Stellate cell activation

The normal liver contains an epithelial component (hepatocytes), an endothelial lining (endothelial cells), tissue macrophages (Kupffer cells), natural killer cells (NK), and perivascular mesenchymal cell, HSC, which are the key fibrogenic cells (26). The cellular elements of the liver are organized within the sinusoid, with the subendothelial space of Disse separating the epithelium from the sinusoidal endothelium. In normal liver this space contains a non electron-dense basement membrane-like matrix which is essential for maintaining the differentiated function of all resident liver cells (27). As the liver becomes fibrotic, the total content of collagens and non-collagenous components increases and it is accompanied by a shift in the type of ECM in the subendothelial space from the normal low density basement membrane-like matrix to interstitial type matrix containing fibril-forming collagens (mostly collagens I and III) (26). HSC activation is a key feature in excessive ECM deposition (27,28).

Under physiological conditions, HSC comprise about 15% of the total number of resident liver cells (28,29). Their main function is storage and homeostasis of vitamin A and other retinoids, which are stored in cytoplasmic lipid droplets as retinyl esters (29,30). HSC regulate the sinusoidal blood flow, produce apolipoproteins, prostaglandins, growth factors, and cytokines all of which contribute to ECM homeostasis (29,30). Synthesis and degradation of normal hepatic ECM is essential for the integrity of the space of Disse and for the intra- and intercellular communication among neighboring cells (29,30).

Following a fibrogenic stimulus, HSC undergo a complex process of activation in which they become transformed from quiescent to activated myofibroblast-like cells (8,26). Phenotypic changes include stretching, nuclear and cellular enlargement, cytoplasmic spreading, elongation of processes to establish contacts among cells, and loss of lipid droplets (26,29,31). As they become activated, HSC increase a-smooth muscle actin (a-sma) and collagen type I protein expression (26-29,31), they proliferate, and migrate to the site of injury where ECM builds up and scarring occurs (26).

The phenomenon of HSC activation takes place as a sequence of well interrelated events (26,28-31). The first steps encompass rapid changes in gene expression, associated with transcriptional events (e.g. COL1A1 and COL1A2 up-regulation), and induction of immediate early genes, which render the cells responsive to cytokines and other local stimuli from paracrine or autocrine origin (26). The subsequent steps incorporate the cellular events that amplify the activated phenotype through enhanced cytokine expression and responsiveness (26).

The perpetuation of HSC activation involves key phenotypic responses mediated by increased cytokine production and remodeling of ECM. These phenotypic responses of HSC include:

1. Proliferation: increased numbers of HSC in injured liver develop at least in part as a response to local growth factors, most of which signal through receptor tyrosine kinases (32,33). Among these factors, platelet-derived growth factor (PDGF) and TGFb are the best characterized and most powerful (34,35).

3. Fibrogenesis: up-regulation of collagen type I synthesis is among the most striking molecular responses of HSC to injury and is regulated at the transcriptional and translational levels (37-40).

4. Matrix degradation: changes in matrix proteolytic activity lead to remodeling of ECM during liver injury, which accelerate HSC activation (37). A family of matrix-metalloproteinases (MMPs) contributes to either pathologic or restorative matrix degradation (37,41,42). MMPs can be either activated through proteolytic cleavage (43), or inhibited by binding to specific inhibitors known as tissue inhibitors of metalloproteinases (TIMPs) (43). MMP-2, MMP-3, MMP-9 and MT-MMP1 are involved in the degradation of the normal subendothelial ECM which is replaced by fibril-forming collagens, which can stimulate HSC growth (44-46). Furthermore, expression of TIMP-1 in activated HSC inhibits MMP-1, the main metalloproteinase responsible for collagen type I degradation in humans (46,47). Sustained TIMP-1 expression is emerging as a key reason why fibrosis progresses (48, 49). MMPs and TIMPs are sensitive to ROS, reactive nitrogen species, cytokines, and growth factors (44-46,48,49) .

5. Chemotaxis: directed migration of activated HSC enhances their accumulation in areas of injury (34,50). PDGF and monocyte chemotactic protein (MCP-1) are chemoattractants toward activated but not quiescent cells (34,51).

6. Retinoids: loss of intracellular vitamin A is remarkable during HSC activation (52), yet it remains unknown whether it is required for HSC to activate, and also which retinoids might accelerate or prevent activation in vivo (52). Retinoids may be directly linked to fibrogenesis as they stimulate the activation of latent TGFb1, thereby increasing its fibrogenic activity (53).

