Hepatocyte Produced Matrix Metalloproteinases Are Regulated by CD147 in Liver Fibrogenesis

Calabrò, S; Maczurek, Annette; Morgan, A.J.; Tu, Thomas; Wen, Victoria W.; Yee, Christine; Mridha, Auvro R.; Lee, Maggie; d’Avigdor, W.; Locarnini, Stephen; McCaughan, Geoffrey W.; Warner, Fiona J.; McLennan, Susan V.; Shackel, Nicholas

doi:10.1371/journal.pone.0090571

Cited by 48 publications

(50 citation statements)

References 65 publications

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“…In situ hybridization and immunohistochemistry on tissue sections and primary isolated hepatocytes showed heterogeneous expression of MMP‐2, MMP‐3, and MMP‐13 as well as TIMP‐1 and TIMP‐2 in lobules in CCl 4 ‐induced fibrosis and with fibrosis resolution . This finding was validated by our group as we have found significant expression of MMP‐2, MMP‐9, MMP‐13, and MMP‐14 in human and murine hepatocytes mediated by the glycoprotein CD147 with liver injury . In vitro hepatocytes were shown to be essential for MMP‐2 activation in untreated HSC cultures, and this has been attributed to hepatocyte‐derived MT2‐MMP .…”

Section: The Case For An Accomplice Role For Hepatocytes In Progressisupporting

confidence: 68%

“…Degradation of fibrous tissue is accompanied by intrahepatic upregulation of MMP‐1, MMP‐2, and MMP‐8 and downregulation of TIMP‐1 and TIMP‐2 . The cellular origins of the MMPs leading to the resolution of fibrosis are HSCs, inflammatory infiltrate (in particular macrophages), and hepatocytes . Further, apoptosis of activated HSCs is known to be an important factor in the resolution of fibrosis .…”

Section: Current Cellular Model Of Liver Injurymentioning

confidence: 99%

“…39 The cellular origins of the MMPs leading to the resolution of fibrosis are HSCs, inflammatory infiltrate (in particular macrophages), and hepatocytes. 40 Further, apoptosis of activated HSCs is known to be an important factor in the resolution of fibrosis. 12 Interestingly, there is evidence that HSC apoptosis is inhibited by TIMP-1, which also decreases in injury resolution through the inhibition of MMP activity.…”

Section: Initiation Of Injurymentioning

confidence: 99%

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Hepatocytes in liver injury: Victim, bystander, or accomplice in progressive fibrosis?

Calabrò

Lee

et al. 2015

J of Gastro and Hepatol

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Chronic liver disease causes significant morbidity and mortality through progressive fibrosis, cirrhosis, and liver cancer. The classical theory of fibrogenesis has hepatic stellate cells (HSCs) as the principal and only significant source of abnormal extracellular matrix (ECM). Further, HSCs have the major role in abnormal ECM turnover. It is the death of hepatocytes, as the initial target of injury, that initiates a sequence of events including the recruitment of inflammatory cells and activation of HSCs. Following this initial response, the ongoing insult to hepatocytes is regarded as perpetuating injury, but otherwise, hepatocytes are regarded as "victims" and "bystanders" in progressive fibrosis. Recent developments, however, challenge this view and suggest the concept of the hepatocyte being an active participant in liver injury. It is clear now that hepatocytes undergo phenotypic changes, adapt to injury, and react to the altered microenvironment. In this review, we describe studies showing that hepatocytes contribute to progressive fibrosis by direct manipulation of the surrounding ECM and through signaling to effector cells, particularly HSCs and intrahepatic immune cells. Together, these findings suggest an active "accomplice" role for the hepatocyte in progressive liver fibrosis and highlight novel pathways that could be targeted for development of future anti-fibrotic therapies.

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Section: The Case For An Accomplice Role For Hepatocytes In Progressisupporting

confidence: 68%

Section: Current Cellular Model Of Liver Injurymentioning

confidence: 99%

Section: Initiation Of Injurymentioning

confidence: 99%

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Hepatocytes in liver injury: Victim, bystander, or accomplice in progressive fibrosis?

