Epigenetic Effects of an Adenosine Derivative in a Wistar Rat Model of Liver Cirrhosis

Rodríguez‐Aguilera, Jesús Rafael; Guerrero‐Hernández, Carlos; Pérez‐Molina, Rosario; Cadena‐del‐Castillo, Carla Elizabeth; Vaca, Rebeca Pérez‐Cabeza de; Guerrero‐Celis, Nuria; Domínguez‐López, Mariana; Murillo‐de‐Ozores, Adrián Rafael; Arzate-Mejía, Rodrigo G.; Recillas‐Targa, Félix; Sánchez, Victoria Chagoya de

doi:10.1002/jcb.26192

Cited by 15 publications

(21 citation statements)

References 37 publications

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“…During different stages of chronic liver injury, 5hmC was found reduced, while hepatic stellate cells became transdifferentiated [111]. Consistent with these data, global 5hmC was shown to be reduced in a rat model of CCl4-induced cirrhosis [112]. It is important to note the recent availability of liver methylome and hydroxymethylome data on Wistar and Sprague-Dawley rats, as well as the genome-wide distribution of enhancer related chromatin marks (i.e., H3K4me1 and H3K27ac), which could represent a baseline reference for future studies of liver pathology [113].…”

Section: Perspectives and Concluding Remarkssupporting

confidence: 77%

5-Hydroxymethylcytosine (5hmC), or How to Identify Your Favorite Cell

2018

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Abstract:Recently described as the sixth base of the DNA macromolecule, the precise role of 5-hydroxymethylcytosine (5hmC) is the subject of debate. Early studies indicate that it is functionally distinct from cytosine DNA methylation (5mC), and there is evidence for 5hmC being a stable derivate of 5mC, rather than just an intermediate of demethylation. Moreover, 5hmC events correlate in time and space with key differentiation steps in mammalian cells. Such events span the three embryonic germ layers and multiple progenitor cell subtypes, suggesting a general mechanism. Because of the growing understanding of the role of progenitor cells in disease origin, we attempted to provide a detailed summary on the currently available literature supporting 5hmC as a key player in adult progenitor cell differentiation. This summary consolidates the emerging role for 5hmC in defining cellular fate.

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Section: Perspectives and Concluding Remarkssupporting

confidence: 77%

5-Hydroxymethylcytosine (5hmC), or How to Identify Your Favorite Cell

2018

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“…With these results and in order to assess DNA methylation dynamics, 5hmC levels were measured and a similar behavior to the one observed with 5mC, a reduction of 5hmC in cirrhosis in concordance with group of Mann findings, was found [89]. Treatment with IFC-305 triggers a regaining of both 5mC and 5hmC [16]. These results together suggest that there is a perturbation of DNA methylation dynamic during cirrhosis, while IFC-305 is able to modulate this dynamic, possibly reducing chromosome instability.…”

Section: Gene Expression Deregulation In Cirrhosis and Ifc-305 Modulasupporting

confidence: 70%

“…Rats are intraperitoneal treated with 0.04 g/kg body weight of CCl 4 three times per week, during 10 weeks. After this time it is possible to observe a liver distortion, the formation of nodules, bilirubin accumulation and hepatomegaly [16], the generation of a fibrotic area of 16% of the tissue, and a reduction in parenchyma surface to around 78%. As a consequence of these liver architecture changes, there are alterations of liver function: serum samples of cirrhotic rats display elevated AST, ALT, and bilirubin levels and albumin are relatively reduced [17].…”

Section: Biochemical and Physiological Alteration Of Liver During Cirmentioning

confidence: 99%

“…IFC-305 is able to reduce the levels to healthy-like levels for three fibrogenic genes (Fn1, Col1a1,andTgfb1), C9, Apob1 and Hdac3; meanwhile, this compound generates the increasing expression of Pparg and Cps1 recovering the levels of the healthy liver and partially restoring the levels of Ass1 [17]. Analyzing proteins, we could identify an increment in collagen I and HDAC3 and a reduction of PPARγ during cirrhosis, and the treatment with IFC-305 resembles the healthy-like levels of these three proteins [16]. Thus, through this quantitative analysis of expression and protein levels, IFC-305 shows capabilities to modulate the gene expression of some important genes involved in liver fibrogenesis.…”

Section: Gene Expression Deregulation In Cirrhosis and Ifc-305 Modulamentioning

confidence: 99%

“…We have previously shown that adenosine can modulate trans-methylation reactions, like methylation of phospholipids, via regulation of S-adenosylmethionine (SAM) levels [87], so that we make an approach to SAM levels and found that during cirrhosis, the amount of this molecule is diminished, whereas IFC-305 treatment restored the physiological levels; this suggests that during cirrhosis, it could be an imbalance of methylation reactions, and IFC-305, like adenosine, could also regulate this process [16].…”

Section: Gene Expression Deregulation In Cirrhosis and Ifc-305 Modulamentioning

confidence: 99%

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Molecular and Cellular Aspects of Cirrhosis and How an Adenosine Derivative Could Revert Fibrosis

Rodríguez‐Aguilera¹,

Vaca²,

Guerrero‐Celis³

et al. 2019

Liver Cirrhosis - Debates and Current Challenges

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Hepatic fibrosis occurs in response to persistent liver damage and is characterized by an excessive accumulation of extracellular matrix. When the damage is prolonged, there is a chronic inflammation and persistent hepatic fibrosis eventually leads to cirrhosis, where in addition to the scar, there is an important vascular remodeling associated with portal hypertension and, if decompensated, leads to death or can develop hepatocellular carcinoma. We have been studying the pharmacologic functions of adenosine, finding that a derivative of this nucleoside, IFC-305, shows hepatoprotective effects in a CCl 4-induced rat cirrhosis model where it reverses liver fibrosis through modulation of fibrosis-related genes and by ameliorating hepatic function. Furthermore, this compound has the property to rescue cell cycle inhibition in vivo, prevents hepatic stellate cell activation, modulates antiinflammatory macrophage polarization, and favors a chromatin context that could decrease the genomic instability and characteristics of cirrhosis, enabling the recovery of gene expression profile. Here we show results that contribute to the comprehension of molecular and cellular mechanism of cirrhosis, give the opportunity to suggest biomarkers to the early diagnostic of this pathology, and constitute the fundaments to suggest IFC-305 as a coadjuvant for treatment of this disease.

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