Extracellular Vesicles Enriched with Moonlighting Metalloproteinase Are Highly Transmissive, Pro-Tumorigenic, and Trans-Activates Cellular Communication Network Factor (CCN2/CTGF): CRISPR against Cancer

Matrix metalloproteinase 3 (MMP3) plays multiple roles in extracellular proteolysis as well as intracellular transcription, prompting a new definition of moonlighting metalloproteinase (MMP), according to a definition of protein moonlighting (or gene sharing), a phenomenon by which a protein can per...

Descripción completa

Detalles Bibliográficos
Autores principales: Okusha, Yuka, Eguchi, Takanori, Tran, Manh T., Sogawa, Chiharu, Yoshida, Kaya, Itagaki, Mami, Taha, Eman A., Ono, Kisho, Aoyama, Eriko, Okamura, Hirohiko, Kozaki, Ken-ichi, Calderwood, Stuart K., Takigawa, Masaharu, Okamoto, Kuniaki
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2020
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7226423/
https://www.ncbi.nlm.nih.gov/pubmed/32260433
http://dx.doi.org/10.3390/cancers12040881
_version_ 1783534284220399616
author Okusha, Yuka
Eguchi, Takanori
Tran, Manh T.
Sogawa, Chiharu
Yoshida, Kaya
Itagaki, Mami
Taha, Eman A.
Ono, Kisho
Aoyama, Eriko
Okamura, Hirohiko
Kozaki, Ken-ichi
Calderwood, Stuart K.
Takigawa, Masaharu
Okamoto, Kuniaki
author_facet Okusha, Yuka
Eguchi, Takanori
Tran, Manh T.
Sogawa, Chiharu
Yoshida, Kaya
Itagaki, Mami
Taha, Eman A.
Ono, Kisho
Aoyama, Eriko
Okamura, Hirohiko
Kozaki, Ken-ichi
Calderwood, Stuart K.
Takigawa, Masaharu
Okamoto, Kuniaki
author_sort Okusha, Yuka
collection PubMed
description Matrix metalloproteinase 3 (MMP3) plays multiple roles in extracellular proteolysis as well as intracellular transcription, prompting a new definition of moonlighting metalloproteinase (MMP), according to a definition of protein moonlighting (or gene sharing), a phenomenon by which a protein can perform more than one function. Indeed, connective tissue growth factor (CTGF, aka cellular communication network factor 2 (CCN2)) is transcriptionally induced as well as cleaved by MMP3. Moreover, several members of the MMP family have been found within tumor-derived extracellular vesicles (EVs). We here investigated the roles of MMP3-rich EVs in tumor progression, molecular transmission, and gene regulation. EVs derived from a rapidly metastatic cancer cell line (LuM1) were enriched in MMP3 and a C-terminal half fragment of CCN2/CTGF. MMP3-rich, LuM1-derived EVs were disseminated to multiple organs through body fluid and were pro-tumorigenic in an allograft mouse model, which prompted us to define LuM1-EVs as oncosomes in the present study. Oncosome-derived MMP3 was transferred into recipient cell nuclei and thereby trans-activated the CCN2/CTGF promoter, and induced CCN2/CTGF production in vitro. TRENDIC and other cis-elements in the CCN2/CTGF promoter were essential for the oncosomal responsivity. The CRISPR/Cas9-mediated knockout of MMP3 showed significant anti-tumor effects such as the inhibition of migration and invasion of tumor cells, and a reduction in CCN2/CTGF promoter activity and fragmentations in vitro. A high expression level of MMP3 or CCN2/CTGF mRNA was prognostic and unfavorable in particular types of cancers including head and neck, lung, pancreatic, cervical, stomach, and urothelial cancers. These data newly demonstrate that oncogenic EVs-derived MMP is a transmissive trans-activator for the cellular communication network gene and promotes tumorigenesis at distant sites.
