Radiation therapy induces immunosenescence mediated by p90RSK

Masaki Imanishi; Haizi Cheng; Sivareddy Kotla; Anita Deswal; Nhat Tu Le; Eduardo Chini; Kyung Ae Ko; Venkata S.K. Samanthapudi; Ling Ling Lee; Joerg Herrmann; Xiaolei Xu; Cielito Reyes-Gibby; Sai Ching J. Yeung; Keri L. Schadler; Syed Wamique Yusuf; Zhongxing Liao; Roza Nurieva; El ad David Amir; Jared K. Burks; Nicolas L. Palaskas; John P. Cooke; Steven H. Lin; Michihiro Kobayashi; Momoko Yoshimoto; Jun Ichi Abe

doi:10.3389/fcvm.2022.988713

Radiation therapy induces immunosenescence mediated by p90RSK

Masaki Imanishi, Haizi Cheng, Sivareddy Kotla, Anita Deswal, Nhat Tu Le, Eduardo Chini, Kyung Ae Ko, Venkata S.K. Samanthapudi, Ling Ling Lee, Joerg Herrmann, Xiaolei Xu, Cielito Reyes-Gibby, Sai Ching J. Yeung, Keri L. Schadler, Syed Wamique Yusuf, Zhongxing Liao, Roza Nurieva, El ad David Amir, Jared K. Burks, Nicolas L. PalaskasJohn P. Cooke, Steven H. Lin, Michihiro Kobayashi, Momoko Yoshimoto, Jun Ichi Abe

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

Abstract

Radiation therapy (RT) to the chest increases the patients’ risk of cardiovascular disease (CVD). A complete understanding of the mechanisms by which RT induces CVD could lead to specific preventive, therapeutic approaches. It is becoming evident that both genotoxic chemotherapy agents and radiation induce mitochondrial dysfunction and cellular senescence. Notably, one of the common phenotypes observed in cancer survivors is accelerated senescence, and immunosenescence is closely related to both cancer risk and CVD development. Therefore, suppression of immunosenescence can be an ideal target to prevent cancer treatment-induced CVD. However, the mechanism(s) by which cancer treatments induce immunosenescence are incompletely characterized. We isolated peripheral blood mononuclear cells (PBMCs) before and 3 months after RT from 16 thoracic cancer patients. We characterized human immune cell lineages and markers of senescence, DNA damage response (DDR), efferocytosis, and determinants of clonal hematopoiesis of indeterminant potential (CHIP), using mass cytometry (CyTOF). We found that the frequency of the B cell subtype was decreased after RT. Unsupervised clustering of the CyTOF data identified 138 functional subsets of PBMCs. Compared with baseline, RT increased TBX21 (T-bet) expression in the largest B cell subset of Ki67^–/DNMT3a⁺naïve B cells, and T-bet expression was correlated with phosphorylation of p90RSK expression. CD38 expression was also increased in naïve B cells (CD27^–) and CD8⁺ effector memory CD45RA T cells (T_EMRA). In vitro, we found the critical role of p90RSK activation in upregulating (1) CD38⁺/T-bet⁺ memory and naïve B, and myeloid cells, (2) senescence-associated β-gal staining, and (3) mitochondrial reactive oxygen species (ROS) after ionizing radiation (IR). These data suggest the crucial role of p90RSK activation in immunosenescence. The critical role of p90RSK activation in immune cells and T-bet induction in upregulating atherosclerosis formation has been reported. Furthermore, T-bet directly binds to the CD38 promoter region and upregulates CD38 expression. Since both T-bet and CD38 play a significant role in the process of immunosenescence, our data provide a cellular and molecular mechanism that links RT-induced p90RSK activation and the immunosenescence with T-bet and CD38 induction observed in thoracic cancer patients treated by RT and suggests that targeting the p90RSK/T-bet/CD38 pathway could play a role in preventing the radiation-associated CVD and improving cancer prognosis by inhibiting immunosenescence.

