MiR‐21 role in aspirin‐dependent PPARα and multidrug resistance protein 4 upregulation

Massimi, Isabella; Alemanno, Laura; Guarino, Maria; Guerriero, Raffaella; Frati, Luigi; Biasucci, Luigi M.; Pulcinelli, Fabio

doi:10.1002/rth2.12104

Cited by 6 publications

(3 citation statements)

References 32 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…These data are in line withAn et al (2018) who observed a significant decrease in IL-1β mRNA levels by clopidogrel treatment.Likewise,clopidogrel significantly decreased the hepatic expressions of TIMP1 and TGF-β1, compared toαnaphthylisothiocyanate (xenobiotic)-exposed protease activated receptor-4 in mice treated with vehicle (Joshi et al, 2016). Regarding PPARα, rarelydata linking PPARα with clopidogrel, but contrarily to the present study, Massimi et al (2018) showed that, cells treated with Aspirin, an anti-platelet drug, had up-regulated PPARα mRNA. Anti-platelet treatment by clopidogrel in NALFD ameliorated the hepatic inflammation (Sitia et al, 2013) and abolished vascular inflammatory responses and remodeling (An et al, 2018), as platelet granules contain a variety of factors including TGFβ that are secreted upon platelet activation (Denslow et al, 2017),and a linear correlation of plasma TIMP1 levels and platelet count has been observed by the lower circulating TIMP1 levels in patients on clopidogrel treatment (Nagy et al, 2016).…”

Section: Discussionsupporting

confidence: 48%

Grape Seed Proanthocyanidin Extract And Antiplatelet drug (Clopidogrel) Alleviates Nonalcoholic Fatty Liver Disease Via Inhibition Of Hepatic Inflammation In Rats

Hussein

zaid

Azab

et al. 2021

Benha Veterinary Medical Journal

View full text Add to dashboard Cite

Non-alcoholic fatty liver disease (NAFLD) is a complex disease caused by a number of different pathogenic processes as a result of the systemic interaction between the liver and several other organs. Grape seeds proanthocyanidins extract (GSPE) potency in the liver is associated with improvement of the hepatic enzyme activities as their powerful antioxidant property results from its ability to directly scavenge free radicals and/or chelate metals. Thirty-two male albino rats were assigned into 4 equal groups of 8 rats as: Normal control group (G1): Rats fed ordinary normal diet for 12 weeks. NAFLD group (G2): Rats provided with HFD-diet for 6 weeks for NAFLD induction, followed by ordinary normal diet for another 6 weeks. NAFLD + GSPE treated group (G3): Rats fed HFD for 6 weeks (NAFLD) followed by administration of GSPE for another 6 weeks. NAFLD + GSPE + clopidogrel treated group (G4): Rats fed HFD for 6 weeks, followed by administration of GSPE and clopidogrel for additional 6 weeks. The results revealed that treatment with GSPE or in combination with clopidogrel (G3, G4) significantly decreased the higher activities of serum AST, ALT and γ GT in NAFLD induced rats (G2). Interestingly, the gene expressions ofIL-1β, PPARα, TGF-β1 and TIMP1 inliver tissue significantly down regulated in GSPE (G3) and GSPE + clopidogrel (G4) treated groups as compared with NAFLD group (G2). In conclusion, treatment with GSPE and in combination with clopidogrel is alternative therapiesand powerful anti-inflammatory, protect liver cells against fatty liver disease via restoring the hepatocytes function and inflammatory mediators.

show abstract

Section: Discussionsupporting

confidence: 48%

Grape Seed Proanthocyanidin Extract And Antiplatelet drug (Clopidogrel) Alleviates Nonalcoholic Fatty Liver Disease Via Inhibition Of Hepatic Inflammation In Rats

Hussein

zaid

Azab

et al. 2021

Benha Veterinary Medical Journal

View full text Add to dashboard Cite

show abstract

“…[2][3][4][5][6] Studies have shown that chronic use of aspirin can enhance expression of several proteins that can potentially affect cardiovascular outcomes. 7,8 In particular, it has been demonstrated that aspirin modulates miRNAs 9,10 and gene expression, such as the nuclear receptor PPARα modulation resulting in an increase in platelet MRP4. 11 Importantly, increased expression of MRP4 in platelets contributes to HARPR.…”

