IL-17RC is critically required to maintain baseline A20 production to repress JNK isoform-dependent tumor-specific proliferation

Chi Yan; Yang Lei; Tong Jun Lin; David W. Hoskin; Averil Ma; Jun Wang

doi:10.18632/oncotarget.17820

IL-17RC is critically required to maintain baseline A20 production to repress JNK isoform-dependent tumor-specific proliferation

Chi Yan, Yang Lei, Tong Jun Lin, David W. Hoskin, Averil Ma, Jun Wang

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

8 Citations (Scopus)

Abstract

The IL-17/IL-17R axis has controversial roles in cancer, which may be explained by tumor-specific results. Here, we describe a novel molecular mechanism underlying IL-17RC-controlled tumor-specific proliferation. Triggered by IL-17RC knockdown (KD), B16 melanoma and 4T1 carcinoma cells inversely altered homeostatic tumor proliferation and tumor growth in vitro and in vivo. In contrast to the existing dogma that IL-17RCdependent signaling activates the JNK pathway, IL-17RC KD in both tumor cell lines caused aberrant expression and activation of different JNK isoforms along with markedly diminished levels of the ubiquitin-editing enzyme A20. We demonstrated that differential up-regulation of JNK1 and JNK2 in the two tumor cell lines was responsible for the reciprocal regulation of c-Jun activity and tumor-specific proliferation. Furthermore, we showed that A20 reconstitution of IL-17RCKD clones with expression of full-length A20, but not a truncation-mutant, reversed aberrant JNK1/JNK2 activities and tumor-specific proliferation. Collectively, our study reveals a critical role of IL-17RC in maintaining baseline A20 production and a novel role of the IL-17RC-A20 axis in controlling JNK isoform-dependent tumor-specific homeostatic proliferation.

Original language	English
Pages (from-to)	43153-43168
Number of pages	16
Journal	Oncotarget
Volume	8
Issue number	26
DOIs	https://doi.org/10.18632/oncotarget.17820
Publication status	Published - 2017

Bibliographical note

Funding Information:
We would like to thank Dr. Ryan Noyce for assistance with viral transductions, Dr. Lei Yue for assistance with the EMSA experiment, as well as Ms. Qianni Hu and Dr. Ian Alwayn for assistance in conducting immunohistochemical staining. CY is supported by a graduate student scholarship from IWK Health Centre and received a trainee award from the Beatrice Hunter Cancer Research Institute with funds provided by the Cancer Research Training Program as part of The Terry Fox Foundation Strategic Health Research Training Program in Cancer Research in CIHR. Canadian Breast Cancer Foundation-Atlantic Region, Breast Cancer Society of Canada, QEII Foundation

Publisher Copyright:
© Yan et al.

ASJC Scopus Subject Areas

Oncology

UN SDGs

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

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10.18632/oncotarget.17820

Cite this

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title = "IL-17RC is critically required to maintain baseline A20 production to repress JNK isoform-dependent tumor-specific proliferation",

abstract = "The IL-17/IL-17R axis has controversial roles in cancer, which may be explained by tumor-specific results. Here, we describe a novel molecular mechanism underlying IL-17RC-controlled tumor-specific proliferation. Triggered by IL-17RC knockdown (KD), B16 melanoma and 4T1 carcinoma cells inversely altered homeostatic tumor proliferation and tumor growth in vitro and in vivo. In contrast to the existing dogma that IL-17RCdependent signaling activates the JNK pathway, IL-17RC KD in both tumor cell lines caused aberrant expression and activation of different JNK isoforms along with markedly diminished levels of the ubiquitin-editing enzyme A20. We demonstrated that differential up-regulation of JNK1 and JNK2 in the two tumor cell lines was responsible for the reciprocal regulation of c-Jun activity and tumor-specific proliferation. Furthermore, we showed that A20 reconstitution of IL-17RCKD clones with expression of full-length A20, but not a truncation-mutant, reversed aberrant JNK1/JNK2 activities and tumor-specific proliferation. Collectively, our study reveals a critical role of IL-17RC in maintaining baseline A20 production and a novel role of the IL-17RC-A20 axis in controlling JNK isoform-dependent tumor-specific homeostatic proliferation.",

author = "Chi Yan and Yang Lei and Lin, {Tong Jun} and Hoskin, {David W.} and Averil Ma and Jun Wang",

