Triple knockdown of CDC37, HSP90-alpha and HSP90-beta diminishes extracellular vesicles-driven malignancy events and macrophage M2 polarization in oral cancer

Kisho Ono; Chiharu Sogawa; Hotaka Kawai; Manh Tien Tran; Eman A. Taha; Yanyin Lu; May Wathone Oo; Yuka Okusya; Hirohiko Okamura; Soichiro Ibaragi; Masaharu Takigawa; Ken-ichi Kozaｋi; Hitoshi Nagatsuka; Akira Sasaki; Kuniaki Okamoto; Stuart K. Calderwood; Takanori Eguchi

doi:10.1080/20013078.2020.1769373

Triple knockdown of CDC37, HSP90-alpha and HSP90-beta diminishes extracellular vesicles-driven malignancy events and macrophage M2 polarization in oral cancer

Kisho Ono, Chiharu Sogawa, Hotaka Kawai, Manh Tien Tran, Eman A. Taha, Yanyin Lu, May Wathone Oo, Yuka Okusya, Hirohiko Okamura, Soichiro Ibaragi, Masaharu Takigawa, Ken-ichi Kozaｋi, Hitoshi Nagatsuka, Akira Sasaki, Kuniaki Okamoto, Stuart K. Calderwood, Takanori Eguchi

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

34 Citations (Scopus)

Abstract

Evidence has been accumulating to indicate that extracellular vesicles (EVs), including exosomes, released by cancer cells can foster tumour progression. The molecular chaperones–CDC37, HSP90α and HSP90β play key roles in cancer progression including epithelial-mesenchymal transition (EMT), although their contribution to EVs-mediated cell–cell communication in tumour microenvironment has not been thoroughly examined. Here we show that triple depletion of the chaperone trio attenuates numerous cancer malignancy events exerted through EV release. Metastatic oral cancer-derived EVs (MEV) were enriched with HSP90α HSP90β and cancer-initiating cell marker CD326/EpCAM. Depletion of these chaperones individually induced compensatory increases in the other chaperones, whereas triple siRNA targeting of these molecules markedly diminished the levels of the chaperone trio and attenuated EMT. MEV were potent agents in initiating EMT in normal epithelial cells, a process that was attenuated by the triple chaperone depletion. The migration, invasion, and in vitro tumour initiation of oral cancer cells were significantly promoted by MEV, while triple depletion of CDC37/HSP90α/β reversed these MEV-driven malignancy events. In metastatic oral cancer patient-derived tumours, HSP90β was significantly accumulated in infiltrating tumour-associated macrophages (TAM) as compared to lower grade oral cancer cases. HSP90-enriched MEV-induced TAM polarization to an M2 phenotype, a transition known to support cancer progression, whereas the triple chaperone depletion attenuated this effect. Mechanistically, the triple chaperone depletion in metastatic oral cancer cells effectively reduced MEV transmission into macrophages. Hence, siRNA-mediated knockdown of the chaperone trio (CDC37/HSP90α/HSP90β) could potentially be a novel therapeutic strategy to attenuate several EV-driven malignancy events in the tumour microenvironment. Abbreviations: CDC37: cell division control 37; EMT: epithelial-mesenchymal transmission; EV: extracellular vesicles; HNSCC: head and neck squamous cell carcinoma; HSP90: heat shock protein 90; TAM: tumour-associated macrophage.

Original language	English
Article number	1769373
Journal	Journal of Extracellular Vesicles
Volume	9
Issue number	1
DOIs	https://doi.org/10.1080/20013078.2020.1769373
Publication status	Published - Jan 1 2020

Keywords

CDC37
Extracellular vesicles
HSP90
epithelial-mesenchymal transition
oral cancer
tetraspanin
tumour-associated macrophage

ASJC Scopus subject areas

Histology
Cell Biology

UN SDGs

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

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10.1080/20013078.2020.1769373

