Quercetin inhibits the expression of MYC and CYP2E1 and reduces oxidative stress in the myocardium of spontaneously hypertensive rats

Maksymchuk, Oksana; Shysh, Angela; Kotliarova, A.B.

doi:10.18388/abp.2020_6517

Cited by 4 publications

(6 citation statements)

References 24 publications

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“…A study demonstrated that quercetin significantly declines oxidative stress by reducing the expression of CYP2E1 resulting in diminish lipid peroxidation or free radical generation. [76] The other three compounds also showed favorable docking scores with CYP2E1. The regulation of hepatic CYP2E1's physiological expression is principally governed by the transcription factors hepatocyte nuclear factor-alpha (HNF-α) and NF-kB in the context of inflammatory conditions.…”

Section: Discussionmentioning

confidence: 92%

“…The protein‐ligand interaction image presented shows quercetin forms hydrogen bonds with three residues, Val388, Asn220, and Asp102, of CYP2E1 (Supplementary file). A study demonstrated that quercetin significantly declines oxidative stress by reducing the expression of CYP2E1 resulting in diminish lipid peroxidation or free radical generation [76] . The other three compounds also showed favorable docking scores with CYP2E1.…”

Section: Discussionmentioning

confidence: 99%

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Longevity Spinach (Gynura procumbens) Ameliorated Oxidative Stress and Inflammatory Mediators in Cisplatin‐Induced Organ Dysfunction in Rats: Comprehensive in vivo and in silico Studies

Chandra Shill,

El‐Nashar,

Prova Mollick

et al. 2024

Chemistry & Biodiversity

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This study aimed to investigate the efficacy of Gynura procumbens (GP) leaf extract against cisplatin (CP)‐induced hepatorenal complications in Wister albino rats. Additionally, it aims to detect pol‐yphenolic compounds using high‐performance liquid chromatography with diode‐array detection (HPLC‐DAD). The rats were treated intraperitoneally with CP (7.5mg/kg) to mediate hepatorenal damage. They were then treated with GP extract (75 and 150mg/kg, P.O.) for 7 consecutive days. CP‐mediated hepatorenal biomarkers like alkaline phosphatase, alanine aminotransferase, aspar‐tate aminotransferase, creatinine and blood urea nitrogen levels were normalized by GP extract in a dose‐dependent manner. Similarly, it significantly reduced CP‐induced oxidative stress inducers including nitric oxide and advanced oxidative protein products. Besides, it enhanced the antioxi‐dant enzymes, and glutathione levels. Histopathological studies showed that CP caused collagen accumulation in the liver and kidney tissues. GP extract drained the collagen mass and acted against hepatorenal damage. Ellagic acid, gallic acid, quercetin hydrate, kaempferol, and rutin hydrate were revealed in GP extract. In‐silico modelling showed good docking scores of the polyphenolic compounds with molecular targets including CYP4502E1, NF‐κB, caspase‐3, and TNF‐α. GP could be an effective therapeutic option for management of anticancer drugs’ complications like CP‐induced organ damage, although clinical studies are required to establish herbal formulation.

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Section: Discussionmentioning

confidence: 92%

Section: Discussionmentioning

confidence: 99%

Longevity Spinach (Gynura procumbens) Ameliorated Oxidative Stress and Inflammatory Mediators in Cisplatin‐Induced Organ Dysfunction in Rats: Comprehensive in vivo and in silico Studies

Chandra Shill,

El‐Nashar,

Prova Mollick

et al. 2024

Chemistry & Biodiversity

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“…The myocardium of spontaneously hypertensive rats (SHRs) overexpresses MYC and its downstream target CYP2E1, whose overexpression leads to oxidative stress and other pathological processes. Long-term treatment with quercetin, a flavonoid with potential cardiovascular beneficial effects, resulted in a significant reduction of blood pressure with concomitant downregulation of MYC and CYP2E1, significantly improving the prooxidant-antioxidant profile ( Maksymchuk et al, 2023 ). Whether downregulation of MYC alone would reduce blood pressure, CYP2E1 expression, and curb the oxidative stress, still remains to be seen.…”

Section: Myc’s Involvement In Diseases and Conditionsmentioning

confidence: 99%

MYC: there is more to it than cancer

Zacarías-Fluck,

Soucek,

Whitfield

2024

Front. Cell Dev. Biol.