note = "Funding Information: We would like to thank Dr. Ryan Noyce for assistance with viral transductions, Dr. Lei Yue for assistance with the EMSA experiment, as well as Ms. Qianni Hu and Dr. Ian Alwayn for assistance in conducting immunohistochemical staining. CY is supported by a graduate student scholarship from IWK Health Centre and received a trainee award from the Beatrice Hunter Cancer Research Institute with funds provided by the Cancer Research Training Program as part of The Terry Fox Foundation Strategic Health Research Training Program in Cancer Research in CIHR. Canadian Breast Cancer Foundation-Atlantic Region, Breast Cancer Society of Canada, QEII Foundation Publisher Copyright: {\textcopyright} Yan et al.",

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doi = "10.18632/oncotarget.17820",

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AU - Yan, Chi

AU - Lei, Yang

AU - Lin, Tong Jun

AU - Hoskin, David W.

AU - Ma, Averil

AU - Wang, Jun

N1 - Funding Information: We would like to thank Dr. Ryan Noyce for assistance with viral transductions, Dr. Lei Yue for assistance with the EMSA experiment, as well as Ms. Qianni Hu and Dr. Ian Alwayn for assistance in conducting immunohistochemical staining. CY is supported by a graduate student scholarship from IWK Health Centre and received a trainee award from the Beatrice Hunter Cancer Research Institute with funds provided by the Cancer Research Training Program as part of The Terry Fox Foundation Strategic Health Research Training Program in Cancer Research in CIHR. Canadian Breast Cancer Foundation-Atlantic Region, Breast Cancer Society of Canada, QEII Foundation Publisher Copyright: © Yan et al.

PY - 2017

Y1 - 2017

N2 - The IL-17/IL-17R axis has controversial roles in cancer, which may be explained by tumor-specific results. Here, we describe a novel molecular mechanism underlying IL-17RC-controlled tumor-specific proliferation. Triggered by IL-17RC knockdown (KD), B16 melanoma and 4T1 carcinoma cells inversely altered homeostatic tumor proliferation and tumor growth in vitro and in vivo. In contrast to the existing dogma that IL-17RCdependent signaling activates the JNK pathway, IL-17RC KD in both tumor cell lines caused aberrant expression and activation of different JNK isoforms along with markedly diminished levels of the ubiquitin-editing enzyme A20. We demonstrated that differential up-regulation of JNK1 and JNK2 in the two tumor cell lines was responsible for the reciprocal regulation of c-Jun activity and tumor-specific proliferation. Furthermore, we showed that A20 reconstitution of IL-17RCKD clones with expression of full-length A20, but not a truncation-mutant, reversed aberrant JNK1/JNK2 activities and tumor-specific proliferation. Collectively, our study reveals a critical role of IL-17RC in maintaining baseline A20 production and a novel role of the IL-17RC-A20 axis in controlling JNK isoform-dependent tumor-specific homeostatic proliferation.

AB - The IL-17/IL-17R axis has controversial roles in cancer, which may be explained by tumor-specific results. Here, we describe a novel molecular mechanism underlying IL-17RC-controlled tumor-specific proliferation. Triggered by IL-17RC knockdown (KD), B16 melanoma and 4T1 carcinoma cells inversely altered homeostatic tumor proliferation and tumor growth in vitro and in vivo. In contrast to the existing dogma that IL-17RCdependent signaling activates the JNK pathway, IL-17RC KD in both tumor cell lines caused aberrant expression and activation of different JNK isoforms along with markedly diminished levels of the ubiquitin-editing enzyme A20. We demonstrated that differential up-regulation of JNK1 and JNK2 in the two tumor cell lines was responsible for the reciprocal regulation of c-Jun activity and tumor-specific proliferation. Furthermore, we showed that A20 reconstitution of IL-17RCKD clones with expression of full-length A20, but not a truncation-mutant, reversed aberrant JNK1/JNK2 activities and tumor-specific proliferation. Collectively, our study reveals a critical role of IL-17RC in maintaining baseline A20 production and a novel role of the IL-17RC-A20 axis in controlling JNK isoform-dependent tumor-specific homeostatic proliferation.

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IL-17RC is critically required to maintain baseline A20 production to repress JNK isoform-dependent tumor-specific proliferation

Abstract

Bibliographical note

ASJC Scopus Subject Areas

UN SDGs

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