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Ono, K., Sogawa, C., Kawai, H., Tran, M. T., Taha, E. A., Lu, Y., Oo, M. W., Okusya, Y., Okamura, H., Ibaragi, S., Takigawa, M., Kozaｋi, K., Nagatsuka, H., Sasaki, A., Okamoto, K., Calderwood, S. K., & Eguchi, T. (2020). Triple knockdown of CDC37, HSP90-alpha and HSP90-beta diminishes extracellular vesicles-driven malignancy events and macrophage M2 polarization in oral cancer. Journal of Extracellular Vesicles, 9(1), [1769373]. https://doi.org/10.1080/20013078.2020.1769373

Ono, K, Sogawa, C, Kawai, H, Tran, MT, Taha, EA, Lu, Y, Oo, MW, Okusya, Y, Okamura, H , Ibaragi, S , Takigawa, M, Kozaｋi, K, Nagatsuka, H, Sasaki, A, Okamoto, K, Calderwood, SK & Eguchi, T 2020, 'Triple knockdown of CDC37, HSP90-alpha and HSP90-beta diminishes extracellular vesicles-driven malignancy events and macrophage M2 polarization in oral cancer', Journal of Extracellular Vesicles, vol. 9, no. 1, 1769373. https://doi.org/10.1080/20013078.2020.1769373

@article{141ef3b94e30422d988d2085b8e7fde8,

title = "Triple knockdown of CDC37, HSP90-alpha and HSP90-beta diminishes extracellular vesicles-driven malignancy events and macrophage M2 polarization in oral cancer",

abstract = "Evidence has been accumulating to indicate that extracellular vesicles (EVs), including exosomes, released by cancer cells can foster tumour progression. The molecular chaperones–CDC37, HSP90α and HSP90β play key roles in cancer progression including epithelial-mesenchymal transition (EMT), although their contribution to EVs-mediated cell–cell communication in tumour microenvironment has not been thoroughly examined. Here we show that triple depletion of the chaperone trio attenuates numerous cancer malignancy events exerted through EV release. Metastatic oral cancer-derived EVs (MEV) were enriched with HSP90α HSP90β and cancer-initiating cell marker CD326/EpCAM. Depletion of these chaperones individually induced compensatory increases in the other chaperones, whereas triple siRNA targeting of these molecules markedly diminished the levels of the chaperone trio and attenuated EMT. MEV were potent agents in initiating EMT in normal epithelial cells, a process that was attenuated by the triple chaperone depletion. The migration, invasion, and in vitro tumour initiation of oral cancer cells were significantly promoted by MEV, while triple depletion of CDC37/HSP90α/β reversed these MEV-driven malignancy events. In metastatic oral cancer patient-derived tumours, HSP90β was significantly accumulated in infiltrating tumour-associated macrophages (TAM) as compared to lower grade oral cancer cases. HSP90-enriched MEV-induced TAM polarization to an M2 phenotype, a transition known to support cancer progression, whereas the triple chaperone depletion attenuated this effect. Mechanistically, the triple chaperone depletion in metastatic oral cancer cells effectively reduced MEV transmission into macrophages. Hence, siRNA-mediated knockdown of the chaperone trio (CDC37/HSP90α/HSP90β) could potentially be a novel therapeutic strategy to attenuate several EV-driven malignancy events in the tumour microenvironment. Abbreviations: CDC37: cell division control 37; EMT: epithelial-mesenchymal transmission; EV: extracellular vesicles; HNSCC: head and neck squamous cell carcinoma; HSP90: heat shock protein 90; TAM: tumour-associated macrophage.",

keywords = "CDC37, Extracellular vesicles, HSP90, epithelial-mesenchymal transition, oral cancer, tetraspanin, tumour-associated macrophage",

author = "Kisho Ono and Chiharu Sogawa and Hotaka Kawai and Tran, {Manh Tien} and Taha, {Eman A.} and Yanyin Lu and Oo, {May Wathone} and Yuka Okusya and Hirohiko Okamura and Soichiro Ibaragi and Masaharu Takigawa and Ken-ichi Kozaｋi and Hitoshi Nagatsuka and Akira Sasaki and Kuniaki Okamoto and Calderwood, {Stuart K.} and Takanori Eguchi",