Calabrò

Lee

et al. 2015

J of Gastro and Hepatol

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“…Furthermore, hepatocytes have been investigated as a source of TIMPs and other matrix modulators protein. Thus, they could play a role in processes of fibrogenesis and fibrosis regeneration 59 . Fibrosis progresses by HSCs, and hepatocyte damage deteriorates 20 .…”

Section: Discussionmentioning

confidence: 99%

Anti-fibrotic Effects of Synthetic Oligodeoxynucleotide for TGF-β1 and Smad in an Animal Model of Liver Cirrhosis

Kim

et al. 2017

Molecular Therapy - Nucleic Acids

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Liver fibrosis is characterized by changes in tissue architecture and extracellular matrix composition. Liver fibrosis affects not only hepatocytes but also the non-parenchymal cells such as hepatic stellate cells (HSCs), which are essential for maintaining an intact liver structure and function. Transforming growth factor β1 (TGF-β1) is a multifunctional cytokine that induces liver fibrosis through activation of Smad signaling pathways. To improve a new therapeutic approach, synthetic TGF-β1/Smad oligodeoxynucleotide (ODN) was used to suppress both TGF-β1 expression and Smad transcription factor using a combination of antisense ODN and decoy ODN. The aims of this study are to investigate the anti-fibrotic effects of TGF-β1/Smad ODN on simultaneous suppressions of both Smad transcription factor and TGF-β1 mRNA expression in the hepatic fibrosis model in vitro and in vivo. Synthetic TGF-β1/Smad ODN effectively inhibits Smad binding activity and TGF-β1 expression. TGF-β1/Smad ODN attenuated the epithelial mesenchymal transition (EMT) and activation of HSCs in TGF-β1-induced AML12 and HSC-T6 cells. TGF-β1/Smad ODN prevented the fibrogenesis and deposition of collagen in CCl4-treated mouse model. Synthetic TGF-β1/Smad ODN demonstrates anti-fibrotic effects that are mediated by the suppression of fibrogenic protein and inflammatory cytokines. Therefore, synthetic TGF-β1/Smad ODN has substantial therapeutic feasibility for the treatment of liver fibrotic diseases.

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“…14 MMPs act as a part of a proteolytic network, in which proteases activate each other by processing inactive proforms. For instance, it has been shown that proMMP-2 is activated by MT-MMP-1 (MMP-14) in complex with TIMP-2, 15 and further MMP-2 and MT-MMP-1 are activated by proMMP-13.…”

mentioning

confidence: 99%

Metalloproteinases in liver fibrosis: current insights

Zbodakova¹,

Chalupský²,

Turečková³

et al. 2017

MNM

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Liver fibrosis is defined by excessive deposition of extracellular matrix. The fibrotic conditions result from the imbalance between synthesis and deposition of fibrous tissues and decomposition of these matrix proteins. This process can be reversed as a regular part of the healing process after hepatic damage or can become chronic. When the protein matrix synthesis predominates and the decomposition is suppressed, fibrosis will progress into irreversible cirrhosis or steatosis. Among the molecular players involved in fibrotic liver diseases, metalloproteinases of matrix metalloproteinase (MMP) and a disintegrin and metalloproteinase (ADAM) families are critical in the development of liver fibrosis and its resolution. Previously, MMPs were recognized as extracellular matrix degrading enzymes. Currently, they are also known as mediators in a variety of processes related to immunity and tissue repair. In this article, we have reviewed the models of liver fibrosis and findings on MMPs and ADAMs in hepatic fibrosis conditions.

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Hepatocyte Produced Matrix Metalloproteinases Are Regulated by CD147 in Liver Fibrogenesis

Cited by 48 publications

References 65 publications

Hepatocytes in liver injury: Victim, bystander, or accomplice in progressive fibrosis?

Hepatocytes in liver injury: Victim, bystander, or accomplice in progressive fibrosis?

Anti-fibrotic Effects of Synthetic Oligodeoxynucleotide for TGF-β1 and Smad in an Animal Model of Liver Cirrhosis

Metalloproteinases in liver fibrosis: current insights

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