Original language	English (US)
Article number	988713
Journal	Frontiers in Cardiovascular Medicine
Volume	9
DOIs	https://doi.org/10.3389/fcvm.2022.988713
State	Published - Nov 7 2022

Keywords

CD38
T-bet
immunosenescence
p90RSK
radiotherapy

ASJC Scopus subject areas

Cardiology and Cardiovascular Medicine

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10.3389/fcvm.2022.988713

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Imanishi, M., Cheng, H., Kotla, S., Deswal, A., Le, N. T., Chini, E., Ko, K. A., Samanthapudi, V. S. K., Lee, L. L., Herrmann, J., Xu, X., Reyes-Gibby, C., Yeung, S. C. J., Schadler, K. L., Yusuf, S. W., Liao, Z., Nurieva, R., Amir, E. A. D., Burks, J. K., ... Abe, J. I. (2022). Radiation therapy induces immunosenescence mediated by p90RSK. Frontiers in Cardiovascular Medicine, 9, [988713]. https://doi.org/10.3389/fcvm.2022.988713

Imanishi, M, Cheng, H, Kotla, S, Deswal, A, Le, NT, Chini, E, Ko, KA, Samanthapudi, VSK, Lee, LL, Herrmann, J, Xu, X, Reyes-Gibby, C, Yeung, SCJ, Schadler, KL, Yusuf, SW, Liao, Z, Nurieva, R, Amir, EAD, Burks, JK, Palaskas, NL, Cooke, JP, Lin, SH, Kobayashi, M, Yoshimoto, M & Abe, JI 2022, 'Radiation therapy induces immunosenescence mediated by p90RSK', Frontiers in Cardiovascular Medicine, vol. 9, 988713. https://doi.org/10.3389/fcvm.2022.988713

@article{7f063dd135664d4ebd5e40b15049a353,

title = "Radiation therapy induces immunosenescence mediated by p90RSK",

abstract = "Radiation therapy (RT) to the chest increases the patients{\textquoteright} risk of cardiovascular disease (CVD). A complete understanding of the mechanisms by which RT induces CVD could lead to specific preventive, therapeutic approaches. It is becoming evident that both genotoxic chemotherapy agents and radiation induce mitochondrial dysfunction and cellular senescence. Notably, one of the common phenotypes observed in cancer survivors is accelerated senescence, and immunosenescence is closely related to both cancer risk and CVD development. Therefore, suppression of immunosenescence can be an ideal target to prevent cancer treatment-induced CVD. However, the mechanism(s) by which cancer treatments induce immunosenescence are incompletely characterized. We isolated peripheral blood mononuclear cells (PBMCs) before and 3 months after RT from 16 thoracic cancer patients. We characterized human immune cell lineages and markers of senescence, DNA damage response (DDR), efferocytosis, and determinants of clonal hematopoiesis of indeterminant potential (CHIP), using mass cytometry (CyTOF). We found that the frequency of the B cell subtype was decreased after RT. Unsupervised clustering of the CyTOF data identified 138 functional subsets of PBMCs. Compared with baseline, RT increased TBX21 (T-bet) expression in the largest B cell subset of Ki67–/DNMT3a+na{\"i}ve B cells, and T-bet expression was correlated with phosphorylation of p90RSK expression. CD38 expression was also increased in na{\"i}ve B cells (CD27–) and CD8+ effector memory CD45RA T cells (TEMRA). In vitro, we found the critical role of p90RSK activation in upregulating (1) CD38+/T-bet+ memory and na{\"i}ve B, and myeloid cells, (2) senescence-associated β-gal staining, and (3) mitochondrial reactive oxygen species (ROS) after ionizing radiation (IR). These data suggest the crucial role of p90RSK activation in immunosenescence. The critical role of p90RSK activation in immune cells and T-bet induction in upregulating atherosclerosis formation has been reported. Furthermore, T-bet directly binds to the CD38 promoter region and upregulates CD38 expression. Since both T-bet and CD38 play a significant role in the process of immunosenescence, our data provide a cellular and molecular mechanism that links RT-induced p90RSK activation and the immunosenescence with T-bet and CD38 induction observed in thoracic cancer patients treated by RT and suggests that targeting the p90RSK/T-bet/CD38 pathway could play a role in preventing the radiation-associated CVD and improving cancer prognosis by inhibiting immunosenescence.",

keywords = "CD38, T-bet, immunosenescence, p90RSK, radiotherapy",

author = "Masaki Imanishi and Haizi Cheng and Sivareddy Kotla and Anita Deswal and Le, {Nhat Tu} and Eduardo Chini and Ko, {Kyung Ae} and Samanthapudi, {Venkata S.K.} and Lee, {Ling Ling} and Joerg Herrmann and Xiaolei Xu and Cielito Reyes-Gibby and Yeung, {Sai Ching J.} and Schadler, {Keri L.} and Yusuf, {Syed Wamique} and Zhongxing Liao and Roza Nurieva and Amir, {El ad David} and Burks, {Jared K.} and Palaskas, {Nicolas L.} and Cooke, {John P.} and Lin, {Steven H.} and Michihiro Kobayashi and Momoko Yoshimoto and Abe, {Jun Ichi}",