7. Cytokine release: increased production and activity of cytokines is critical for perpetuation of HSC activation (22,50). ECM is also an important reservoir for growth factors including TGFb1, PDGF, VEGF, fibroblast growth factor (FGF), hepatocyte growth factor (HGF), and platelet activating factor (PAF) (22,32,50). Finally, HSC also release neutrophil and monocyte chemoattractants that can amplify inflammation during liver injury, including colony stimulating factor (CSF), monocyte chemotactic protein-1 (MCP-1), interleukin-6, and cytokine-induced neutrophil chemoattractant/IL-8 (CINC) (54-57). Anti-fibrogenic cytokines produced by HSC have also been identified, in particular IL-10 (58) and TNFa (59).

Alcohol and liver fibrosis

Chronic alcohol liver injury leads to fibrosis, with the subsequent disruption of the liver architecture, and impairment of hepatic metabolism (15,60). The cross-talk between parenchymal and non-parenchymal cells and the excessive production of ECM components are main features in the development of hepatic injury and fibrosis (38,40). Soluble factors, such as cytokines, chemokines, and ROS are candidate mediators for the induction of the fibrogenic response (26,32,40,61). Reactive nitrogen species may also play a role. Initiation of HSC activation is mainly due to paracrine stimulation by injured hepatocytes/bile duct cells, inflammatory cells, activated macrophages and neutrophils, or to early changes in ECM composition (26,32,40). Perpetuation results form autocrine and paracrine stimulation, as well as from accelerated ECM remodeling (26,32,40).

-Paracrine effect of hepatocytes. Alcohol metabolism via CYP2E1 leads ROS production and lipid peroxidation-end products (62). Acetaldehyde, ROS, and long-chain polyunsaturated fatty acids can activate HSC in a paracrine mode (62-65). Acetaldehyde induces COL1A1 and COL1A2 through a TGFb-dependent mechanism (63,64). TGF-b is considered to be the most potent pro-fibrogenic cytokine (35,66). It suppresses hepatocyte proliferation, stimulates HSC activation, promotes ECM production, and mediates hepatocyte apoptosis (3,35,53,67-69). ROS and lipid peroxidation products MDA and 4-HNE can increase collagen type I production in HSC (70-76). ROS also modulate the binding of transcription factors (e.g. c-Jun/AP1, NFkB, Sp1, and Smads) which modulate COL1A1 and COL1A2 transactivation in HSC (27,40,77-79).

-Paracrine effect of Kupffer cells. Ethanol impairs gut permeability leading to overgrowth of Gram negative bacteria (82-85). Endotoxin or lipopolysaccharide (LPS), a component of the Gram negative bacterial wall, translocates from the intestinal lumen into the portal circulation triggering Kupffer cell activation (82-85). Influx of Kupffer cells coincides with the appearance of HSC activation markers (e.g. PDGFRb and a-sma) (86). Kupffer cells may stimulate matrix synthesis, cell proliferation, and release of retinoids by HSC through the actions of cytokines and reactive species (57). They can also influence HSC through secretion of MMP-9 because it can activate latent TGFb1, stimulating HSC collagen I synthesis (87). Lastly, Kupffer cells generate ROS either via NADPH oxidase (88), xanthine oxidase (89), mitochondria (89), or possibly CYP2E1 (90), which in turn, may enhance HSC activation and collagen I synthesis (13,91). These effects are enhanced under ethanol treatment, and a role for polyunsaturated fatty acids should be considered as critical components which promote injury in several in vitro and in vivo models of ethanol administration (85,92). Kupffer cells also produce nitric oxide (NO), which can counterbalance the stimulatory effects of ROS by reducing HSC proliferation, contractility, and collagen I production; however, NO may also react with O₂^.- to generate peroxynitrite (ONOO-), whose potential effects on HSC collagen I production are unknown and worth exploring. TNFa acts as an antifibrogenic, down-regulating COL1A1 and COL1A2 promoters both in humans and in rodents (40,59,93).