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MYC is a pleiotropic transcription factor involved in multiple cellular processes. While its mechanism of action and targets are not completely elucidated, it has a fundamental role in cellular proliferation, differentiation, metabolism, ribogenesis, and bone and vascular development. Over 4 decades of research and some 10,000 publications linking it to tumorigenesis (by searching PubMed for “MYC oncogene”) have led to MYC becoming a most-wanted target for the treatment of cancer, where many of MYC’s physiological functions become co-opted for tumour initiation and maintenance. In this context, an abundance of reviews describes strategies for potentially targeting MYC in the oncology field. However, its multiple roles in different aspects of cellular biology suggest that it may also play a role in many additional diseases, and other publications are indeed linking MYC to pathologies beyond cancer. Here, we review these physiological functions and the current literature linking MYC to non-oncological diseases. The intense efforts towards developing MYC inhibitors as a cancer therapy will potentially have huge implications for the treatment of other diseases. In addition, with a complementary approach, we discuss some diseases and conditions where MYC appears to play a protective role and hence its increased expression or activation could be therapeutic.

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“…In the case of high-density microsomes obtained from rats exposed to ethanol, a reduced GSH/GSSG ratio of 2.9:1 was observed, indicating an elevated level of oxidative stress following ethanol consumption [162]. The increased oxidative stress was associated with the up-regulated expression of CYP2E1, as demonstrated by the presence of 4-hydroxynonenal (4-HNE) protein adducts in adipocytes and an elevation in ADIPO carbonylation [163][164][165][166]. While overexpression of CYP2E1 in 3T3-L1 adipocytes did not affect intracellular ADIPO concentration [161], ethanol culture did lead to the inhibition of ADIPO release into the extracellular medium.…”

Section: Adipomentioning

confidence: 99%

Alcohol, White Adipose Tissue, and Brown Adipose Tissue: Mechanistic Links to Lipogenesis and Lipolysis

Wang

et al. 2023

Nutrients

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According to data from the World Health Organization, there were about 3 million deaths caused by alcohol consumption worldwide in 2016, of which about 50% were related to liver disease. Alcohol consumption interfering with the normal function of adipocytes has an important impact on the pathogenesis of alcoholic liver disease. There has been increasing recognition of the crucial role of adipose tissue in regulating systemic metabolism, far beyond that of an inert energy storage organ in recent years. The endocrine function of adipose tissue is widely recognized, and the significance of the proteins it produces and releases is still being investigated. Alcohol consumption may affect white adipose tissue (WAT) and brown adipose tissue (BAT), which interact with surrounding tissues such as the liver and intestines. This review briefly introduces the basic concept and classification of adipose tissue and summarizes the mechanism of alcohol affecting lipolysis and lipogenesis in WAT and BAT. The adipose tissue–liver axis is crucial in maintaining lipid homeostasis within the body. Therefore, this review also demonstrates the effects of alcohol consumption on the adipose tissue–liver axis to explore the role of alcohol consumption in the crosstalk between adipose tissue and the liver.

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Quercetin inhibits the expression of MYC and CYP2E1 and reduces oxidative stress in the myocardium of spontaneously hypertensive rats

Cited by 4 publications

References 24 publications

Longevity Spinach (Gynura procumbens) Ameliorated Oxidative Stress and Inflammatory Mediators in Cisplatin‐Induced Organ Dysfunction in Rats: Comprehensive in vivo and in silico Studies

Longevity Spinach (Gynura procumbens) Ameliorated Oxidative Stress and Inflammatory Mediators in Cisplatin‐Induced Organ Dysfunction in Rats: Comprehensive in vivo and in silico Studies

MYC: there is more to it than cancer

Alcohol, White Adipose Tissue, and Brown Adipose Tissue: Mechanistic Links to Lipogenesis and Lipolysis

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