note = "Funding Information: This work was partially supported by the National Institutes of Health (NIH) to J-iA (grants HL-149303 and AI-156921), and JC (grants HL148338, HL133254, and HL157790), N-TL (grants HL-134740 and HL-149303), RN (grants HL141966 and HL143520), and MY (grant AI121197), the Cancer Prevention and Research Institute of Texas (CPRIT) to J-iA and KS (grant RP190256), RN (grant RP190326), and JC (grant RP200619), the Ted Nash Long Life Foundation to MY, and from Institutional Research Grant to RN. This research performed in the Flow Cytometry and Cellular Imaging Facility (NC) was supported in part by the National Institutes of Health through MD Anderson{\textquoteright}s Support (grant CA016672). Publisher Copyright: Copyright {\textcopyright} 2022 Imanishi, Cheng, Kotla, Deswal, Le, Chini, Ko, Samanthapudi, Lee, Herrmann, Xu, Reyes-Gibby, Yeung, Schadler, Yusuf, Liao, Nurieva, Amir, Burks, Palaskas, Cooke, Lin, Kobayashi, Yoshimoto and Abe.",

year = "2022",

month = nov,

day = "7",

doi = "10.3389/fcvm.2022.988713",

language = "English (US)",

volume = "9",

journal = "Frontiers in Cardiovascular Medicine",

issn = "2297-055X",

}

TY - JOUR

T1 - Radiation therapy induces immunosenescence mediated by p90RSK

AU - Imanishi, Masaki

AU - Cheng, Haizi

AU - Kotla, Sivareddy

AU - Deswal, Anita

AU - Le, Nhat Tu

AU - Chini, Eduardo

AU - Ko, Kyung Ae

AU - Samanthapudi, Venkata S.K.

AU - Lee, Ling Ling

AU - Herrmann, Joerg

AU - Xu, Xiaolei

AU - Reyes-Gibby, Cielito

AU - Yeung, Sai Ching J.

AU - Schadler, Keri L.

AU - Yusuf, Syed Wamique

AU - Liao, Zhongxing

AU - Nurieva, Roza

AU - Amir, El ad David

AU - Burks, Jared K.

AU - Palaskas, Nicolas L.

AU - Cooke, John P.

AU - Lin, Steven H.

AU - Kobayashi, Michihiro

AU - Yoshimoto, Momoko

AU - Abe, Jun Ichi

N1 - Funding Information: This work was partially supported by the National Institutes of Health (NIH) to J-iA (grants HL-149303 and AI-156921), and JC (grants HL148338, HL133254, and HL157790), N-TL (grants HL-134740 and HL-149303), RN (grants HL141966 and HL143520), and MY (grant AI121197), the Cancer Prevention and Research Institute of Texas (CPRIT) to J-iA and KS (grant RP190256), RN (grant RP190326), and JC (grant RP200619), the Ted Nash Long Life Foundation to MY, and from Institutional Research Grant to RN. This research performed in the Flow Cytometry and Cellular Imaging Facility (NC) was supported in part by the National Institutes of Health through MD Anderson’s Support (grant CA016672). Publisher Copyright: Copyright © 2022 Imanishi, Cheng, Kotla, Deswal, Le, Chini, Ko, Samanthapudi, Lee, Herrmann, Xu, Reyes-Gibby, Yeung, Schadler, Yusuf, Liao, Nurieva, Amir, Burks, Palaskas, Cooke, Lin, Kobayashi, Yoshimoto and Abe.