note = "Funding Information: This work was supported by JSPS KAKENHI, grant numbers [17K11642 (T.E.), 17K11643 (C.S., T.E.), 17K11669 (K.Oh., T.E.), 19K24072 (K.On.), 16K11722-JM (T.E., H.N.), 19K10288-JM (H.N.), 18K09789-KN (H.N., T.E), JP16K11441 (H.N.), JP20H03888 (H.N., T.E.), 19H03817 (M.T., T.E.), 19H04051 (H.O., T.E.) and 20K09904 (C.S., T.E., K.Ok.)], Ryobi Teien Memorial Foundation Grant (K.Ok., C.S., T.E.), Suzuken Memorial Foundation Grant (T.E.) and NIH Grant CA176326-05 (SKC). This paper is dedicated to the memory of one of our mentors, Professor Ken-ichi Kozaki, who passed away on 29 May 2016. The authors thank Haruo Urata for the operation of TEM, Tomonari Kasai and Masaharu Seno for particle size analysis using ELS-8000, Kazuko Kobayashi for the operation of Zetasizer, Eriko Aoyama for maintenance of HCS analyzer. The authors thank Manabu Itoh and Kazuya Arai at JSR for technical advice in NCP. The authors thank Keisuke Nakano for illuminating discussion and encouraging support. Publisher Copyright: {\textcopyright} 2020, {\textcopyright} 2020 The Author(s). Published by Informa UK Limited, trading as Taylor & Francis Group on behalf of The International Society for Extracellular Vesicles.",

year = "2020",

month = jan,

day = "1",

doi = "10.1080/20013078.2020.1769373",

language = "English",

volume = "9",

journal = "Journal of Extracellular Vesicles",

issn = "2001-3078",

publisher = "Taylor and Francis Ltd.",

number = "1",

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TY - JOUR

T1 - Triple knockdown of CDC37, HSP90-alpha and HSP90-beta diminishes extracellular vesicles-driven malignancy events and macrophage M2 polarization in oral cancer

AU - Ono, Kisho

AU - Sogawa, Chiharu

AU - Kawai, Hotaka

AU - Tran, Manh Tien

AU - Taha, Eman A.

AU - Lu, Yanyin

AU - Oo, May Wathone

AU - Okusya, Yuka

AU - Okamura, Hirohiko

AU - Ibaragi, Soichiro

AU - Takigawa, Masaharu

AU - Kozaｋi, Ken-ichi

AU - Nagatsuka, Hitoshi

AU - Sasaki, Akira

AU - Okamoto, Kuniaki

AU - Calderwood, Stuart K.

AU - Eguchi, Takanori

N1 - Funding Information: This work was supported by JSPS KAKENHI, grant numbers [17K11642 (T.E.), 17K11643 (C.S., T.E.), 17K11669 (K.Oh., T.E.), 19K24072 (K.On.), 16K11722-JM (T.E., H.N.), 19K10288-JM (H.N.), 18K09789-KN (H.N., T.E), JP16K11441 (H.N.), JP20H03888 (H.N., T.E.), 19H03817 (M.T., T.E.), 19H04051 (H.O., T.E.) and 20K09904 (C.S., T.E., K.Ok.)], Ryobi Teien Memorial Foundation Grant (K.Ok., C.S., T.E.), Suzuken Memorial Foundation Grant (T.E.) and NIH Grant CA176326-05 (SKC). This paper is dedicated to the memory of one of our mentors, Professor Ken-ichi Kozaki, who passed away on 29 May 2016. The authors thank Haruo Urata for the operation of TEM, Tomonari Kasai and Masaharu Seno for particle size analysis using ELS-8000, Kazuko Kobayashi for the operation of Zetasizer, Eriko Aoyama for maintenance of HCS analyzer. The authors thank Manabu Itoh and Kazuya Arai at JSR for technical advice in NCP. The authors thank Keisuke Nakano for illuminating discussion and encouraging support. Publisher Copyright: © 2020, © 2020 The Author(s). Published by Informa UK Limited, trading as Taylor & Francis Group on behalf of The International Society for Extracellular Vesicles.

