glioblastoma and is characterized by decreased CD4 T-cell counts and downregulation of major histocompatibility complex class II expression on peripheral blood monocytes in patients. This immunosuppression is a critical barrier to the successful development of immunotherapies for glioblastoma. We recapitulated the immunosuppression observed in glioblastoma patients in the C57BL/6 mouse and investigated the aetiology of low CD4 T-cell counts. We determined that thymic involution was a hallmark feature of immunosuppression in three distinct models of brain cancer, including mice harbouring GL261 glioma, B16 melanoma, and in a spontaneous model of diffuse intrinsic pontine glioma. In addition to thymic involution, we determined that tumour growth in the brain induced significant splenic involution, reductions in peripheral T cells, reduced MHC II expression on blood leucocytes, and a modest increase in bone marrow resident CD4 T cells. Using parabiosis we report that thymic involution, declines in peripheral T-cell counts, and reduced major histocompatibility complex class II expression levels were mediated through circulating blood-derived factors. Conversely, T-cell sequestration in the bone marrow was not governed through circulating factors. Serum isolated from glioma-bearing mice potently inhibited proliferation and functions of T cells both in vitro and in vivo. Interestingly, the factor responsible for immunosuppression in serum is non-steroidal and of high molecular weight. Through further analysis of neurological disease models, we determined that the immunosuppression was not unique to cancer itself, but rather occurs in response to brain injury. Non-cancerous acute neurological insults also induced significant thymic involution and rendered serum immunosuppressive. Both thymic involution and serum-derived immunosuppression were reversible upon clearance of brain insults. These findings demonstrate that brain cancers cause multifaceted immunosuppression and pinpoint circulating factors as a target of intervention to restore immunity.

AB - Immunosuppression of unknown aetiology is a hallmark feature of glioblastoma and is characterized by decreased CD4 T-cell counts and downregulation of major histocompatibility complex class II expression on peripheral blood monocytes in patients. This immunosuppression is a critical barrier to the successful development of immunotherapies for glioblastoma. We recapitulated the immunosuppression observed in glioblastoma patients in the C57BL/6 mouse and investigated the aetiology of low CD4 T-cell counts. We determined that thymic involution was a hallmark feature of immunosuppression in three distinct models of brain cancer, including mice harbouring GL261 glioma, B16 melanoma, and in a spontaneous model of diffuse intrinsic pontine glioma. In addition to thymic involution, we determined that tumour growth in the brain induced significant splenic involution, reductions in peripheral T cells, reduced MHC II expression on blood leucocytes, and a modest increase in bone marrow resident CD4 T cells. Using parabiosis we report that thymic involution, declines in peripheral T-cell counts, and reduced major histocompatibility complex class II expression levels were mediated through circulating blood-derived factors. Conversely, T-cell sequestration in the bone marrow was not governed through circulating factors. Serum isolated from glioma-bearing mice potently inhibited proliferation and functions of T cells both in vitro and in vivo. Interestingly, the factor responsible for immunosuppression in serum is non-steroidal and of high molecular weight. Through further analysis of neurological disease models, we determined that the immunosuppression was not unique to cancer itself, but rather occurs in response to brain injury. Non-cancerous acute neurological insults also induced significant thymic involution and rendered serum immunosuppressive. Both thymic involution and serum-derived immunosuppression were reversible upon clearance of brain insults. These findings demonstrate that brain cancers cause multifaceted immunosuppression and pinpoint circulating factors as a target of intervention to restore immunity.

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KW - glioblastoma

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Brain cancer induces systemic immunosuppression through release of non-steroid soluble mediators

Abstract

Keywords

ASJC Scopus subject areas

UN SDGs

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