format Online
Article
Text
id pubmed-7226423
institution National Center for Biotechnology Information
language English
publishDate 2020
publisher MDPI
record_format MEDLINE/PubMed
spelling pubmed-72264232020-05-18 Extracellular Vesicles Enriched with Moonlighting Metalloproteinase Are Highly Transmissive, Pro-Tumorigenic, and Trans-Activates Cellular Communication Network Factor (CCN2/CTGF): CRISPR against Cancer Okusha, Yuka Eguchi, Takanori Tran, Manh T. Sogawa, Chiharu Yoshida, Kaya Itagaki, Mami Taha, Eman A. Ono, Kisho Aoyama, Eriko Okamura, Hirohiko Kozaki, Ken-ichi Calderwood, Stuart K. Takigawa, Masaharu Okamoto, Kuniaki Cancers (Basel) Article Matrix metalloproteinase 3 (MMP3) plays multiple roles in extracellular proteolysis as well as intracellular transcription, prompting a new definition of moonlighting metalloproteinase (MMP), according to a definition of protein moonlighting (or gene sharing), a phenomenon by which a protein can perform more than one function. Indeed, connective tissue growth factor (CTGF, aka cellular communication network factor 2 (CCN2)) is transcriptionally induced as well as cleaved by MMP3. Moreover, several members of the MMP family have been found within tumor-derived extracellular vesicles (EVs). We here investigated the roles of MMP3-rich EVs in tumor progression, molecular transmission, and gene regulation. EVs derived from a rapidly metastatic cancer cell line (LuM1) were enriched in MMP3 and a C-terminal half fragment of CCN2/CTGF. MMP3-rich, LuM1-derived EVs were disseminated to multiple organs through body fluid and were pro-tumorigenic in an allograft mouse model, which prompted us to define LuM1-EVs as oncosomes in the present study. Oncosome-derived MMP3 was transferred into recipient cell nuclei and thereby trans-activated the CCN2/CTGF promoter, and induced CCN2/CTGF production in vitro. TRENDIC and other cis-elements in the CCN2/CTGF promoter were essential for the oncosomal responsivity. The CRISPR/Cas9-mediated knockout of MMP3 showed significant anti-tumor effects such as the inhibition of migration and invasion of tumor cells, and a reduction in CCN2/CTGF promoter activity and fragmentations in vitro. A high expression level of MMP3 or CCN2/CTGF mRNA was prognostic and unfavorable in particular types of cancers including head and neck, lung, pancreatic, cervical, stomach, and urothelial cancers. These data newly demonstrate that oncogenic EVs-derived MMP is a transmissive trans-activator for the cellular communication network gene and promotes tumorigenesis at distant sites. MDPI 2020-04-04 /pmc/articles/PMC7226423/ /pubmed/32260433 http://dx.doi.org/10.3390/cancers12040881 Text en © 2020 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Okusha, Yuka
Eguchi, Takanori
Tran, Manh T.
Sogawa, Chiharu
Yoshida, Kaya
Itagaki, Mami
Taha, Eman A.
Ono, Kisho
Aoyama, Eriko
Okamura, Hirohiko
Kozaki, Ken-ichi
Calderwood, Stuart K.
