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

Abstract: 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 t… Show more

“…Earlier studies showed that MMPs constituted a large family of zinc/calcium-dependent endopeptidases, playing key roles in extracellular matrix (ECM) remodeling because of their ability to degrade numerous components of ECM (such as collagens and proteoglycans) and non-ECM proteins (such as adhesion molecules, cytokines, protease inhibitors, and membrane receptors) [24]. Later studies have shown that matrix metalloproteinase 3 (MMP3) was a bifunctional protein that acted as a proteolytic enzyme and a transcriptional factor, playing crucial roles in tumor progression [30][31][32]. Therefore, we defined MMP3 as a moonlighting protein, as it plays multiple roles in the cells as a proteinase as well as a transcription factor [32,33].…”

“…Later studies have shown that matrix metalloproteinase 3 (MMP3) was a bifunctional protein that acted as a proteolytic enzyme and a transcriptional factor, playing crucial roles in tumor progression [30][31][32]. Therefore, we defined MMP3 as a moonlighting protein, as it plays multiple roles in the cells as a proteinase as well as a transcription factor [32,33]. It has been shown that some members of MMPs were expressed at high levels in particular cancer types and promoted tumor progression.…”

“…It has been shown that some members of MMPs were expressed at high levels in particular cancer types and promoted tumor progression. We have compared protumorigenic phenotypes of rapidly metastatic murine cancer cell line LuM1 with a parental cancer cell line Colon26 (aka CT26) [31,32,[34][35][36] and shown that MMP3 and MMP9 were highly expressed in LuM1 cells. The RNA interference (RNAi)-mediated knockdown of MMP3 and/or MMP9 significantly attenuated tumor growth and metastasis in the tumor allograft mouse model [31].…”

“…The RNA interference (RNAi)-mediated knockdown of MMP3 and/or MMP9 significantly attenuated tumor growth and metastasis in the tumor allograft mouse model [31]. Most recently, we established MMP3-knockout (KO) cells using CRISPR/Cas9 genome editing technology on the LuM1 cells and then compared the oncogenic effects of MMP3-KO cells versus LuM1 cells [32]. This study indicated that knockout of Mmp3 results in a significant inhibition of tumor growth in vivo, cellular migration and invasion in vitro [32].…”

“…Most recently, we established MMP3-knockout (KO) cells using CRISPR/Cas9 genome editing technology on the LuM1 cells and then compared the oncogenic effects of MMP3-KO cells versus LuM1 cells [32]. This study indicated that knockout of Mmp3 results in a significant inhibition of tumor growth in vivo, cellular migration and invasion in vitro [32]. However, a mechanism of how MMP3 enriched EVs influences the characteristics of EVs and tumors has not been completed yet.…”

Knockout of MMP3 Weakens Solid Tumor Organoids and Cancer Extracellular Vesicles

“…Earlier studies showed that MMPs constituted a large family of zinc/calcium-dependent endopeptidases, playing key roles in extracellular matrix (ECM) remodeling because of their ability to degrade numerous components of ECM (such as collagens and proteoglycans) and non-ECM proteins (such as adhesion molecules, cytokines, protease inhibitors, and membrane receptors) [24]. Later studies have shown that matrix metalloproteinase 3 (MMP3) was a bifunctional protein that acted as a proteolytic enzyme and a transcriptional factor, playing crucial roles in tumor progression [30][31][32]. Therefore, we defined MMP3 as a moonlighting protein, as it plays multiple roles in the cells as a proteinase as well as a transcription factor [32,33].…”

“…Later studies have shown that matrix metalloproteinase 3 (MMP3) was a bifunctional protein that acted as a proteolytic enzyme and a transcriptional factor, playing crucial roles in tumor progression [30][31][32]. Therefore, we defined MMP3 as a moonlighting protein, as it plays multiple roles in the cells as a proteinase as well as a transcription factor [32,33]. It has been shown that some members of MMPs were expressed at high levels in particular cancer types and promoted tumor progression.…”

“…It has been shown that some members of MMPs were expressed at high levels in particular cancer types and promoted tumor progression. We have compared protumorigenic phenotypes of rapidly metastatic murine cancer cell line LuM1 with a parental cancer cell line Colon26 (aka CT26) [31,32,[34][35][36] and shown that MMP3 and MMP9 were highly expressed in LuM1 cells. The RNA interference (RNAi)-mediated knockdown of MMP3 and/or MMP9 significantly attenuated tumor growth and metastasis in the tumor allograft mouse model [31].…”

“…The RNA interference (RNAi)-mediated knockdown of MMP3 and/or MMP9 significantly attenuated tumor growth and metastasis in the tumor allograft mouse model [31]. Most recently, we established MMP3-knockout (KO) cells using CRISPR/Cas9 genome editing technology on the LuM1 cells and then compared the oncogenic effects of MMP3-KO cells versus LuM1 cells [32]. This study indicated that knockout of Mmp3 results in a significant inhibition of tumor growth in vivo, cellular migration and invasion in vitro [32].…”

“…Most recently, we established MMP3-knockout (KO) cells using CRISPR/Cas9 genome editing technology on the LuM1 cells and then compared the oncogenic effects of MMP3-KO cells versus LuM1 cells [32]. This study indicated that knockout of Mmp3 results in a significant inhibition of tumor growth in vivo, cellular migration and invasion in vitro [32]. However, a mechanism of how MMP3 enriched EVs influences the characteristics of EVs and tumors has not been completed yet.…”

Knockout of MMP3 Weakens Solid Tumor Organoids and Cancer Extracellular Vesicles

Extracellular Vesicle-Associated Moonlighting Proteins: Heat Shock Proteins and Metalloproteinases

Protocol for CRISPR/Cas Genome Editing for Investigating Cell Communication Network