PY - 2022/11/7

Y1 - 2022/11/7

N2 - Radiation therapy (RT) to the chest increases the patients’ risk of cardiovascular disease (CVD). A complete understanding of the mechanisms by which RT induces CVD could lead to specific preventive, therapeutic approaches. It is becoming evident that both genotoxic chemotherapy agents and radiation induce mitochondrial dysfunction and cellular senescence. Notably, one of the common phenotypes observed in cancer survivors is accelerated senescence, and immunosenescence is closely related to both cancer risk and CVD development. Therefore, suppression of immunosenescence can be an ideal target to prevent cancer treatment-induced CVD. However, the mechanism(s) by which cancer treatments induce immunosenescence are incompletely characterized. We isolated peripheral blood mononuclear cells (PBMCs) before and 3 months after RT from 16 thoracic cancer patients. We characterized human immune cell lineages and markers of senescence, DNA damage response (DDR), efferocytosis, and determinants of clonal hematopoiesis of indeterminant potential (CHIP), using mass cytometry (CyTOF). We found that the frequency of the B cell subtype was decreased after RT. Unsupervised clustering of the CyTOF data identified 138 functional subsets of PBMCs. Compared with baseline, RT increased TBX21 (T-bet) expression in the largest B cell subset of Ki67–/DNMT3a+naïve B cells, and T-bet expression was correlated with phosphorylation of p90RSK expression. CD38 expression was also increased in naïve B cells (CD27–) and CD8+ effector memory CD45RA T cells (TEMRA). In vitro, we found the critical role of p90RSK activation in upregulating (1) CD38+/T-bet+ memory and naïve B, and myeloid cells, (2) senescence-associated β-gal staining, and (3) mitochondrial reactive oxygen species (ROS) after ionizing radiation (IR). These data suggest the crucial role of p90RSK activation in immunosenescence. The critical role of p90RSK activation in immune cells and T-bet induction in upregulating atherosclerosis formation has been reported. Furthermore, T-bet directly binds to the CD38 promoter region and upregulates CD38 expression. Since both T-bet and CD38 play a significant role in the process of immunosenescence, our data provide a cellular and molecular mechanism that links RT-induced p90RSK activation and the immunosenescence with T-bet and CD38 induction observed in thoracic cancer patients treated by RT and suggests that targeting the p90RSK/T-bet/CD38 pathway could play a role in preventing the radiation-associated CVD and improving cancer prognosis by inhibiting immunosenescence.

AB - Radiation therapy (RT) to the chest increases the patients’ risk of cardiovascular disease (CVD). A complete understanding of the mechanisms by which RT induces CVD could lead to specific preventive, therapeutic approaches. It is becoming evident that both genotoxic chemotherapy agents and radiation induce mitochondrial dysfunction and cellular senescence. Notably, one of the common phenotypes observed in cancer survivors is accelerated senescence, and immunosenescence is closely related to both cancer risk and CVD development. Therefore, suppression of immunosenescence can be an ideal target to prevent cancer treatment-induced CVD. However, the mechanism(s) by which cancer treatments induce immunosenescence are incompletely characterized. We isolated peripheral blood mononuclear cells (PBMCs) before and 3 months after RT from 16 thoracic cancer patients. We characterized human immune cell lineages and markers of senescence, DNA damage response (DDR), efferocytosis, and determinants of clonal hematopoiesis of indeterminant potential (CHIP), using mass cytometry (CyTOF). We found that the frequency of the B cell subtype was decreased after RT. Unsupervised clustering of the CyTOF data identified 138 functional subsets of PBMCs. Compared with baseline, RT increased TBX21 (T-bet) expression in the largest B cell subset of Ki67–/DNMT3a+naïve B cells, and T-bet expression was correlated with phosphorylation of p90RSK expression. CD38 expression was also increased in naïve B cells (CD27–) and CD8+ effector memory CD45RA T cells (TEMRA). In vitro, we found the critical role of p90RSK activation in upregulating (1) CD38+/T-bet+ memory and naïve B, and myeloid cells, (2) senescence-associated β-gal staining, and (3) mitochondrial reactive oxygen species (ROS) after ionizing radiation (IR). These data suggest the crucial role of p90RSK activation in immunosenescence. The critical role of p90RSK activation in immune cells and T-bet induction in upregulating atherosclerosis formation has been reported. Furthermore, T-bet directly binds to the CD38 promoter region and upregulates CD38 expression. Since both T-bet and CD38 play a significant role in the process of immunosenescence, our data provide a cellular and molecular mechanism that links RT-induced p90RSK activation and the immunosenescence with T-bet and CD38 induction observed in thoracic cancer patients treated by RT and suggests that targeting the p90RSK/T-bet/CD38 pathway could play a role in preventing the radiation-associated CVD and improving cancer prognosis by inhibiting immunosenescence.

KW - CD38

KW - T-bet

KW - immunosenescence

KW - p90RSK

KW - radiotherapy

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U2 - 10.3389/fcvm.2022.988713

DO - 10.3389/fcvm.2022.988713

M3 - Article

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VL - 9

JO - Frontiers in Cardiovascular Medicine

JF - Frontiers in Cardiovascular Medicine

SN - 2297-055X

M1 - 988713

ER -

Radiation therapy induces immunosenescence mediated by p90RSK

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