Section: Introductionmentioning

confidence: 99%

Aspirin-Dependent Effects on Purinergic P2Y1 Receptor Expression

et al. 2019

Self Cite

View full text Add to dashboard Cite

Chronic treatment with aspirin in healthy volunteers (HVs) is associated with recovery of adenosine diphosphate (ADP)-induced platelet activation. The purinergic P2Y1 receptor exerts its effects via a Gq-protein, which is the same biochemical pathway activated by thromboxane-A2 receptor. We hypothesized that recovery of ADP-induced platelet activation could be attributed to increased P2Y1 expression induced by chronic aspirin exposure. We performed a multi-phase investigation which embraced both in vitro and in vivo experiments conducted in (1) human megakaryoblastic DAMI cells, (2) human megakaryocytic progenitor cell cultures, (3) platelets obtained from HVs treated with aspirin and (4) platelets obtained from aspirin-treated patients. DAMI cells treated with aspirin or WY14643 (PPARα agonist) had a significant up-regulation of P2Y1 mRNA, which was shown to be a PPARα-dependent process. In human megakaryocytic progenitors, in the presence of aspirin or WY14643, P2Y1 mRNA expression was higher than in mock culture. P2Y1 expression increased in platelets obtained from HVs treated with aspirin for 8 weeks. Platelets obtained from patients who were on aspirin for more than 2 months had increased P2Y1 expression and ADP-induced aggregation compared with patients on aspirin treatment for less than a month. Overall, our results suggest that aspirin induces genomic changes in megakaryocytes leading to P2Y1 up-regulation and that PPARα is the nuclear receptor involved in this regulation. Since P2Y1 is coupled to the same Gq-protein of thromboxane-A2 receptor, platelet adaptation in response to pharmacological inhibition seems not to be receptor specific, but may involve other receptors with the same biochemical pathway.

show abstract

“…Aspirin (50 μ mol/L) therapy in human megakaryocytes reduced miR-21 and upregulated MRP4. miR-21 inhibited MRP4 and PPAR α transcription, and aspirin prevented these events [ 74 ].…”

Section: Effects Of Aspirin On Ncrnas In Different Conditionsmentioning

confidence: 99%

Noncoding RNA Roles in Pharmacogenomic Responses to Aspirin: New Molecular Mechanisms for an Old Drug

Tabari

Mishan

Moradi

et al. 2021

BioMed Research International

View full text Add to dashboard Cite

Aspirin, as one of the most frequently prescribed drugs, can have therapeutic effects on different conditions such as cardiovascular and metabolic disorders and malignancies. The effects of this common cardiovascular drug are exerted through different molecular and cellular pathways. Altered noncoding RNA (ncRNA) expression profiles during aspirin treatments indicate a close relationship between these regulatory molecules and aspirin effects through regulating gene expressions. A better understanding of the molecular networks contributing to aspirin efficacy would help optimize efficient therapies for this very popular drug. This review is aimed at discussing and highlighting the identified interactions between aspirin and ncRNAs and their targeting pathways and better understanding pharmacogenetic responses to aspirin.

show abstract

MiR‐21 role in aspirin‐dependent PPARα and multidrug resistance protein 4 upregulation

Cited by 6 publications

References 32 publications

Grape Seed Proanthocyanidin Extract And Antiplatelet drug (Clopidogrel) Alleviates Nonalcoholic Fatty Liver Disease Via Inhibition Of Hepatic Inflammation In Rats

Grape Seed Proanthocyanidin Extract And Antiplatelet drug (Clopidogrel) Alleviates Nonalcoholic Fatty Liver Disease Via Inhibition Of Hepatic Inflammation In Rats

Aspirin-Dependent Effects on Purinergic P2Y1 Receptor Expression

Noncoding RNA Roles in Pharmacogenomic Responses to Aspirin: New Molecular Mechanisms for an Old Drug

Contact Info

Product

Resources

About