Takigawa, Masaharu
Okamoto, Kuniaki
Extracellular Vesicles Enriched with Moonlighting Metalloproteinase Are Highly Transmissive, Pro-Tumorigenic, and Trans-Activates Cellular Communication Network Factor (CCN2/CTGF): CRISPR against Cancer
title Extracellular Vesicles Enriched with Moonlighting Metalloproteinase Are Highly Transmissive, Pro-Tumorigenic, and Trans-Activates Cellular Communication Network Factor (CCN2/CTGF): CRISPR against Cancer
title_full Extracellular Vesicles Enriched with Moonlighting Metalloproteinase Are Highly Transmissive, Pro-Tumorigenic, and Trans-Activates Cellular Communication Network Factor (CCN2/CTGF): CRISPR against Cancer
title_fullStr Extracellular Vesicles Enriched with Moonlighting Metalloproteinase Are Highly Transmissive, Pro-Tumorigenic, and Trans-Activates Cellular Communication Network Factor (CCN2/CTGF): CRISPR against Cancer
title_full_unstemmed Extracellular Vesicles Enriched with Moonlighting Metalloproteinase Are Highly Transmissive, Pro-Tumorigenic, and Trans-Activates Cellular Communication Network Factor (CCN2/CTGF): CRISPR against Cancer
title_short Extracellular Vesicles Enriched with Moonlighting Metalloproteinase Are Highly Transmissive, Pro-Tumorigenic, and Trans-Activates Cellular Communication Network Factor (CCN2/CTGF): CRISPR against Cancer
title_sort extracellular vesicles enriched with moonlighting metalloproteinase are highly transmissive, pro-tumorigenic, and trans-activates cellular communication network factor (ccn2/ctgf): crispr against cancer
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7226423/
https://www.ncbi.nlm.nih.gov/pubmed/32260433
http://dx.doi.org/10.3390/cancers12040881
work_keys_str_mv AT okushayuka extracellularvesiclesenrichedwithmoonlightingmetalloproteinasearehighlytransmissiveprotumorigenicandtransactivatescellularcommunicationnetworkfactorccn2ctgfcrispragainstcancer
AT eguchitakanori extracellularvesiclesenrichedwithmoonlightingmetalloproteinasearehighlytransmissiveprotumorigenicandtransactivatescellularcommunicationnetworkfactorccn2ctgfcrispragainstcancer
AT tranmanht extracellularvesiclesenrichedwithmoonlightingmetalloproteinasearehighlytransmissiveprotumorigenicandtransactivatescellularcommunicationnetworkfactorccn2ctgfcrispragainstcancer
AT sogawachiharu extracellularvesiclesenrichedwithmoonlightingmetalloproteinasearehighlytransmissiveprotumorigenicandtransactivatescellularcommunicationnetworkfactorccn2ctgfcrispragainstcancer
AT yoshidakaya extracellularvesiclesenrichedwithmoonlightingmetalloproteinasearehighlytransmissiveprotumorigenicandtransactivatescellularcommunicationnetworkfactorccn2ctgfcrispragainstcancer
AT itagakimami extracellularvesiclesenrichedwithmoonlightingmetalloproteinasearehighlytransmissiveprotumorigenicandtransactivatescellularcommunicationnetworkfactorccn2ctgfcrispragainstcancer
AT tahaemana extracellularvesiclesenrichedwithmoonlightingmetalloproteinasearehighlytransmissiveprotumorigenicandtransactivatescellularcommunicationnetworkfactorccn2ctgfcrispragainstcancer
AT onokisho extracellularvesiclesenrichedwithmoonlightingmetalloproteinasearehighlytransmissiveprotumorigenicandtransactivatescellularcommunicationnetworkfactorccn2ctgfcrispragainstcancer
AT aoyamaeriko extracellularvesiclesenrichedwithmoonlightingmetalloproteinasearehighlytransmissiveprotumorigenicandtransactivatescellularcommunicationnetworkfactorccn2ctgfcrispragainstcancer
AT okamurahirohiko extracellularvesiclesenrichedwithmoonlightingmetalloproteinasearehighlytransmissiveprotumorigenicandtransactivatescellularcommunicationnetworkfactorccn2ctgfcrispragainstcancer
AT kozakikenichi extracellularvesiclesenrichedwithmoonlightingmetalloproteinasearehighlytransmissiveprotumorigenicandtransactivatescellularcommunicationnetworkfactorccn2ctgfcrispragainstcancer
AT calderwoodstuartk extracellularvesiclesenrichedwithmoonlightingmetalloproteinasearehighlytransmissiveprotumorigenicandtransactivatescellularcommunicationnetworkfactorccn2ctgfcrispragainstcancer
AT takigawamasaharu extracellularvesiclesenrichedwithmoonlightingmetalloproteinasearehighlytransmissiveprotumorigenicandtransactivatescellularcommunicationnetworkfactorccn2ctgfcrispragainstcancer
AT okamotokuniaki extracellularvesiclesenrichedwithmoonlightingmetalloproteinasearehighlytransmissiveprotumorigenicandtransactivatescellularcommunicationnetworkfactorccn2ctgfcrispragainstcancer

Ejemplares similares