-Paracrine effect of sinusoidal endothelial cells. Injury of sinusoidal endothelial cells by ROS and acetaldehyde stimulates the production of certain fibronectin isoforms, such as leptin, which may activate HSC (94). Moreover, damaged endothelial cells convert latent TGF-b1 into its active form (22,95). Also, sinusoidal endothelial cells increase the expression of vascular endothelial growth factor (VEGF) in response to injury (96). VEGF binds to its receptors in HSC and promote their activation enhancing the expression of procollagen type I (96).

-Paracrine and autocrine effect of HSC. Activated HSC secrete inflammatory chemokines e.g. TNFa, TGFb, IL6, and PDGF which regulate collagen type I at the transcriptional and translational level (28,33,40,50,97). Activated HSC also secrete angiotensin II, which induces fibrogenic actions via NADPH oxidase (41,42). HSC are the master regulators for ECM remodeling. An expanding family of matrix-metalloproteinases (MMPs) contributes to either pathologic or restorative matrix degradation (41,42). These enzymes fall into five categories based on substrate specificity: interstitial collagenases (MMP-1, -8, -13), gelatinases (MMP-2, -9), stromelysins (MMP-3, -7, -10, -11), membrane-type metalloproteinases (MMP-14 or MT1-MMP, -15, -16, -17, -24, -25) and metalloelastase (MMP-12) (41,42). Metalloproteinases can be either activated through proteolytic cleavage, or inhibited by binding to specific inhibitors known as tissue inhibitors of metalloproteinases (TIMPs) (45). Liver ‘pathologic' matrix degradation refers to early disruption of the normal subendothelial matrix which occurs through the actions of four enzymes: MMP-2 and MMP-9, which degrade type IV collagen; MT1-MMP, which activates latent MMP-2; and MMP-3, which degrades proteoglycans and glycoproteins, and also activates latent collagenases (43). Failure to degrade the accumulated scar is a major reason why fibrosis progresses to cirrhosis (7). In humans, MMP-1 (in rats, MMP-13) is the main protease which degrades type I collagen, the principal collagenous protein in liver fibrosis (98). Alternatively, it is possible that other enzymes such as MT1-MMP and MMP-2 may have interstitial collagenase activity (98). More importantly, progressive fibrosis is associated with marked increases in TIMP-1 and TIMP-2 (44,46), leading to a net decrease in protease activity, and therefore matrix accumulation. HSC are the major source of these inhibitors (44,46).

-Role of innate immunity. Alcohol consumption mediates suppression of the innate immunity as decreases NK cells activity and their numbers (99,100). The liver immune system is comprised of Kupffer cells, NK cells, NK-T cells and interferon alpha and gamma (IFNa and IFNg). NK cells may kill activated HSC while IFNa and IFNg block TGF-b1 signaling and HSC activation (101,102).

Reversion and treatment

Current questionable trends of thought suggest that reversion of fibrosis may happen by inducing apoptosis or necrosis of activated HSC, or less likely by transformation of activated HSC to a more quiescent phenotype.

-Apoptosis of activated HSC. Spontaneous resolution of experimental fibrosis is associated with the clearance of collagen type I-producing a-sma positive myofibroblasts (activated HSC and transdifferentiated portal fibroblasts) (103). HSC clearance has been attributed to the induction of apoptosis (103). Apoptosis of myofibroblasts is associated with decreased expression of TIMP1, which protects activated HSC from apoptosis, and increased MMP-1 activity in the liver (103).

-Reverse trans-differentiation of activated HSC to quiescent phenotype. One theoretical approach to reverse fibrosis is the reverse trans-differentiation of activated HSC to a more quiescent phenotype. Quiescent HSC are full of vitamin A and triglycerides which are depleted in the activated HSC (26,28). The adipogenic/lipogenic transcriptional regulation conferred by PPAR, LXR, and SREBP-1c is required for the maintenance of the fat-storing quiescence phenotype of HSC (104). Expression of these transcription factors is lost in activated HSC (104). On the other hand, treatment of the activated HSC with an adipocyte differentiation cocktail or ectopic expression of PPARg or SREBP-1c causes their reversal to the quiescent phenotype (105-107).

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Correspondence:
Natalia Nieto.
Department of Medicine.
Division of Lier Diseases.
Mount Sinai School of Medicine.
Box 1123. 1425 Madison Avenue.
Room 11-76.
New York 10029. USA. ]]> Fax: 1-212-849-2574.
e-mail: natalia.nieto@mssm.edu

Recibido: 06-09-06.
Aceptado: 06-09-06.