PY - 2020/1/1

Y1 - 2020/1/1

N2 - Evidence has been accumulating to indicate that extracellular vesicles (EVs), including exosomes, released by cancer cells can foster tumour progression. The molecular chaperones–CDC37, HSP90α and HSP90β play key roles in cancer progression including epithelial-mesenchymal transition (EMT), although their contribution to EVs-mediated cell–cell communication in tumour microenvironment has not been thoroughly examined. Here we show that triple depletion of the chaperone trio attenuates numerous cancer malignancy events exerted through EV release. Metastatic oral cancer-derived EVs (MEV) were enriched with HSP90α HSP90β and cancer-initiating cell marker CD326/EpCAM. Depletion of these chaperones individually induced compensatory increases in the other chaperones, whereas triple siRNA targeting of these molecules markedly diminished the levels of the chaperone trio and attenuated EMT. MEV were potent agents in initiating EMT in normal epithelial cells, a process that was attenuated by the triple chaperone depletion. The migration, invasion, and in vitro tumour initiation of oral cancer cells were significantly promoted by MEV, while triple depletion of CDC37/HSP90α/β reversed these MEV-driven malignancy events. In metastatic oral cancer patient-derived tumours, HSP90β was significantly accumulated in infiltrating tumour-associated macrophages (TAM) as compared to lower grade oral cancer cases. HSP90-enriched MEV-induced TAM polarization to an M2 phenotype, a transition known to support cancer progression, whereas the triple chaperone depletion attenuated this effect. Mechanistically, the triple chaperone depletion in metastatic oral cancer cells effectively reduced MEV transmission into macrophages. Hence, siRNA-mediated knockdown of the chaperone trio (CDC37/HSP90α/HSP90β) could potentially be a novel therapeutic strategy to attenuate several EV-driven malignancy events in the tumour microenvironment. Abbreviations: CDC37: cell division control 37; EMT: epithelial-mesenchymal transmission; EV: extracellular vesicles; HNSCC: head and neck squamous cell carcinoma; HSP90: heat shock protein 90; TAM: tumour-associated macrophage.

AB - Evidence has been accumulating to indicate that extracellular vesicles (EVs), including exosomes, released by cancer cells can foster tumour progression. The molecular chaperones–CDC37, HSP90α and HSP90β play key roles in cancer progression including epithelial-mesenchymal transition (EMT), although their contribution to EVs-mediated cell–cell communication in tumour microenvironment has not been thoroughly examined. Here we show that triple depletion of the chaperone trio attenuates numerous cancer malignancy events exerted through EV release. Metastatic oral cancer-derived EVs (MEV) were enriched with HSP90α HSP90β and cancer-initiating cell marker CD326/EpCAM. Depletion of these chaperones individually induced compensatory increases in the other chaperones, whereas triple siRNA targeting of these molecules markedly diminished the levels of the chaperone trio and attenuated EMT. MEV were potent agents in initiating EMT in normal epithelial cells, a process that was attenuated by the triple chaperone depletion. The migration, invasion, and in vitro tumour initiation of oral cancer cells were significantly promoted by MEV, while triple depletion of CDC37/HSP90α/β reversed these MEV-driven malignancy events. In metastatic oral cancer patient-derived tumours, HSP90β was significantly accumulated in infiltrating tumour-associated macrophages (TAM) as compared to lower grade oral cancer cases. HSP90-enriched MEV-induced TAM polarization to an M2 phenotype, a transition known to support cancer progression, whereas the triple chaperone depletion attenuated this effect. Mechanistically, the triple chaperone depletion in metastatic oral cancer cells effectively reduced MEV transmission into macrophages. Hence, siRNA-mediated knockdown of the chaperone trio (CDC37/HSP90α/HSP90β) could potentially be a novel therapeutic strategy to attenuate several EV-driven malignancy events in the tumour microenvironment. Abbreviations: CDC37: cell division control 37; EMT: epithelial-mesenchymal transmission; EV: extracellular vesicles; HNSCC: head and neck squamous cell carcinoma; HSP90: heat shock protein 90; TAM: tumour-associated macrophage.

KW - CDC37

KW - Extracellular vesicles

KW - HSP90

KW - epithelial-mesenchymal transition

KW - oral cancer

KW - tetraspanin

KW - tumour-associated macrophage

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Triple knockdown of CDC37, HSP90-alpha and HSP90-beta diminishes extracellular vesicles-driven malignancy events and macrophage M2 polarization in oral cancer

Abstract

Keywords

ASJC Scopus subject areas

UN SDGs

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